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Maksym Pogorielov Sumy State University, Ukraine

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Eugenia Husak Sumy State University, Ukraine

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Alexandr Solodivnik Sumy State University, Ukraine

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Sergii Zhdanov Sumy State University, Ukraine

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In recent years, the paradigm about the metal with improved corrosion resistance for application in surgery and orthopedy was broken. The new class of biodegradable metal emerges as an alternative for biomedical implants. These metals corrode gradually with an appropriate host response and release of corrosion products. And it is absolutely necessary to use essential metals metabolized by hosting organism with local and general nontoxic effect. Magnesium serves this aim best; it plays the essential role in body metabolism and should be completely excreted within a few days after degradation. This review summarizes data from Mg discovery and its first experimental and clinical application of modern concept of Mg alloy development. We focused on biodegradable metal application in general surgery and orthopedic practice and showed the advantages and disadvantages Mg alloys offer. We focused on methods of in vitro and in vivo investigation of degradable Mg alloys and correlation between these methods. Based on the observed data, a better way for new alloy pre-clinical investigation is suggested. This review analyzes possible alloying elements that improve corrosion rate, mechanical properties, and gives the appropriate host response.

Abstract

In recent years, the paradigm about the metal with improved corrosion resistance for application in surgery and orthopedy was broken. The new class of biodegradable metal emerges as an alternative for biomedical implants. These metals corrode gradually with an appropriate host response and release of corrosion products. And it is absolutely necessary to use essential metals metabolized by hosting organism with local and general nontoxic effect. Magnesium serves this aim best; it plays the essential role in body metabolism and should be completely excreted within a few days after degradation. This review summarizes data from Mg discovery and its first experimental and clinical application of modern concept of Mg alloy development. We focused on biodegradable metal application in general surgery and orthopedic practice and showed the advantages and disadvantages Mg alloys offer. We focused on methods of in vitro and in vivo investigation of degradable Mg alloys and correlation between these methods. Based on the observed data, a better way for new alloy pre-clinical investigation is suggested. This review analyzes possible alloying elements that improve corrosion rate, mechanical properties, and gives the appropriate host response.

Introduction

In the last decades, the paradigm establishing that implants must be inert and corrosion resistant has been displaced by the advent of a new class of metallic biomaterials: biodegradable metallic materials [1]. Compared with other materials, these metals have high impact strength, high wear resistance, high ductility, and toughness [2]. Hence, these metals are used in orthopedy, general, and cardiovascular surgeries because of their appropriate mechanical and corrosion properties after providing structural support for a certain period to complete both the regeneration and the healing processes.

Iron (Fe), zinc (Zn), and magnesium (Mg) are considered as the basic biodegradable materials for medical application. Mechanical parameters of these three pure metals are shown in TableI.

Table I

Mechanical parameters and degradation rate of pure Fe, Zn, and Mg used for medical applications (compare the stainless steel)

Yield strength (MPa)Tensile strength (MPa)Elongation (%)In vitro degradation rate (mm year−1)
316L SS: annealed19049040
Pure Fe: annealed150200400.16
Pure Zn: as cast17200.20.2
Pure Mg: as cast208613407

Among these metals, Fe is an interesting candidate for biodegradable materials in terms of its mechanical properties. Because of its higher elastic modulus, Fe has a high radial strength, which is helpful in making materials with thinner struts. It has also high ductility, which is helpful during the implantation when the material is plastically deformed [3]. The first biodegradable metallic stent was fabricated from Armco® iron (Fe > 99.8%) and implanted in descending aorta of New Zealand white rabbits in 2001 [4]. The results from the implantation of the first Fe stent showed no significant evidence of either an inflammatory response or neointimal proliferation, and organ examination did not reveal any systemic toxicity. However, the slow degradation rate (0.16 mm year−1) and the ferromagnetic nature of pure Fe led to problems when these materials were used as implantable devices [5]. The addition of manganese (Mn) increases the degradation rate up to 0.44 mm year−1, but still it does not have wide application.

Zn-based alloys may also be promising candidates for biodegradable implants. The advantages of Zn-based alloys are its low melting point and low reactivity in molten state. Therefore, they can be prepared by simple melting, gravity, or die casting in air atmosphere and hot forming [6]. Zn alloys do not show local or general toxicity or other biological compatibility [7]. However, one drawback of pure Zn as potential biodegradable metal lies in that pure Zn has quite low strength and plasticity.

Mg and its alloys are biocompatible materials with appropriate biomechanical parameters that can corrode completely in biological media. These properties make them promising candidates for biomedical applications [8]. Degradation of Mg under the physiological conditions avoids reoperation to remove bone implant. In recent century, Mg alloys were extensively investigated, but still they are not used as the optimal material for controlling biodegradation and tailoring alloy composition and microstructure depending on texture, grain size, manufacturing method, and postprocessing techniques [9–11].

This review summarize the discovery of Mg and its alloys for biomedical application. Furthermore, it also summarizes the different fields of Mg alloy application and mechanisms of Mg degradation (both in vitro and in vivo).

Mg Discovery and Its First Biomedical Application

Mg was first identified by Sir Humphry Davy in 1808 (Fig.1), and in 1833, it was first extracted by Michael Faraday using electrolysis [12]. In the mid-19th century, it was produced by small companies in Germany, the USA, and the UK for pyrotechnical and photographical applications.

Fig. 1.
Fig. 1.

Left: Sir Humphry Davy (17 December 1778 – 29 May 1829), English chemist, who discovered Mg in 1808; Right: Dr. Erwin Payr (17 February 1871 – 6 April 1946). Austrian–German surgeon, a pioneer in medical application of Mg

Citation: Interventional Medicine and Applied Science Interventional Medicine and Applied Science 9, 1; 10.1556/1646.9.2017.1.04

The first medical application of Mg alloy was reported in 1878, when Huse used wire as ligature to stop bleeding from radial artery (2 cases) and during the operation for varicocele [12]. In all cases, the application of Mg ligature was successful, but the further researches on this application were not carried out until Payr reported other possible Mg applications in 1900 [13, 14].

Mg in Surgery

Payr was a pioneer in medical application of Mg; he carried out both human and animal testings. In his first experiment in 1900, he used Mg vessel connectors in animal femoral artery [13, 14]. The original image from the Payr article is shown in Fig.2A. He proved that the connection of the vessel ends became solid after 8 days and observed a severely thickened intima layer at the anastomosis, with a fibrous ring on the outer side at that point. In the same study, he also suggested that only the intravascularly placed Mg tubes exhibited thrombotic blood clotting at the end of the tubes, which, however, never closed the remaining lumen. Also, no thrombosis was observed with extravascularly placed Mg tubes. He recommended using Mg plates and sheets for well-vascularized organ suturing and treatment of cavernous hemangioma and large vessel aneurysms [17–19]. He proved that hemostasis was effective after the partial liver excision on animal model using Mg sheet, and then, he successfully applied this method in a human case. In the animal model, he suggested that the resorption time of Mg plates after hemostasis varied from 50% resorption after 3 weeks to minor corrosion after 5 weeks. Two years later, in 1905, Payr and Martina showed that hemostatic effect after Mg sheets application was because of the tamponade effect of hydrogen gas [17]. In 1900, he carried out his first successful treatment of hemangioma in a 14-year-old girl. Few years later, he suggested that treatment with Mg arrow was only beneficial for treating subcutaneous cavernous hemangioma [19]. In 1914, Sonntag confirmed Payr’s results in several clinical cases [20]. Finally, Payr suggested the use Mg tubes for sutures of nerves and used this technique both in animal experiments and in human cases (7 nerves) [14]. During the experiments, he observed several round cells and granular tissue formation around the corroding Mg [14]. The granular tissue was highly vascularized and contained giant cells with metallic particles and leucocytes. He also found that the strong activation of blood clotting was because of the corroding Mg implant [17].

Fig. 2.
Fig. 2.

(A) Mg vessel connectors (extravasal Mg rings – left column, two-part connectors – right column) designed by Payr [15]. (B) Mg connector for intestine anastomosis, designed by Chlumsky in 1900 [16]

Citation: Interventional Medicine and Applied Science Interventional Medicine and Applied Science 9, 1; 10.1556/1646.9.2017.1.04

At the same time, Chlumsky suggested the use of Mg tubes as connectors for intestine anastomosis, but he used high-purity Mg, which corroded homogeneously (Fig.2B). The corroding rate of the connectors was between 2 and 4 weeks, depending on their anatomical localization [21]. Also, Chlumsky interposed 0.1–0.8-mm-thick Mg sheets between the freshly separated bone surfaces in the knee joints of dogs and rabbits, proving the complete corrosion after 18 days. Both in animal and human cases, Chlumsky prevented joint stiffness and restored the joint motion [16]. But later observation showed that all neo-joints became stiff over the years.

In 1903, Hopfner used Mg cylinders for vessel anastomosis and observed thrombosis in vessels with diameter <3 mm. He suggested that thrombosis was because of the extensive intima lesion during the operation and recommended to use Mg for anastomosing of large vessels [22].

In 1910, Lespinasse used Mg metallic ring plates with punched holes for extravasal sutures [23]. The Mg ring plates were found to maintain their original shape for about 30 days before they began to break down and completely degrade within 80–100 days. The Mg rings were tied firmly together, but not so tight to cut the intima and cause vessel necrosis. Lespinasse did not observe any thrombosis or secondary vessels constriction.

In 1917, Andrews used the absorbable Mg clips and staples for successful hemostasis in the brain, deep wounds, and intestinal anastomosis [24]. Unlike the previous researches, he used both pure metals and Mg alloys for different applications. He made alloys with aluminum (Al), cadmium (Cd), and Zn, but soon discovered that all these alloys were too hard and brittle and could not be used for cardiovascular application. In 1924, Seelig found that the available Mg wires on the market were too brittle. So, he used pure Mg produced by distillation in vacuum to obtain more ductile Mg wires. Also, noble metals, such as gold and silver (Ag), were alloyed with Mg to increase its ductility. But after some experiments, he suggested that these wires had a low tensile strength and were not sufficiently pliable [25]. Two years later, Glass had unsuccessful results from two hemangioma treatments using Mg alloy. The additional animal experiments showed that Mg was not beneficial for large and purely cavernous hemangioma [26]. The same inappropriate results were obtained in 1981 after Mg arrow treatment of 27 hemangioma patients [27]. But in 1928, Hoffheinz and Dimitroff found that Mg corroded fast in well cavernous hemangioma with its transformation in connective tissue in rabbit model [28].

