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乳腺癌中细胞通讯相关的连续组织、协同过表达的蛋白编码基因的揭示。

The Revelation of Continuously Organized, Co-Overexpressed Protein-Coding Genes with Roles in Cellular Communications in Breast Cancer.

机构信息

Cancer Research Program, Rajiv Gandhi Centre for Biotechnology, Thiruvananthapuram 695014, India.

PhD Program, Manipal Academy of Higher Education, Manipal 576104, India.

出版信息

Cells. 2022 Nov 28;11(23):3806. doi: 10.3390/cells11233806.

Abstract

Many human cancers, including breast cancer, are polygenic and involve the co-dysregulation of multiple regulatory molecules and pathways. Though the overexpression of genes and amplified chromosomal regions have been closely linked in breast cancer, the notion of the co-upregulation of genes at a single locus remains poorly described. Here, we describe the co-overexpression of 34 continuously organized protein-coding genes with diverse functions at 8q.24.3(143437655-144326919) in breast and other cancer types, the CanCord34 genes. In total, 10 out of 34 genes have not been reported to be overexpressed in breast cancer. Interestingly, the overexpression of CanCord34 genes is not necessarily associated with genomic amplification and is independent of hormonal or HER2 status in breast cancer. CanCord34 genes exhibit diverse known and predicted functions, including enzymatic activities, cell viability, multipotency, cancer stem cells, and secretory activities, including extracellular vesicles. The co-overexpression of 33 of the CanCord34 genes in a multivariant analysis was correlated with poor survival among patients with breast cancer. The analysis of the genome-wide RNAi functional screening, cell dependency fitness, and breast cancer stem cell databases indicated that three diverse overexpressed CanCord34 genes, including a component of spliceosome PUF60, a component of exosome complex EXOSC4, and a ribosomal biogenesis factor BOP1, shared roles in cell viability, cell fitness, and stem cell phenotypes. In addition, 17 of the CanCord34 genes were found in the microvesicles (MVs) secreted from the mesenchymal stem cells that were primed with MDA-MB-231 breast cancer cells. Since these MVs were important in the chemoresistance and dedifferentiation of breast cancer cells into cancer stem cells, these findings highlight the significance of the CanCord34 genes in cellular communications. In brief, the persistent co-overexpression of CanCord34 genes with diverse functions can lead to the dysregulation of complementary functions in breast cancer. In brief, the present study provides new insights into the polygenic nature of breast cancer and opens new research avenues for basic, preclinical, and therapeutic studies in human cancer.

摘要

许多人类癌症,包括乳腺癌,是多基因的,并涉及多个调节分子和途径的共同失调。尽管在乳腺癌中已经密切关联了基因的过度表达和扩增的染色体区域,但单个基因座的基因共同上调的概念仍描述得很差。在这里,我们描述了在乳腺癌和其他癌症类型中,在 8q.24.3(143437655-144326919) 上连续组织的 34 个具有不同功能的蛋白质编码基因的共同过度表达,即 CanCord34 基因。总的来说,在乳腺癌中,有 10 个基因没有被报道过度表达。有趣的是,CanCord34 基因的过度表达不一定与基因组扩增有关,并且在乳腺癌中与激素或 HER2 状态无关。CanCord34 基因具有多种已知和预测的功能,包括酶活性、细胞活力、多能性、癌症干细胞和分泌活性,包括细胞外囊泡。在多变量分析中,33 个 CanCord34 基因的共同过度表达与乳腺癌患者的不良生存相关。对全基因组 RNAi 功能筛选、细胞依赖性适应性和乳腺癌干细胞数据库的分析表明,三种不同的过度表达的 CanCord34 基因,包括剪接体 PUF60 的一个成分、外泌体复合物 EXOSC4 的一个成分和核糖体生物发生因子 BOP1,在细胞活力、细胞适应性和干细胞表型中发挥作用。此外,在被 MDA-MB-231 乳腺癌细胞预激活的间充质干细胞分泌的微泡 (MVs) 中发现了 17 个 CanCord34 基因。由于这些 MVs 对乳腺癌细胞的化疗耐药性和去分化为癌症干细胞至关重要,这些发现突出了 CanCord34 基因在细胞通讯中的重要性。简而言之,具有不同功能的 CanCord34 基因的持续共同过度表达可能导致乳腺癌中互补功能的失调。简而言之,本研究为乳腺癌的多基因性质提供了新的见解,并为人类癌症的基础、临床前和治疗研究开辟了新的研究途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81bf/9741223/1c16c797953d/cells-11-03806-g001.jpg

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