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2. Study of Viral Photoinactivation by UV-C Light and Photosensitizer Using a Pseudotyped Model.

Author

Sadraeian, M, Junior, FFP, Miranda, M, Galinskas, J, Fernandes, RS, da Cruz, EF, Fu, L, Zhang, L, Diaz, RS, Cabral-Miranda, G, Guimarães, FEG, Sadraeian, M, Junior, FFP, Miranda, M, Galinskas, J, Fernandes, RS, da Cruz, EF, Fu, L, Zhang, L, Diaz, RS, Cabral-Miranda, G, and Guimarães, FEG

Abstract

Different light-based strategies have been investigated to inactivate viruses. Herein, we developed an HIV-based pseudotyped model of SARS-CoV-2 (SC2) to study the mechanisms of virus inactivation by using two different strategies; photoinactivation (PI) by UV-C light and photodynamic inactivation (PDI) by Photodithazine photosensitizer (PDZ). We used two pseudoviral particles harboring the Luciferase-IRES-ZsGreen reporter gene with either a SC2 spike on the membrane or without a spike as a naked control pseudovirus. The mechanism of viral inactivation by UV-C and PDZ-based PDI were studied via biochemical characterizations and quantitative PCR on four levels; free-cell viral damage; viral cell entry; DNA integration; and expression of reporter genes. Both UV-C and PDZ treatments could destroy single stranded RNA (ssRNA) and the spike protein of the virus, with different ratios. However, the virus was still capable of binding and entering into the HEK 293T cells expressing angiotensin-converting enzyme 2 (ACE-2). A dose-dependent manner of UV-C irradiation mostly damages the ssRNA, while PDZ-based PDI mostly destroys the spike and viral membrane in concentration and dose-dependent manners. We observed that the cells infected by the virus and treated with either UV-C or PDZ-based PDI could not express the luciferase reporter gene, signifying the viral inactivation, despite the presence of RNA and DNA intact genes.

Published
2022

4. Safety and potential impact of auranofin on the viral reservoir in HIV positive individuals under mega-ART

Author

Diaz, R.S., primary, Giron, L.B., additional, Galinskas, J., additional, Dias, D., additional, Hunter, J., additional, Tenore, S., additional, Gosuen, G., additional, Samer, S., additional, Umaki, M., additional, Shoaib Arif, M., additional, Nutini, M., additional, Luca Shytaj, I., additional, Lucic, B., additional, Lusic, M., additional, Janini, M., additional, Sucupira, M.C., additional, and Savarino, A., additional

Published
2017
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8. People living with HIV co-infected with the Kaposi Sarcoma-associated Herpes Virus have a distinct HIV Tat profile and higher rates of antiretroviral virologic failure, more evident among those with Kaposi's sarcoma.

Author

Suterio DG, Hunter JR, Tenore SB, Pimentel SR, Galinskas J, Dias DA, Bellini DC, Ferreira PA, and Diaz RS

Subjects
Humans, Male, Female, Adult, Middle Aged, HIV-1 genetics, HIV-1 drug effects, Genetic Variation, Viral Load, Anti-Retroviral Agents therapeutic use, CD4 Lymphocyte Count, Sarcoma, Kaposi virology, HIV Infections complications, HIV Infections drug therapy, HIV Infections virology, Herpesvirus 8, Human genetics, tat Gene Products, Human Immunodeficiency Virus genetics, Coinfection virology, Coinfection drug therapy
Abstract