In 1951, Stone and Lord used thrombogenic materials for successful intravascular clotting in aortic aneurysms. They used pure Mg wires (0.025 inch diameter) and Mg–Al wires (0.03 inch diameter) in dogs’ aortas as double-coiled wires. They found that Mg wires were twice as thrombogenic as stainless steel and that the thrombogenic potential of Al-alloyed Mg wires was as much as three times higher than that of stainless steel. The pure Mg wire was very brittle, while the addition of 2% Al allowed bending and clinical application. Stone and Lord stated that both wires were suitable for the intended application, while the Mg–2% Al exhibited higher thrombogenic potential than commercially pure Mg [29].

Mg in Orthopedic Practice

Mg and its alloys have several advantages for orthopedic surgery. Materials currently used for this purpose, including stainless steel, titanium, cobalt–chromium, and zirconium (Zr) alloys, have limitation because of the possible release of toxic ions during corrosion or wear processes and noncompliance with elastic module of natural bone [30, 31]. Also, metallic materials for permanent fixtures should be removed after a few months that lead to possible complication and the increase of treatment cost [32]. In contrast to other metals, Mg has density and elastic module close to natural bone [33]. During the degradation, Mg alloy releases nontoxic MgO that is most completely excreted in the urine [34]. Also, there are some evidences that Mg has stimulatory effect on the new bone tissue growth [35–37].

Possible Mg implants, such as pins, nails, wires, and plates, were developed by Payr in 1900 [13]. But the first practical application of Mg alloy in orthopedy was carried out by Lambotte in 1906 [38]. After the clinical failure of performing metal osteosynthesis of fractured tibia for 17-year-old child, he used Mg plates with six steel screws. But after the operation, the extensive subcutaneous gas cavities formed were treated by removing the fragments of Mg plates on the eighth day. So, the electrochemically developed Mg, which degraded extensively between the Mg plate and the steel screws. After some animal experiments, Lambotte and Verbrugge found total Mg resorption between 7 and 10 months after implantation. Later clinical investigations of pure Mg without steel screw showed successful results with children suffering from bone fracture (Fig.3). Thus, they recommended to use Mg implants in Bennett fractures, scaphoid fractures, foot surgery, clavicular fractures, carpus fractures, phalanx and metacarpal fractures, radius epiphyseal fractures, lower arm diaphyseal fractures, supra and condylar fractures in children, humeral head fractures, malleolus fractures, oblique tibial fractures, and pertrochanteric fractures [39].

Fig. 3.
Fig. 3.

Supracondylar humerus fracture of a child, fixated with Mg nail by Lambotte (A) and results after several months with total Mg nail corrosion (no gas cavities observed) (B) [38]

Citation: Interventional Medicine and Applied Science Interventional Medicine and Applied Science 9, 1; 10.1556/1646.9.2017.1.04

But, in 1913, Groves investigated Mg as intramedullary peg and suggested that it cannot be used for orthopedy because of the formation of abscess cavities and quick degradation before fracture healing [40]. Later, Zierold proved the stimulation of connective tissue production and acceleration of new bone growth during alloy application [41]. In 1920, Verbrugge investigated Mg alloy with 8 wt. % of Al in animal experiments and clinical cases and found the resorption of Mg after 6–8 months with no signs of inflammation and tissue irritation. Thus, concluding that gas formation was not damaging any tissue. He demonstrated callus formation in 21 clinical cases, in which there was no reaction of skin, soft tissues, bone, and joints to corroded Mg products [42].

After some animal trials, in 1938, McBrigge reported that pure Mg plates were not suitable for bone reconstruction because of its fast degradation time. But he observed that Mg screw was more resistant to corrosion compared with the plates and should be used for bone surgery [43]. Later, McBride used Mg–Al–Mn alloy for bone grafting and fracture fixation in 20 patients (Fig.4). He did not observe any inflammatory or systemic reaction and slow degradation rate of new alloy. McBride reported that Mg had positive effect on periosteal tissue and callus deposition [44]. Two years later, Maier reported about two positive cases of fracture healing using spindle-shaped Mg sheets. Subcutaneous implantation of Mg implants in rabbit showed corrosion and formation of gas cavities with strong periosteal reaction. Maier [45] suggested that MgO, as a product of corrosion, had irritant effect on bone cells and stimulated periosteal reaction.

Fig. 4.
Fig. 4.

Rotation-resistant osteosynthesis with Mg–Mn metal plate, provided by McBride [44]

Citation: Interventional Medicine and Applied Science Interventional Medicine and Applied Science 9, 1; 10.1556/1646.9.2017.1.04

Troitskii and Tsitrin in 1944 used Mg alloy with small amount of Cd for treatment of 34 patients with different bone fractures. Of the 34 patients, only 9 were unsuccessful because of infection. In other cases, complete bone healing with no inflammatory reaction around implants was observed; also, they did not find any correlation between Mg degradation and concentration in blood serum. Corrosion process was slow and complete within 10–12 months. At the same time, they also reported that some implants were resorbed in 3–5 weeks because of incensement of acidity level in the fracture zone [46]. In 1945, similar positive result of 2 fracture healing was reported by Znamenskii. He used Mg with 10 wt. % of Al, and implants were not detected in the fracture zone in 6 months after grafting [47].

In 1972, Borodkin et al. used Mg alloy with rare earth elements. The alloy was composed of 0.4–4 wt. % rare earth metal, 0.05–1.2 wt. % Cd, 0.05–1.0 wt. % calcium (Ca) or Al, and variable, trace (0.8%) levels of Mn, Ag, Zr, or silicon (Si). They showed the slow degradation of complex alloy in 5–10 months in vivo, but they did not report about trace element distribution and any complications [48].

From 2001 to 2005, Witte et al. studied in vivo degradation of 4 Mg alloys – with Al and Zn (3 wt. % Al + 1 wt. % Zn and 9 wt. % Al + 1 wt. % Zn) and with rare earth elements (4 wt. % of yttrium (Y) + 3 wt. % of neodymium, cerium, and dysprosium and 4 wt. % of lithium (Li) + 4 wt. % of Al + 2 wt. % of cerium, lanthanum, neodymium, and praseodymium). Microtomography showed alloy degradation in 18 weeks after operation with significant increase of bone formation compared with the control group (polylactide rod). They proved the slowest corrosion rate in Li–Al-rare elements alloy. The rare elements were detected in the corrosion layer in the presence of amorphous Ca3(PO2)4, but not in the surrounding bone tissue [49].

In recent years, several researchers have investigated different Mg alloys for increasing its degradation stability, mechanical properties, and biological response. Trincă et al. (2015) suggested the use of an alloy based on Mg with addition of 0.4% Ca and 0.5% Si and carrying out an Si concentration gradient of 0.25 mm depth from the sample surface to inside. In the case of the tibiae implant, the variation of the main biochemical and histological parameters sustained normal evolution of the bone fracture with a short resorption stage on the background of a relatively constant bone formation rate. The specific histological stains showed the intense and active bone formation after 2 weeks of implantation, whereas after the 4th week, the bone remodeling process had already started. X-Ray and computed tomography (CT) registered the presence of experimentally created defect in the tibia and revealed some of the bone-specific recovery stages in relation with the biodegradation process of the implant sample [50].

In 2015, Wang implanted Mg–Zn–Zr alloy cylinders into the femoral condyles of Japanese big-eared white rabbits. In the 24th week, the implant was more obscure and the density of the surrounding cancellous bone increased. Micro-CT confirmed that new bone tissue on the surface of the residual alloy implant increased between 12th and 24th week. On 12th week, many cavities in the cancellous bone tissue around the implant were noted with a CT value, similar to a gas value, and increased by the 24th week. The histological examination of hard tissue slices showed that bone tissue was visibly attached to the alloy in the femoral condyle at the 12th week. The trabecular bone tissues became more intact and dense, and the cavities were filled with soft tissue at 24th week. In general, gas produced by the degradation of the Mg–Zn–Zr alloy can cause cavitation within cancellous bone, which does not affect osteogenesis around Mg alloy [51].

Pan et al. developed the new wrought Mg–2Sn–1Ca wt. % (TX21) and Mg–2Sn–1Ca–2Zn wt. % (TXZ212) alloys with high strength and ductility, simultaneously produced by conventional casting, homogenization, and indirect extrusion. They proved that the high strengths were because of the high number density of nano-Mg–Sn–Ca phases, G.P. zones, and ultra-fine grain size (∼0.8 μm) [52]. In the same year, fine-grained Mg–1.8Gd–1Zn–0.1Zr (at.%) alloy with long-period stacking ordered (LPSO) phase was obtained via solid solution (SS) treatment plus multipass equal-channel angular pressing (ECAP). The effects on post-ECAP rolling on microstructure changes and deformation characteristics of the Mg alloy were investigated. The results showed that the fine-grained alloy after 16 ECAP at 658 K had yield strength of 334.4 MPa with an elongation of 22.5%. The grain refinement with LPSO formed and improved the strength and ductility of the ECAPed alloy simultaneously, indicating good plastic formability [53]. But the in vivo experiment was not performed, and the biodegradation rate was not studied.

Yang Liu added 2 × 1017 ions cm−2 of Ag, Fe, and Y to the Mg–1Ca alloy using metal vapor vacuum arc technique. Y-ion implantation induced an Mg/Ca-deficient outer oxidized layer, and the distribution of Y along with depth was more homogeneous. Both electrochemical and immersion tests revealed the accelerated corrosion rate of Ag-implanted Mg–1Ca and Fe-implanted Mg–1Ca, whereas Y-ion implantation showed a short period of protection as enhanced corrosion resistance was obtained by electrochemical test, but accelerated corrosion rate was found by long-period immersion test. Indirect cytotoxicity assay indicated good cytocompatibility of Y-implanted Mg–1Ca [54].

