胰岛素分泌、β细胞质量和胰岛血流灌注的早期缺陷先于 BioBreeding 大鼠自身免疫 1 型糖尿病的发病。
Early deficits in insulin secretion, beta cell mass and islet blood perfusion precede onset of autoimmune type 1 diabetes in BioBreeding rats.
机构信息
Lund University Diabetes Centre, Clinical Research Centre, Skåne University Hospital (SUS), Jan Waldentrömsgata 35, SE-20502, Malmö, Sweden.
Umeå Centre for Molecular Medicine, Umeå University, Umeå, Sweden.
出版信息
Diabetologia. 2018 Apr;61(4):896-905. doi: 10.1007/s00125-017-4512-z. Epub 2017 Dec 6.
AIMS/HYPOTHESIS: Genetic studies show coupling of genes affecting beta cell function to type 1 diabetes, but hitherto no studies on whether beta cell dysfunction could precede insulitis and clinical onset of type 1 diabetes are available.
METHODS
We used 40-day-old BioBreeding (BB) DRLyp/Lyp rats (a model of spontaneous autoimmune type 1 diabetes) and diabetes-resistant DRLyp/+ and DR+/+ littermates (controls) to investigate beta cell function in vivo, and insulin and glucagon secretion in vitro. Beta cell mass was assessed by optical projection tomography (OPT) and morphometry. Additionally, measurements of intra-islet blood flow were performed using microsphere injections. We also assessed immune cell infiltration, cytokine expression in islets (by immunohistochemistry and qPCR), as well as islet Glut2 expression and ATP/ADP ratio to determine effects on glucose uptake and metabolism in beta cells.
RESULTS
DRLyp/Lyp rats were normoglycaemic and without traces of immune cell infiltrates. However, IVGTTs revealed a significant decrease in the acute insulin response to glucose compared with control rats (1685.3 ± 121.3 vs 633.3 ± 148.7; p < 0.0001). In agreement, insulin secretion was severely perturbed in isolated islets, and both first- and second-phase insulin release were lowered compared with control rats, while glucagon secretion was similar in both groups. Interestingly, after 5-7 days of culture of islets from DRLyp/Lyp rats in normal media, glucose-stimulated insulin secretion (GSIS) was improved; although, a significant decrease in GSIS was still evident compared with islets from control rats at this time (7393.9 ± 1593.7 vs 4416.8 ± 1230.5 pg islet h; p < 0.0001). Compared with controls, OPT of whole pancreas from DRLyp/Lyp rats revealed significant reductions in medium (4.1 × 10 ± 9.5 × 10 vs 3.8 × 10 ± 5.8 × 10 μm; p = 0.044) and small sized islets (1.6 × 10 ± 5.1 × 10 vs 1.4 × 10 ± 4.5 × 10 μm; p = 0.035). Finally, we found lower intra-islet blood perfusion in vivo (113.1 ± 16.8 vs 76.9 ± 11.8 μl min [g pancreas]; p = 0.023) and alterations in the beta cell ATP/ADP ratio in DRLyp/Lyp rats vs control rats.
CONCLUSIONS/INTERPRETATION: The present study identifies a deterioration of beta cell function and mass, and intra-islet blood flow that precedes insulitis and diabetes development in animals prone to autoimmune type 1 diabetes. These underlying changes in islet function may be previously unrecognised factors of importance in type 1 diabetes development.
目的/假设:遗传研究表明,影响β细胞功能的基因与 1 型糖尿病有关,但迄今为止,尚无关于β细胞功能障碍是否先于胰岛炎和 1 型糖尿病临床发作的研究。
方法
我们使用 40 天大的 BioBreeding(BB)DRLyp/Lyp 大鼠(自发性自身免疫 1 型糖尿病模型)和糖尿病抗性 DRLyp/+和 DR+/+同窝仔鼠(对照),在体内研究β细胞功能,并在体外研究胰岛素和胰高血糖素分泌。通过光学投影断层扫描(OPT)和形态计量学评估β细胞质量。此外,还通过微球注射测量胰岛内血流。我们还评估了免疫细胞浸润、胰岛中细胞因子的表达(通过免疫组织化学和 qPCR),以及胰岛 Glut2 表达和 ATP/ADP 比值,以确定对β细胞葡萄糖摄取和代谢的影响。
结果
DRLyp/Lyp 大鼠血糖正常,无免疫细胞浸润迹象。然而,IVGTT 显示,与对照组相比,急性葡萄糖刺激胰岛素反应明显降低(1685.3±121.3 比 633.3±148.7;p<0.0001)。与此一致,分离的胰岛中胰岛素分泌严重紊乱,第一和第二相胰岛素释放均降低,而两组的胰高血糖素分泌相似。有趣的是,在正常培养基中培养 DRLyp/Lyp 大鼠胰岛 5-7 天后,葡萄糖刺激的胰岛素分泌(GSIS)得到改善;尽管此时与对照组相比,GSIS 仍明显降低(7393.9±1593.7 比 4416.8±1230.5 pg 胰岛 h;p<0.0001)。与对照组相比,DRLyp/Lyp 大鼠全胰腺的 OPT 显示中等大小(4.1×10±9.5×10 比 3.8×10±5.8×10 μm;p=0.044)和小胰岛(1.6×10±5.1×10 比 1.4×10±4.5×10 μm;p=0.035)的大小显著减少。最后,我们发现体内胰岛内血流灌注降低(113.1±16.8 比 76.9±11.8 μl·min[g 胰腺];p=0.023),DRLyp/Lyp 大鼠与对照组相比,β细胞 ATP/ADP 比值发生改变。
结论/解释:本研究确定了易发生自身免疫 1 型糖尿病的动物中β细胞功能和质量的恶化,以及胰岛内血流的恶化,这些变化先于胰岛炎和糖尿病的发展。这些胰岛功能的潜在变化可能是以前未被认识到的 1 型糖尿病发展的重要因素。
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