Kaposi sarcoma (KS) is a neoplasm of vascular origin that promotes angiogenesis and the growth of endothelial cells triggered by the Kaposi Sarcoma-associated Herpes Virus (KSHV). When associated with HIV, KSHV becomes more aggressive and rapidly evolves. The HIV-1 TAT protein can be essential in developing AIDS-associated KS by promoting angiogenesis and increasing KSHV replication. Therefore, we evaluated the genetic profile of the first exon of tat gene among groups of people living with HIV (PLHIV) with (case group, n = 36) or without KS, this later with (positive control group, n = 46) and without KSHV infection (negative control group, n = 24); all individuals under antiretroviral therapy. The genetic diversity, the DN/DS ratio, and the genetic entropy of the first exon of tat were higher in the case group, followed by the positive control group, which was higher than the negative control group. The number of tat codons under positive selection was seven in the case group, six in the positive control group, and one in the negative control group. The prevalence of HIV viral loads below the detection limit was equal in the case and positive control groups, which were lower than in the negative control group. The mean CD4+ T cell counts were higher in the negative control group, followed by the positive control group, and followed by the case group. These results emphasize the negative influence of KSHV in antiretroviral treatment, as well as the HIV-specific TAT profile among PLHIV who developed KS., (© 2024 Wiley Periodicals LLC.)

Published
2024
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9. Dolutegravir-associated resistance mutations after first-line treatment failure in Brazil.

Author

Diaz RS, Hunter JR, Camargo M, Dias D, Galinskas J, Nassar I, de Lima IB, Caldeira DB, Sucupira MC, and Schechter M

Subjects
Humans, Brazil, Lamivudine pharmacology, Lamivudine therapeutic use, Mutation, Anti-Retroviral Agents, Tenofovir, Treatment Failure, Reverse Transcriptase Inhibitors pharmacology, Reverse Transcriptase Inhibitors therapeutic use, HIV Infections drug therapy
Abstract

Background: Since January 2017, the recommended first-line antiretroviral regimen in Brazil is the fixed-dose combination of tenofovir plus lamivudine with dolutegravir (TL + D). According to the literature, integrase resistance-associated mutations (INRAMs) are rarely found upon virologic failure to first-line dolutegravir plus two nucleoside reverse transcriptase inhibitors. We evaluated the HIV antiretroviral genotypic resistance profile of patients referred for genotyping in the public health system who failed first-line TL + D after at least six months of therapy on or before December 31, 2018., Methods: HIV Sanger sequences of the pol gene were generated from plasma of patients with confirmed virologic failure to first-line TL + D in the Brazilian public health system before December 31, 2018., Results: One hundred thirteen individuals were included in the analysis. Major INRAMs were detected in seven patients (6.19%), four with R263K, one with G118R, one with E138A, and one with G140R. Four patients with major INRAMs also had the K70E and M184V mutations in the RT gene. Sixteen (14.2%) additional individuals presented minor INRAMs, and five (4,42%) patients had both major and minor INRAMS. Thirteen (11.5%) patients also presented mutations in the RT gene selected by tenofovir and lamivudine, including four with both the K70E and M184V mutations and four with only M184V. The integrase mutations L101I and T124A, which are in the in vitro pathway for integrase inhibitor resistance, were found in 48 and 19 patients, respectively. Mutations not related to TL + D, thus probable transmitted resistance mutations (TDR), were present in 28 patients (24.8%): 25 (22.1%) to nucleoside reverse transcriptase inhibitors, 19 (16.8%) to non-nucleoside reverse transcriptase inhibitors, and 6 (5.31%) to protease inhibitors., Conclusions: In marked contrast to previous reports, we report a relatively high frequency of INRAMs among selected patients failing first-line TL + D in the public health system in Brazil. Possible reasons for this discrepancy include delays in detecting virologic failure, patients inadvertently on dolutegravir monotherapy, TDR, and/or infecting subtype., (© 2023. The Author(s).)

Published
2023
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10. Re-emergence of mayaro virus and coinfection with chikungunya during an outbreak in the state of Tocantins/Brazil.

Author

Dos Santos Souza Marinho R, Duro RLS, Bellini Caldeira D, Galinskas J, Oliveira Mota MT, Hunter J, Rodrigues Teles MDA, de Pádua Milagres FA, Sobhie Diaz R, Shinji Kawakubo F, and Vasconcelos Komninakis S

Subjects
Brazil epidemiology, Disease Outbreaks, Humans, Chikungunya Fever diagnosis, Chikungunya Fever epidemiology, Chikungunya virus genetics, Coinfection epidemiology, Dengue epidemiology
Abstract

