Abstract

Two key cellular processes, namely transcription and replication, require the opening of the DNA double helix and act differently on the two DNA strands, generating different mutational patterns (mutational asymmetry) that may result, after long evolutionary time, in different nucleotide compositions on the two DNA strands (compositional asymmetry). We elaborate on the simplest model of neutral substitution rates that takes into account the strand asymmetries generated by the transcription and replication processes. Using perturbation theory, we then solve the time evolution of the DNA composition under strand-asymmetric substitution rates. In our minimal model, the compositional and substitutional asymmetries are predicted to decompose into a transcription- and a replication-associated components. The transcription-associated asymmetry increases in magnitude with transcription rate and changes sign with gene orientation while the replication-associated asymmetry is proportional to the replication fork polarity. These results are confirmed experimentally in the human genome, using substitution rates obtained by aligning the human and chimpanzee genomes using macaca and orangutan as outgroups, and replication fork polarity determined in the HeLa cell line as estimated from the derivative of the mean replication timing. When further investigating the dynamics of compositional skew evolution, we show that it is not at equilibrium yet and that its evolution is an extremely slow process with characteristic time scales of several hundred Myrs.

Highlights

  • A clear relationship between replication and compositional asymmetry was first established in prokaryotic genomes by Lobry [11]

  • We recover the result of Lobry [32]: if the substitution rate matrix is symmetrical (PR1), the compositional skews are null at equilibrium (PR2): if M = M s (PR1) ST∗ A = SG∗ C = 0 (PR2). (46)

  • We analysed strand asymmetry using the replication fork polarity determined in the HeLa cell line, as a substitute to germline replication fork polarity

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Summary

About the role of the replication fork polarity in genome evolution

This article is published with open access at Springerlink.com

Introduction
Transcription and replication as strand symmetry breaking processes
Parity rule type 1
Parity rule type 2
Transcription is a strand-asymmetric process
Replication is a strand asymmetric process
From mutations to substitutions
Substitution rates in intergenic regions
Substitution rates in genic regions
Molecular mechanisms
Other examples of molecular mechanisms
Analysis of substitution rates in the human genome
General formalism
Time evolution of the composition
Exploiting strand exchange symmetry
Numerical simulations
Strand asymmetry establishment
Perturbative analysis
From substitutional to compositional asymmetries
Numerical tests
The observed compositional skews were generated over several hundreds Myrs
Discussion
Are the replication-associated asymmetries overestimated?
Findings
Effect of gene expression on substitution rates
Full Text
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