首页> 外文期刊>Journal of molecular histology >Ghrelin, ghrelin-O-acyl transferase, nucleobindin-2esfatin-1 and prohormone convertases in the pancreatic islets of Sprague Dawley rats during development
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Ghrelin, ghrelin-O-acyl transferase, nucleobindin-2esfatin-1 and prohormone convertases in the pancreatic islets of Sprague Dawley rats during development

机译:Sprague Dawley大鼠胰岛发育过程中Ghrelin,Ghrelin-O-酰基转移酶,nucleobindin-2 / nesfatin-1和激素原转化酶

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摘要

Ghrelin and nesfatin-1 are regulators of blood glucose and energy balance. Prohormone convertases (PCs) enable processing of ghrelin and nesfatin-1 from its precursors. An acylation, enabled by ghrelin O-acyl transferase (GOAT) is critical for many of the biological actions of ghrelin. To date, there is no research on the developmental expression of GOAT, and the co-expression of both NUCB2esfatin-1 and prohormone convertases in the pancreas. The objective of this research was to immunolocalize ghrelin, GOAT, NUCB2esfatin-1, PC1/3 and PC2 in the pancreas during fetal and postnatal periods of Sprague Dawley (SD) rats using immunohistochemical analysis. GOAT mRNA in the rat pancreas during development was also determined. In the pancreas, not all islet cells immunopositive for GOAT are immunoreactive for ghrelin on postnatal (P) days 20, 27 and adult. GOAT mRNA expression in the pancreas at P27 was higher than the expression levels in rest of the developmental stages tested. Both PC1/3 and PC2 are co-expressed with NUCB2esfatin-1 on embryonic (E) day E21, P13, P20. While similar co-localization was also found in P27 for NUCB2esfatin-1 and PC1/3, NUCB2esfatin-1 and PC2 were found in distinct populations of cells in P27. Some ghrelin and GOAT positive cells stained for nesfatin-1 as well. Meanwhile, no co-localization of somatostatin and glucaon with nesfatin-1 was found in the pancreas of SD rats. Our findings suggest that the endocrine pancreas can produce and process precursors of ghrelin and nesfatin-1 to make bioactive forms of both peptides.
机译:Ghrelin和nesfatin-1是血糖和能量平衡的调节剂。激素原转化酶(PCs)可以从其前体中加工生长素释放肽和nesfatin-1。由生长素释放肽O-酰基转移酶(GOAT)促成的酰化对于生长素释放肽的许多生物作用至关重要。迄今为止,还没有关于GOAT的发育表达以及NUCB2 / nesfatin-1和激素原转化酶在胰腺中共表达的研究。这项研究的目的是使用免疫组织化学分析技术,在Sprague Dawley(SD)大鼠的胎儿和出生后的胰腺中对生长素释放肽,GOAT,NUCB2 / nesfatin-1,PC1 / 3和PC2进行免疫定位。还确定了大鼠胰腺发育过程中的GOAT mRNA。在胰腺中,并非所有对GOAT呈阳性的胰岛细胞在出生后(P)第20、27天和成年后都对生长素释放肽具有免疫反应性。 P27时胰腺中的GOAT mRNA表达高于其余发育阶段的表达水平。 PC1 / 3和PC2均与NUCB2 / nesfatin-1在胚胎(E)天E21,P13,P20共表达。虽然在P27中还发现了NUCB2 / nesfatin-1和PC1 / 3的相似共定位,但在P27中不同的细胞群中却发现了NUCB2 / nesfatin-1和PC2。一些生长素释放肽和GOAT阳性细胞也对nesfatin-1染色。同时,在SD大鼠的胰腺中未发现生长抑素和葡聚糖与nesfatin-1的共定位。我们的发现表明,内分泌胰腺可以产生和处理ghrelin和nesfatin-1的前体,从而形成两种肽的生物活性形式。

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