Objective: To perform a molecular screening to detect infections by the mayaro virus and possible coinfections with Chikungunya during an outbreak in the state of Tocantins/Brazil in 2017., Results: Of a total 102 samples analyzed in this study, 6 cases were identified with simultaneous infection between mayaro and chikungunya viruses (5.88%). In these 6 samples, the mean Cycle threshold (Ct) for CHIKV was 26.87 (SD ± 10.54) and for MAYV was 29.58 (SD ± 6.34). The mayaro sequences generated showed 95-100% identity to other Brazilian sequences of this virus and with other MAYV isolates obtained from human and arthropods in different regions of the world. The remaining samples were detected with CHIKV monoinfection (41 cases), DENV monoinfection (50 cases) and coinfection between CHIKV/DENV (5 cases). We did not detect MAYV monoinfections., (© 2022. The Author(s).)

Published
2022
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11. Study of Viral Photoinactivation by UV-C Light and Photosensitizer Using a Pseudotyped Model.

Author

Sadraeian M, Junior FFP, Miranda M, Galinskas J, Fernandes RS, da Cruz EF, Fu L, Zhang L, Diaz RS, Cabral-Miranda G, and Guimarães FEG

Abstract

Different light-based strategies have been investigated to inactivate viruses. Herein, we developed an HIV-based pseudotyped model of SARS-CoV-2 (SC2) to study the mechanisms of virus inactivation by using two different strategies; photoinactivation (PI) by UV-C light and photodynamic inactivation (PDI) by Photodithazine photosensitizer (PDZ). We used two pseudoviral particles harboring the Luciferase-IRES-ZsGreen reporter gene with either a SC2 spike on the membrane or without a spike as a naked control pseudovirus. The mechanism of viral inactivation by UV-C and PDZ-based PDI were studied via biochemical characterizations and quantitative PCR on four levels; free-cell viral damage; viral cell entry; DNA integration; and expression of reporter genes. Both UV-C and PDZ treatments could destroy single stranded RNA (ssRNA) and the spike protein of the virus, with different ratios. However, the virus was still capable of binding and entering into the HEK 293T cells expressing angiotensin-converting enzyme 2 (ACE-2). A dose-dependent manner of UV-C irradiation mostly damages the ssRNA, while PDZ-based PDI mostly destroys the spike and viral membrane in concentration and dose-dependent manners. We observed that the cells infected by the virus and treated with either UV-C or PDZ-based PDI could not express the luciferase reporter gene, signifying the viral inactivation, despite the presence of RNA and DNA intact genes.

Published
2022
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12. Pre-Exposure Prophylaxis Failure With a Multiple Drug-Resistant HIV-1 Clade C Virus in Brazil.

Author

Diaz RS, Grangeiro A, Estevam DL, Galinskas J, Dias D, and Schechter M

Subjects
Brazil epidemiology, Humans, Anti-HIV Agents therapeutic use, HIV Infections drug therapy, HIV Infections prevention & control, HIV-1 genetics, Pre-Exposure Prophylaxis
Abstract

Competing Interests: R.S.D. has received research grants from ViiV, Sanofi, J&J, and Gilead and has received honoraria for participating in GSK, ViiV, MSD, Janssen, and Gilead advisory boards; D.L.E. has received honoraria for participating in GSK, ViiV, and Gilead and advisory boards; MS has received research grants from ViiV, GSK, Janssen, MSD, and Gilead and has received honoraria for participating in GSK, ViiV, MSD, Janssen, and Gilead advisory boards. The remaining authors have no funding or conflicts of interest to disclose.

Published
2022
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13. Immunogenicity of personalized dendritic-cell therapy in HIV-1 infected individuals under suppressive antiretroviral treatment: interim analysis from a phase II clinical trial.