Hofstetter investigated the effect of trace impurity elements on the degradation behavior of high-strength Mg alloys of type ZX50 (Mg–5Zn–0.3Ca). It is shown that trace impurity elements increased the degradation rate, predominantly in the initial period of the tests, and also increase the material’s susceptibility to localize corrosion attack. These effects are explained on the basis of the corrosion potential of the intermetallic phases presented in the alloys [15].

The recent study of different statuses of Mg–strontium (Sr) showed that the as-cast Mg–Sr alloy exhibited a rapid degradation rate compared with the as-extruded alloy because of the intergranular distribution of the second phase and micro-galvanic corrosion. However, the initial degradation could be tailored by the coating protection, which was proved to be cytocompatible and also suitable for bone repair observed by in vivo implantation. The integrated fracture calluses formed and bridged the fracture gap without gas bubble accumulation, meanwhile the substitutes simultaneously degraded. In conclusion, the as-cast Mg–Sr alloy with coating is potential to be used for bone substitute alternative [55].

Zhou et al. developed extruded Mg–1Mn–2Zn–xNd alloys (x = 0.5, 1.0, 1.5 mass%). The experimental results indicated that all extruded Mg–1Mn–2Zn–xNd alloys show good ductility and much higher mechanical strength than that of cast pure Mg and natural bone. The tensile strength and elongation of the extruded alloys increase with an increase in neodymium content. Their compressive strength does not change significantly with an increase in neodymium content. The extruded alloys show good biocompatibility and much higher corrosion resistance than that of cast pure Mg [56].

In summary, an ideal Mg alloy (for degradation rate, in vivo response, and mechanical strength) is still not found.

Mg Alloy Degradation

The great challenge is to tailor implant degradation in a manner that is suitable for a biological environment [8]. The best way for Mg alloy production for orthopedic and surgery application is still investigated. The fast resorption can lead to mechanical instability before complete bone healing, but the low degradation can lead to the inappropriate host response. The basic conditions that determine the corrosion rate are alloy compound and environment around implant. In aqueous media, Mg alloy degrades during the electrochemical reaction known as a corrosion and produces magnesium hydroxide (Mg(OH)2) and hydrogen gas. Mg(OH)2 is not soluble and forms a protective layer on alloy surface. When the chloride concentration is above 30 mmol/l, it converts into the soluble MgCl2. Chloride content in body fluids is about 150 mmol/l, and degradation of Mg alloy starts just after their insertion to the organism [57].

The degradation rate of Mg depends on several factors (Fig.5). Sanchez et al. reviewed more than 100 papers for in vitro (23 alloys) and in vivo (20 alloys) degradation, and pointed on different time of degradation and the absence of correlation data between in vitro and in vivo experiments [8].

Fig. 5.
Fig. 5.

Factors that can change Mg and Mg alloy degradation

Citation: Interventional Medicine and Applied Science Interventional Medicine and Applied Science 9, 1; 10.1556/1646.9.2017.1.04

The methods of in vitro degradation include electrochemical tests, hydrogen evolution, and mass/volume loss after immersion test [8]. Electrochemical test is simple and reproducible, but it leads to acceleration of corrosion that does not correlate with in vivo degradation [58]. For example, degradation rate using immersion method for pure Mg reported by Zhang was 0.26 mm year−1 [59], whereas degradation rate using electrochemical method was 2.52 mm year−1 [60]. The methods of mass or volume loss are similar to in vivo conditions but have some limitations. For example, mass loss without removing the corrosion products can lead to negative degradation rate [61].

The main challenge during the corrosion test is choosing the media for experiment. For this test, solution that simulates in vivo environment should be used. The best test media for this purpose are Hank’s solution, simulated body fluid (SBF), Earle’s balanced salt solution (EBSS), or minimum essential medium (MEM). The ion concentration in SBF is very similar to blood plasma, but MEM contains glucose, amino acid, and vitamins [8]. MEM and EBSS contain a slightly lower amount of Ca and Mg compared with blood [62] (TableII). Using different media, it is possible to obtain different valuable results. For the pure Mg, corrosion rate measured by immersion in EBSS and reported by Walker was 0.39 mm year−1 [63], whereas in SBF and Hank’s solution, it was 1.39 [64] and 2.05 mm year−1, [65] respectively. It is also likely that with alloying Mg – degradation rate for Ca–P coating – an increase from 0.25 mm year−1 in Hanks solution [66] to 1.88 mm year−1 in SBF [67]. It should be noted that not only methods but also solution can influence the degradation rate.

Table II

The ions and glucose level in blood and experimental media for testing of biodegradability

Ions and organic composition (mmol/l)Blood plasmaSBFMEMEBSSHank’s solution
Na135.0–145.0142.0143.0144.0142.0
K3.5–5.35.85.45.45.8
Mg1.5–2.30.80.40.40.8
Cl103.0145.0125.0125.0145.0
Ca2.1–2.82.51.81.82.5
HPO40.8–1.50.40.91.00.4
SO40.4–0.60.80.40.40.8
HCO318.0–23.04.226.026.04.2
Glucose3.5–5.55.65.6

Experimental temperature can significantly influence degradation of Mg alloy in vitro. Pure Mg degrades two times faster at 37 °C compared with 20 °C. The same authors demonstrated that the temperature increases up to 40 °C and accelerates corrosion rate by 50% compared with 37 °C [68]. This finding shows potential risk of extensive Mg alloy corrosion after implantation, especially during the inflammatory processes.

The influence of pH solution on Mg corrosion was described in several publications [63, 69–71]. They showed that using buffering system for keeping constant pH around material was very important for the appropriate experiment results. The nonbuffered solution leads to pH increase, formation of protective layer on alloy surface, and decrease of corrosion rate. The best buffering solution that mimics in vivo environment is NaHCO3/CO2 buffers. It maintains pH in neutral regimen, and corrosion will not be stopped [8].

To mimic in vivo environment, we need to use a dynamic test. In static immersion test, protective layer on Mg alloy should be formed because we did not remove degradation products. The last can lead to changes in solution environment and stop corrosion. Shi et al. showed that degradation rate of AZ31 Mg alloy during the static condition (0.3 mm year−1) was five times lower compared with the dynamic condition (1.5 mm year−1). Moreover, dynamic experiment significantly correlates with in vivo experiment (1 mm year−1) [72].

All these data show that the ideal conditions for in vitro Mg and its alloy corrosion test are still investigated, and the main parameters of this research are solution compound, temperature, and pH.

In vivo Mg resorption was completed from a few weeks to more than 1 year, depending on type of Mg alloy and host tissue environment. The first Mg plate application reported a fast degradation because of electrochemical reaction with stainless steel screws [38]. Recent research showed slower degradation in vivo, but all factors that determine Mg alloy corrosion in animal and human body are still not found.

Sanchez in her review summarized data of more than 50 papers for Mg alloy degradation [8]. She did not find any correlation between alloy compound and degradation rate. Pure Mg corrosion rate varies from 0.33 mm year−1 after subcutaneous implantation [63] to 0.86 mm year−1 in femur implantation model [73]. Mg–Al–Zn alloy degrades faster in rabbit compared with the rats during the bone no-intramedullary implantation: 1.64 mm year−1 [49] compared with 0.168 mm year−1 [74]. In the same case, intramedullary implantation in femur of Mg–Zn–Ca–Mn alloy corrodes three times faster after the intramuscular implantation insertion [65, 75].

Based on enumerated data, we cannot choose the main causes that influence Mg corrosion in vivo. The first is animal model that involves the experiment and anatomical region of implantation. Animals have different water contents and blood flow that can influence the removing of degradation products. Water content in human bone tissue is 43.9% and it significantly increases in rabbit bone tissue up to 58.1%. For example, blood flow increases from rat (2.3 ml/min/100 g) to rabbit (19.1 ml/min/100 g) and human (120 ml/min/100 g). Water content in skin is significantly higher in all animal models as well as in human, but blood flow in rabbit skin decreases to 12.7 ml/min/100 g. The amount of water and blood flow can affect the removal of degradation product and prevent the formation of protective layer on alloy surface [57].

Chloride-contained environment can transform Mg(OH)2 into soluble MgCl2 that accelerates corrosion. But the level of chlorine ion depends not only on the species but even on the tissue and body condition. This factor can significantly decrease corrosion rate and is probably the main factor that determines the difference between in vitro and in vivo experiments [49, 76].

As mentioned previously, pH is one of the factors that determine degradation rate in vitro. After the metal implantation, tissue response such as inflammation or foreign body reaction can be observed. It can lead to formation of stable corrosion layer in first term after the surgical procedure [77]. Body fluid ion concentration as well as temperature can also change the rate of Mg corrosion [78].

By comparing the data for in vitro and in vivo degradation, it can be observed that different corrosion rates depend on numerous factors. In vitro test gives only general information about alloy degradation, and this information should be used for planning in vitro investigation. But the last aspect does not answer the key question—how does alloy will corrode in clinical case? Only the systematic analysis of clinical trials and in vivo animal studies with different conditions can give complete information about the relations between the degradable Mg alloy and the hosting organ.

Mg Alloying Elements

Pure Mg implants have low corrosion resistance and unsatisfactory properties, and Mg fast degradation and distribution over the body may cause clinical complications. The main purpose of developing a alloy is to improve the mechanical properties, corrosion resistance, and the production cost [57]. The basic elements used for Mg alloying are Al, Ca, copper, Fe, Li, Mn, nickel, Sr, Y, zinc, Zr, and rare earth elements [49, 77, 79–82]. But the alloy properties also depend on intermetallic compound and microstructural effect based on the processing route.

Witte [57] classified Mg alloys into three groups: (1) pure Mg with trace of other elements, (2) Al-containing Mg alloy, and (3) Al-free Mg alloys. The most used Al-contained alloys are Al–Zn, Al-rare elements, Al–Ca, Li–Al, and Al–Li-rare elements [83, 84]. The most typical Al-free composites are Mg–Mn–rare elements, Mg–Mn–Zn, Mg–Yt–Zn, and Mg–Ca [85]. Nontoxic alloying elements should be used for humans.

