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鸟嘌呤核苷酸交换、GTP水解与突变型ras蛋白转化潜能之间的关系。

Relationship among guanine nucleotide exchange, GTP hydrolysis, and transforming potential of mutated ras proteins.

作者信息

Feig L A, Cooper G M

机构信息

Department of Biochemistry, Tufts University School of Medicine, Boston, Massachusetts 02111.

出版信息

Mol Cell Biol. 1988 Jun;8(6):2472-8. doi: 10.1128/mcb.8.6.2472-2478.1988.

Abstract

The effect of a series of mutations on the transforming potential of normal human rasH has been compared with their effects on GTPase and guanine nucleotide exchange rates of p21. The mutation Val-146 resulted in partial activation of transforming potential which could be attributed to a greater than 1,000-fold-increased rate of nucleotide exchange in the absence of an effect on GTPase. In contrast, the more modest enhancement of exchange rate (approximately 100-fold) which resulted from the mutation Met-14 did not affect biological activity. The partially activating mutation Thr-59 was found to result in both a 5-fold reduction in GTPase and a 10-fold increase in nucleotide exchange. However, the nontransforming mutant Ile-59 displayed a comparable decrease in GTPase without an effect on nucleotide exchange. The activating effect of the Thr-59 mutation may thus represent a combined effect of reduced GTPase and increased exchange. Similarly, the strongly activating mutation Leu-61 resulted in a fivefold increase in nucleotide exchange in addition to decreased GTPase, whereas weakly activating mutations at position 61 (Trp and Pro) resulted only in decreased GTPase without affecting nucleotide exchange rates. Finally, combining the two mutations Met-14 and Ile-59, which alone had no effect on biological activity, yielded a double mutant with a 20-fold increased transforming potential, demonstrating a synergistic effect of these two mutations. Overall, these results indicate that large increases in nucleotide exchange can activate ras transforming potential in the absence of decreased GTPase and that relatively modest increases in nucleotide exchange can act synergistically with decreased GTPase to contribute to ras activation.

摘要

已将一系列突变对正常人rasH转化潜能的影响与其对p21的GTP酶活性和鸟嘌呤核苷酸交换速率的影响进行了比较。Val-146突变导致转化潜能部分激活,这可归因于在不影响GTP酶的情况下核苷酸交换速率增加了1000倍以上。相比之下,Met-14突变导致的交换速率适度增强(约100倍)并未影响生物学活性。发现部分激活突变Thr-59导致GTP酶活性降低5倍,核苷酸交换增加10倍。然而,非转化突变体Ile-59的GTP酶活性有类似降低,但对核苷酸交换没有影响。因此,Thr-59突变的激活作用可能代表了GTP酶降低和交换增加的综合作用。同样,强激活突变Leu-61除了导致GTP酶降低外,还使核苷酸交换增加了五倍,而61位的弱激活突变(Trp和Pro)仅导致GTP酶降低,而不影响核苷酸交换速率。最后,将单独对生物学活性无影响的两个突变Met-14和Ile-59组合,产生了一个转化潜能增加20倍的双突变体,证明了这两个突变的协同作用。总体而言,这些结果表明,在GTP酶不降低的情况下,核苷酸交换的大幅增加可激活ras的转化潜能,而核苷酸交换的相对适度增加可与GTP酶降低协同作用,促进ras激活。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/374f/363447/99262841d777/molcellb00066-0218-a.jpg

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