Author

de Almeida Baptista MV, da Silva LT, Samer S, Oshiro TM, Shytaj IL, Giron LB, Pena NM, Cruz N, Gosuen GC, Ferreira PRA, Cunha-Neto E, Galinskas J, Dias D, Sucupira MCA, de Almeida-Neto C, Salomão R, da Silva Duarte AJ, Janini LM, Hunter JR, Savarino A, Juliano MA, and Diaz RS

Subjects
CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Cell- and Tissue-Based Therapy, Dendritic Cells, Humans, HIV Infections drug therapy, HIV-1
Abstract

Background: We developed a personalized Monocyte-Derived Dendritic-cell Therapy (MDDCT) for HIV-infected individuals on suppressive antiretroviral treatment and evaluated HIV-specific T-cell responses., Methods: PBMCs were obtained from 10 HIV + individuals enrolled in trial NCT02961829. Monocytes were differentiated into DCs using IFN-α and GM-CSF. After sequencing each patient's HIV-1 Gag and determining HLA profiles, autologous Gag peptides were selected based on the predicted individual immunogenicity and used to pulse MDDCs. Three doses of the MDDCT were administered every 15 days. To assess immunogenicity, patients' cells were stimulated in vitro with autologous peptides, and intracellular IL-2, TNF, and interferon-gamma (IFN-γ) production were measured in CD4 + and CD8 + T-cells., Results: The protocol of ex-vivo treatment with IFN-α and GM-CSF was able to induce maturation of MDDCs, as well as to preserve their viability for reinfusion. MDDCT administration was associated with increased expression of IL-2 in CD4 + and CD8 + T-cells at 15 and/or 30 days after the first MDDCT administration. Moreover, intracellular TNF and IFN-γ expression was significantly increased in CD4 + T-cells. The number of candidates that increased in vitro the cytokine levels in CD4 + and CD8 + T cells upon stimulation with Gag peptides from baseline to day 15 and from baseline to day 30 and day 120 after MDDCT was significant as compared to Gag unstimulated response. This was accompanied by an increasing trend in the frequency of polyfunctional T-cells over time, which was visible when considering both cells expressing two and three out of the three cytokines examined., Conclusions: MDDC had a mature profile, and this MDDCT promoted in-vitro T-cell immune responses in HIV-infected patients undergoing long-term suppressive antiretroviral treatment. Trial registration NCT02961829: (Multi Interventional Study Exploring HIV-1 Residual Replication: a Step Towards HIV-1 Eradication and Sterilizing Cure, https://www.clinicaltrials.gov/ct2/show/NCT02961829 , posted November 11th, 2016)., (© 2021. The Author(s).)

Published
2022
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14. Corrigendum to "Nitazoxanide superiority to placebo to treat moderate COVID-19 - A Pilot prove of concept randomized double-blind clinical trial." [EClinicalMedicine 37 (2021) 100981].

Author

Blum VF, Cimerman S, Hunter JR, Tierno P, Lacerda A, Soeiro A, Cardoso F, Bellei NC, Maricato J, Mantovani N, Vassao M, Dias D, Galinskas J, Janini LMR, Santos-Oliveira JR, Da-Cruz AM, and Diaz RS

Abstract

[This corrects the article DOI: 10.1016/j.eclinm.2021.100981.]., (© 2021 The Authors.)

Published
2021
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15. Nitazoxanide superiority to placebo to treat moderate COVID-19 - A Pilot prove of concept randomized double-blind clinical trial.

Author

Blum VF, Cimerman S, Hunter JR, Tierno P, Lacerda A, Soeiro A, Cardoso F, Bellei NC, Maricato J, Mantovani N, Vassao M, Dias D, Galinskas J, Janini LMR, Santos-Oliveira JR, Da-Cruz AM, and Diaz RS

