Analysis of the activity of c-kit immunopositive alpha-cells of the pancreas in exogenous infusions and endogenously formed pathology

Current issues in pharmacy and medicine: science and practice Pub Date : 2023-03-10 DOI:10.14739/2409-2932.2023.1.273223

T. Ivanenko

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Abstract

There are a number of factors and agents that change the population of endocrinocytes and their secretory activity depending on various conditions and experimentally formed pathologies. These include the impact of intermittent hypoxic hypoxia; experimentally formed pathology (diabetes); genetically formed pathology (arterial hypertension), direct effect on endocrinocytes of the pancreas with their own pathophysiological mechanism. In this context, it is interesting to analyze the state of the progenitor potential of alpha cells depending on the living conditions of the organism, its effects, and developing pathological conditions in it. The aim of the work is to determine the activity of the proliferative factor c-kit in alpha cells under exogenous factors – intermittent hypoxic hypoxia and endogenously formed pathology – arterial hypertension and diabetes. Materials and methods. The study was conducted on the pancreas of SHR and Wistar rats. Glucagon and c-kit in pancreatic islets were determined by the immunofluorescence method. The immunofluorescence reaction was studied with an AxioImager-M2 fluorescence microscope. Results. Analysis of the c-kit positive alpha-cell index in rats with diabetes showed a 5-fold increase. This was explained by the fact, that the development of hyperglycemia in diabetes mellitus was characterized not only by an increased level of glucose in the blood due to insufficient insulin production but also due to an increase in the number of alpha cells, their active proliferation and possible transdifferentiation from beta cells. The number of c-kit positive alpha cells in SHR rats decreased. This may indicate that these changes were not so related to a violation of the modulation of the transcription factor, but to the participation of neurogenic mechanisms. The decrease in c-kit positive alpha cells in animals with hypoxic hypoxia can be explained by transdifferentiation (remodeling) changes, aimed at suppressing proliferative processes in alpha endocrinocytes. Conclusions. The increase in the number of c-kit positive alpha cells in rats with diabetes is explained by the fact, that the development of hyperglycemia in diabetes is characterized not only by an increased level of glucose in the blood due to insufficient insulin production but also by an increase in the number of alpha cells, their active proliferation and possible transdifferentiation from beta cells. A decrease in the number of c-kit positive alpha cells in SHR rats may indicate that these changes are not so much related to a violation of the modulation of the transcription factor, but to the participation of neurogenic mechanisms. The decrease in c-kit positive alpha cells in animals with hypoxic hypoxia can be explained by transdifferentiation (remodeling) changes, aimed at suppressing proliferative processes in alpha endocrinocytes.

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外源性输注和内源性病理胰腺c-kit免疫阳性α细胞活性分析

根据不同的条件和实验形成的病理，有许多因素和因子可以改变内分泌细胞的数量及其分泌活性。这些包括间歇性缺氧的影响;实验形成的病理(糖尿病);遗传形成的病理(动脉性高血压)，直接作用于胰腺的内分泌细胞有其自身的病理生理机制。在这种情况下，分析α细胞的祖细胞潜能的状态取决于生物体的生存条件、其作用和在生物体中发展的病理条件是很有趣的。这项工作的目的是确定在外源性因素(间歇性缺氧)和内源性病理(动脉高血压和糖尿病)下α细胞中增殖因子c-kit的活性。材料和方法。以SHR大鼠和Wistar大鼠胰腺为研究对象。采用免疫荧光法测定胰岛胰高血糖素和c-kit水平。用AxioImager-M2荧光显微镜观察免疫荧光反应。对糖尿病大鼠的c-kit阳性α细胞指数进行分析，结果显示升高了5倍。这可以用以下事实来解释:糖尿病的高血糖症的发展不仅表现为由于胰岛素分泌不足而导致血液中葡萄糖水平升高，而且还表现为α细胞数量的增加、它们的活跃增殖和β细胞的可能转分化。SHR大鼠c-kit阳性α细胞数量减少。这可能表明这些变化与转录因子调节的破坏无关，而是与神经源性机制的参与有关。缺氧动物c-kit阳性α细胞的减少可以通过转分化(重塑)改变来解释，其目的是抑制α内分泌细胞的增殖过程。糖尿病大鼠c-kit阳性α细胞数量的增加可以解释为:糖尿病高血糖的发展不仅以胰岛素分泌不足导致血液中葡萄糖水平升高为特征，而且还以α细胞数量的增加、它们的活跃增殖和β细胞的可能转分化为特征。SHR大鼠c-kit阳性α细胞数量的减少可能表明这些变化与转录因子调节的破坏无关，而与神经源性机制的参与有关。缺氧动物c-kit阳性α细胞的减少可以通过转分化(重塑)改变来解释，旨在抑制α内分泌细胞的增殖过程。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Current issues in pharmacy and medicine: science and practice

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