HIV-1 Protease as DNA Immunogen against Drug Resistance in HIV-1 Infection: DNA Immunization with Drug Resistant HIV-1 Protease Protects Mice from Challenge with Protease-Expressing Cells.
Stefan PetkovAthina KilpeläinenEkaterina O BayurovaAnastasia LatanovaDzeina MezaleIlse FridrihsoneElizaveta S StarodubovaJurģis JansonsAlesja DudorovaIlya V GordeychukBritta WahrenMaria G IsaguliantsPublished in: Cancers (2022)
DNA immunization with HIV-1 protease (PR) is advanced for immunotherapy of HIV-1 infection to reduce the number of infected cells producing drug-resistant virus. A consensus PR of the HIV-1 FSU_A strain was designed, expression-optimized, inactivated (D25N), and supplemented with drug resistance (DR) mutations M46I, I54V, and V82A common for FSU_A. PR variants with D25N/M46I/I54V (PR_Ai2mut) and with D25N/M46I/I54V/V82A (PR_Ai3mut) were cloned into the DNA vaccine vector pVAX1, and PR_Ai3mut, into a lentiviral vector for the transduction of murine mammary adenocarcinoma cells expressing luciferase 4T1luc2. BALB/c mice were DNA-immunized by intradermal injections of PR_Ai, PR_Ai2mut, PR_Ai3mut, vector pVAX1, or PBS with electroporation. All PR variants induced specific CD8+ T-cell responses revealed after splenocyte stimulation with PR-derived peptides. Splenocytes of mice DNA-immunized with PR_Ai and PR_Ai2mut were not activated by peptides carrying V82A, whereas splenocytes of PR_Ai3mut-immunized mice recognized both peptides with and without V82A mutation. Mutations M46I and I54V were immunologically silent. In the challenge study, DNA immunization with PR_Ai3mut protected mice from the outgrowth of subcutaneously implanted adenocarcinoma 4T1luc2 cells expressing PR_Ai3mut; a tumor was formed only in 1/10 implantation sites and no metastases were detected. Immunizations with other PR variants were not protective; all mice formed tumors and multiple metastasis in the lungs, liver, and spleen. CD8+ cells of PR_Ai3mut DNA-immunized mice exhibited strong IFN-γ/IL-2 responses against PR peptides, while the splenocytes of mice in other groups were nonresponsive. Thus, immunization with a DNA plasmid encoding inactive HIV-1 protease with DR mutations suppressed the growth and metastatic activity of tumor cells expressing PR identical to the one encoded by the immunogen. This demonstrates the capacity of T-cell response induced by DNA immunization to recognize single DR mutations, and supports the concept of the development of immunotherapies against drug resistance in HIV-1 infection. It also suggests that HIV-1-infected patients developing drug resistance may have a reduced natural immune response against DR HIV-1 mutations causing an immune escape.
Keyphrases
- antiretroviral therapy
- artificial intelligence
- drug resistant
- circulating tumor
- human immunodeficiency virus
- hiv infected patients
- immune response
- induced apoptosis
- single molecule
- hiv positive
- hiv infected
- high fat diet induced
- cell free
- hiv aids
- hepatitis c virus
- squamous cell carcinoma
- hiv testing
- cell cycle arrest
- gene expression
- oxidative stress
- escherichia coli
- acinetobacter baumannii
- small cell lung cancer
- dna methylation
- type diabetes
- metabolic syndrome
- wild type
- cell proliferation
- machine learning
- deep learning
- cell death
- radiation therapy
- poor prognosis
- skeletal muscle
- cystic fibrosis
- south africa
- diabetic rats
- high glucose
- locally advanced
- endoplasmic reticulum stress