Abstract

Background: The absence of specific antivirals to treat COVID-19 leads to the repositioning of candidates' drugs. Nitazoxanide (NTZ) has a broad antiviral effect., Methods: This was a randomized, double-blind pilot clinical trial comparing NTZ 600 mg BID versus Placebo for seven days among 50 individuals (25 each arm) with SARS-COV-2 RT-PCR+ (PCR) that were hospitalized with mild respiratory insufficiency from May 20 th , 2020, to September 21 st , 2020 (ClinicalTrials.gov NCT04348409). Clinical and virologic endpoints and inflammatory biomarkers were evaluated. A five-point scale for disease severity (SSD) was used., Findings: Two patients died in the NTZ arm compared to 6 in the placebo arm ( p  = 0.564). NTZ was superior to placebo when considering SSD ( p  < 0001), the mean time for hospital discharge (6.6 vs. 14 days, p  = 0.021), and negative PCR at day 21 ( p  = 0.035), whereas the placebo group presented more adverse events ( p  = 0.04). Among adverse events likely related to the study drug, 14 were detected in the NTZ group and 22 in placebo ( p  = 0.24). Among the 30 adverse events unlikely related, 21 occurred in the placebo group ( p  = 0.04). A decrease from baseline was higher in the NTZ group for d-Dimer ( p  = 0.001), US-RCP ( p  < 0.002), TNF ( p  < 0.038), IL-6 ( p  < 0.001), IL-8 ( p  = 0.014), HLA DR. on CD4 + T lymphocytes ( p  < 0.05), CD38 in CD4 + and CD8 + T (both p  < 0.05), and CD38 and HLA-DR. on CD4+ ( p  < 0.01)., Interpretation: Compared to placebo in clinical and virologic outcomes and improvement of inflammatory outcomes, the superiority of NTZ warrants further investigation of this drug for moderate COVID-19 in larger clinical trials. A higher incidence of adverse events in the placebo arm might be attributed to COVID-19 related symptoms., Competing Interests: VB exerts activities of clinical research at FQM Farmoquímica, sponsor of the study. AL reports grants from FQM, during the conduct of the study; personal fees from Daiicho Sankyo Brasil, Pfizer, Mantecorp Indústria Química e Farmacêutica, Libs Farmacêutica, Sanofi-Aventis; grants, personal fees and non-financial support from Janssen Pharmaceutical; personal fees and non-financial support from Cristalia Produtos Químicos e Farmacêuticos; grants and personal fees from Eli Lilly; grants from H. Lundbeck A/S, Servier Laboratories, Hoffman-La Roche, Forum Pharmaceuticals, Biophytis, Ganentech, Cellavita, Celltrion (outside the submitted work). JG, DD, JH, and NM report personal fees from FMQ during the conduct of the study. SC reports grants from FQM during the conduct of the study; grants from MERCK SHARP & DOME, NOVARTIS, ROCHE, ABBVIE, GILEAD, and PFIZER (outside the submitted work). Other authors do not have any conflict of interest to declare., (© 2021 The Authors.)

Published
2021
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16. Evidence of genomic information and structural restrictions of HIV-1 PR and RT gene regions from individuals experiencing antiretroviral virologic failure.

Author

de Carvalho Lima EN, Lima RSA, Piqueira JRC, Sucupira MC, Camargo M, Galinskas J, and Diaz RS

Subjects
Drug Resistance, Viral genetics, Genome, Viral, HIV Infections virology, HIV Protease chemistry, HIV Reverse Transcriptase chemistry, HIV-1 enzymology, HIV-1 isolation & purification, Humans, Mutation, Treatment Failure, Anti-HIV Agents pharmacology, HIV Infections drug therapy, HIV Protease genetics, HIV Reverse Transcriptase genetics, HIV-1 genetics
Abstract

Objectives: This study analyzed Protease-PR and Reverse Transcriptase-RT HIV-1 genomic information entropy metrics among patients under antiretroviral virologic failure, according to the numbers of virologic failures or resistance mutations., Methods: For this purpose, we used genomic sequences from PR and RT of HIV-1 from a cohort of chronic patients followed up at São Paulo Hospital., Results: Informational entropy proportionally increases with the number of antiretroviral virologic failures in PR and RT (p < .001). Affected regions of PR were related to catalytic and structural functions, such as Fulcrum (K20) Flap (M46) and Cantilever (A71). In RT, this occurred at Fingers (E44) and Palm (K219). Informational entropy increases according to the number of resistance mutations in PR and RT (p < .001). Higher PR entropy was proportional to the resistance mutation numbers in Fulcrum (L10), Active site (L24) Flap (M46), Cantilever (L63) and near Interface (L90). In RT, they related to regions responsible for protein stability such as Fingers (T39) and Palm (L100)., Conclusions: The antiretroviral selective pressure affects HIV genomic informational entropy at the PR and RT regions, leading to the emergence of more unstable virions. Mapping the three-dimensional structure in these HIV-1 proteins is relevant to designing new antiretroviral targeting resistant strains., Competing Interests: Declaration of Competing Interest The authors have no declarations or conflicts of interest associated with this work., (Copyright © 2019 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2020
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17. Nicotinamide activates latent HIV-1 ex vivo in ART suppressed individuals, revealing higher potency than the association of two methyltransferase inhibitors, chaetocin and BIX01294.

