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Arginine limitation drives a directed codon-dependent DNA sequence evolution response in colorectal cancer cells.


ABSTRACT: Utilization of specific codons varies between organisms. Cancer represents a model for understanding DNA sequence evolution and could reveal causal factors underlying codon evolution. We found that across human cancer, arginine codons are frequently mutated to other codons. Moreover, arginine limitation-a feature of tumor microenvironments-is sufficient to induce arginine codon-switching mutations in human colon cancer cells. Such DNA codon switching events encode mutant proteins with arginine residue substitutions. Mechanistically, arginine limitation caused rapid reduction of arginine transfer RNAs and the stalling of ribosomes over arginine codons. Such selective pressure against arginine codon translation induced an adaptive proteomic shift toward low-arginine codon-containing genes, including specific amino acid transporters, and caused mutational evolution away from arginine codons-reducing translational bottlenecks that occurred during arginine starvation. Thus, environmental availability of a specific amino acid can influence DNA sequence evolution away from its cognate codons and generate altered proteins.

SUBMITTER: Hsu DJ 

PROVIDER: S-EPMC9821863 | biostudies-literature | 2023 Jan

REPOSITORIES: biostudies-literature

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Arginine limitation drives a directed codon-dependent DNA sequence evolution response in colorectal cancer cells.

Hsu Dennis J DJ   Gao Jenny J   Yamaguchi Norihiro N   Pinzaru Alexandra A   Wu Qiushuang Q   Mandayam Nandan N   Liberti Maria M   Heissel Søren S   Alwaseem Hanan H   Tavazoie Saeed S   Tavazoie Sohail F SF  

Science advances 20230106 1


Utilization of specific codons varies between organisms. Cancer represents a model for understanding DNA sequence evolution and could reveal causal factors underlying codon evolution. We found that across human cancer, arginine codons are frequently mutated to other codons. Moreover, arginine limitation-a feature of tumor microenvironments-is sufficient to induce arginine codon-switching mutations in human colon cancer cells. Such DNA codon switching events encode mutant proteins with arginine r  ...[more]

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