Relan N K, Yang Y, Beqaj S, Miner J H, Schuger L
Department of Pathology, Wayne State University School of Medicine, Detroit, Michigan 48201, USA.
J Cell Biol. 1999 Dec 13;147(6):1341-50. doi: 10.1083/jcb.147.6.1341.
Bronchial smooth muscle (SM) mesenchymal cell precursors change their shape from round to spread/elongated while undergoing differentiation. Here we show that this change in cell shape induces the expression of laminin (LM) alpha2 chain not present in round mesenchymal cells. LM alpha2 expression is reversible and switched on and off by altering the cell's shape in culture. In comparison, the expression of LM beta1 and gamma1 remains unchanged. Functional studies showed that mesenchymal cell spreading and further differentiation into SM are inhibited by an antibody against LM alpha2. Dy/dy mice express very low levels of LM alpha2 and exhibit congenital muscular dystrophy. Lung SM cells isolated from adult dy/dy mice spread defectively and synthesized less SM alpha-actin, desmin, and SM-myosin than controls. These deficiencies were completely corrected by exogenous LM-2. On histological examination, dy/dy mouse airways and gastrointestinal tract had shorter SM cells, and lungs from dy/dy mice contained less SM-specific protein. The intestine, however, showed compensatory hyperplasia, perhaps related to its higher contractile activity. This study therefore demonstrated a novel role for the LM alpha2 chain in SM myogenesis and showed that its decrease in dy/dy mice results in abnormal SM.
支气管平滑肌(SM)间充质细胞前体在分化过程中其形状从圆形变为伸展/拉长状。在此我们表明,这种细胞形状的改变会诱导圆形间充质细胞中不存在的层粘连蛋白(LM)α2链的表达。LMα2的表达是可逆的,可通过在培养中改变细胞形状来开启和关闭。相比之下,LMβ1和γ1的表达保持不变。功能研究表明,抗LMα2抗体可抑制间充质细胞的伸展以及向SM的进一步分化。dy/dy小鼠表达极低水平的LMα2,并表现出先天性肌营养不良。从成年dy/dy小鼠分离出的肺SM细胞伸展存在缺陷,且与对照相比,合成的SMα-肌动蛋白、结蛋白和SM-肌球蛋白更少。这些缺陷可通过外源性LM-2完全纠正。组织学检查显示,dy/dy小鼠的气道和胃肠道的SM细胞较短,dy/dy小鼠的肺中含有的SM特异性蛋白较少。然而,肠道显示出代偿性增生,这可能与其较高的收缩活性有关。因此,本研究证明了LMα2链在SM肌生成中的新作用,并表明其在dy/dy小鼠中的减少会导致SM异常。
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