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Single genome retrieval of context-dependent variability in mutation rates for human germline.

Published version
Peer-reviewed

Type

Article

Change log

Authors

Sahakyan, Aleksandr  ORCID logo  https://orcid.org/0000-0002-8343-3594
Balasubramanian, Shankar  ORCID logo  https://orcid.org/0000-0002-0281-5815

Abstract

BACKGROUND: Accurate knowledge of the core components of substitution rates is of vital importance to understand genome evolution and dynamics. By performing a single-genome and direct analysis of 39,894 retrotransposon remnants, we reveal sequence context-dependent germline nucleotide substitution rates for the human genome.

RESULTS: The rates are characterised through rate constants in a time-domain, and are made available through a dedicated program (Trek) and a stand-alone database. Due to the nature of the method design and the imposed stringency criteria, we expect our rate constants to be good estimates for the rates of spontaneous mutations. Benefiting from such data, we study the short-range nucleotide (up to 7-mer) organisation and the germline basal substitution propensity (BSP) profile of the human genome; characterise novel, CpG-independent, substitution prone and resistant motifs; confirm a decreased tendency of moieties with low BSP to undergo somatic mutations in a number of cancer types; and, produce a Trek-based estimate of the overall mutation rate in human.

CONCLUSIONS: The extended set of rate constants we report may enrich our resources and help advance our understanding of genome dynamics and evolution, with possible implications for the role of spontaneous mutations in the emergence of pathological genotypes and neutral evolution of proteomes.

Description

Keywords

cancer, context-dependence, genome composition, germline, nucleotide substitutions, somatic mutations, spontaneous mutations

Journal Title

BMC Genomics

Conference Name

Journal ISSN

1471-2164
1471-2164

Volume Title

18

Publisher

BioMed Central
Sponsorship
Wellcome Trust (099232/Z/12/Z)
Cancer Research UK (18618)
This research was supported by the Herchel Smith Fund and Cancer Research UK (C9681/A18618). S.B. is a Wellcome Trust Senior Investigator (099232/Z/12/Z).