A steric gate prevents mutagenic dATP incorporation opposite 8-oxo-deoxyguanosine in mitochondrial DNA polymerases

Artículo

 

Te invitamos a leer el artículo "A steric gate prevents mutagenic dATP incorporation opposite 8-oxo-deoxyguanosine in mitochondrial DNA polymerases" publicado en FEBS Journal, ​a cargo del profesor investigador de la Unidad de Genómica Avanzada del Cinvestav Dr. Luis Gabriel Brieba de Castro, Profesor Investigador de la UGA.

Autores: Noe Baruch-Torres / Carlos H. Trasviña-Arenas / Alexandru Ionut Gilea/ Upeksha C. Dissanayake/ Missael Molina Jiménez/ Paola L. García-Medel / Corina Díaz-Quezada / Tiziana Lodi G / Andrés Cisneros / Enrico Baruffini / Luis G. Brieba

  1. Unidad de Genómica Avanzada, Centro de Investigación y de Estudios Avanzados (Cinvestav), Irapuato, Mexico 

  2. Department of Biochemistry and Molecular Biology, University of Texas Medical Branch, Galveston, TX, USA 

  3. Sealy Center for Structural Biology and Molecular Biophysics, Galveston, TX, USA

  4. Centro de Investigación sobre el Envejecimiento, Centro de Investigación y de Estudios Avanzados (Cinvestav) Unidad Sede Sur, Mexico City, Mexico

  5. Department of Chemistry, Life Sciences and Environmental Sustainability, University of Parma, Italy

  6. Department of Chemistry and Biochemistry, University of Texas at Dallas, Richardson, TX, USA

  7. Department of Physics, University of Texas at Dallas, Richardson, TX, USA

Felicitamos al estudiantado y profesorado que contribuyeron en esta investigación por su arduo trabajo.

Summary:

Reactive oxygen species (ROS) generate DNA lesions that alter genome integrity. Among those DNA lesions, 7,8-dihydro-8-oxo-2′-deoxyguanosine (8-oxodG) is particularly mutagenic. 8-oxodG efficiently incorporates deoxycytidine monophosphate (dCMP) and deoxyadenosine monophosphate (dAMP) via base pairing mediated by its anti and syn conformations, respectively. In family-A DNA polymerases (DNAPs), the amino acids responsible for modulating dCMP or dAMP incorporation across 8-oxodG are located in a determined structural position. Those residues are a conserved tyrosine located at the N terminus of the α-helix O and a nonconserved residue located six amino acids after this conserved tyrosine. In yeast mitochondrial DNAP (DNA-directed DNA polymerase gamma MIP1 [Mip1]), those residues correspond to amino acids Y757 and F763. We hypothesized that the phenyl group of the F763 residue impinges on the syn conformation of 8-oxodG, therefore reducing dAMP misincorporation. Here, we measured dCMP and dAMP incorporation across 8-oxodG using wild-type and F763 Mip1 mutants. Our data suggest that both residue F763 and the universally conserved Y757 assemble a steric gate that obtrudes the 8-oxodG(syn) conformation. As the human orthologue of Mip1, DNA polymerase gamma (HsPolγ) or DNAP γ, also harbors phenylalanine at the corresponding position to Mip1-F763, the steric gate mechanism might similarly be responsible for controlling HsPolγ's fidelity when tolerating 8-oxodG lesions.

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11/11/2024 01:41:23 p. m.
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