As a widely used element for Mg alloying with maximum solubility of 12.7 wt. %, Al can provide both solid strengthening solution and precipitation. Witte et al. reported that increase of the Al content lowers the liquidus and solidus temperature lines and enhances the castability of alloys with high Al solidus [57]. The Al addition of Mg alloys leads to the improvement of strength and the small increase of density (the density of Al is close to that of Mg), but it causes the decrease of elongation [86]. Insoluble Al2O3 will be formed in the corrosion products layer in alloys containing Al and Mg during corrosion [87]. Al should be used carefully because of its possible biological complications such as risk factor in Alzheimer’s disease, muscle damage, and decrease of activities of osteoclasts [88–90].

Zn is a nontoxic element that plays significant role in human metabolism as a co-factor for some enzymes, and it is essential for immune system [91, 92]. The consumption of Zn in amounts higher than the upper limit (40 mg/day) is generally considered relatively nontoxic, and amounts approaching 100 mg/day can be tolerated for a few days [93]. Zn is an important alloying element with a relatively high solubility in Mg—up to 6.2 wt. %. Zn content that is up to 4 wt. % significantly increases the ultimate tensile strength and elongation of as-cast Mg–Zn alloys, but any higher percentage of Zn would lead to the reduction of both properties and decrease the corrosion resistance of the alloy [94]. But it was shown that amorphous Mg–Zn-based alloys containing about 5.0 wt. % of Zn had excellent strength, high corrosion resistance, low hydrogen evolution rate, and good biocompatibility in animals; therefore, these are promising candidates for biodegradable bone implants. But problems arise from a quite difficult preparation of metallic glasses and especially forming them to a final product. The common processes involved rapid solidification of melt that limited the maximum thickness of amorphous alloys to hundreds of micrometers [95]. In amount <2 wt. % Zn contributes to strength because of SS strengthening, but larger amount leads to embrittlement in combination with Al [83]. The mechanical and degradation properties being the main concerns, the Mg–Zn alloys with low Zn content (<4 wt. %) were further alloyed by adding the third alloying elements, including Ca [96], Mn [97], Sr, Y, and Zr [98].

Ca is the most abundant mineral in the human body, and it is strictly regulated by homeostasis of skeletal, renal, and intestinal mechanisms. It plays a significant role in bone function, vascular, and heart physiology [99]. The solubility of Ca in Mg is about 1.34 wt. %, and under the equilibrium conditions, Ca contributes to solid strengthening solution and precipitation. It also acts to some extent as a grain-refining agent and additionally contributes to grain boundary strengthening. In binary Mg–Ca alloys, the Laves phase Mg2Ca is formed, whereas in Al-containing alloys, the Laves phase Al2Ca is formed first. Both phases improve creep resistance because of SS strengthening, precipitation strengthening, and grain boundary pinning. Mg2Ca intermetallic phase is brittle, which can act as potential sources for cracking to occur and indicates a negative effect on the ductility of Mg, and it also accelerates the degradation because of galvanic corrosion. In the Mg–Ca system, Mg2Ca is the only second phase besides α-Mg and distributes around grain boundaries. Wan et al. [100] reported that 0.6 wt. % of Ca addition could improve the bending and compressive strength of pure Mg, whereas a higher Ca addition deteriorated these properties. Large amounts of Ca (>1 wt. %) can lead to problems during casting like hot tearing or sticking [57]. Zn, Y, and Sr were introduced in the Mg–Ca binary alloys to optimize their mechanical and degradation properties [101]. The introduction of Zn (2.31 wt. %) into the as-cast Mg–3Ca alloy can improve the strength and ductility of the alloy, and its presence supports the formation of the eutectic phase (a-Mg + Mg2Ca + Ca2Mg6Zn3) that leads to a decreased degradation rate of the alloy [102]. Ca-contained alloy positively influences the cell viability and proliferation rate [103].

Mn is an essential element that plays important role in metabolic cycle of lipids, amino acids, and carbohydrates. It also influences the function of immune system, bone growth, and blood clotting [104]. In Mg alloy, Mn is mainly used to enhance ductility. More important is the formation of Al–Mn intermetallic phases in Al-containing Mg alloys. These phases can pick-up Fe and can therefore be used to control the corrosion of Mg alloys because of the detrimental effect of Fe on the corrosion behavior [57]. Several researches show nontoxic influence of Mn during cell culturing, but its poisonous effect from Mg alloys on the cell viability and the proliferation has also been observed [57].

Zr is a powerful grain refiner for Mg alloys; it is usually used in alloys containing Zn, RE, Y, and thorium, and it cannot be used together with Al and Mn as they form stable compounds with Zr [105]. Recently, the Mg–Zr alloys had attracted considerable attention because of their high-specific damping capacity (around 80%), which may help to suppress the vibrations generated during movement and stress at the implant/bone interface [106]. It was indicated that 1 wt. % of Zr addition in Mg resulted in significant improvement of the strength and ductility of the metal and reduced the degradation rate by 50%, and co-addition of Sr and Sn could effectively reduce the degradation of as-cast Mg–Zr–Ca alloy [107]. Some authors investigated alloys with a wide range of Zr content 1–5 wt. % and showed that the degradation rate increased with increasing Zr content [108].

Rare earth elements are used both in Al-contained and Al-free alloys for changing final alloy mechanical properties, resorption rate, and biological response. We need to balance between possible toxicity and benefit. For Mg alloy processing, several rare elements have been used, such as cerium (Ce), lanthanum (La), neodymium (Nd) and praseodymium (Pr), gadolinium (Gd), terbium (Tb), dysprosium (Dy), holmium (Ho), erbium (Er), thulium (Tm), ytterbium (Yb), and lutetium (Lu) [57, 109]. Usually, they are used in combination with other alloying elements, but currently, there are some Mg alloys containing only rare earth elements.

Alloying elements can significantly improve mechanical properties, control corrosion rate, and influence biological response on Mg alloy. But it is difficult to choose the best alloy, and to do this, we need some more in vitro and in vivo experiments and clinical investigation.

Conclusion

Since 1900, after the first experimental application, Mg and its alloys were applied during different clinical cases, but they were not widely used because of uncontrolled corrosion and excessive hydrogen formation. It led to implant failure and clinical complications. There are two ways of biodegradable implants improvement – alloying elements addition and new methods of alloy casting to change intermetallic phases and grain. There are many bi- and poly-phase alloys created with improvement properties, but their biological response and long-term clinical results are still not completely clear.

In vitro and in vivo studies have been used for evaluation of degradation rate and host response. There is no correlation between these methods and should be used together for better alloy assessment. The best method for in vitro degradation is emersion in medium that simulates body environment, such as SBF, MEM, or EBSS. Electrochemical method and emersion in saline solution do not give reliable results. The results of in vivo research depend on animal species, implant anatomical location, and some physiological parameters, such as pH, blood flow speed, and chloride ion concentration. All these parameters could significantly change corrosion rate and host response.

Authors’ contribution

MP: idea, manuscript design, article writing and revising (introduction, conclusion, Mg alloy degradation). EH: article writing and revising (Mg alloying elements). AS: article writing and revising (Mg in surgery). SZ: article writing and revising (Mg in orthopedics practice).

Conflict of interest

The authors declared that they have no conflict of interest.

References

  • 1.

    Fagali NS , Grilloa CA , Puntarulo S , Fernández Lorenzo de Mele MA : Cytotoxicity of corrosion products of degradable Fe-based stents: Relevance of pH and insoluble products. Colloids Surf B Biointerfaces 128, 480488 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 2.

    Moravej M , Mantovani D : Biodegradable metals for cardiovascular stent application: Interests and new opportunities. Int J Mol Sci 12, 42504270 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 3.

    Mani G , Feldman MD , Patel D , Agrawal CM : Coronary stents: A materials perspective. Biomaterials 28, 16891710 (2007)

  • 4.

    Peuster M , Wohlsein P , Brugmann M , Ehlerding M , Seidler K , Fink C , Brauer H , Fischer A , Hausdorf G : A novel approach to temporary stenting: Degradable cardiovascular stents produced from corrodible metal – Results 6–18 months after implantation into New Zealand white rabbits. Heart 86, 563569 (2001)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 5.

    Purnama A , Hermawan H , Couet J , Mantovani D : Assessing the biocompatibility of degradable metallic materials: State-of-the-art and focus on the potential of genetic regulation. Acta Biomater 6, 18001807 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 6.

    Kubásek J , Vojtěch D , Jablonská E , Pospíšilová I , Lipov J , Ruml T : Structure, mechanical characteristics and in vitro degradation, cytotoxicity, genotoxicity and mutagenicity of novel biodegradable Zn–Mg alloys. Mater Sci Eng C Mater Biol Appl 58, 2435 (2016)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 7.

    Murni NS , Dambatta MS , Yeap SK , Froemming GR , Hermawan H : Cytotoxicity evaluation of biodegradable Zn-3Mg alloy toward normal human osteoblast cells. Mater Sci Eng C 49, 560566 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 8.

    Sanchez AH , Luthringer BJ , Feyerabend F , Willumeit R : Mg and Mg alloys: How comparable are in vitro and in vivo corrosion rates? A review. Acta Biomater 13, 1631 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 9.

    Liu C , Xin Y , Tang G , Chu PK : Influence of heat treatment on degradation behavior of bio-degradable die-cast AZ63 magnesium alloy in simulated body fluid. Mater Sci Eng A 456, 350357 (2007)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 10.

    Wang Y , Liu G , Fan Z : A new heat treatment procedure for rheo-diecast AZ91D magnesium alloy. Scripta Mater 54, 903908 (2006)

  • 11.

    Zeng RC , Zhang J , Huang WJ , Dietzel W , Kainer KU , Blawert C , Wei KE : Review of studies on corrosion of magnesium alloys. Trans Nonferr Metal Soc China 16, 763771 (2006)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 12.

