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自体微移植物在胶原-糖胺聚糖支架中用于糖尿病伤口愈合的新应用。

Novel application of autologous micrografts in a collagen-glycosaminoglycan scaffold for diabetic wound healing.

作者信息

Panayi Adriana C, Haug Valentin, Liu Qinxin, Wu Mengfan, Karvar Mehran, Aoki Shimpo, Ma Chenhao, Hamaguchi Ryoko, Endo Yori, Orgill Dennis P

机构信息

Department of Surgery, Division of Plastic Surgery, Brigham and Women's Hospital and Harvard Medical School, Boston, MA 02115, United States of America.

Department of Hand, Plastic and Reconstructive Surgery, Microsurgery, Burn Center, BG Trauma Center Ludwigshafen, University of Heidelberg, Ludwigshafen 67071, Germany.

出版信息

Biomed Mater. 2021 Mar 5;16(3). doi: 10.1088/1748-605X/abc3dc.

Abstract

Therapeutic strategies that successfully combine two techniques-autologous micrografting and biodegradable scaffolds-offer great potential for improved wound repair and decreased scarring. In this study we evaluate the efficacy of a novel modification of a collagen-glycosaminoglycan (collagen-GAG) scaffold with autologous micrografts using a murine dorsal wound model. db/db mice underwent a full thickness 1.0 cmdorsal wound excision and were treated with a collagen-GAG scaffold (CGS group), a modified collagen-GAG scaffold (CGS + MG group) or simple occlusive dressing (Blank group). The modified scaffold was created by harvesting full thickness micrografts and transplanting these into the collagen-GAG membrane. Parameters of wound healing, including cellular proliferation, collagen deposition, keratinocyte migration, and angiogenesis were assessed. The group treated with the micrograft-modified scaffold healed at a faster rate, showed greater cellular proliferation, collagen deposition, and keratinocyte migration with higher density and greater maturity of microvessels. The grafts remained viable within the scaffold with no evidence of rejection. Keratinocytes were shown to migrate from the wound border and from the micrograft edges towards the center of the wound, while cellular proliferation was present both at the wound border and wound bed. We report successful treatment of diabetic wounds with a novel collagen-GAG scaffold modified with full-thickness automicrografts. Differences in cellular migration and proliferation offer maiden evidence on the mechanisms of wound healing. Clinically, the successful scaffold engraftment, micrograft viability and improved wound healing offer promising results for the development of a new therapeutic modality for wound repair.

摘要

成功结合自体微移植和可生物降解支架这两种技术的治疗策略,为改善伤口修复和减少瘢痕形成提供了巨大潜力。在本研究中,我们使用小鼠背部伤口模型评估了一种新型改良的胶原-糖胺聚糖(collagen-GAG)支架与自体微移植相结合的疗效。db/db小鼠接受了1.0厘米全层背部伤口切除,并分别用胶原-GAG支架(CGS组)、改良胶原-GAG支架(CGS + MG组)或简单封闭敷料(空白组)进行治疗。改良支架是通过采集全层微移植组织并将其移植到胶原-GAG膜中制成的。评估了伤口愈合的参数,包括细胞增殖、胶原沉积、角质形成细胞迁移和血管生成。接受微移植改良支架治疗的组愈合速度更快,细胞增殖、胶原沉积和角质形成细胞迁移更明显,微血管密度更高且成熟度更好。移植物在支架内保持存活,无排斥迹象。角质形成细胞从伤口边缘和微移植边缘向伤口中心迁移,而细胞增殖在伤口边缘和伤口床均有出现。我们报告了用全层自体微移植改良的新型胶原-GAG支架成功治疗糖尿病伤口的情况。细胞迁移和增殖的差异为伤口愈合机制提供了初步证据。临床上,成功的支架植入、微移植存活及改善的伤口愈合为开发新的伤口修复治疗方法提供了有希望的结果。

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