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工程化胰岛-细胞微粒杂合体与生物黏附性 FK506 载药聚合物微球用于异种胰岛移植的局部免疫调节。

Engineering "cell-particle hybrids" of pancreatic islets and bioadhesive FK506-loaded polymeric microspheres for local immunomodulation in xenogeneic islet transplantation.

机构信息

College of Pharmacy, Yeungnam University, Gyeongsan, Gyeongbuk, 38541, South Korea.

College of Pharmacy, Keimyung University, Daegu, 42601, South Korea.

出版信息

Biomaterials. 2019 Nov;221:119415. doi: 10.1016/j.biomaterials.2019.119415. Epub 2019 Aug 6.

Abstract

Host immune response remains an obstacle in cell-replacement therapy for treating type I diabetes. Long-term systemic immunosuppression results in suboptimal efficacy and adverse reactions. Thus, "cell-particle hybrids" of pancreatic islets and tissue-adhesive, polydopamine-coated, FK506-loaded biodegradable microspheres (PD-FK506-MS) were developed to locally modulate the immune response at the transplantation site. Coating of FK506-MS with PD enabled the rapid formation of stable cell-particle hybrids without significant changes in islet viability and functionality. Extremely low quantities of FK506 (approximately 600 ng per recipient) sustainably released from cell-particle hybrids effectively prolonged survival of xenogeneic islet graft. Interestingly, FK506 exhibited extended bioavailability in the grafts but was undetectable in systemic circulation and other tissues. Moreover, mRNA expression of inflammatory cytokines was significantly inhibited in the PD-FK506-MS-containing grafts but not in lymphoid organs. This study presents a promising platform that facilitates the translation of local immunomodulation towards an effective strategy with improved safety profiles for treating type I diabetes.

摘要

宿主免疫反应仍然是细胞替代疗法治疗 1 型糖尿病的障碍。长期全身免疫抑制导致疗效不佳和不良反应。因此,开发了胰岛和组织黏附、聚多巴胺涂层、FK506 负载的可生物降解微球(PD-FK506-MS)的“细胞-颗粒杂交体”,以在移植部位局部调节免疫反应。FK506-MS 的 PD 涂层使得能够在不显著改变胰岛活力和功能的情况下快速形成稳定的细胞-颗粒杂交体。从细胞-颗粒杂交体中持续释放的极低量 FK506(每个受者约 600ng)有效地延长了异种胰岛移植物的存活时间。有趣的是,FK506 在移植物中表现出延长的生物利用度,但在全身循环和其他组织中无法检测到。此外,炎性细胞因子的 mRNA 表达在含有 PD-FK506-MS 的移植物中显著受到抑制,但在淋巴器官中未受到抑制。这项研究提出了一个有前途的平台,促进了局部免疫调节向治疗 1 型糖尿病的有效策略的转化,提高了安全性。

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