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胰岛源性促肾上腺皮质激素样肽对胰岛素释放调节的旁分泌作用的证据。

Evidence for the paracrine action of islet-derived corticotropin-like peptides on the regulation of insulin release.

作者信息

Borelli M I, Estivariz F E, Gagliardino J J

机构信息

Centro de Endocrinologia Experimental y Aplicada, Universidad Nacional de La Plata, Argentina.

出版信息

Metabolism. 1996 May;45(5):565-70. doi: 10.1016/s0026-0495(96)90025-6.

DOI:10.1016/s0026-0495(96)90025-6
PMID:8622598
Abstract

In view of recent evidence for the endogenous synthesis of proopiomelanocortin (POMC) by pancreatic islets, we have assessed (1) the release of POMC-derived corticotropin (ACTH)-like peptides (ACTH-LP) from isolated perifused rat islets, and (2) the potential paracrine modulatory effect on insulin output of these putative secretagogues. Islets perifused at a glucose concentration of 3.3 mmol/L secreted ACTH-LP at 0.15 +/- 0.005 ng/islet/10 min, which was increased by 17-fold at 16.7 mmol/L glucose. Islets statically incubated with different concentrations of medium glucose plus synthetic 1-39ACTH at 55 pmol/L showed a significant increase of insulin release at 8 (by 79%) and 16 (by 119%) mmol/L glucose, but not at 4 mmol/L. To determine the possible cis-directed effects of these endogenously released islet ACTH-LP on insulin secretion, we either blocked their biological action by immunoneutralization with an ACTH-specific antiserum or prevented their receptor interaction by addition of the ACTH-inhibiting polypeptide (CIP) to the incubation medium. In the presence of 16.7 mmol/L glucose, the rate of insulin output decreased by approximately 25% upon exposure to the antiserum and by approximately 50% in the presence of CIP. The foregoing observations would therefore suggest that both (1) the elaboration of ACTH-LP by isolated perifused islets and (2) the stimulation of islet insulin release by exogenous 1-39ACTH in static incubation occur as a function of glucose concentration in the incubation medium, and that (3) the newly-secreted endogenous ACTH-LP operate in a cis mode to enhance islet insulin output in a manner analogous to that of exogenously added ACTH species. These results strongly support the view that islet-elaborated ACTH-LP are important physiological paracrine modulators of insulin secretion.

摘要

鉴于近期有证据表明胰岛可内源性合成阿片促黑皮质素原(POMC),我们评估了:(1)从分离的经灌流大鼠胰岛中释放POMC衍生的促肾上腺皮质激素(ACTH)样肽(ACTH-LP)的情况;(2)这些假定的促分泌素对胰岛素分泌的潜在旁分泌调节作用。在葡萄糖浓度为3.3 mmol/L的条件下进行灌流的胰岛,以0.15±0.005 ng/胰岛/10分钟的速率分泌ACTH-LP,在葡萄糖浓度为16.7 mmol/L时增加了17倍。将胰岛与不同浓度的培养基葡萄糖以及55 pmol/L的合成1-39ACTH进行静态孵育,结果显示在葡萄糖浓度为8(增加79%)和16 mmol/L(增加119%)时胰岛素释放显著增加,但在4 mmol/L时未增加。为了确定这些内源性释放的胰岛ACTH-LP对胰岛素分泌可能的顺式定向作用,我们要么用ACTH特异性抗血清进行免疫中和来阻断其生物学作用,要么通过向孵育培养基中添加ACTH抑制多肽(CIP)来阻止其与受体的相互作用。在存在16.7 mmol/L葡萄糖的情况下,暴露于抗血清后胰岛素分泌速率下降约25%,在存在CIP的情况下下降约50%。因此,上述观察结果表明:(1)分离的经灌流胰岛分泌ACTH-LP以及(2)在静态孵育中外源1-39ACTH刺激胰岛胰岛素释放均是孵育培养基中葡萄糖浓度的函数,并且(3)新分泌的内源性ACTH-LP以顺式模式发挥作用,以类似于外源添加的ACTH的方式增强胰岛胰岛素分泌。这些结果有力地支持了胰岛产生的ACTH-LP是胰岛素分泌重要的生理性旁分泌调节因子这一观点。

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