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FGF-7 expression enhances the performance of bioengineered skin.

作者信息

Erdag Gulsun, Medalie Daniel A, Rakhorst Hinne, Krueger Gerald G, Morgan Jeffrey R

机构信息

Center for Engineering in Medicine and Surgery, Massachusetts General Hospital and Harvard Medical School and Shriners Hospital for Children, Boston, MA 02114, USA.

出版信息

Mol Ther. 2004 Jul;10(1):76-85. doi: 10.1016/j.ymthe.2004.04.013.

Abstract

To improve the performance of bioengineered skin, we used a recombinant retrovirus encoding FGF-7 to modify diploid human keratinocytes genetically. Control or FGF-7-expressing keratinocytes were seeded onto acellular human dermis to form bioengineered skin. Gene-modified skin secreted significant levels of FGF-7 and formed a thicker and hyperproliferative epidermis with about four times the number of cells per square centimeter. Secretion of an endogenous trophic factor, VEGF, was increased approximately 5-fold. Migration of FGF-7-expressing keratinocytes was stimulated as was the self-healing of bioengineered skin expressing FGF-7. When tested in a bacterial infection model, the antimicrobial properties of FGF-7-expressing skin were increased >500-fold against both gram-negative and gram-positive bacteria. After transplantation to full-thickness wounds on athymic mice, skin expressing FGF-7 was revascularized more rapidly. These results demonstrate that genetic modification can be used to enhance performance and that expression of FGF-7 augments several properties important to the wound-healing properties of bioengineered skin.

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