    Witte F : Reprint of: The history of biodegradable magnesium implants: A review. Acta Biomater 23, 2840 (2015)

  • 13.

    Payr E : Beiträge zur Technik der Blutgefäss – und Nervennaht nebst Mittheilungen über die Verwendung eines resorbirbaren Metalles in der Chirurgie [Contributions to the technique of blood vessel and nerve suture, as well as the use of a resorbable metal in surgery]. Arch Klin Chir 62, 6793 (1900)

    • Search Google Scholar
    • Export Citation
  • 14.

    Payr E : Blutgefäß- und Nervennaht (nebst Mittheilung über die Verwendung eines resorbirbaren Metalles in der Chirurgie) [Blood vessel and nerve suture (in addition to the use of a resorbable metal in surgery)]. Centralblatt Chir 28, 3137 (1901)

    • Search Google Scholar
    • Export Citation
  • 15.

    Hofstetter J , Martinelli E , Pogatscher S , Schmutz P , Povoden-Karadeniz E , Weinberg AM , Uggowitzer PJ , Löffler JF : Influence of trace impurities on the in vitro and in vivo degradation of biodegradable Mg–5Zn–0.3Ca alloys. Acta Biomater 23, 347353 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 16.

    Chlumsky V : Über die Wiederherstellung der Beweglichkeit des Gelenkes bei Ankylose [On restoring the mobility of the joint with ankyloses]. Centralblatt Chir 27, 921925 (1900)

    • Search Google Scholar
    • Export Citation
  • 17.

    Payr E , Martina A : Experimentelle und klinische Beiträge zur Lebernaht und leberresection (Magnesiumplattennaht) [Experimental and clinical contributions to the liver suture and liver resection (magnesium plate seam)]. Arch Klin Chir 77, 962998 (1905)

    • Search Google Scholar
    • Export Citation
  • 18.

    Payr E : Ueber Verwendung von Magnesium zur Behandlung von Blutgefässerkrankungen [On the use of magnesium for the treatment of blood vessel diseases]. Deut Z Chir 63, 503511 (1902)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 19.

    Payr E : Zur Technik der Behandlung kavernöser Tumoren [The technique of treating cavernous tumors]. Zentralblatt Chir 30, 233234 (1903)

    • Search Google Scholar
    • Export Citation
  • 20.

    Sonntag E : Die Hämangiome und ihre Behandlung [The hemangiomas and their treatment]. Ergebn Chir Orthop 8, 1156 (1914)

  • 21.

    Chlumsky V : Beiträge zur Darmknopffrage [Contribution to the intestine]. Mitt Grenzgebieten Med Chir 3, 416451 (1907)

  • 22.

    Höpfner E : Ueber Gefässnaht, Gefässtransplantation und Replantation von amputierten Extremitäten [About vascular suture, vascular transplantation and replantation of amputated limbs]. Arch Klin Chir 70, 417471 (1903)

    • Search Google Scholar
    • Export Citation
  • 23.

    Lespinasse VD : A practical mechanical method of end-to-end anastomosis of blood-vessels: Using absorbable magnesium rings. JAMA 55, 17851790 (1910)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 24.

    Andrews EW : Absorbable metal clips as substitutes for ligatures in wound closure. JAMA 28, 278281 (1917)

  • 25.

    Seelig MG : A study of magnesium wire as an absorbable suture and ligature material. Arch Surg 8, 669680 (1924)

  • 26.

    Glass E : Klinische und experimentelle Untersuchungen uber die Payrsche Magnesiumpfeil behandlung von Angiomen [Clinical and experimental studies of the Payr’s magnesium wires in treatment of angiomas]. Deut Z Chir 194, 352366 (1926)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 27.

    Wilflingseder P , Martin R , Papp C : Magnesium seeds in the treatment of lymph- and haemangiomata. Chir Plast 6, 105116 (1981)

  • 28.

    Hoffheinz S , Dimitroff N : Experimentelle Studie uber die Resorption parental zugefuhrten metallischen Magnesiums [Experimental study of the absorption parentally fed metallic magnesium]. Deut Z Chir 208, 346353 (1928)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 29.

    Stone P , Lord JW Jr : An experimental study of the thrombogenic properties of magnesium and magnesium–aluminum wire in the dog’s aorta. Surgery 30, 987993 (1951)

    • Search Google Scholar
    • Export Citation
  • 30.

    Nagels J , Stokdijk M , Rozing PM : Stress shielding and bone resorption shoulder arthroplasty. J Shoulder Elbow Surg 12, 3539 (2003)

  • 31.

    Wang ML , Nesti LJ , Tuli R , Lazatin J , Danielson KG , Sharkey PF , Tuan RS : Titanium particles suppress expression of osteoblastic phenotype in human mesenchymal stem cells. J Orthop Res 20, 11751184 (2002)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 32.

    Park JB , Kim YK (2003): Metallic biomaterials. In: Biomaterials: Principles and Application, eds Park JB, Bronzino JD, CRC Press, Boca Raton, pp. 120

    • Search Google Scholar
    • Export Citation
  • 33.

    DeGarmo PE (1979): Materials and Processes in Manufacturing. Collin Macmillan, New York, USA

  • 34.

    Saris NE , Mervaala E , Karppanen H , Khawaja JA , Lewenstam A : Magnesium: An update on physiological, clinical and analytical aspects. Clin Chim Acta 294, 126 (2000)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 35.

    Revell PA , Damien E , Zhang XS , Evans P , Howlett CR : The effect of magnesium ions on bone bonding to hydroxyapatite. Key Eng Mater 254–256, 447450 (2004)

    • Search Google Scholar
    • Export Citation
  • 36.

    Yamasaki Y , Yoshida Y , Okazaki M , Shimazu A , Uchida T , Kubo T , Akagawa Y , Hamada Y , Takahashi J , Matsuura N : Synthesis of functionally graded MgCO3 apatite accelerating osteoblast adhesion. J Biomed Mater Res A 62, 99105 (2002)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 37.

    Zreiqat H , Howlett CR , Zannettino A , Evans P , Schulze-Tanzil G , Knabe C , Shakibaei M : Mechanisms of magnesium-stimulated adhesion of osteoblastic cells to commonly used orthopaedic implants. J Biomed Mater Res 62, 175184 (2002)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 38.

    Lambotte A : Lutilisation du magnesium comme materiel perdu dans losteosynthese [The use of magnesium as material for osteosynthesis]. Bull Mem Soc Nat Chir 28, 13251334 (1932)

    • Search Google Scholar
    • Export Citation
  • 39.

    Verbrugge J : Le matériel métallique résorbable en chirurgie osseuse [Resorbable metallic material in bone surgery]. Presse Med 23, 460465 (1934)

    • Search Google Scholar
    • Export Citation
  • 40.

    Groves E : An experimental study of the operative treatment of fractures. Br J Surg 1, 438501 (1913)

  • 41.

    Zierold AA : Reaction of bone to various metals. Arch Surg 9, 365412 (1924)

  • 42.

    Verbrugge J : L’utilisation du magnésium dans le traitement chirurgical des fractures [The use of magnesium in the surgical treatment of fractures]. Bull Mém Soc Nat Cir 59, 813823 (1937)

    • Search Google Scholar
    • Export Citation
  • 43.

    McBride ED : Absorbable metal in bone surgery. JAMA 111, 24642467 (1938)

  • 44.

    McBride ED : Magnesium screw and nail transfixion in fractures. South Med J 31, 508515 (1938)

  • 45.

    Maier O : Uber die Verwendbarkeit von Leichtmetallen in der Chirurgie (metallisches Magnesium als Reizmittel zur Knochenneubildung) [About the availability of light metals in surgery (metallic magnesium as a stimulant for bone formation)]. Deut Z Chir 253, 552556 (1940)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 46.

    Troitskii VV , Tsitrin DN : The resorbing metallic alloy ‘Osteosinthezit’ as material for fastening broken bone. Khirurgiia 8, 4144 (1944)

    • Search Google Scholar
    • Export Citation
  • 47.

    Znamenskii MS : Metallic osteosynthesis by means of an apparatus made of resorbing metal. Khirurgiia 12, 6063 (1945)

  • 48.

    Borodkin VS , Savitsky E , Sivash KM , Stroganov GB , Terekhova V , Tikhova NM , Volkov MV : Magnesium-base alloys for use in bone surgery. US Patent No. 3687135A (1972)

    • Search Google Scholar
    • Export Citation
  • 49.

    Witte F , Kaese V , Haferkamp H , Switzer E , Meyer-Lindenberg C , Wirth CJ , Windhagen H : In vivo corrosion of four magnesium alloys and the associated bone response. Biomaterials 26, 35573563 (2005)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 50.

    Trincă LC , Fântânariu M , Solcan C , Trofin AL , Burtan L , Acatrinei DM , Stanciu S , Istrate B , Munteanu C : In vivo degradation behavior and biological activity of some new Mg–Ca alloys with concentration’s gradient of Si for bone grafts. Appl Surf Sci 352, 140150 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 51.

    Wang J , Jiang H , Bi Y , Sun J , Chen M , Liu D : Effects of gas produced by degradation of Mg–Zn–Zr Alloy on cancellous bone tissue. Mater Sci Eng C Mater Biol Appl 55, 556561 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 52.

    Pan H , Qin G , Xu M , Fu H , Ren Y , Pan F , Gao Z , Zhao C , Yang Q , She J , Song B : Enhancing mechanical properties of Mg–Sn alloys by combining addition of Ca and Zn. Mater Des 83, 736744 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 53.

    Lu F , Ma A , Jiang J , Chen J , Song D , Yuan Y , Chen J , Yang D : Enhanced mechanical properties and rolling formability of fine-grained Mg–Gd–Zn–Zr alloy produced by equal-channel angular pressing. J Alloys Compounds 643, 2833 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 54.

    Liu Y , Bian D , Wu Y , Li N , Qiu K , Zheng Y , Han Y : Influence of biocompatible metal ions (Ag, Fe, Y) on the surface chemistry, corrosion behavior and cytocompatibility of Mg–1Ca alloy treated with MEVVA. Colloids Surf B Biointerfaces 133, 99107 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 55.

