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链脲佐菌素增强小鼠胰腺干细胞/祖细胞,并在部分胰腺切除术后再生糖尿病胰腺。

Mouse Pancreas Stem/Progenitor Cells Get Augmented by Streptozotocin and Regenerate Diabetic Pancreas After Partial Pancreatectomy.

机构信息

Stem Cell Biology Department, ICMR- National Institute for Research in Reproductive Health, Jehangir Merwanji Street Parel, Mumbai, 400 012, India.

Experimental Animal Facility, ICMR-National Institute for Research in Reproductive Health, Jehangir Merwanji Street, Parel, Mumbai, 400 012, India.

出版信息

Stem Cell Rev Rep. 2020 Feb;16(1):144-158. doi: 10.1007/s12015-019-09919-x.

Abstract

Existence of stem cells in adult pancreas remains contentious. Single cells suspensions obtained by collagenase and trypsin digestion separately from adult mouse pancreas and pancreatic islets were spun at 1000 rpm (250 g) to collect the cells. At this speed the stem/ progenitor cells remained buoyant and were further enriched by spinning the supernatant at 3000 rpm (1000 g). Two distinct populations of stem cells were detected including pluripotent, very small (2-6 μm) embryonic-like stem cells (VSELs) that expressed nuclear OCT-4A and pluripotent transcripts (Oct-4A, Sox2, Nanog, Stella) and slightly bigger progenitors, pancreatic stem cells (PSCs) that expressed cytoplasmic OCT-4B and PDX-1. Streptozotocin treated diabetic pancreas showed an increase in numbers of VSELs (2-6 μm, 7AAD-, LIN-CD45-SCA1+ cells) and up-regulation of transcripts specific for stem/ progenitor cells. Diabetic mice were further subjected to partial pancreatectomy to study involvement of VSELs/ PSCs during regeneration. VSELs/ PSCs were mobilized in large numbers, were observed in the lumen of blood vessels and PCNA expression suggested their proliferation. Initially, new acini assembled to regenerate the exocrine pancreas and later by Day 30, neogenesis of islets was observed in the vicinity of the blood vessels and pancreatic ducts by the differentiation of endogenous VSELs/ PSCs which may be targeted to regenerate diabetic pancreas in clinical settings.

摘要

成年胰腺中干细胞的存在仍然存在争议。分别用胶原酶和胰蛋白酶从成年小鼠胰腺和胰岛中消化获得的单细胞悬液以 1000rpm(250g)离心以收集细胞。在这个速度下,干细胞/祖细胞保持浮力,并通过以 3000rpm(1000g)离心上清液进一步富集。检测到两种不同的干细胞群,包括多能的、非常小的(2-6μm)类似胚胎的干细胞(VSELs),其表达核 OCT-4A 和多能转录物(Oct-4A、Sox2、Nanog、Stella)和稍大的祖细胞,胰腺干细胞(PSCs),表达细胞质 OCT-4B 和 PDX-1。链脲佐菌素处理的糖尿病胰腺显示 VSELs(2-6μm,7AAD-,LIN-CD45-SCA1+细胞)数量增加,并上调干细胞/祖细胞特异性转录物。糖尿病小鼠进一步接受部分胰腺切除术,以研究 VSELs/PSCs 在再生过程中的参与。大量动员 VSELs/PSCs,观察到血管管腔中的细胞,并通过 PCNA 表达提示其增殖。最初,新的腺泡组装以再生外分泌胰腺,后来在第 30 天,观察到血管附近和胰腺导管处的胰岛新生,这可能是通过内源性 VSELs/PSCs 的分化来靶向再生糖尿病胰腺的。

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