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通过注射免疫保护胰岛实现糖尿病的长期逆转。

Long-term reversal of diabetes by the injection of immunoprotected islets.

作者信息

Soon-Shiong P, Feldman E, Nelson R, Heintz R, Yao Q, Yao Z, Zheng T, Merideth N, Skjak-Braek G, Espevik T

机构信息

Islet Transplant Center, Wadsworth Medical Center, Los Angeles, CA 90073.

出版信息

Proc Natl Acad Sci U S A. 1993 Jun 15;90(12):5843-7. doi: 10.1073/pnas.90.12.5843.

DOI:10.1073/pnas.90.12.5843
PMID:8516335
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC46819/
Abstract

The intraperitoneal injection of insulin-producing islets immunoprotected by an alginate-poly(amino acid) membrane is a potential method of reversing diabetes without the need for lifelong immunosuppression. Previous attempts to demonstrate this technology in large animals have failed, preventing application in humans. We have determined that key factors responsible for these past failures include cytokine (interleukins 1 and 6 and tumor necrosis factor) stimulation by mannuronic acid monomers from alginate capsules with weak mechanical integrity, which results in fibroblast proliferation. With this insight, we formulated mechanically stable microcapsules by using alginate high in guluronic acid content and report prolonged reversal of diabetes in the spontaneous diabetic dog model by the intraperitoneal injection of encapsulated canine islet allografts. Euglycemia, independent of any exogenous insulin requirement, was noted for up to 172 days. Graft survival, evidenced by positive C-peptide release, was noted for as long as 726 days in a recipient receiving a single injection of immunoprotected islets. Histological evidence of viable islets retrieved from the peritoneal cavity 6 months posttransplant confirmed the biocompatibility and immunoprotective nature of this capsule formulation. The finding that intraperitoneal injection of alginate-immunoprotected islets, a minimally invasive surgical procedure, is effective in prolonged (> 1 year) maintenance of glycemic control, without the need for lifelong immunosuppression, may have significant implications for the future therapy of type I diabetes in humans.

摘要

经藻酸盐 - 聚氨基酸膜免疫保护的胰岛素分泌胰岛腹腔注射,是一种无需终身免疫抑制即可逆转糖尿病的潜在方法。此前在大型动物中证明这项技术的尝试均告失败,从而无法应用于人类。我们已经确定,导致过去这些失败的关键因素包括机械完整性较弱的藻酸盐胶囊中的甘露糖醛酸单体刺激细胞因子(白细胞介素1和6以及肿瘤坏死因子),这会导致成纤维细胞增殖。基于这一认识,我们通过使用古洛糖醛酸含量高的藻酸盐制备了机械稳定的微胶囊,并报告了通过腹腔注射封装的犬胰岛同种异体移植物,在自发性糖尿病犬模型中糖尿病得到了长期逆转。在长达172天的时间里,观察到血糖正常,且无需任何外源性胰岛素。在接受单次免疫保护胰岛注射的受体中,C肽释放阳性证明移植物存活长达726天。移植后6个月从腹腔中取出的活胰岛的组织学证据证实了这种胶囊制剂的生物相容性和免疫保护特性。腹腔注射藻酸盐免疫保护的胰岛这种微创外科手术,能够有效长期(>1年)维持血糖控制,且无需终身免疫抑制,这一发现可能对未来人类I型糖尿病的治疗具有重大意义。

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Proc Natl Acad Sci U S A. 1993 Jun 15;90(12):5843-7. doi: 10.1073/pnas.90.12.5843.
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本文引用的文献

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Microencapsulated islets as bioartificial endocrine pancreas.微囊化胰岛作为生物人工内分泌胰腺
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Immunoisolation of pancreatic B cells by microencapsulation. An in vitro study.通过微囊化对胰腺β细胞进行免疫隔离。一项体外研究。
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Microencapsulated hepatocytes as a bioartificial liver.微囊化肝细胞作为一种生物人工肝
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Designing a retrievable and scalable cell encapsulation device for potential treatment of type 1 diabetes.设计一种可回收和可扩展的细胞封装装置,用于潜在治疗 1 型糖尿病。
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Synthesis and Evaluation of a Sodium Alginate-4-Aminosalicylic Acid Based Microporous Hydrogel for Potential Viscosupplementation for Joint Injuries and Arthritis-Induced Conditions.基于海藻酸钠-4-氨基水杨酸的微孔水凝胶的合成与评价,用于关节损伤和关节炎相关病症的潜在粘弹性补充治疗
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3D Cell Culture in Alginate Hydrogels.藻酸盐水凝胶中的3D细胞培养
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The effects of pancreas transplantation on the glomerular structure of renal allografts in patients with insulin-dependent diabetes.胰腺移植对胰岛素依赖型糖尿病患者同种异体肾移植肾小球结构的影响。
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The role of CD4+ helper T cells in the destruction of microencapsulated islet xenografts in nod mice.CD4 +辅助性T细胞在NOD小鼠微囊化胰岛异种移植破坏中的作用
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