Mitochondrial Haplotype and Mito-nuclear Matching Drive Somatic Mutation and Selection Throughout Ageing

Overview

Journal Nat Ecol Evol

Publisher Springer Nature

Specialty Biology

Date 2024 Feb 16

PMID 38361161

Authors

Isabel M Serrano

Misa Hirose

Charles C Valentine

Sharon Roesner

Elizabeth Schmidt

Gabriel Pratt

Lindsey Williams

Jesse Salk

Saleh Ibrahim

Peter H Sudmant

Affiliations

Soon will be listed here.

Abstract

Mitochondrial genomes co-evolve with the nuclear genome over evolutionary timescales and are shaped by selection in the female germline. Here we investigate how mismatching between nuclear and mitochondrial ancestry impacts the somatic evolution of the mitochondrial genome in different tissues throughout ageing. We used ultrasensitive duplex sequencing to profile ~2.5 million mitochondrial genomes across five mitochondrial haplotypes and three tissues in young and aged mice, cataloguing ~1.2 million mitochondrial somatic and ultralow-frequency inherited mutations, of which 81,097 are unique. We identify haplotype-specific mutational patterns and several mutational hotspots, including at the light strand origin of replication, which consistently exhibits the highest mutation frequency. We show that rodents exhibit a distinct mitochondrial somatic mutational spectrum compared with primates with a surfeit of reactive oxygen species-associated G > T/C > A mutations, and that somatic mutations in protein-coding genes exhibit signatures of negative selection. Lastly, we identify an extensive enrichment in somatic reversion mutations that 're-align' mito-nuclear ancestry within an organism's lifespan. Together, our findings demonstrate that mitochondrial genomes are a dynamically evolving subcellular population shaped by somatic mutation and selection throughout organismal lifetimes.

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