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LMNA突变在原代卫星细胞和C2C12细胞成肌分化中的作用

THE ROLE OF LMNA MUTATIONS IN MYOGENIC DIFFERENTIATION OF PRIMARY SATELLITE CELLS AND C2C12 CELLS.

作者信息

Perepelina K I, Smolina N A, Zabirnik A S, Dmitrieva R I, Malashicheva A B, Kostareva A A

出版信息

Tsitologiia. 2017;59(2):117-24.

Abstract

Nuclear lamins form nuclear lamina localized under the inner nuclear membrane. It was previously considered that the nuclear lamina predominantly plays a structural role, however, its involvement have been recently described in the regulatory processes such as chromatin organization and gene transcription. It is known that mutations in the LMNA gene lead to the development of a large number of diseases, laminopathies, which mainly affect mesenchymal tissue. Nowadays, the mechanisms by which the lamina can regulate cell differentiation remain incompletely understood. In the present work, we have studied the effect of LMNA gene mutations on the process of muscle differentiation of primary satellite cells and Ñ2Ñ12 cell line. The genome of satellite cells and Ñ2Ñ12 cell line was modified by the introduction of lentiviral constructs encoding LMNA G232E associated with the development of muscular dystrophy Emery—Dreyfus and LMNA R571S associated with the development of dilated cardiomyopathy. The morphology of the cells was estimated using immunofluorescence, the expression level of myogenic genes were analyzed by qPCR. We have shown that the analyzed mutations reduce the ability of cells to differentiate, to fuse and to form myotubes. We have suggested that it is due to enhanced expression of markers at the early stages and to reduced expression markers at the late stages of myogenesis. Therefore, mutations in nuclear lamins can influence the process of muscle differentiation.

摘要

核纤层蛋白形成位于内核膜下方的核纤层。以前人们认为核纤层主要起结构作用,然而,最近已有研究表明其参与了诸如染色质组织和基因转录等调控过程。已知LMNA基因突变会导致大量疾病,即核纤层蛋白病的发生,这些疾病主要影响间充质组织。如今,核纤层调节细胞分化的机制仍未完全清楚。在本研究中,我们研究了LMNA基因突变对原代卫星细胞和C2C12细胞系肌肉分化过程的影响。通过引入编码与Emery-Dreyfus型肌营养不良症相关的LMNA G232E和与扩张型心肌病相关的LMNA R571S的慢病毒构建体,对卫星细胞和C2C12细胞系的基因组进行了修饰。使用免疫荧光评估细胞形态,通过qPCR分析成肌基因的表达水平。我们发现,所分析的突变降低了细胞分化、融合及形成肌管的能力。我们认为这是由于成肌早期标志物表达增强以及成肌后期标志物表达降低所致。因此,核纤层蛋白的突变会影响肌肉分化过程。

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