    Han J , Wan P , Ge Y , Fan X , Tan L , Li J , Yang K : Tailoring the degradation and biological response of a magnesium–strontium alloy for potential bone substitute application. Mater Sci Eng C 58, 799811 (2016)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 56.

    Zhou YL , Li Y , Luo DM , Ding Y , Hodgson P : Microstructures, mechanical and corrosion properties and biocompatibility of as extruded Mg–Mn–Zn–Nd alloys for biomedical applications. Mater Sci Eng C Mater Biol Appl 49, 93100 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 57.

    Witte F , Hort N , Vogt C , Cohen S , Kainer KU , Willumeit R , Feyerabend F : Degradable biomaterials based on magnesium corrosion. Curr Opin Solid State Mater Sci 12, 6372 (2008)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 58.

    Zhen Z , Xi T-F , Zheng Y-F : A review on in vitro corrosion performance test of biodegradable metallic materials. Trans Nonferr Metal Soc China 23, 22832293 (2013)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 59.

    Zhang S , Zhang X , Zhao C , Li J , Song Y , Xie C , Tao H , Zhang Y , He Y , Jiang Y , Bian Y : Research on an Mg–Zn alloy as a degradable biomaterial. Acta Biomater 6, 626640 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 60.

    Wen Z , Wu C , Dai C , Yang F : Corrosion behaviors of Mg and its alloys with different Al contents in a modified simulated body fluid. J Alloys Compounds 488, 392399 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 61.

    Seitz JM , Collier K , Wulf E , Bormann D , Bach FW : Comparison of the corrosion behavior of coated and uncoated magnesium alloys in an in vitro corrosion environment. Adv Eng Mater 13, 313323 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 62.

    Kirkland NT , Lespagnol L , Birbilis N , Staiger MP : A survey of bio-corrosion rates of magnesium alloys. Corros Sci 52, 287291 (2010)

  • 63.

    Walker J , Shadanbaz S , Kirkland NT , Stace E , Woodfield T , Staiger MP , Diaz GJ : Magnesium alloys: Predicting in vivo corrosion with in vitro immersion testing. J Biomed Mater Res B Appl Biomater 100, 11341141 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 64.

    Gu X , Zheng Y , Cheng Y , Zhong S , Xi T : In vitro corrosion and biocompatibility of binary magnesium alloys. Biomaterials 30, 484498 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 65.

    Zainal Abidin NI , Rolfe B , Owen H , Malisano J , Martin D , Hofstetter J , Uggowitzer PJ , Atrens A : The in vivo and in vitro corrosion of high-purity magnesium and magnesium alloys WZ21 and AZ91. Corros Sci 75, 354366 (2013)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 66.

    Wang H , Shi Z : In vitro biodegradation behavior of magnesium and magnesium alloy. J Biomed Mater Res B Appl Biomater 98, 203209 (2011)

  • 67.

    Barfield W , Colbath G , DesJardins JD , Yuehuei HA , Hartsock LA : The potential of magnesium alloy use in orthopaedic surgery. Curr Pract Orthop Surg 23, 146150 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 68.

    Kirkland NT , Birbilis N , Staiger MP : Assessing the corrosion of biodegradable magnesium implants: A critical review of current methodologies and their limitations. Acta Mater 8, 925936 (2012)

    • Search Google Scholar
    • Export Citation
  • 69.

    Muller WD , de Mele MF , Nascimento ML , Zeddies M : Degradation of magnesium and its alloys: Dependence on the composition of the synthetic biological media. J Biomed Mater Res A 90, 487495 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 70.

    Yamamoto A , Hiromoto S : Effect of inorganic salts, amino acids and proteins on the degradation of pure magnesium in vitro. Mater Sci Eng C 29, 15591568 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 71.

    Yang L , Zhang E : Biocorrosion behavior of magnesium alloy in different simulated fluids for biomedical application. Mater Sci Eng C Mater Biol Appl 29, 16911696 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 72.

    Shi Z , Liu M , Atrens A : Measurement of the corrosion rate of magnesium alloys using Tafel extrapolation. Corros Sci 52, 579588 (2010)

  • 73.

    Yang W , Zhang Y , Yang J , Tan L , Yang K : Potential antiosteoporosis effect of biodegradable magnesium implanted in STZ-induced diabetic rats. J Biomed Mater Res A 99, 386394 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 74.

    Chai H , Guo L , Wang X , Gao X , Liu K , Fu Y , Guan J , Tan L , Yang K : In vitro and in vivo evaluations on osteogenesis and biodegradability of a beta-tricalcium phosphate coated magnesium alloy. J Biomed Mater Res A 100, 293304 (2011)

    • Search Google Scholar
    • Export Citation
  • 75.

    Kraus T , Fischerauer SF , Hanzi AC , Uggowitzer PJ , Loffler JF , Weinberg AM : Magnesium alloys for temporary implants in osteosynthesis: In vivo studies of their degradation and interaction with bone. Acta Biomater 8, 12301238 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 76.

    Badawy WA , Hilal NH , El-Rabiee M , Nady H : Electrochemical behavior of Mg and some Mg alloys in aqueous solutions of different pH. Electrochim Acta 55, 18801887 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 77.

    Witte F , Fischer J , Nellesen J , Crostack HA , Kaese V , Pisch A , Beckmann F , Windhagen H : In vitro and in vivo corrosion measurements of magnesium alloys. Biomaterials 27, 10131018 (2006)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 78.

    Erdmann N , Bondarenko A , Hewicker-Trautwein M , Angrisani N , Reifenrath J , Lucas A , Meyer-Lindenberg A : Evaluation of the soft tissue biocompatibility of MgCa0.8 and surgical steel 316L in vivo: A comparative study in rabbits. Biomed Eng Online 9, 63 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 79.

    Muller WD , Nascimento ML , Zeddies M , Córsico M , Gassa LM , Mele MA : Magnesium and its alloys as degradable biomaterials: Corrosion studies using potentiodynamic and EIS electrochemical techniques. Mater Res 10, 510 (2007)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 80.

    Witte F , Ulrich H , Rudert M , Willbold E : Biodegradable magnesium scaffolds: Part 1: Appropriate inflammatory response. J Biomed Mater Res A 81, 748756 (2007)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 81.

    Xu LP , Yu GN , Zhang E , Pan F , Yang K : In vivo corrosion behavior of Mg–Mn–Zn alloy for bone implant: Application. J Biomed Mater Res A 83, 703711 (2007)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 82.

    Zhang GD , Huang JJ , Yang K , Zhang BC , Ai HJ : Experimental study of in vivo implantation of a magnesium alloy at early stage. Acta Metall Sin 43, 11861190 (2007)

    • Search Google Scholar
    • Export Citation
  • 83.

    Avedesian MM (1999): Magnesium and Magnesium Alloys. ASM International, Materials Park, OH

  • 84.

    Bach FW , Schaper M , Jaschik C : Influence of lithium on hcp magnesium alloys. Mater Sci Forum 419–422, 10371042 (2003)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 85.

    Friedrich HE , Mordike BL (2006): Magnesium Technology. Springer-Verlag, Berlin – Heidelberg

  • 86.

    Wu RZ , Qu ZK , Zhang ML : Reviews on the influences of alloying elements on the microstructure and mechanical properties of Mg–Li base alloys. Rev Adv Mater Sci 24, 3543 (2010)

    • Search Google Scholar
    • Export Citation
  • 87.

    Wang Y , Lim CS , Lim CV , Yong MS , Teo EK , Moh LN : In vitro studying corrosion behaviour of biocorrodible Mg alloys. Mater Sci Eng C Mater Biol Appl 31, 579587 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 88.

    Ferreira PC , Piai Kde A , Takayanagui AM , Segura-Munoz SI : Aluminum as a risk factor for Alzheimer’s disease. Rev Lat Am Enfermagem 16, 151157 (2008)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 89.

    Okazaki Y , Rao S , Ito Y , Tateishi T : Corrosion resistance, mechanical properties, corrosion fatigue strength and cytocompatibility of new Ti alloys without Al and V. Biomaterials 19, 11971215 (1998)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 90.

    Shingde M , Hughes J , Boadle R , Wills EJ , Pamphlett R : Macrophagic myofasciitis associated with vaccine-derived aluminium. Med J Aust 183, 145146 (2005)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 91.

    Lastra MD , Pastelin R , Camacho A , Monroy B , Aguilar AE : Zinc intervention on macrophages and lymphocytes response. J Trace Elem Med Biol 15, 510 (2001)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 92.

    Saltman PD , Strause LG : The role of trace minerals in osteoporosis. J Am Coll Nutr 12, 384389 (1993)

  • 93.

    Bowen PK , Drelich J , Goldman J : Zinc exhibits ideal physiological corrosion behavior for bioabsorbable stents. Adv Mater 25, 25772582 (2013)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 94.

    Zhang B , Wang Y , Geng L (2011): Research on Mg-Zn-Ca alloy as degradable biomaterial. In: Biomaterials – Physics and Chemistry, ed Pignatello R, InTech, Rijeka, pp. 183204

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 95.

    Bruno Z , Peter JU , Jörg FL : MgZnCa glasses without clinically observable hydrogen evolution for biodegradable implants. Nat Mater 8, 887891 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 96.

    Zhang B , Hou Y , Wang X , Wang Y , Geng L : Mechanical properties, degradation performance and cytotoxicity of Mg–Zn–Ca biomedical alloys with different compositions. Mater Sci Eng C Mater Biol Appl 31, 16671673 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 97.

    Zhang E , Yin D , Xu L , Yang L , Yang K : Microstructure, mechanical and corrosion properties and biocompatibility of Mg–Zn–Mn alloys for biomedical application. Mater Sci Eng C Mater Biol Appl 29, 987993 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 98.

    Huan Z , Leeflang M , Zhou J , Fratila-Apachitei L , Duszczyk J : In vitro degradation behavior and cytocompatibility of Mg–Zn–Zr alloys. J Mater Sci Mater Med 21, 26232635 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 99.