Author

Samer S, Arif MS, Giron LB, Zukurov JPL, Hunter J, Santillo BT, Namiyama G, Galinskas J, Komninakis SV, Oshiro TM, Sucupira MC, Janini LM, and Diaz RS

Subjects
Adult, CD4-Positive T-Lymphocytes, Female, Gene Expression Regulation, Viral, Humans, Leukocytes, Mononuclear virology, Male, Middle Aged, Piperazines pharmacology, Viral Load drug effects, Viral Tropism drug effects, Virus Latency, Young Adult, Azepines pharmacology, HIV Infections virology, HIV-1 drug effects, Methyltransferases antagonists & inhibitors, Niacinamide pharmacology, Quinazolines pharmacology, Virus Activation drug effects
Abstract

Background: Latent HIV-1 is a major hurdle in obtaining HIV-1 sustained virological remission (SVR). Here we explored histone deacetylation inhibition property of nicotinamide (NAM; n=17) for the first time in comparison to a combination of methyltransferase inhibitors (MTIs; Chaetocin and BIX01294; n=25) to reactivate latent HIV ex vivo in CD8-depleted PBMCs from antiretroviral treated aviremic individuals., Results: NAM reactivated HIV-1 from 13/17 (76.4%) samples compared to 20/25 (80.0%) using MTIs with mean viral load (VLs) of 4.32 and 3.22 log 10 RNA copies/mL, respectively (p=0.004). Mean purging time after NAM and MTIs stimulation was 5.1 and 6.75 days, respectively (p=0.73). Viral purging in autologous cultures exhibited blunted HIV recovery with fluctuating VLs followed by a complete viral extinction when expanded in allogenic system. Electron microscopy from five supernatants revealed anomalous viral particles, with lack of complete viral genomes when characterized by ultradeep sequencing through metagenomics approach (n=4)., Conclusion: NAM alone was more potent HIV-1 activator than combination of MTIs, with potential of clinical use., (Copyright © 2020 Sociedade Brasileira de Infectologia. Published by Elsevier España, S.L.U. All rights reserved.)

Published
2020
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18. Potential impact of the antirheumatic agent auranofin on proviral HIV-1 DNA in individuals under intensified antiretroviral therapy: Results from a randomised clinical trial.

Author

Diaz RS, Shytaj IL, Giron LB, Obermaier B, Della Libera E Jr, Galinskas J, Dias D, Hunter J, Janini M, Gosuen G, Ferreira PA, Sucupira MC, Maricato J, Fackler O, Lusic M, and Savarino A

Subjects
Antiretroviral Therapy, Highly Active, CD4 Lymphocyte Count, DNA, Viral drug effects, DNA, Viral genetics, HIV Fusion Inhibitors therapeutic use, HIV Infections drug therapy, HIV Integrase Inhibitors therapeutic use, HIV-1 drug effects, Heterocyclic Compounds, 3-Ring therapeutic use, Humans, Maraviroc therapeutic use, Oxazines, Piperazines, Pyridones, Antirheumatic Agents therapeutic use, Auranofin therapeutic use, HIV-1 genetics, Proviruses drug effects, Proviruses genetics, Virus Latency drug effects
Abstract

