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丝素蛋白支架结构调控骨髓单核细胞的炎症反应和植入。

Silk Fibroin Scaffold Architecture Regulates Inflammatory Responses and Engraftment of Bone Marrow-Mononuclear Cells.

机构信息

School of Medical Sciences, Faculty of Health and Medicine, The University of Sydney, Sydney, NSW, 2006, Australia.

Charles Perkins Centre, The University of Sydney, Sydney, NSW, 2006, Australia.

出版信息

Adv Healthc Mater. 2021 Aug;10(16):e2100615. doi: 10.1002/adhm.202100615. Epub 2021 May 7.

DOI:10.1002/adhm.202100615
PMID:33963682
Abstract

Despite being one of the most clinically trialed cell therapies, bone marrow-mononuclear cell (BM-MNC) infusion has largely failed to fulfill its clinical promise. Implanting biomimetic scaffolds at sites of injury prior to BM-MNC infusion is a promising approach to enhance BM-MNC engraftment and therapeutic function. Here, it is demonstrated that scaffold architecture can be leveraged to regulate the immune responses that drive BM-MNC engraftment. Silk scaffolds with thin fibers and low porosity (LP) impairs immune activation in vitro compared with thicker fiber, high porosity (HP) scaffolds. Using the authors' established in vivo bioluminescent BM-MNC tracking model, they showed that BM-MNCs home to and engraft in greater numbers in HP scaffolds over 14 days. Histological analysis reveals thicker fibrous capsule formation, with enhanced collagen deposition in HP compared to LP scaffolds consistent with substantially more native CD68 macrophages and CD4 T cells, driven by their elevated pro-inflammatory M1 and Th1 phenotypes, respectively. These results suggest that implant architecture impacts local inflammation that drives differential engraftment and remodeling behavior of infused BM-MNC. These findings inform the future design of biomimetic scaffolds that may better enhance the clinical effectiveness of BM-MNC infusion therapy.

摘要

尽管骨髓单核细胞(BM-MNC)输注是最具临床试验的细胞疗法之一,但它在很大程度上未能实现其临床承诺。在 BM-MNC 输注之前,在损伤部位植入仿生支架是增强 BM-MNC 植入和治疗功能的一种很有前途的方法。在这里,研究表明支架结构可用于调节驱动 BM-MNC 植入的免疫反应。与较厚纤维、高孔隙率(HP)支架相比,具有细纤维和低孔隙率(LP)的丝质支架在体外可削弱免疫激活。使用作者建立的体内生物发光 BM-MNC 跟踪模型,他们表明在 14 天内,HP 支架中 BM-MNC 归巢和植入的数量更多。组织学分析显示,HP 支架中形成的纤维囊更厚,与 LP 支架相比,胶原蛋白沉积增强,这与更多的天然 CD68 巨噬细胞和 CD4 T 细胞一致,这分别由其升高的促炎 M1 和 Th1 表型驱动。这些结果表明,植入物结构会影响局部炎症,从而影响输注的 BM-MNC 的不同植入和重塑行为。这些发现为未来设计仿生支架提供了信息,这些支架可能会更好地增强 BM-MNC 输注疗法的临床效果。

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