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猿猴肉瘤病毒转化细胞中v-sis基因产物的细胞内周转、新型分泌及有丝分裂活性细胞内形式。对细胞内环自分泌转化的意义。

Intracellular turnover, novel secretion, and mitogenically active intracellular forms of v-sis gene product in simian sarcoma virus-transformed cells. Implications for intracellular loop autocrine transformation.

作者信息

Lokeshwar V B, Huang S S, Huang J S

机构信息

Department of Biochemistry and Molecular Biology, St. Louis University School of Medicine, Missouri 63104.

出版信息

J Biol Chem. 1990 Jan 25;265(3):1665-75.

PMID:2153139
Abstract

In simian sarcoma virus (SSV)-transformed cells (SSV-NRK, SSV-NIH 3T3, and SSV-NP1 cells), the v-sis gene product was synthesized as a 36-kDa glycopolypeptide with one endoglycosidase (Endo) H-sensitive oligosaccharide chain and formed a dimer (p72) with a half-time of less than 5 min. p72 was proteolytically processed to generate sequentially p68 and p58 in the endoplasmic reticulum/Golgi complex, p44 in the post-Golgi complex compartments, and p27 in an endosomal/lysosomal compartment. A portion (20-30%) of p72 and p68 later became Endo H-resistant but Endo F-sensitive. During processing, the v-sis gene products exhibited rapid turnover, possibly in the endoplasmic reticulum and/or Golgi complex. The rate of turnover correlated with the tumorigenicity previously reported in these SSV-transformed cells. All three SSV-transformed cells secreted v-sis gene product (p44). p44 was secreted but remained tightly associated with the cell surface. This novel secretion provided an efficient system for the interaction of p44 with the cell surface platelet-derived growth factor receptor which resulted in the intracellular formation of p27. A fraction of secreted p44 was converted extracellularly to a 27-kDa product (extracellular p27) after a longer time in culture. The identical N-terminal amino acid sequence of p44 and extracellular p27 (H2N-SLGSLSVAEPAMIA) indicated a preferential site (Lys110-Arg111) for the proteolytic processing. The intracellular turnover of the v-sis gene product and its correlation with tumorigenicity as well as the demonstration of mitogenically active intracellular forms of v-sis gene product support the hypothesis of intracellular loop autocrine transformation.

摘要

在猿猴肉瘤病毒(SSV)转化的细胞(SSV-NRK、SSV-NIH 3T3和SSV-NP1细胞)中,v-sis基因产物被合成为一种36 kDa的糖多肽,带有一条对内切糖苷酶(Endo)H敏感的寡糖链,并形成一个半衰期小于5分钟的二聚体(p72)。p72在内质网/高尔基体复合体中被蛋白水解加工,依次产生p68和p58,在高尔基体后复合体区室产生p44,在内体/溶酶体区室产生p27。一部分(20 - 30%)的p72和p68后来变得对Endo H有抗性但对Endo F敏感。在加工过程中,v-sis基因产物表现出快速周转,可能在内质网和/或高尔基体复合体中。周转速率与先前报道的这些SSV转化细胞中的致瘤性相关。所有三种SSV转化细胞都分泌v-sis基因产物(p44)。p44被分泌,但仍与细胞表面紧密结合。这种新的分泌为p44与细胞表面血小板衍生生长因子受体的相互作用提供了一个高效系统,导致细胞内形成p27。培养较长时间后,一部分分泌的p44在细胞外被转化为一种27 kDa的产物(细胞外p27)。p44和细胞外p27相同的N端氨基酸序列(H2N-SLGSLSVAEPAMIA)表明了蛋白水解加工的一个优先位点(Lys110 - Arg111)。v-sis基因产物的细胞内周转及其与致瘤性的相关性,以及v-sis基因产物有丝分裂活性细胞内形式的证明支持了细胞内环自分泌转化的假说。

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