Antiretroviral therapy (ART) is typically composed of a combination of three antiretroviral drugs and is the treatment of choice for people with human immunodeficiency virus type 1/acquired immune deficiency syndrome (HIV-1/AIDS). However, it is unable to impact on viral reservoirs, which harbour latent HIV-1 genomes that are able to reignite the infection upon treatment suspension. The aim of this study was to provide an estimate of the safety of the disease-modifying antirheumatic agent auranofin and its impact on the HIV-1 reservoir in humans under intensified ART. For this purpose, an interim analysis was conducted of three of the six arms of the NCT02961829 clinical trial (five patients each) with: no intervention, i.e. continuation of first-line ART; intensified ART (ART + dolutegravir and maraviroc); and intensified ART plus auranofin. Auranofin treatment was found to be well tolerated. No major adverse events were detected apart from a transient decrease in CD4 + T-cell counts at Weeks 8 and 12. Auranofin decreased total viral DNA in peripheral blood mononuclear cells compared with ART-only regimens at Week 20 (P = 0.036) and induced a decrease in integrated viral DNA as quantified by Alu PCR. Despite the limited number of patient-derived sequences available in this study, phylogenetic analyses of nef sequences support the idea that auranofin may impact on the viral reservoir. [ClinicalTrials.gov ID: NCT02961829]., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published
2019
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19. Impact of antiretroviral resistance and virological failure on HIV-1 informational entropy.

Author

Lima ENC, Piqueira JRC, Camargo M, Galinskas J, Sucupira MC, and Diaz RS

Subjects
Anti-Retroviral Agents administration & dosage, Brazil, CD4 Lymphocyte Count, Genetic Fitness, HIV Infections drug therapy, HIV-1 enzymology, HIV-1 genetics, Humans, Treatment Failure, Viral Load, Anti-Retroviral Agents pharmacology, Drug Resistance, Viral, HIV Infections virology, HIV Integrase genetics, HIV Protease genetics, HIV-1 drug effects, Mutation
Abstract

Objectives: The present study investigated the relationship between genomic variability and resistance of HIV-1 sequences in protease (PR) and reverse transcriptase (RT) regions of the pol gene. In addition, we analysed the resistance among 651 individuals presenting antiretroviral virological failure, from 2009 to 2011, in the state of São Paulo, Brazil., Methods: The genomic variability was quantified by using informational entropy methods and the relationship between resistance and replicative fitness, as inferred by the residual viral load and CD4+ T cell count., Results: The number of antiretroviral schemes is related to the number of resistance mutations in the HIV-1 PR (α = 0.2511, P = 0.0003, R2 = 0.8672) and the RT (α = 0.7892, P = 0.0001, R2 = 0.9141). Increased informational entropy rate is related to lower levels of HIV-1 viral loads (α = -0.0121, P = 0.0471, R2 = 0.7923), lower levels of CD4+ T cell counts (α = -0.0120, P = 0.0335, R2 = 0.8221) and a higher number of antiretroviral resistance-related mutations., Conclusions: Less organized HIV genomes as inferred by higher levels of informational entropy relate to less competent host immune systems, lower levels of HIV replication and HIV genetic evolution as a consequence of antiretroviral resistance.

Published
2018
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20. Pace of Coreceptor Tropism Switch in HIV-1-Infected Individuals after Recent Infection.

Author

Arif MS, Hunter J, Léda AR, Zukurov JPL, Samer S, Camargo M, Galinskas J, Kallás EG, Komninakis SV, Janini LM, Sucupira MC, and Diaz RS

Subjects
Adult, CD4 Lymphocyte Count, CD4-CD8 Ratio, Coinfection virology, False Positive Reactions, Female, HIV Infections virology, HIV-1 genetics, Humans, Male, Middle Aged, Viral Load immunology, Virus Attachment, Virus Internalization, Young Adult, GB virus C metabolism, HIV Infections transmission, HIV-1 metabolism, Receptors, CCR5 metabolism, Receptors, CXCR4 metabolism, Receptors, HIV metabolism, Viral Tropism physiology
Abstract

