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Alpha-, Delta- and PP-cells

机译:Alpha,Delta和PP电池

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Islet non-β-cells, the α- δ- and pancreatic polypeptide cells (PP-cells), are important components of islet architecture and intercellular communication. In α-cells, glucagon is found in electron-dense granules; granule exocytosis is calcium-dependent via P/Q-type Ca~(2+)-channels, which may be clustered at designated cell membrane sites. Somatostatin-containing δ-cells are neuron-like, creating a network for intra-islet communication. Somatostatin 1-28 and 1-14 have a short bioactive half-life, suggesting inhibitory action via paracrine signaling. PP-cells are the most infrequent islet cell type. The embryologically separate ventral pancreas anlage contains PP-rich islets that are morphologically diffuse and α-cell deficient. Tissue samples taken from the head region are unlikely to be representative of the whole pancreas. PP has anorexic effects on gastro-intestinal function and alters insulin and glucagon secretion. Islet architecture is disrupted in rodent diabetic models, diabetic primates and human Type 1 and Type 2 diabetes, with an increased α-cell population and relocation of non-β-cells to central areas of the islet. In diabetes, the transdifferentiation of non-β-cells, with changes in hormone content, suggests plasticity of islet cells but cellular function may be compromised. Understanding how diabetes-related disordered islet structure influences intra-islet cellular communication could clarify how non-β-cells contribute to the control of islet function.
机译:胰岛非β细胞,α-δ细胞和胰多肽细胞(PP细胞)是胰岛结构和细胞间通讯的重要组成部分。在α细胞中,胰高血糖素存在于电子致密颗粒中。颗粒胞吐作用是通过P / Q型Ca〜(2 +)-通道钙依赖性的,该通道可能聚集在指定的细胞膜部位。含有促生长素抑制素的δ细胞呈神经元样,从而形成了胰岛内部通讯网络。生长抑素1-28和1-14具有较短的生物活性半衰期,表明通过旁分泌信号传导具有抑制作用。 PP细胞是最不常见的胰岛细胞类型。胚胎分离的腹胰肛门包含富含PP的胰岛,这些胰岛形态上分散且α细胞缺陷。从头部区域采集的组织样本不太可能代表整个胰腺。 PP对肠胃功能有厌食作用,并会改变胰岛素和胰高血糖素的分泌。在啮齿动物糖尿病模型,糖尿病灵长类动物以及人类1型和2型糖尿病中,胰岛结构受到破坏,α细胞数量增加,非β细胞迁移至胰岛中心区域。在糖尿病中,非β细胞的转分化以及激素含量的变化提示胰岛细胞具有可塑性,但细胞功能可能受到损害。了解与糖尿病相关的无序的胰岛结构如何影响胰岛内的细胞通讯可以阐明非β细胞如何促进胰岛功能的控制。

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