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用c-fms序列“替换”v-fms的COOH末端截短会显著降低转化潜能。

"Replacement" of COOH-terminal truncation of v-fms with c-fms sequences markedly reduces transformation potential.

作者信息

Browning P J, Bunn H F, Cline A, Shuman M, Nienhuis A W

出版信息

Proc Natl Acad Sci U S A. 1986 Oct;83(20):7800-4. doi: 10.1073/pnas.83.20.7800.

Abstract

Protooncogenes when transduced by retroviruses may undergo structural modifications that render their gene products oncogenic. The c-fms gene encodes a transmembrane protein with tyrosine kinase activity that is very similar or identical to the receptor for the monocyte-macrophage colony-stimulating factor. Its transforming homologue (v-fms) in the Susan McDonough strain feline sarcoma virus causes fibrosarcomas in cats. Molecular cloning and sequence analysis of the cDNA that encodes the cytoplasmic domain of the human c-fms gene shows that the product of the transduced viral homologue, v-fms, is truncated at the COOH-terminal end. The COOH-terminal 40 amino acids of the c-fms gene product are replaced in the v-fms gene product by 11 amino acids encoded by the retroviral genome. Hybrid v-fms/c-fms genes, in which either the entire cytoplasmic domain or the COOH-terminal coding sequences of the v-fms gene were replaced by the corresponding segments of the c-fms gene, had a reduced ability to transform fibroblasts despite a high level of encoded protein on the cell surface. These data indicate that the COOH-terminal modifications contribute to the transforming potential of the v-fms viral oncogene product.

摘要

原癌基因在被逆转录病毒转导时可能会发生结构修饰,使其基因产物具有致癌性。c-fms基因编码一种具有酪氨酸激酶活性的跨膜蛋白,该蛋白与单核细胞 - 巨噬细胞集落刺激因子的受体非常相似或相同。其在苏珊·麦克多诺猫肉瘤病毒中的转化同源物(v-fms)可在猫体内引发纤维肉瘤。对编码人c-fms基因胞质结构域的cDNA进行分子克隆和序列分析表明,转导的病毒同源物v-fms的产物在COOH末端被截断。c-fms基因产物的COOH末端40个氨基酸在v-fms基因产物中被逆转录病毒基因组编码的11个氨基酸所取代。杂合的v-fms/c-fms基因,其中v-fms基因的整个胞质结构域或COOH末端编码序列被c-fms基因的相应片段所取代,尽管细胞表面编码蛋白水平很高,但转化成纤维细胞的能力却降低了。这些数据表明,COOH末端修饰有助于v-fms病毒癌基因产物的转化潜能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/985e/386809/d93ed22115e8/pnas00324-0247-a.jpg

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