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在成年大鼠胰腺损伤模型中,间充质细胞对于上皮导管细胞向β细胞的成熟及功能发挥是必需的。

Mesenchymal cells are required for epithelial duct cell-to-beta cell maturation and function in an injured adult pancreas in the rat.

作者信息

Manda Juziel Kampando, Page Benedict John, Tchokonte-Nana Venant

机构信息

Islet and MSK Research Group, Anatomy and Histology, Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Stellenbosch University, Francie van Zijl road Tygerberg, Cape Town 7500, South Africa.

Islet and MSK Research Group, Anatomy and Histology, Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Stellenbosch University, Francie van Zijl road Tygerberg, Cape Town 7500, South Africa.

出版信息

Acta Histochem. 2017 Sep;119(7):689-695. doi: 10.1016/j.acthis.2017.08.004. Epub 2017 Aug 26.

Abstract

The islet, the endocrine portion of the pancreas - develops from an invagination of the pancreatic duct epithelial cells (PDECs) into the surrounding tissue. The contact of the PDECs with mesenchymal cells (MSCs) may be an essential drive for endocrine cell fate. During pancreatic development, cells that express Neurogenin-3 (Ngn3) biomarker are precursors of insulin- producing beta cells. These precursors have been reported in the neogenesis of islets from adult tissues following the surgical ligation of the main pancreatic duct (PDL). But the capacity of these precursors to induce the appropriate signals to complete the entire neogenesis program has been questioned. We studied the fate of co-culture of PDECs and MSCs from the ligated adult pancreas and established the exact location of adult stem- or progenitor-like cells that give rise to beta cells. PDECs were cultured in direct contact with or without MSCs in serum-containing culture media. The cytomorphology of the cells in co-cultures was determined and the immunocytochemical study of the cells was carried out using anti-Ngn3, anti-insulin and anti-cytokeratin-7 (CK7) antibodies. Both the PDEC/MSC- and PDEC/MSC+ cultures showed out- pocketing from duct epithelium by the end of the second week, which are distinct as cell clusters only in PDEC/MSC+ cells later in week four, exhibiting numerous branching ducts. Co-expression of Ngn3 with insulin was observed in both cultures from the second week. However, characterizations of these Ngn3+ cells in the PDEC/MSC+ culture revealed that these cells also co-expressed a CK7 biomarker. This study provides new evidence of the ductal epithelial nature of beta cells in injured adult pancreata; and that the mesenchymal stromal cells are required to sustain Ngn3 expression for beta cell maturation and function.

摘要

胰岛是胰腺的内分泌部分,由胰腺导管上皮细胞(PDEC)向周围组织内陷发育而成。PDEC与间充质细胞(MSC)的接触可能是内分泌细胞命运的关键驱动因素。在胰腺发育过程中,表达神经源蛋白3(Ngn3)生物标志物的细胞是产生胰岛素的β细胞的前体。这些前体已在成年组织胰岛新生中被报道,即在主胰管结扎(PDL)后。但这些前体诱导适当信号以完成整个新生程序的能力受到了质疑。我们研究了成年结扎胰腺中PDEC与MSC共培养的命运,并确定了产生β细胞的成年干细胞样或祖细胞样细胞的确切位置。PDEC在含血清培养基中与MSC直接接触或不接触的情况下进行培养。确定了共培养细胞的细胞形态,并使用抗Ngn3、抗胰岛素和抗细胞角蛋白7(CK7)抗体对细胞进行了免疫细胞化学研究。到第二周结束时,PDEC/MSC - 和PDEC/MSC + 培养物均显示出从导管上皮向外突出,到第四周后期,只有PDEC/MSC + 细胞中的这些突出物作为细胞簇明显可见,并呈现出许多分支导管。从第二周起,在两种培养物中均观察到Ngn3与胰岛素的共表达。然而,对PDEC/MSC + 培养物中这些Ngn3 + 细胞的表征显示,这些细胞还共表达CK7生物标志物。本研究为损伤成年胰腺中β细胞的导管上皮性质提供了新证据;并且间充质基质细胞是β细胞成熟和功能维持Ngn3表达所必需的。

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