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从研究酸-碱转运体基因的体细胞突变中,我们能了解到癌症方面的什么信息?

What can we learn about acid-base transporters in cancer from studying somatic mutations in their genes?

机构信息

Department of Physiology, Anatomy and Genetics, University of Oxford, Parks Road, Oxford, OX1 3PT, UK.

出版信息

Pflugers Arch. 2024 Apr;476(4):673-688. doi: 10.1007/s00424-023-02876-y. Epub 2023 Nov 24.

Abstract

Acidosis is a chemical signature of the tumour microenvironment that challenges intracellular pH homeostasis. The orchestrated activity of acid-base transporters of the solute-linked carrier (SLC) family is critical for removing the end-products of fermentative metabolism (lactate/H) and maintaining a favourably alkaline cytoplasm. Given the critical role of pH homeostasis in enabling cellular activities, mutations in relevant SLC genes may impact the oncogenic process, emerging as negatively or positively selected, or as driver or passenger mutations. To address this, we performed a pan-cancer analysis of The Cancer Genome Atlas simple nucleotide variation data for acid/base-transporting SLCs (ABT-SLCs). Somatic mutation patterns of monocarboxylate transporters (MCTs) were consistent with their proposed essentiality in facilitating lactate/H efflux. Among all cancers, tumours of uterine corpus endometrial cancer carried more ABT-SLC somatic mutations than expected from median tumour mutation burden. Among these, somatic mutations in SLC4A3 had features consistent with meaningful consequences on cellular fitness. Definitive evidence for ABT-SLCs as 'cancer essential' or 'driver genes' will have to consider microenvironmental context in genomic sequencing because bulk approaches are insensitive to pH heterogeneity within tumours. Moreover, genomic analyses must be validated with phenotypic outcomes (i.e. SLC-carried flux) to appreciate the opportunities for targeting acid-base transport in cancers.

摘要

酸中毒是肿瘤微环境的化学特征,挑战细胞内 pH 稳态。溶质载体(SLC)家族的酸碱转运体的协调活动对于去除发酵代谢的终产物(乳酸/H)和维持有利的碱性细胞质至关重要。鉴于 pH 稳态在使细胞活动成为可能方面的关键作用,相关 SLC 基因的突变可能会影响致癌过程,作为负选择或正选择,或作为驱动或乘客突变出现。为了解决这个问题,我们对癌症基因组图谱简单核苷酸变异数据进行了泛癌分析,研究了酸碱转运 SLC(ABT-SLC)。单羧酸转运体(MCT)的体细胞突变模式与其在促进乳酸/H 外排中的预期必需性一致。在所有癌症中,子宫体子宫内膜癌的 ABT-SLC 体细胞突变比从中位数肿瘤突变负担预期的要多。在这些突变中,SLC4A3 的体细胞突变具有对细胞适应性产生有意义影响的特征。ABT-SLC 作为“癌症必需”或“驱动基因”的明确证据将不得不考虑基因组测序中的微环境背景,因为批量方法对肿瘤内 pH 异质性不敏感。此外,必须通过表型结果(即 SLC 携带的通量)验证基因组分析,以了解在癌症中靶向酸碱转运的机会。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f7c/11006749/bd6c236a6ba1/424_2023_2876_Fig1_HTML.jpg

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