Literature DB >> 34199989

Cellular Immune Response Induced by DNA Immunization of Mice with Drug Resistant Integrases of HIV-1 Clade A Offers Partial Protection against Growth and Metastatic Activity of Integrase-Expressing Adenocarcinoma Cells.

Maria Isaguliants1,2,3,4, Olga Krotova3,5, Stefan Petkov1, Juris Jansons2,6, Ekaterina Bayurova3,4, Dzeina Mezale2, Ilze Fridrihsone2, Athina Kilpelainen1, Philip Podschwadt1, Yulia Agapkina7, Olga Smirnova3,5, Linda Kostic1, Mina Saleem1, Oleg Latyshev3, Olesja Eliseeva3, Anastasia Malkova8, Tatiana Gorodnicheva9, Britta Wahren1, Ilya Gordeychuk3,4,10, Elizaveta Starodubova5,11, Anastasia Latanova3,5,11.   

Abstract

Therapeutic DNA-vaccination against drug-resistant HIV-1 may hinder emergence and spread of drug-resistant HIV-1, allowing for longer successful antiretroviral treatment (ART) up-to relief of ART. We designed DNA-vaccines against drug-resistant HIV-1 based on consensus clade A integrase (IN) resistant to raltegravir: IN_in_r1 (L74M/E92Q/V151I/N155H/G163R) or IN_in_r2 (E138K/G140S/Q148K) carrying D64V abrogating IN activity. INs, overexpressed in mammalian cells from synthetic genes, were assessed for stability, route of proteolytic degradation, and ability to induce oxidative stress. Both were found safe in immunotoxicity tests in mice, with no inherent carcinogenicity: their expression did not enhance tumorigenic or metastatic potential of adenocarcinoma 4T1 cells. DNA-immunization of mice with INs induced potent multicytokine T-cell response mainly against aa 209-239, and moderate IgG response cross-recognizing diverse IN variants. DNA-immunization with IN_in_r1 protected 60% of mice from challenge with 4Tlluc2 cells expressing non-mutated IN, while DNA-immunization with IN_in_r2 protected only 20% of mice, although tumor cells expressed IN matching the immunogen. Tumor size inversely correlated with IN-specific IFN-γ/IL-2 T-cell response. IN-expressing tumors displayed compromised metastatic activity restricted to lungs with reduced metastases size. Protective potential of IN immunogens relied on their immunogenicity for CD8+ T-cells, dependent on proteasomal processing and low level of oxidative stress.

Entities:  

Keywords:  ART; HIV-1; T-cell response; antibodies; immunotoxicity; integrase; lentiviral transduction; metastasis; murine adenocarcinoma 4T1luc2 cells; resistance to tumor growth; therapeutic DNA vaccine; tumor growth

Year:  2021        PMID: 34199989      PMCID: PMC8226624          DOI: 10.3390/microorganisms9061219

Source DB:  PubMed          Journal:  Microorganisms        ISSN: 2076-2607


  102 in total

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1.  Murine Models of Chronic Viral Infections and Associated Cancers.

Authors:  D V Avdoshina; A S Kondrashova; M G Belikova; E O Bayurova
Journal:  Mol Biol       Date:  2022-10-05       Impact factor: 1.540

  1 in total

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