Molecular Biology and Evolution, Vol 15, 957-966, Copyright © 1998 by Society for Molecular Biology and Evolution
A Reyes, C Gissi, G Pesole and C Saccone
The base composition of 25 complete mammalian mitochondrial (mt) genomes
has been analyzed taking into account all three codon positions (P1230 and
fourfold degenerate sites (P4FD) of H-strand genes. In the nontranscribed L
strand, G is the less represented base and A is the most represented one in
all cases, while C and T differ among species. H-strand protein-coding
genes show an asymmetric distribution of the four bases between the two
strands. The asymmetry indexes AT and GC skews on P4FD are much higher than
those on P123, suggesting the existence of asymmetrical directional
mutation pressure. Relationships between the compositional features and
transcription of replication processes have been investigated in order to
find a possible mechanism that could explain the origin of this asymmetry.
AT and GC skews, the base composition in fourfold degenerate sites, and the
number of variable sites for each gene are significantly correlated with
the duration of single-stranded state of the H-stranded genes during
replication. We tested different replication-related hypotheses, such as
the existence of biased dNTP pools, gamma DNA polymerase mispairing, and
the asymmetric replication itself. Most of them failed to explain the
observed results, hydrolytic deaminations being the only one in agreement
with our data. Thus, we hypothesize that one of the crucial processes for
the origin of asymmetric and biased base composition of mammalian
mitochondrial genomes is the spontaneous deamination of C and A in the H
strand during replication.
ORIGINAL ARTICLE
Asymmetrical directional mutation pressure in the mitochondrial genome of mammals
Centro di Studio sui Mitocondri e Metabolismo Energetico, Consiglio Nazionale delle Recerche, Bari, Italy.
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