Senescent fibroblasts beta-galactosidase induced by extracellular vesicles obtained from MSC-iPSC under the action of various modulators

IF 0.1 Q4 MEDICINE, GENERAL & INTERNAL
I. Cazan
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Abstract

(Abstract): The absolute majority of published experimental data involve mesenchymal stem cells, although the possibilities offered by the use of pluripotent stem cells reprogrammed from mesenchymal stem cells are practically infinite. Aim : The goal of our study was represented by tracking the effects of stimulation and inhibition of multiple functional, intracellular pathways of senescent dermal fibroblasts in culture, in the presence of microvesicles released from pluripotent stem cells reprogrammed from mesenchymal stem cells. Material and methods : We used flow cytometry to measure the production of the be-ta-galactosidase level by dermal fibroblasts in culture after 30 passages and ultraviolet treatment. Results : Reduction of β-galactosidase concentrations in senescent dermal fibroblasts was evident upon administration of exosomes (approximately 20% on average) and exosomes co-administered with: LY-294002 (a highly selective PI3K kinase inhibitor, 41% on average); nutlin-3 (which stabilizes the non-genomic actions of p53, respectively the MDM2/p53 pathway, 63% on average); rapamycin (which stimulates autophagy and the mTOR pathway and related ones, 62% on average); and metformin (a pharmacologically active substance, considered a reprogrammer of energy metabolism, 73% on average). Conclusions : Exosomes derived from pluripotent stem cells induced from mesenchymal stem cells, administered in the culture medium of senescent dermal fibroblasts, can modify the degree and evolution of the senescence of these last cells by potentiating, activating, or stimulating some intracellular pathways of biological signal transduction, but especially through epigenetic reprogramming of energy metabolism.
多种调节剂作用下MSC-iPSC细胞外囊泡诱导衰老成纤维细胞β -半乳糖苷酶的研究
(摘要):绝大多数已发表的实验数据涉及间充质干细胞,尽管使用间充质干细胞重编程的多能干细胞提供的可能性实际上是无限的。目的:我们的研究目的是通过追踪在培养中,在间充质干细胞重编程的多能干细胞释放的微泡存在的情况下,刺激和抑制衰老真皮成纤维细胞的多种功能细胞内通路的影响。材料与方法:采用流式细胞术检测体外培养的皮肤成纤维细胞经30代及紫外线处理后β -半乳糖苷酶的生成水平。结果:衰老真皮成纤维细胞中β-半乳糖苷酶浓度明显降低,外泌体(平均约20%)和外泌体与:LY-294002(一种高选择性PI3K激酶抑制剂,平均41%)共同施用;nutlin-3(稳定p53的非基因组作用,分别是MDM2/p53通路,平均63%);雷帕霉素(刺激自噬和mTOR途径及相关途径,平均62%);二甲双胍(一种药理活性物质,被认为是能量代谢的重新编程器,平均为73%)。结论:间充质干细胞诱导的多能干细胞衍生的外泌体,在衰老的真皮成纤维细胞培养基中,可以通过增强、激活或刺激一些细胞内的生物信号转导途径,特别是通过表观遗传重编程的能量代谢,来改变这些末代细胞的衰老程度和进化。
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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