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非人灵长类动物的内分泌胰腺:发育、再生潜能与化生

The non-human primate endocrine pancreas: development, regeneration potential and metaplasia.

作者信息

Wolfe-Coote S, Louw J, Woodroof C, Du Toit D F

机构信息

Experimental Biology Programme, MRC, Cape, South Africa.

出版信息

Cell Biol Int. 1996 Feb;20(2):95-101. doi: 10.1006/cbir.1996.0013.

DOI:10.1006/cbir.1996.0013
PMID:8935153
Abstract

An investigation into the development of the Vervet monkey endocrine pancreas revealed a sequence of occurrence of pancreatic peptides that differed from previous reports in mice, dog and human with PP and somatostatin occurring before glucagon and insulin. All four pancreatic peptides were identified, immunohistochemically, in only one of the pancreatic primordial buds, before fusion of the two buds to form the pancreas. This questions the hypothesis that the heterogeneous endocrine cell distribution seen in the adult pancreas is due to the contribution of only PP cells by the ventral bud and non-PP cells by the dorsal bud. Co-localization of glucagon and PP was observed extensively in the developing pancreas and the predominant expression of one over the other in an apparently organized non-random manner accounted for the glucagon- and PP-rich areas seen in the developing pancreas. A small number of cells immunoreactive to glucagon and PP were also observed in the adult. Reports of plasticity of differentiation of other pancreatic cells led us to investigate regeneration potential of the adult monkey pancreas. Partial obstruction of the Vervet monkey main pancreatic duct, by cellophane wrapping, resulted in duct cell proliferation and differentiation to form new endocrine tissue in a way that mimics normal organogenesis. Focal areas of hepatocytes were found in the regenerated pancreas of one monkey, illustrating further the latent developmental capabilities of adult pancreas cells. These findings could lead to interesting new therapies for pancreas and liver disease.

摘要

对绿猴内分泌胰腺发育的一项研究揭示了胰腺肽出现的顺序,该顺序与之前关于小鼠、狗和人类的报道不同,胰多肽(PP)和生长抑素在胰高血糖素和胰岛素之前出现。在两个胰腺原基芽融合形成胰腺之前,通过免疫组织化学方法仅在其中一个胰腺原基芽中鉴定出了所有四种胰腺肽。这对以下假设提出了质疑:成年胰腺中所见的异质性内分泌细胞分布是由于腹侧芽仅贡献PP细胞,背侧芽贡献非PP细胞。在发育中的胰腺中广泛观察到胰高血糖素和PP的共定位,并且一种肽相对于另一种肽以明显有组织的非随机方式的主要表达解释了发育中的胰腺中富含胰高血糖素和PP的区域。在成年个体中也观察到少量对胰高血糖素和PP有免疫反应的细胞。关于其他胰腺细胞分化可塑性的报道促使我们研究成年猴胰腺的再生潜力。通过玻璃纸包裹对绿猴主胰管进行部分阻塞,导致导管细胞增殖并分化形成新的内分泌组织,其方式类似于正常器官发生。在一只猴子再生的胰腺中发现了局灶性肝细胞区域,进一步说明了成年胰腺细胞潜在的发育能力。这些发现可能会为胰腺和肝脏疾病带来有趣的新疗法。

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