出典(authority):フリー百科事典『ウィキペディア(Wikipedia)』「2015/06/28 18:59:35」(JST)
Artificial skin refers to a collagen scaffold that induces regeneration of skin in mammals. The term was used in the late 1970s and early 1980s to describe a new treatment for massive burns. It was later discovered that treatment of deep skin wounds in adult animals and humans with this scaffold induces regeneration of the dermis. It has been developed commercially under the name IntegraTM and is used in massively burned patients, during plastic surgery of the skin, and in treatment of chronic skin wounds.
Alternatively, the term “artificial skin” sometimes is used to refer to skin-like tissue grown in a laboratory, or to flexible semiconductor materials that can sense touch for those with prosthetic limbs.
The skin is the largest organ in the human body.[1] Skin is made up of three layers, the epidermis, dermis and the fat layer, also called the hypodermis. The epidermis is the outer layer of skin that keeps vital fluids in and harmful bacteria out of the body. The dermis is the inner layer of skin that contains blood vessels, nerves, hair follicles, oil, and sweat glands.[2] Severe damage to large areas of skin exposes the human organism to dehydration and infections that can result in death.
Traditional ways of dealing with large losses of skin have been to use skin grafts from the patient (autografts) or from an unrelated donor or a cadaver. The former approach has the disadvantage that there may not be enough skin available, while the latter suffers from the possibility of rejection or infection. Until the late twentieth century, skin grafts were constructed from the patient's own skin. This became a problem when skin had been damaged extensively, making it impossible to treat severely injured patients entirely with autografts.[3]
A process for inducing regeneration in skin was invented by Dr. Ioannis V. Yannas (then Assistant Professor in the Fibers and Polymers Division, Department of Mechanical Engineering, Massachusetts Institute of Technology, Cambridge MA) and Dr. John F. Burke (then Chief of Staff, Shriners Burns Institute, Boston MA). Their initial objective was to discover a wound cover that would protect severe skin wounds from infection by accelerating wound closure. Several kinds of grafts made of synthetic and natural polymers were prepared and tested in a guinea pig animal model. By late 1970s it was evident that the original objective was not reached. Instead, these experimental grafts typically did not affect the speed of wound closure. In one case, however, a particular type of collagen graft led to significant delay of wound closure.[4] Careful study of histology samples revealed that grafts that delayed wound closure induced the synthesis of new dermis de novo at the injury site, instead of forming scar, which is the normal outcome of the spontaneous wound healing response. This was the first demonstration of regeneration of a tissue (dermis) that does not regenerate by itself in the adult mammal.[5][6][7][8][9][10] After the initial discovery, further research led to the composition and fabrication of grafts that were evaluated in clinical trials.[9][11] These grafts were synthesized as a graft copolymer of microfibrillar type I collagen and a glycosaminoglycan, chondroitin-6-sulfate, fabricated into porous sheets by freeze-drying, and then cross-linked by dehydrothermal treatment.[12] Control of the structural features of the collagen scaffold (average pore size, degradation rate and surface chemistry) was eventually found to be a critical prerequisite for its unusual biological activity.
