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Gellan Gum-Hyaluronic Acid Spongy-like Hydrogels and Cells from Adipose Tissue Synergize Promoting Neoskin Vascularization

机译:结冷胶透明质酸海绵状水凝胶和来自脂肪组织的细胞协同促进新皮血管化。

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Currently available substitutes for skin wound healing often result in the formation of nonfunctional neotissue. Thus, urgent care is still needed to promote an effective and complete regeneration. To meet this need, we proposed the assembling of a construct that takes advantage of cell-adhesive gellan gum-hyaluronic acid (GG-HA) spongy-like hydrogels and a powerful cell-machinery obtained from adipose tissue, human adipose stem cells (hASCs), and microvascular endothelial cells (hAMECs). In addition to a cell-adhesive character, GG-HA spongy-like hydrogels overpass limitations of traditional hydrogels, such as reduced physical stability and limited manipulation, due to improved microstructural arrangement characterized by pore wall thickening and increased mean pore size. The proposed constructs combining cellular mediators of the healing process within the spongy-like hydrogels that intend to recapitulate skin matrix aim to promote neoskin vascularization. Stable and off-the-shelf dried GG-HA polymeric networks, rapidly rehydrated at the time of cell seeding then depicting features of both sponges and hydrogels, enabled the natural cell entrapment/encapsulation and attachment supported by cell-polymer interactions. Upon transplantation into mice full-thickness excisional wounds, GG-HA spongy-like hydrogels absorbed the early inflammatory cell infiltrate and led to the formation of a dense granulation tissue. Consequently, spongy-like hydrogel degradation was observed, and progressive wound closure, re-epithelialization, and matrix remodelling was improved in relation to the control condition. More importantly, GG-HA spongy-like hydrogels promoted a superior neovascularization, which was enhanced in the presence of human hAMECs, also found in the formed neovessels. These observations highlight the successful integration of a valuable matrix and prevascularization cues to target angiogenesiseovascularization in skin full-thickness excisional wounds.
机译:当前可用的皮肤伤口愈合的替代物经常导致无功能的新组织的形成。因此,仍然需要紧急护理以促进有效和完全的再生。为了满足这一需求,我们提出了一种利用细胞粘附性吉兰糖-透明质酸(GG-HA)海绵状水凝胶和从脂肪组织,人脂肪干细胞(hASCs)获得的强大细胞机械的构造进行组装)和微血管内皮细胞(hAMEC)。除具有细胞粘附特性外,GG-HA海绵状水凝胶还克服了传统水凝胶的局限性,例如由于孔壁增厚和平均孔径增大而改善的微结构排列,降低了物理稳定性和限制了操作。拟议的构建体在旨在重塑皮肤基质的海绵状水凝胶中结合了愈合过程的细胞介体,旨在促进新皮肤血管形成。稳定且现成的干燥GG-HA聚合物网络在细胞接种时迅速重新水化,然后描绘了海绵和水凝胶的特征,使得细胞-聚合物相互作用能够支持天然的细胞捕获/包封和附着。移植至小鼠全层切除伤口后,GG-HA海绵状水凝胶吸收了早期炎症细胞的浸润并导致了致密的肉芽组织的形成。因此,观察到海绵状的水凝胶降解,并且相对于对照条件,进行性伤口闭合,再上皮化和基质重塑得到改善。更重要的是,GG-HA海绵状水凝胶促进了优异的新血管形成,在人类hAMEC的存在下也增强了血管新生,在形成的新血管中也有发现。这些观察结果突出了有价值的基质和血管形成前线索的成功整合,以靶向皮肤全层切除伤口中的血管生成/新生血管形成。

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