Characteristics of nuclear architectural abnormalities of myotubes differentiated from Lmna^H222P/H222P skeletal muscle cells.

IF 1.5 4区生物学 Q4 CELL BIOLOGY

In Vitro Cellular & Developmental Biology. Animal Pub Date : 2024-08-01 Epub Date: 2024-05-09 DOI:10.1007/s11626-024-00915-1

Eiji Wada, Nao Susumu, Motoshi Kaya, Yukiko K Hayashi

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Abstract

The presence of nuclear architectural abnormalities is a hallmark of the nuclear envelopathies, which are a group of diseases caused by mutations in genes encoding nuclear envelope proteins. Mutations in the lamin A/C gene cause several diseases, named laminopathies, including muscular dystrophies, progeria syndromes, and lipodystrophy. A mouse model carrying with the Lmna^H222P/H222P mutation (H222P) was shown to develop severe cardiomyopathy but only mild skeletal myopathy, although abnormal nuclei were observed in their striated muscle. In this report, we analyzed the abnormal-shaped nuclei in myoblasts and myotubes isolated from skeletal muscle of H222P mice, and evaluated the expression of nuclear envelope proteins in these abnormal myonuclei. Primary skeletal muscle cells from H222P mice proliferated and efficiently differentiated into myotubes in vitro, similarly to those from wild-type mice. During cell proliferation, few abnormal-shaped nuclei were detected; however, numerous markedly abnormal myonuclei were observed in myotubes from H222P mice on days 5 and 7 of differentiation. Time-lapse observation demonstrated that myonuclei with a normal shape maintained their normal shape, whereas abnormal-shaped myonuclei remained abnormal for at least 48 h during differentiation. Among the abnormal-shaped myonuclei, 65% had a bleb with a string structure, and 35% were severely deformed. The area and nuclear contents of the nuclear blebs were relatively stable, whereas the myocytes with nuclear blebs were actively fused within primary myotubes. Although myonuclei were markedly deformed, the deposition of DNA damage marker (γH2AX) or apoptotic marker staining was rarely observed. Localizations of lamin A/C and emerin were maintained within the blebs, strings, and severely deformed regions of myonuclei; however, lamin B1, nesprin-1, and a nuclear pore complex protein were absent in these abnormal regions. These results demonstrate that nuclear membranes from H222P skeletal muscle cells do not rupture and are resistant to DNA damage, despite these marked morphological changes.

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从 LmnaH222P/H222P 骨骼肌细胞分化出的肌管的核结构异常特征

核结构异常是核包膜病的一个特征，核包膜病是由编码核包膜蛋白的基因突变引起的一组疾病。片层蛋白 A/C基因突变会导致多种疾病，包括肌肉萎缩症、早衰综合征和脂肪营养不良症，这些疾病被命名为片层病。一种携带 LmnaH222P/H222P 突变（H222P）的小鼠模型被证明会出现严重的心肌病，但只有轻微的骨骼肌病，尽管在它们的横纹肌中观察到了异常的细胞核。在本报告中，我们分析了从 H222P 小鼠骨骼肌中分离出的肌母细胞和肌管中的异常形核，并评估了这些异常肌核中核包膜蛋白的表达。与野生型小鼠的骨骼肌细胞相似，H222P 小鼠的骨骼肌原代细胞在体外增殖并高效分化为肌管。在细胞增殖过程中，很少检测到形状异常的核，但在分化的第 5 天和第 7 天，在 H222P 小鼠的肌管中观察到大量明显异常的肌核。延时观察结果表明，形状正常的肌核可保持正常形状，而形状异常的肌核在分化过程中至少48小时仍保持异常。在形状异常的肌核中，65%的肌核呈串珠状结构，35%的肌核严重变形。核出血点的面积和核内容物相对稳定，而有核出血点的肌细胞则在原发性肌管内积极融合。虽然肌核明显变形，但很少观察到DNA损伤标记（γH2AX）或凋亡标记染色沉积。在肌核的出血点、串和严重畸形区域，层粘连蛋白A/C和emerin的定位保持不变；但在这些异常区域，层粘连蛋白B1、nesprin-1和一种核孔复合体蛋白却不存在。这些结果表明，尽管H222P骨骼肌细胞的核膜发生了这些明显的形态学变化，但它们不会破裂，并能抵抗DNA损伤。

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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来源期刊

In Vitro Cellular & Developmental Biology. Animal 生物-发育生物学

CiteScore

3.70

自引率

4.80%

发文量

审稿时长

3 months

期刊介绍： In Vitro Cellular & Developmental Biology - Animal is a journal of the Society for In Vitro Biology (SIVB). Original manuscripts reporting results of research in cellular, molecular, and developmental biology that employ or are relevant to organs, tissue, tumors, and cells in vitro will be considered for publication. Topics covered include: Biotechnology; Cell and Tissue Models; Cell Growth/Differentiation/Apoptosis; Cellular Pathology/Virology; Cytokines/Growth Factors/Adhesion Factors; Establishment of Cell Lines; Signal Transduction; Stem Cells; Toxicology/Chemical Carcinogenesis; Product Applications.