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致癌 Ras 变异体在秀丽隐杆线虫中的功能差异。

Functional distinction in oncogenic Ras variant activity in Caenorhabditis elegans.

机构信息

Department of Molecular Genetics, Ohio State University, 484 West 12th Avenue, Columbus, OH 43210, USA.

出版信息

Dis Model Mech. 2024 Aug 1;17(8). doi: 10.1242/dmm.050577. Epub 2024 Aug 14.

Abstract

Ras genes are important oncogenes that are frequently mutated in cancer. Human oncogenic variants exhibit functional distinctions in terms of their representation in different cancer types, impact on cellular targets and sensitivity to pharmacological treatments. However, how these distinct variants influence and respond to the cellular networks in which they are embedded is poorly understood. To identify novel participants in the complex interplay between Ras genotype and cell interaction networks in vivo, we have developed and tested an experimental framework using a simple vulva-development assay in the nematode C. elegans. Using this system, we evaluated a set of Ras oncogenic substitution changes at G12, G13 and Q61. We found that these variants fall into distinct groups based on phenotypic differences, sensitivity to gene dosage and inhibition of the downstream kinase MEK and their response to genetic modulators that influence Ras activity in a non-autonomous manner. Together, our results demonstrated that oncogenic C. elegans Ras variants exhibit clear distinctions in how they interface with the vulva-development network and showed that extracellular modulators yield variant-restricted effects in vivo.

摘要

Ras 基因是重要的致癌基因,在癌症中经常发生突变。人类致癌变体在不同癌症类型中的表现、对细胞靶标的影响以及对药物治疗的敏感性方面存在功能差异。然而,这些不同的变体如何影响和响应它们所嵌入的细胞网络还知之甚少。为了确定 Ras 基因型与细胞相互作用网络在体内复杂相互作用中的新参与者,我们开发并测试了一种使用线虫 C. elegans 中简单的生殖道发育测定的实验框架。使用该系统,我们评估了一组 G12、G13 和 Q61 处的 Ras 致癌替代变化。我们发现,这些变体根据表型差异、对基因剂量的敏感性以及对下游激酶 MEK 的抑制作用以及对以非自主方式影响 Ras 活性的遗传调节剂的反应,分为不同的组。总之,我们的结果表明,致癌的 C. elegans Ras 变体在与生殖道发育网络的接口方面表现出明显的差异,并表明细胞外调节剂在体内产生变体特异性的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1275/11340813/e7abd69487fc/dmm-17-050577-g1.jpg

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