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小鼠内分泌胰腺的前体细胞共表达胰岛素、胰高血糖素以及神经元蛋白酪氨酸羟化酶和神经肽Y,但不表达胰多肽。

Precursor cells of mouse endocrine pancreas coexpress insulin, glucagon and the neuronal proteins tyrosine hydroxylase and neuropeptide Y, but not pancreatic polypeptide.

作者信息

Teitelman G, Alpert S, Polak J M, Martinez A, Hanahan D

机构信息

Department of Anatomy and Cell Biology, SUNY Health Science Center, Brooklyn 11203.

出版信息

Development. 1993 Aug;118(4):1031-9. doi: 10.1242/dev.118.4.1031.

Abstract

The early progenitor cells to the pancreatic islets in the mouse have been characterized so as to re-examine their possible lineage relationships to the four islet cell types found in mature islets. Insulin and glucagon were both first expressed at embryonic day 9.5, and many cells coexpressed these two markers, as shown by light and electron microscopic analysis using double-label immunohistochemistry. Incubation of embryonic pancreas with 1% glutaraldehyde, a fixative commonly used by electron microscopists, abolished this reactivity, thereby explaining reported difficulties in detecting these precursor cells. Using antisera specific for neuropeptide Y (NPY) a peptide with considerable homology to pancreatic polypeptide (PP), we show that NPY first appears with insulin and glucagon immunoreactivity at E9.5, and is co-expressed with glucagon in a majority of adult alpha cells. As we have previously reported, PP itself is first detectable immunocytochemically at postnatal day 1 with PP-specific antibodies. However, antibodies raised against bovine PP are shown by dot blotting to recognize NPY with comparable avidity, indicating that a recent report of islet progenitor cells containing PP at E9.5 (Herrera, P. L., Huarte, J., Sanvito, F., Meda, P., Orci, L. and Vassalli, J. D. (1991) Development 113, 1257-1265), actually represents cross-reactivity to NPY. The data support a model in which early precursor cells to the endocrine pancreas co-activate and co-express a set of islet cell hormone and neural genes, whose expression is both selectively increased and extinguished as development proceeds, concomitant with a restriction to the patterns of expression characteristic of mature islet cell types.

摘要

小鼠胰岛的早期祖细胞已得到鉴定,以便重新审视它们与成熟胰岛中发现的四种胰岛细胞类型可能存在的谱系关系。胰岛素和胰高血糖素均在胚胎第9.5天首次表达,许多细胞共表达这两种标志物,这通过使用双标记免疫组织化学的光镜和电镜分析得以证实。用1%戊二醛(电子显微镜工作者常用的一种固定剂)孵育胚胎胰腺,消除了这种反应性,从而解释了此前报道的在检测这些前体细胞时遇到的困难。利用针对神经肽Y(NPY,一种与胰多肽(PP)具有相当同源性的肽)的抗血清,我们发现NPY在胚胎第9.5天首次与胰岛素和胰高血糖素免疫反应性一同出现,并且在大多数成年α细胞中与胰高血糖素共表达。正如我们之前所报道的,PP本身在出生后第1天用PP特异性抗体首次可通过免疫细胞化学检测到。然而,通过斑点印迹法显示,针对牛PP产生的抗体以相当的亲和力识别NPY,这表明最近一篇报道中提到的在胚胎第9.5天含有PP的胰岛祖细胞(赫雷拉,P.L.,瓦尔泰,J.,桑维托,F.,梅达,P.,奥尔西,L.和瓦萨利,J.D.(1991年)《发育》113卷,1257 - 1265页),实际上代表了与NPY的交叉反应性。这些数据支持了一个模型,即内分泌胰腺的早期前体细胞共同激活并共表达一组胰岛细胞激素和神经基因,随着发育的进行,这些基因的表达既有选择性地增加,也有熄灭,同时伴随着向成熟胰岛细胞类型特征性表达模式的限制。

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