    Renkema KY , Alexander RT , Bindels RJ , Hoenderop JG : Calcium and phosphate homeostasis: Concerted interplay of new regulators. Ann Med 40, 8291 (2008)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 100.

    Wan Y , Xiong G , Luo H , He F , Huang Y , Zhou X : Preparation and characterization of a new biomedical magnesium–calcium alloy. Mater Des 29, 20342037 (2008)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 101.

    Li Y , Hodgson P , Wen CE : The effects of calcium and yttrium additions on the microstructure, mechanical properties and biocompatibility of biodegradable magnesium alloys. J Mater Sci 46, 365371 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 102.

    Du H , Wei ZJ , Liu XW , Zhang EL : Effects of Zn on the microstructure, mechanical property and bio-corrosion property of Mg–3Ca alloys for biomedical application. Mater Chem Phys 125, 568575 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 103.

    Kirkland NT , Birbilis N , Walker J , Woodfield T , Dias GJ , Staiger MP : In vitro dissolution of magnesium–calcium binary alloys: Clarifying the unique role of calcium additions in bioresorbable magnesium implant alloys. Biomed Mater Res B Appl Biomater 95, 91100 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 104.

    Aschner M , Guilarte TR , Schneider JS , Zheng W : Manganese: Recent advances in understanding its transport and neurotoxicity. Toxicol Appl Pharmacol 221, 131147 (2007)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 105.

    Friedrich HE , Mordike BL (2005): Magnesium Technology – Metallurgy, Design Date, Applications. Springer-Verlag, Berlin – Heidelberg – New York

    • Search Google Scholar
    • Export Citation
  • 106.

    Tsai MH , Chen MS , Lin LH , Lin MH , Wu CZ , Ou KL , Yu CH : Effect of heat treatment on the microstructures and damping properties of biomedical Mg–Zr alloy. J Alloys Compounds 509, 813819 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 107.

    Zhang W , Li M , Chen Q , Hu W , Zhang W , Xin W : Effects of Sr and Sn on microstructure and corrosion resistance of Mg–Zr–Ca magnesium alloy for biomedical applications. Mater Des 39, 379383 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 108.

    Li Y , Wen C , Mushahary D , Sravanthi R , Harishankar N , Pande G , Hodgson P : Mg–Zr–Sr alloys as biodegradable implant materials. Acta Biomater 8, 31773188 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 109.

    MEL (2005): Magnesium Elektron Datasheet 467: Elektron WE43

  • 1.

    Fagali NS , Grilloa CA , Puntarulo S , Fernández Lorenzo de Mele MA : Cytotoxicity of corrosion products of degradable Fe-based stents: Relevance of pH and insoluble products. Colloids Surf B Biointerfaces 128, 480488 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 2.

    Moravej M , Mantovani D : Biodegradable metals for cardiovascular stent application: Interests and new opportunities. Int J Mol Sci 12, 42504270 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 3.

    Mani G , Feldman MD , Patel D , Agrawal CM : Coronary stents: A materials perspective. Biomaterials 28, 16891710 (2007)

  • 4.

    Peuster M , Wohlsein P , Brugmann M , Ehlerding M , Seidler K , Fink C , Brauer H , Fischer A , Hausdorf G : A novel approach to temporary stenting: Degradable cardiovascular stents produced from corrodible metal – Results 6–18 months after implantation into New Zealand white rabbits. Heart 86, 563569 (2001)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 5.

    Purnama A , Hermawan H , Couet J , Mantovani D : Assessing the biocompatibility of degradable metallic materials: State-of-the-art and focus on the potential of genetic regulation. Acta Biomater 6, 18001807 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 6.

    Kubásek J , Vojtěch D , Jablonská E , Pospíšilová I , Lipov J , Ruml T : Structure, mechanical characteristics and in vitro degradation, cytotoxicity, genotoxicity and mutagenicity of novel biodegradable Zn–Mg alloys. Mater Sci Eng C Mater Biol Appl 58, 2435 (2016)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 7.

    Murni NS , Dambatta MS , Yeap SK , Froemming GR , Hermawan H : Cytotoxicity evaluation of biodegradable Zn-3Mg alloy toward normal human osteoblast cells. Mater Sci Eng C 49, 560566 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 8.

    Sanchez AH , Luthringer BJ , Feyerabend F , Willumeit R : Mg and Mg alloys: How comparable are in vitro and in vivo corrosion rates? A review. Acta Biomater 13, 1631 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 9.

    Liu C , Xin Y , Tang G , Chu PK : Influence of heat treatment on degradation behavior of bio-degradable die-cast AZ63 magnesium alloy in simulated body fluid. Mater Sci Eng A 456, 350357 (2007)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 10.

    Wang Y , Liu G , Fan Z : A new heat treatment procedure for rheo-diecast AZ91D magnesium alloy. Scripta Mater 54, 903908 (2006)

  • 11.

    Zeng RC , Zhang J , Huang WJ , Dietzel W , Kainer KU , Blawert C , Wei KE : Review of studies on corrosion of magnesium alloys. Trans Nonferr Metal Soc China 16, 763771 (2006)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 12.

    Witte F : Reprint of: The history of biodegradable magnesium implants: A review. Acta Biomater 23, 2840 (2015)

  • 13.

    Payr E : Beiträge zur Technik der Blutgefäss – und Nervennaht nebst Mittheilungen über die Verwendung eines resorbirbaren Metalles in der Chirurgie [Contributions to the technique of blood vessel and nerve suture, as well as the use of a resorbable metal in surgery]. Arch Klin Chir 62, 6793 (1900)

    • Search Google Scholar
    • Export Citation
  • 14.

    Payr E : Blutgefäß- und Nervennaht (nebst Mittheilung über die Verwendung eines resorbirbaren Metalles in der Chirurgie) [Blood vessel and nerve suture (in addition to the use of a resorbable metal in surgery)]. Centralblatt Chir 28, 3137 (1901)

    • Search Google Scholar
    • Export Citation
  • 15.

    Hofstetter J , Martinelli E , Pogatscher S , Schmutz P , Povoden-Karadeniz E , Weinberg AM , Uggowitzer PJ , Löffler JF : Influence of trace impurities on the in vitro and in vivo degradation of biodegradable Mg–5Zn–0.3Ca alloys. Acta Biomater 23, 347353 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 16.

    Chlumsky V : Über die Wiederherstellung der Beweglichkeit des Gelenkes bei Ankylose [On restoring the mobility of the joint with ankyloses]. Centralblatt Chir 27, 921925 (1900)

    • Search Google Scholar
    • Export Citation
  • 17.

    Payr E , Martina A : Experimentelle und klinische Beiträge zur Lebernaht und leberresection (Magnesiumplattennaht) [Experimental and clinical contributions to the liver suture and liver resection (magnesium plate seam)]. Arch Klin Chir 77, 962998 (1905)

    • Search Google Scholar
    • Export Citation
  • 18.

    Payr E : Ueber Verwendung von Magnesium zur Behandlung von Blutgefässerkrankungen [On the use of magnesium for the treatment of blood vessel diseases]. Deut Z Chir 63, 503511 (1902)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 19.

    Payr E : Zur Technik der Behandlung kavernöser Tumoren [The technique of treating cavernous tumors]. Zentralblatt Chir 30, 233234 (1903)

    • Search Google Scholar
    • Export Citation
  • 20.

    Sonntag E : Die Hämangiome und ihre Behandlung [The hemangiomas and their treatment]. Ergebn Chir Orthop 8, 1156 (1914)

  • 21.

    Chlumsky V : Beiträge zur Darmknopffrage [Contribution to the intestine]. Mitt Grenzgebieten Med Chir 3, 416451 (1907)

  • 22.

    Höpfner E : Ueber Gefässnaht, Gefässtransplantation und Replantation von amputierten Extremitäten [About vascular suture, vascular transplantation and replantation of amputated limbs]. Arch Klin Chir 70, 417471 (1903)

    • Search Google Scholar
    • Export Citation
  • 23.

    Lespinasse VD : A practical mechanical method of end-to-end anastomosis of blood-vessels: Using absorbable magnesium rings. JAMA 55, 17851790 (1910)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 24.

    Andrews EW : Absorbable metal clips as substitutes for ligatures in wound closure. JAMA 28, 278281 (1917)

  • 25.

    Seelig MG : A study of magnesium wire as an absorbable suture and ligature material. Arch Surg 8, 669680 (1924)

  • 26.

    Glass E : Klinische und experimentelle Untersuchungen uber die Payrsche Magnesiumpfeil behandlung von Angiomen [Clinical and experimental studies of the Payr’s magnesium wires in treatment of angiomas]. Deut Z Chir 194, 352366 (1926)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 27.

    Wilflingseder P , Martin R , Papp C : Magnesium seeds in the treatment of lymph- and haemangiomata. Chir Plast 6, 105116 (1981)

  • 28.

    Hoffheinz S , Dimitroff N : Experimentelle Studie uber die Resorption parental zugefuhrten metallischen Magnesiums [Experimental study of the absorption parentally fed metallic magnesium]. Deut Z Chir 208, 346353 (1928)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 29.

    Stone P , Lord JW Jr : An experimental study of the thrombogenic properties of magnesium and magnesium–aluminum wire in the dog’s aorta. Surgery 30, 987993 (1951)

    • Search Google Scholar
    • Export Citation
  • 30.

    Nagels J , Stokdijk M , Rozing PM : Stress shielding and bone resorption shoulder arthroplasty. J Shoulder Elbow Surg 12, 3539 (2003)

  • 31.

    Wang ML , Nesti LJ , Tuli R , Lazatin J , Danielson KG , Sharkey PF , Tuan RS : Titanium particles suppress expression of osteoblastic phenotype in human mesenchymal stem cells. J Orthop Res 20, 11751184 (2002)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 32.

    Park JB , Kim YK (2003): Metallic biomaterials. In: Biomaterials: Principles and Application, eds Park JB, Bronzino JD, CRC Press, Boca Raton, pp. 120

    • Search Google Scholar
    • Export Citation
  • 33.

    DeGarmo PE (1979): Materials and Processes in Manufacturing. Collin Macmillan, New York, USA

  • 34.

