胰岛移植的免疫学挑战和当前的观点。

Plamena Kabakchieva, Yavor Assyov, Stavros Gerasoudis, Georgi Vasilev, Monika Peshevska-Sekulovska, Metodija Sekulovski, Snezhina Lazova, Dimitrina Georgieva Miteva, Milena Gulinac, Latchezar Tomov, Tsvetelina Velikova
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摘要

胰岛移植是一种微创手术,旨在通过移植胰岛细胞来逆转1型糖尿病(T1D)患者胰岛素缺乏的影响。总的来说,胰岛移植已经有了很大的改善,细胞替代可能会成为主要的治疗方法。我们回顾胰岛移植作为治疗T1D和面临的免疫学挑战。发表的数据表明,胰岛细胞输血的时间在2到10小时之间变化。大约54%的患者在第一年末获得胰岛素独立性,而只有20%的患者在第二年末保持无胰岛素状态。最终,大多数移植患者在移植后几年内恢复使用某种形式的外源性胰岛素,这就需要在移植前改善免疫因子。我们还讨论了免疫抑制方案,凋亡的供体淋巴细胞,抗tim -1抗体,基于混合嵌合的耐受性诱导,利用乙烯碳二亚胺固定的脾细胞诱导抗原特异性耐受性,移植前输注供体凋亡细胞,B细胞消耗,离体胰岛预处理,诱导局部免疫耐受性,细胞包埋和免疫分离,使用生物材料,免疫调节细胞等。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Islet transplantation-immunological challenges and current perspectives.

Pancreatic islet transplantation is a minimally invasive procedure aiming to reverse the effects of insulin deficiency in patients with type 1 diabetes (T1D) by transplanting pancreatic beta cells. Overall, pancreatic islet transplantation has improved to a great extent, and cellular replacement will likely become the mainstay treatment. We review pancreatic islet transplantation as a treatment for T1D and the immunological challenges faced. Published data demonstrated that the time for islet cell transfusion varied between 2 and 10 h. Approximately 54% of the patients gained insulin independence at the end of the first year, while only 20% remained insulin-free at the end of the second year. Eventually, most transplanted patients return to using some form of exogenous insulin within a few years after the transplantation, which imposed the need to improve immunological factors before transplantation. We also discuss the immunosuppressive regimens, apoptotic donor lymphocytes, anti-TIM-1 antibodies, mixed chimerism-based tolerance induction, induction of antigen-specific tolerance utilizing ethylene carbodiimide-fixed splenocytes, pretransplant infusions of donor apoptotic cells, B cell depletion, preconditioning of isolated islets, inducing local immunotolerance, cell encapsulation and immunoisolation, using of biomaterials, immunomodulatory cells, etc.

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