Several patents were granted to MIT for the discovery of collagen-based grafts that can induce dermis regeneration. U.S. Pat. 4,418,691 (December 6, 1983) was cited by the National Inventors Hall of Fame as the key patent describing the invention of a process for regenerated skin (Inductees Natl Inventors Hall of Fame, 2015[13]). These patents were translated later into a commercial product (IntegraTM) by Integra LifeSciences Corp., a company founded in 1993. IntegraTM grafts received FDA approval in 1996 and since then are being applied worldwide to treat patients who are in need of new skin to treat massive burns, those undergoing plastic surgery of the skin, and patients with chronic skin wounds as well as others who suffer from certain forms of skin cancer. In clinical practice, a thin graft sheet manufactured from the active collagen scaffold is placed on the injury site, which is then covered with a thin sheet of silicone elastomer that protects the wound site from bacterial infection and dehydration. The graft can be seeded with autologous cells (keratinocytes) in order to accelerate wound closure, however the presence of these cells is not required for regenerating the dermis.[8] Grafting skin wounds with IntegraTM leads to the synthesis of normal vascularized and innervated dermis de novo, followed by re-epithelization and formation of epidermis. Although early versions of the scaffold were not capable of regenerating hair follicles and sweat glands, later developments by S.T Boyce and coworkers led to solution of this problem.[14]
The mechanism of regeneration using an active collagen scaffold has been largely clarified. The scaffold retains regenerative activity provided that it has been prepared with appropriate levels of the specific surface (pore size in range 20-125 µm), degradation rate (degradation half-life 14 ± 7 days) and surface chemical features (ligand densities for integrins α1β1 and α2β1 must exceed approximately 200 μΜ α1β1 and α2β1 ligands).[15] It has been hypothesized that specific binding of a sufficient number of contractile cells (myofibroblasts) on the scaffold surface, occurring within a narrow time window, is required for induction of skin regeneration in the presence of this scaffold.[16] Studies with skin wounds have been extended to transected peripheral nerves, and the combined evidence supports a common regeneration mechanism for skin and peripheral nerves using this scaffold.[17]
Research is continually being done on artificial skin. Newer technologies, such as an autologous spray-on skin produced by Avita Medical,[18] are being tested in efforts to accelerate healing and minimize scarring.
The Fraunhofer Institute for Interfacial Engineering and Biotechnology is working towards a fully automated process for producing artificial skin. Their goal is a simple two-layer skin without blood vessels that can be used to study how skin interacts with consumer products, such as creams and medicines. They hope to eventually produce more complex skin that can be used in transplants.[19]
Hanna Wendt, and a team of her colleagues in the Department of Plastic, Hand and Reconstructive Surgery at Medical School Hannover Germany, have found a method for creating artificial skin using spider silk. Before this, however, artificial skin was grown using materials like collagen. These materials did not seem strong enough. Instead, Wendt and her team turned to spider silk, which is known to be 5 times stronger than Kevlar. The silk is harvested by “milking” the silk glands of golden orb web spiders. The silk was spooled as it was harvested, and then it was woven into a rectangular steel frame. The steel frame was 0.7 mm thick and the resulting weave was easy-to-handle, as well as easy to sterilize. Human skin cells were added to the meshwork silk and were found to flourish under an environment providing nutrients, warmth and air. However at this time, using spider silk to grow artificial skin in mass quantities is not practical because of the tedious process of harvesting spider silk.[20]
Australian researchers are currently searching for a new, innovative way to produce artificial skin. This would produce artificial skin quicker, and in a more efficient way. The skin produced would only be 1 millimeter thick and would only be used to rebuild the epidermis. They can also make the skin 1.5 millimeters thick, which would allow the dermis to repair itself if needed. This would require bone marrow from a donation or from the patient's body. The bone marrow would be used as a “seed," and would be placed in the grafts to mimic the dermis. This has been tested on animals and has been proven to work with animal skin. Professor Maitz said, “In Australia, someone with a full-thickness burn to up to 80 per cent of their body surface area has every prospect of surviving the injury…However their quality of life remains questionable as we're unable, at present, to replace the burned skin with normal skin…We're committed to ensuring the pain of survival is worth it, by developing a living skin equivalent.”[21]
Another form of “artificial skin” has been created out of flexible semiconductor materials that can sense touch for those with prosthetic limbs.[22][23] The artificial skin is anticipated to augment robotics in conducting rudimentary jobs that would be considered delicate and require sensitive “touch”.[22][24] Scientists found that by applying a layer of rubber with two parallel electrodes that stored electrical charges inside of the artificial skin, tiny amounts of pressure could be detected. When pressure is exerted, the electrical charge in the rubber is changed and the change is detected by the electrodes. However, the film is so small that when pressure is applied to the skin, the molecules have nowhere to move and become entangled. The molecules also fail to return to their original shape when the pressure is removed.[25] A recent development in the synthetic skin technique has been made by imparting the color changing properties to the thin layer of silicon with the help of artificial ridges which reflect a very specific wavelength of light. By tuning the spaces between these ridges, color to be reflected by the skin can be controlled.[26] This technology can be used in color-shifting camouflages and sensors that can detect otherwise imperceptible defects in buildings, bridges, and aircraft.
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リンク元 | 「人工皮膚」「skin substitute」 |
関連記事 | 「artificial」「skin」 |
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