Fusion to Flaviviral Leader Peptide Targets HIV-1 Reverse Transcriptase for Secretion and Reduces Its Enzymatic Activity and Ability to Induce Oxidative Stress but Has No Major Effects on Its Immunogenic Performance in DNA-Immunized Mice

Author:

Latanova Anastasia123ORCID,Petkov Stefan3,Kuzmenko Yulia1ORCID,Kilpeläinen Athina3ORCID,Ivanov Alexander1ORCID,Smirnova Olga1ORCID,Krotova Olga12ORCID,Korolev Sergey4ORCID,Hinkula Jorma5,Karpov Vadim1ORCID,Isaguliants Maria267ORCID,Starodubova Elizaveta137ORCID

Affiliation:

1. Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, Moscow, Russia

2. Gamaleja Research Center of Epidemiology and Microbiology, Moscow, Russia

3. Department of Microbiology, Tumor and Cell Biology, Karolinska Institutet, Stockholm, Sweden

4. Chemistry Department, Belozersky Research Institute of Physico-Chemical Biology of Lomonosov Moscow State University, Moscow, Russia

5. Linköping University, Linköping, Sweden

6. Riga Stradins University, Riga, Latvia

7. M.P. Chumakov Institute of Poliomyelitis and Viral Encephalities, Russian Academy of Sciences, Moscow, Russia

Abstract

Reverse transcriptase (RT) is a key enzyme in viral replication and susceptibility to ART and a crucial target of immunotherapy against drug-resistant HIV-1. RT induces oxidative stress which undermines the attempts to make it immunogenic. We hypothesized that artificial secretion may reduce the stress and make RT more immunogenic. Inactivated multidrug-resistant RT (RT1.14opt-in) was N-terminally fused to the signal providing secretion of NS1 protein of TBEV (Ld) generating optimized inactivated Ld-carrying enzyme RT1.14oil. Promotion of secretion prohibited proteasomal degradation increasing the half-life and content of RT1.14oil in cells and cell culture medium, drastically reduced the residual polymerase activity, and downmodulated oxidative stress. BALB/c mice were DNA-immunized with RT1.14opt-in or parental RT1.14oil by intradermal injections with electroporation. Fluorospot and ELISA tests revealed that RT1.14opt-in and RT1.14oil induced IFN-γ/IL-2, RT1.14opt-in induced granzyme B, and RT1.14oil induced perforin production. Perforin secretion correlated with coproduction of IFN-γand IL-2 (R=0,97). Both DNA immunogens induced strong anti-RT antibody response. Ld peptide was not immunogenic. Thus, Ld-driven secretion inferred little change to RT performance in DNA immunization. Positive outcome was the abrogation of polymerase activity increasing safety of RT-based DNA vaccines. Identification of the molecular determinants of low cellular immunogenicity of RT requires further studies.

Funder

Russian Foundation for Basic Research

Publisher

Hindawi Limited

Subject

Immunology,General Medicine,Immunology and Allergy

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