    Saris NE , Mervaala E , Karppanen H , Khawaja JA , Lewenstam A : Magnesium: An update on physiological, clinical and analytical aspects. Clin Chim Acta 294, 126 (2000)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 35.

    Revell PA , Damien E , Zhang XS , Evans P , Howlett CR : The effect of magnesium ions on bone bonding to hydroxyapatite. Key Eng Mater 254–256, 447450 (2004)

    • Search Google Scholar
    • Export Citation
  • 36.

    Yamasaki Y , Yoshida Y , Okazaki M , Shimazu A , Uchida T , Kubo T , Akagawa Y , Hamada Y , Takahashi J , Matsuura N : Synthesis of functionally graded MgCO3 apatite accelerating osteoblast adhesion. J Biomed Mater Res A 62, 99105 (2002)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 37.

    Zreiqat H , Howlett CR , Zannettino A , Evans P , Schulze-Tanzil G , Knabe C , Shakibaei M : Mechanisms of magnesium-stimulated adhesion of osteoblastic cells to commonly used orthopaedic implants. J Biomed Mater Res 62, 175184 (2002)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 38.

    Lambotte A : Lutilisation du magnesium comme materiel perdu dans losteosynthese [The use of magnesium as material for osteosynthesis]. Bull Mem Soc Nat Chir 28, 13251334 (1932)

    • Search Google Scholar
    • Export Citation
  • 39.

    Verbrugge J : Le matériel métallique résorbable en chirurgie osseuse [Resorbable metallic material in bone surgery]. Presse Med 23, 460465 (1934)

    • Search Google Scholar
    • Export Citation
  • 40.

    Groves E : An experimental study of the operative treatment of fractures. Br J Surg 1, 438501 (1913)

  • 41.

    Zierold AA : Reaction of bone to various metals. Arch Surg 9, 365412 (1924)

  • 42.

    Verbrugge J : L’utilisation du magnésium dans le traitement chirurgical des fractures [The use of magnesium in the surgical treatment of fractures]. Bull Mém Soc Nat Cir 59, 813823 (1937)

    • Search Google Scholar
    • Export Citation
  • 43.

    McBride ED : Absorbable metal in bone surgery. JAMA 111, 24642467 (1938)

  • 44.

    McBride ED : Magnesium screw and nail transfixion in fractures. South Med J 31, 508515 (1938)

  • 45.

    Maier O : Uber die Verwendbarkeit von Leichtmetallen in der Chirurgie (metallisches Magnesium als Reizmittel zur Knochenneubildung) [About the availability of light metals in surgery (metallic magnesium as a stimulant for bone formation)]. Deut Z Chir 253, 552556 (1940)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 46.

    Troitskii VV , Tsitrin DN : The resorbing metallic alloy ‘Osteosinthezit’ as material for fastening broken bone. Khirurgiia 8, 4144 (1944)

    • Search Google Scholar
    • Export Citation
  • 47.

    Znamenskii MS : Metallic osteosynthesis by means of an apparatus made of resorbing metal. Khirurgiia 12, 6063 (1945)

  • 48.

    Borodkin VS , Savitsky E , Sivash KM , Stroganov GB , Terekhova V , Tikhova NM , Volkov MV : Magnesium-base alloys for use in bone surgery. US Patent No. 3687135A (1972)

    • Search Google Scholar
    • Export Citation
  • 49.

    Witte F , Kaese V , Haferkamp H , Switzer E , Meyer-Lindenberg C , Wirth CJ , Windhagen H : In vivo corrosion of four magnesium alloys and the associated bone response. Biomaterials 26, 35573563 (2005)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 50.

    Trincă LC , Fântânariu M , Solcan C , Trofin AL , Burtan L , Acatrinei DM , Stanciu S , Istrate B , Munteanu C : In vivo degradation behavior and biological activity of some new Mg–Ca alloys with concentration’s gradient of Si for bone grafts. Appl Surf Sci 352, 140150 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 51.

    Wang J , Jiang H , Bi Y , Sun J , Chen M , Liu D : Effects of gas produced by degradation of Mg–Zn–Zr Alloy on cancellous bone tissue. Mater Sci Eng C Mater Biol Appl 55, 556561 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 52.

    Pan H , Qin G , Xu M , Fu H , Ren Y , Pan F , Gao Z , Zhao C , Yang Q , She J , Song B : Enhancing mechanical properties of Mg–Sn alloys by combining addition of Ca and Zn. Mater Des 83, 736744 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 53.

    Lu F , Ma A , Jiang J , Chen J , Song D , Yuan Y , Chen J , Yang D : Enhanced mechanical properties and rolling formability of fine-grained Mg–Gd–Zn–Zr alloy produced by equal-channel angular pressing. J Alloys Compounds 643, 2833 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 54.

    Liu Y , Bian D , Wu Y , Li N , Qiu K , Zheng Y , Han Y : Influence of biocompatible metal ions (Ag, Fe, Y) on the surface chemistry, corrosion behavior and cytocompatibility of Mg–1Ca alloy treated with MEVVA. Colloids Surf B Biointerfaces 133, 99107 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 55.

    Han J , Wan P , Ge Y , Fan X , Tan L , Li J , Yang K : Tailoring the degradation and biological response of a magnesium–strontium alloy for potential bone substitute application. Mater Sci Eng C 58, 799811 (2016)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 56.

    Zhou YL , Li Y , Luo DM , Ding Y , Hodgson P : Microstructures, mechanical and corrosion properties and biocompatibility of as extruded Mg–Mn–Zn–Nd alloys for biomedical applications. Mater Sci Eng C Mater Biol Appl 49, 93100 (2015)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 57.

    Witte F , Hort N , Vogt C , Cohen S , Kainer KU , Willumeit R , Feyerabend F : Degradable biomaterials based on magnesium corrosion. Curr Opin Solid State Mater Sci 12, 6372 (2008)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 58.

    Zhen Z , Xi T-F , Zheng Y-F : A review on in vitro corrosion performance test of biodegradable metallic materials. Trans Nonferr Metal Soc China 23, 22832293 (2013)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 59.

    Zhang S , Zhang X , Zhao C , Li J , Song Y , Xie C , Tao H , Zhang Y , He Y , Jiang Y , Bian Y : Research on an Mg–Zn alloy as a degradable biomaterial. Acta Biomater 6, 626640 (2010)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 60.

    Wen Z , Wu C , Dai C , Yang F : Corrosion behaviors of Mg and its alloys with different Al contents in a modified simulated body fluid. J Alloys Compounds 488, 392399 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 61.

    Seitz JM , Collier K , Wulf E , Bormann D , Bach FW : Comparison of the corrosion behavior of coated and uncoated magnesium alloys in an in vitro corrosion environment. Adv Eng Mater 13, 313323 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 62.

    Kirkland NT , Lespagnol L , Birbilis N , Staiger MP : A survey of bio-corrosion rates of magnesium alloys. Corros Sci 52, 287291 (2010)

  • 63.

    Walker J , Shadanbaz S , Kirkland NT , Stace E , Woodfield T , Staiger MP , Diaz GJ : Magnesium alloys: Predicting in vivo corrosion with in vitro immersion testing. J Biomed Mater Res B Appl Biomater 100, 11341141 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 64.

    Gu X , Zheng Y , Cheng Y , Zhong S , Xi T : In vitro corrosion and biocompatibility of binary magnesium alloys. Biomaterials 30, 484498 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 65.

    Zainal Abidin NI , Rolfe B , Owen H , Malisano J , Martin D , Hofstetter J , Uggowitzer PJ , Atrens A : The in vivo and in vitro corrosion of high-purity magnesium and magnesium alloys WZ21 and AZ91. Corros Sci 75, 354366 (2013)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 66.

    Wang H , Shi Z : In vitro biodegradation behavior of magnesium and magnesium alloy. J Biomed Mater Res B Appl Biomater 98, 203209 (2011)

  • 67.

    Barfield W , Colbath G , DesJardins JD , Yuehuei HA , Hartsock LA : The potential of magnesium alloy use in orthopaedic surgery. Curr Pract Orthop Surg 23, 146150 (2012)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 68.

    Kirkland NT , Birbilis N , Staiger MP : Assessing the corrosion of biodegradable magnesium implants: A critical review of current methodologies and their limitations. Acta Mater 8, 925936 (2012)

    • Search Google Scholar
    • Export Citation
  • 69.

    Muller WD , de Mele MF , Nascimento ML , Zeddies M : Degradation of magnesium and its alloys: Dependence on the composition of the synthetic biological media. J Biomed Mater Res A 90, 487495 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 70.

    Yamamoto A , Hiromoto S : Effect of inorganic salts, amino acids and proteins on the degradation of pure magnesium in vitro. Mater Sci Eng C 29, 15591568 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 71.

    Yang L , Zhang E : Biocorrosion behavior of magnesium alloy in different simulated fluids for biomedical application. Mater Sci Eng C Mater Biol Appl 29, 16911696 (2009)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 72.

    Shi Z , Liu M , Atrens A : Measurement of the corrosion rate of magnesium alloys using Tafel extrapolation. Corros Sci 52, 579588 (2010)

  • 73.

    Yang W , Zhang Y , Yang J , Tan L , Yang K : Potential antiosteoporosis effect of biodegradable magnesium implanted in STZ-induced diabetic rats. J Biomed Mater Res A 99, 386394 (2011)

    • Crossref
    • Search Google Scholar
    • Export Citation
  • 74.

    Chai H , Guo L , Wang X , Gao X , Liu K , Fu Y , Guan J , Tan L , Yang K : In vitro and in vivo evaluations on osteogenesis and biodegradability of a beta-tricalcium phosphate coated magnesium alloy. J Biomed Mater Res A 100, 293304 (2011)

    • Search Google Scholar
    • Export Citation
  • 75.

    Kraus T , Fischerauer SF , Hanzi AC , Uggowitzer PJ , Loffler JF , Weinberg AM : Magnesium alloys for temporary implants in osteosynthesis: In vivo studies of their degradation and interaction with bone. Acta Biomater 8, 12301238 (2012)

    • Crossref