P38 expression in colorectal adenomas: relationships to cell proliferation, stem phenotype and AKT pathway proteins.

Minerva gastroenterologica e dietologica Pub Date : 2020-09-01 Epub Date: 2020-03-24 DOI:10.23736/S1121-421X.20.02667-7

Adriana Handra-Luca, Mouna Bendib, Christina Magkou

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引用次数: 1

Abstract

Background: The P38-protein is known to be expressed in colorectal adenomas (CRA). Expression in low- and high-grade tubular adenomas is decreased when compared to adenocarcinomas and increased with regard to normal mucosa. We aimed to study P38 expression in human CRAs and the relationships to cell proliferation Ki67-protein, stem-phenotype CD133-protein and, to mTOR-protein (AKT pathway).

Methods: The immunohistochemical expression of P38 was evaluated in CRAs on tissue microarrays. Data were analyzed with the Kendall-rank-correlation test.

Results: Nuclear P38 correlated to low-grade dysplasia (Kendall P<0.01/tau=-0.254) and to decreased adenoma size (P<0.01/tau=-0.267). Nuclear P38 also correlated to cytoplasmic or membrane mTOR (P<0.01/tau=-0.223 and P<0.01/tau=-0.340) and to cytoplasmic CD133 (P<0.01/0.293). An inverse relationship was observed to Ki67 (P<0.00/ tau=-0.110).

Conclusions: Our results suggest an interference of P38 with initial steps of colorectal adenomagenesis. The correlation to mTOR suggests a biological crosstalk between the MAPK- and AKT-signaling-pathways in colorectal adenomagenesis at P38 level.

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P38在结直肠腺瘤中的表达:与细胞增殖、干细胞表型和AKT通路蛋白的关系

背景:已知p38蛋白在结直肠腺瘤(CRA)中表达。与腺癌相比，低级别和高级别管状腺瘤的表达减少，而与正常粘膜相比，表达增加。我们旨在研究P38在人CRAs中的表达及其与细胞增殖ki67蛋白、干表型cd133蛋白和mtor蛋白(AKT通路)的关系。方法:采用组织芯片技术检测P38在CRAs中的免疫组化表达。数据分析采用肯德尔秩相关检验。结论:我们的研究结果表明P38与结直肠腺瘤形成的初始阶段存在干扰。与mTOR的相关性表明，在P38水平上，结直肠腺瘤发生过程中，MAPK-和akt -信号通路之间存在生物学上的串扰。

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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Minerva gastroenterologica e dietologica

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