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细胞间和细胞与基质间的相互作用以不同方式调节大鼠肝细胞原代培养物中肝脏基因和细胞骨架基因的表达。

Cell-cell and cell-matrix interactions differentially regulate the expression of hepatic and cytoskeletal genes in primary cultures of rat hepatocytes.

作者信息

Ben-Ze'ev A, Robinson G S, Bucher N L, Farmer S R

机构信息

Department of Biochemistry, Boston University School of Medicine, MA 02118.

出版信息

Proc Natl Acad Sci U S A. 1988 Apr;85(7):2161-5. doi: 10.1073/pnas.85.7.2161.

Abstract

Freshly isolated adult rat hepatocytes exhibit a flat, extended morphology when cultured on dried rat tail collagen in the presence of growth factors; they actively synthesize DNA and express high levels of cytoskeletal mRNAs and proteins (actin, tubulin, cytokeratins, vinculin, alpha-actinin, and desmoplakin), while exhibiting low levels of liver-specific mRNAs (albumin, alpha 1-inhibitor III, and alpha 1-antitrypsin) and limited synthesis and secretion of albumin. Hepatocytes cultured on hydrated gel matrix from the Engelbreth-Holm-Swarm (EHS) mouse tumor form small spherical aggregates and exhibit low DNA, cytoskeletal mRNA, and protein synthesis, while at the same time exhibiting elevated liver-specific mRNAs and albumin production; these cells, therefore, more nearly conform to the program of gene expression seen within the normal animal. Hepatocytes on hydrated rat tail collagen resemble those on dry collagen when cultured at low density, but at high density they form compact trabecular aggregates, synthesize negligible amounts of DNA, and maintain a pattern of gene expression resembling that of hepatocytes seeded on the EHS matrix. If cell morphology is compact, as on EHS or on hydrated rat tail collagen when densely populated, DNA synthesis and expression of cytoskeletal genes are low, while liver-specific mRNAs are abundant. When cells are extended the opposite is the case. Without the growth supplement DNA synthesis is low throughout but gene expression is little affected. These studies point to the importance of cell-cell and cell-matrix interactions in determining the differentiated phenotype of hepatocytes, and they reveal an inverse relationship between cytoskeletal and liver-specific protein expression.

摘要

刚分离出的成年大鼠肝细胞在生长因子存在的情况下,培养于干燥的大鼠尾胶原上时呈现扁平、伸展的形态;它们积极合成DNA并表达高水平的细胞骨架mRNA和蛋白质(肌动蛋白、微管蛋白、细胞角蛋白、纽蛋白、α -辅肌动蛋白和桥粒斑蛋白),同时呈现低水平的肝脏特异性mRNA(白蛋白、α1 -抑制剂III和α1 -抗胰蛋白酶)以及有限的白蛋白合成和分泌。培养于来自恩格尔布雷特 - 霍尔姆 - 斯旺(EHS)小鼠肿瘤的水合凝胶基质上的肝细胞形成小的球形聚集体,并且呈现低水平的DNA、细胞骨架mRNA和蛋白质合成,而与此同时呈现升高的肝脏特异性mRNA和白蛋白产生;因此,这些细胞更接近于正常动物体内所见的基因表达程序。低密度培养时,水合大鼠尾胶原上的肝细胞类似于干燥胶原上的肝细胞,但高密度时它们形成紧密的小梁状聚集体,合成可忽略不计的DNA量,并维持一种类似于接种在EHS基质上的肝细胞的基因表达模式。如果细胞形态紧密,如在EHS上或高密度时在水合大鼠尾胶原上,DNA合成和细胞骨架基因的表达较低,而肝脏特异性mRNA丰富。当细胞伸展时情况则相反。没有生长补充剂时,整个过程中DNA合成较低,但基因表达受影响较小。这些研究指出了细胞 - 细胞和细胞 - 基质相互作用在决定肝细胞分化表型中的重要性,并且揭示了细胞骨架蛋白表达与肝脏特异性蛋白表达之间的负相关关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c55/279949/b480994c1385/pnas00259-0145-a.jpg

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