HIV-1 entry into target cells influences several aspects of HIV-1 pathogenesis, including viral tropism, HIV-1 transmission and disease progression, and response to entry inhibitors. The evolution from CCR5- to CXCR4-using strains in a given human host is still unpredictable. Here we analyzed timing and predictors for coreceptor evolution among recently HIV-1-infected individuals. Proviral DNA was longitudinally evaluated in 66 individuals using Geno2pheno [coreceptor] Demographics, viral load, CD4 + and CD8 + T cell counts, CCR5Δ32 polymorphisms, GB virus C (GBV-C) coinfection, and HLA profiles were also evaluated. Ultradeep sequencing was performed on initial samples from 11 selected individuals. A tropism switch from CCR5- to CXCR4-using strains was identified in 9/49 (18.4%) individuals. Only a low baseline false-positive rate (FPR) was found to be a significant tropism switch predictor. No minor CXCR4-using variants were identified in initial samples of 4 of 5 R5/non-R5 switchers. Logistic regression analysis showed that patients with an FPR of >40.6% at baseline presented a stable FPR over time whereas lower FPRs tend to progressively decay, leading to emergence of CXCR4-using strains, with a mean evolution time of 27.29 months (range, 8.90 to 64.62). An FPR threshold above 40.6% determined by logistic regression analysis may make it unnecessary to further determine tropism for prediction of disease progression related to emergence of X4 strains or use of CCR5 antagonists. The detection of variants with intermediate FPRs and progressive FPR decay over time not only strengthens the power of Geno2pheno in predicting HIV tropism but also indirectly confirms a continuous evolution from earlier R5 variants toward CXCR4-using strains. IMPORTANCE The introduction of CCR5 antagonists in the antiretroviral arsenal has sparked interest in coreceptors utilized by HIV-1. Despite concentrated efforts, viral and human host features predicting tropism switch are still poorly understood. Limited longitudinal data are available to assess the influence that these factors have on predicting tropism switch and disease progression. The present study describes longitudinal tropism evolution in a group of recently HIV-infected individuals to determine the prevalence and potential correlates of tropism switch. We demonstrated here that a low baseline FPR determined by the Geno2pheno [coreceptor] algorithm can predict tropism evolution from CCR5 to CXCR4 coreceptor use., (Copyright © 2017 American Society for Microbiology.)

Published
2017
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21. High prevalence and incidence of HIV-1 in a counseling and testing center in the city of Itajaí, Brazil.

Author

Grinberg G, Giron LB, Knoll RK, Galinskas J, Camargo M, Arif MS, Samer S, Janini LM, Sucupira MC, and Diaz RS

Subjects
Adolescent, Adult, Age Distribution, Aged, Brazil epidemiology, Child, Child, Preschool, Female, Genotype, HIV-1, Humans, Incidence, Infant, Male, Middle Aged, Prevalence, Retrospective Studies, Sex Distribution, Counseling statistics & numerical data, HIV Infections epidemiology
Abstract

Itajaí is a port city in southern Brazil with one of the highest incidence and mortality rates from AIDS in the country. The prevalence and incidence of HIV infection were investigated in 1085 of 3196 new HIV-1 infection cases evaluated in the counseling and testing center of Itajaí from January 2002 to August 2008. Recent infections were assessed using the BED™, and pol region sequencing was performed in 76 samples. The prevalence ranged from 3.08% to 6.17% among women and from 10.26% to 17.36% among men. A total of 17% of infections were classified as recent, with annual incidence varying from 1.6% to 4.8 per 100 patient/year among women and from 2.05% to 8.5 per 100 patient/year among men. Pol sequences were obtained from 38 randomly recent infections selected individuals: 71% were infected by subtype C, 24% B, 2% D, and 2% F1. Among 38 subjects with established infection, 76% were subtype C, and 24% B. Transmitted drug resistance was detected in 18.4% of recent infection subjects (7.8% to nucleoside analog reverse-transcriptase inhibitors, 5.2% to non-nucleoside reverse-transcriptase inhibitors, and 5.2% protease inhibitors) and 5.2% of subjects with established infection had nucleoside analog reverse-transcriptase inhibitors resistance. The high prevalence and incidence of HIV infection in this region is unprecedented in studies involving cases evaluated in the counseling and testing centers in Brazil., (Copyright © 2015 Elsevier Editora Ltda. All rights reserved.)

Published
2015
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