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A mycoplasma high-affinity transport system and the in vitro invasiveness of mouse sarcoma cells.

机译:支原体高亲和力运输系统和小鼠肉瘤细胞的体外侵袭性。

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摘要

FS9 mouse sarcoma cells were previously shown to be highly invasive when confronted with chicken heart fibroblasts using Abercrombie's confronted explant technique. This invasion could be inhibited by addition to the assay of Fab fragments of a monoclonal antibody directed against p37, a protein associated with the surface of FS9 cells. We have cloned and sequenced the gene for p37. We show that it originates from Mycoplasma hyorhinis and that UGA is a tryptophan codon in this organism. We present evidence that the p37 gene is part of an operon encoding two additional proteins which are highly similar to components of the periplasmic binding-protein-dependent transport systems of Gram-negative bacteria, and we suggest that p37 is part of a homologous, high-affinity transport system in M. hyorhinis, a Gram-positive bacterium. We discuss the influence of p37 and M. hyorhinis on contact inhibition of locomotion of mammalian cells.
机译:先前已证明,使用Abercrombie的对峙外植体技术面对鸡心脏成纤维细胞时,FS9小鼠肉瘤细胞具有高度侵袭性。可以通过对针对p37(一种与FS9细胞表面相关的蛋白质)的单克隆抗体的Fab片段进行分析来抑制这种入侵。我们已经克隆并测序了p37的基因。我们显示它起源于支原体,并且UGA是这种生物体中的色氨酸密码子。我们提供的证据表明,p37基因是操纵子的一部分,其编码两个其他蛋白质,这些蛋白质与革兰氏阴性细菌的周质结合蛋白依赖性转运系统的成分高度相似,并且我们建议p37是同源,高表达的一部分革兰氏阳性菌hyorhinis中的α-亲和转运系统。我们讨论了p37和M. hyorhinis对哺乳动物细胞运动的接触抑制的影响。

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