Islet Transplantation Provides Superior Glycemic Control and Maintenance of Better Islet Architecture Compared to Early Insulin Treatment in 50% Pancreatectomized Mice

IF 0.8 4区医学 Q4 IMMUNOLOGY

Transplantation proceedings Pub Date : 2025-07-01 DOI:10.1016/j.transproceed.2025.05.029

Byung-Joon Kim , Heekyoung Park , Jun-Seop Shin , Jin Kuk Kim , Kwang-Won Kim

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引用次数: 0

Abstract

Early insulin intervention is speculated to promote β-cell rest, potentially preserving and regenerating residual β-cells in β-cell-deficient environments, such as recent-onset type 1 diabetes. However, exogenous insulin supplementation is supposed not to be enough to fulfill these beneficial outcomes. To investigate this, we employed a 50% partial pancreatectomy (Px) in mice as a model for β-cell deficiency. Four experimental groups are included: 1. a sham group that underwent 50% Px (sham group), 2. control group that underwent 50% Px with saline injection for 7 days (Px group), 3. insulin group that administered insulin injection for 7 days post-Px (PX+INS group) and 4. islet transplantation group that islet transplantation after 50% Px. (PX+IT group). Intraperitoneal glucose tolerance tests (IPGTTs) were performed at 3- and 7-days postinsulin treatment or IT, and glycemic control was assessed by calculating the area under the curve (AUC) of blood glucose concentrations. Histomorphometric analysis was used to evaluate islet distribution, islet morphology and the composition of β- and α-cells. The results showed significantly improved glucose tolerance at 3- and 7- days in the islet-transplantation group compared to the insulin-treated group. Islet proportions in the pancreas were similar across groups; however, the insulin-treated group exhibited a significant increase in α-cell numbers, with their distribution extending both to the periphery and inner core of the islets. Our findings demonstrate that islet transplantation is superior to insulin treatment for glycemic control following 50% pancreatectomy in mice. Short-term insulin treatment was associated with α-cell expansion and worsened glycemic outcomes. These results suggest that islet transplantation is more effective in β-cell-deficient conditions, and caution is warranted when implementing early preventive insulin interventions.

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与早期胰岛素治疗相比，胰岛移植在50%胰腺切除小鼠中提供了更好的血糖控制和更好的胰岛结构维持。

据推测，早期胰岛素干预可促进β细胞休息，可能在β细胞缺乏的环境中保存和再生剩余的β细胞，如新近发病的1型糖尿病。然而，外源性胰岛素补充被认为不足以实现这些有益的结果。为了研究这一点，我们在小鼠中采用50%部分胰腺切除术（Px）作为β细胞缺乏的模型。实验分为四组：1.试验组；1 .假手术组接受50% Px（假手术组）；2 .对照组给予50% Px加生理盐水注射7 d （Px组）；注射胰岛素7 d组（PX+INS组）；胰岛移植组认为胰岛移植后50% Px。(PX +集团)。分别于胰岛素治疗后3天和7天进行腹腔葡萄糖耐量试验（ipgts），并通过计算血糖浓度曲线下面积（AUC）评估血糖控制情况。采用组织形态学分析评价胰岛分布、胰岛形态及β-和α-细胞组成。结果显示，与胰岛素治疗组相比，胰岛移植组在第3天和第7天的葡萄糖耐量显著改善。各组胰腺中胰岛的比例相似；然而，胰岛素治疗组α-细胞数量显著增加，其分布延伸到胰岛的外围和内核。我们的研究结果表明，胰岛移植在50%胰腺切除术后的小鼠血糖控制方面优于胰岛素治疗。短期胰岛素治疗与α-细胞扩增和血糖结局恶化相关。这些结果表明胰岛移植在β细胞缺乏的情况下更有效，在实施早期预防性胰岛素干预时需要谨慎。

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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来源期刊

Transplantation proceedings 医学-免疫学

CiteScore

1.70

自引率

0.00%

发文量

502

审稿时长

60 days

期刊介绍： Transplantation Proceedings publishes several different categories of manuscripts, all of which undergo extensive peer review by recognized authorities in the field prior to their acceptance for publication. The first type of manuscripts consists of sets of papers providing an in-depth expression of the current state of the art in various rapidly developing components of world transplantation biology and medicine. These manuscripts emanate from congresses of the affiliated transplantation societies, from Symposia sponsored by the Societies, as well as special Conferences and Workshops covering related topics. Transplantation Proceedings also publishes several special sections including publication of Clinical Transplantation Proceedings, being rapid original contributions of preclinical and clinical experiences. These manuscripts undergo review by members of the Editorial Board. Original basic or clinical science articles, clinical trials and case studies can be submitted to the journal?s open access companion title Transplantation Reports.