Mutation Frequencies in HIV-1 Genome in Regions Containing Efficient RNAi Targets As Calculated from Ultra-Deep Sequencing Data


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Abstract

HIV-1 is one of the most variable viruses. The development of gene therapy technology using RNAi for AIDS/HIV-1 treatment is a potential alternative for traditional anti-retroviral therapy. Anti-HIV-1 siRNA should aim to exploit the most conserved viral targets. Using the deep sequencing of potential RNAi targets in 100-nt HIV-1 genome fragments from the clinical HIV-1 subtype A isolates in Russia, we found that the frequencies of all possible transversions and transitions in certain RNAi targets are 3–38 times lower than in adjacent sequences. Therefore, these targets are conserved. We propose the development of these RNAi targets for AIDS/HIV-1 treatment. Deep sequencing also enables the detection of the characteristic mutational bias of RT during the replication of viral RNA.

About the authors

O. V. Kretova

Engelhardt Institute of Molecular Biology

Email: tchurikov@eimb.ru
Russian Federation, Moscow, 119334

M. A. Gorbacheva

Engelhardt Institute of Molecular Biology

Email: tchurikov@eimb.ru
Russian Federation, Moscow, 119334

D. M. Fedoseeva

Engelhardt Institute of Molecular Biology

Email: tchurikov@eimb.ru
Russian Federation, Moscow, 119334

Y. V. Kravatsky

Engelhardt Institute of Molecular Biology

Email: tchurikov@eimb.ru
Russian Federation, Moscow, 119334

V. R. Chechetkin

Engelhardt Institute of Molecular Biology

Email: tchurikov@eimb.ru
Russian Federation, Moscow, 119334

N. A. Tchurikov

Engelhardt Institute of Molecular Biology

Author for correspondence.
Email: tchurikov@eimb.ru
Russian Federation, Moscow, 119334

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