Your search keyword '"Fabiola Di Santo"' showing total 10 results

1. Inhibition of dual/mixed tropic HIV-1 isolates by CCR5-inhibitors in primary lymphocytes and macrophages.

Author

Matteo Surdo, Emanuela Balestra, Patrizia Saccomandi, Fabiola Di Santo, Marco Montano, Domenico Di Carlo, Loredana Sarmati, Stefano Aquaro, Massimo Andreoni, Valentina Svicher, Carlo Federico Perno, and Francesca Ceccherini-Silberstein

Subjects

Medicine, Science

Abstract

BackgroundDual/mixed-tropic HIV-1 strains are predominant in a significant proportion of patients, though little information is available regarding their replication-capacity and susceptibility against CCR5-antagonists in-vitro. The aim of the study was to analyze the replication-capacity and susceptibility to maraviroc of HIV-1 clinical isolates with different tropism characteristics in primary monocyte-derived-macrophages (MDM), peripheral-blood-mononuclear-cells (PBMC), and CD4(+) T-lymphocytes.MethodsTwenty-three HIV-1 isolates were phenotipically and genotipically characterized as R5, X4 or dual (discriminated as R5(+)/X4, R5/X4, R5/X4(+)). Phenotypic-tropism was evaluated by multiple-cycles-assay on U87MG-CD4(+)-CCR5(+)-/CXCR4(+)-expressing cells. Genotypic-tropism prediction was obtained using Geno2Pheno-algorithm (false-positive-rate [FPR] = 10%). Replication-capacity and susceptibility to maraviroc were investigated in human-primary MDM, PBMC and CD4(+) T-cells. AMD3100 was used as CXCR4-inhibitor. Infectivity of R5/Dual/X4-viruses in presence/absence of maraviroc was assessed also by total HIV-DNA, quantified by real-time polymerase-chain-reaction.ResultsAmong 23 HIV-1 clinical isolates, phenotypic-tropism-assay distinguished 4, 17 and 2 viruses with R5-tropic, dual/mixed-, and X4-tropic characteristics, respectively. Overall, viruses defined as R5(+)/X4-tropic were found with the highest prevalence (10/23, 43.5%). The majority of isolates efficiently replicated in both PBMC and CD4(+) T-cells, regardless of their tropism, while MDM mainly sustained replication of R5- or R5(+)/X4-tropic isolates; strong correlation between viral-replication and genotypic-FPR-values was observed in MDM (rho = 0.710;p-value = 1.4e-4). In all primary cells, maraviroc inhibited viral-replication of isolates not only with pure R5- but also with dual/mixed tropism (mainly R5(+)/X4 and, to a lesser extent R5/X4 and R5/X4(+)). Finally, no main differences by comparing the total HIV-DNA with the p24-production in presence/absence of maraviroc were found.ConclusionsMaraviroc is effective in-vitro against viruses with dual-characteristics in both MDM and lymphocytes, despite the potential X4-mediated escape. This suggests that the concept of HIV-entry through one of the two coreceptors "separately" may require revision, and that the use of CCR5-antagonists in patients with dual/mixed-tropic viruses may be a therapeutic-option that deserves further investigations in different clinical settings.

Published

2013

2. The HIV-1 reverse transcriptase polymorphism A98S improves the response to tenofovir disoproxil fumarate + emtricitabine-containing HAART both in vivo and in vitro

Author

Valentina Svicher, Fabio Continenza, Ada Bertoli, Isabella Romeo, Fabiola Di Santo, Enrico Girardi, Nicola Petrosillo, Nicoletta Orchi, Matteo Surdo, Carmela Pinnetti, Carlo Federico Perno, Massimo Andreoni, Giuseppina Liuzzi, Massimo Giuliani, Alessandra Latini, Maria Mercedes Santoro, Valentina Fedele, Claudia Alteri, Antonella d'Arminio Monforte, Anna Artese, Lucia Parrotta, Giosuè Costa, Velia Chiara Di Maio, Andrea Antinori, Francesca Ceccherini-Silberstein, Stefano Alcaro, Stefania Carta, Rita Bellagamba, and Caterina Gori

Subjects

Adult, Male, 0301 basic medicine, Microbiology (medical), HAART, Anti-HIV Agents, Immunology, Docking analysis, HIV-1, Reverse transcriptase, Virological success, HIV Infections, Pharmacology, Emtricitabine, Microbiology, Peripheral blood mononuclear cell, Virus, 03 medical and health sciences, In vivo, Antiretroviral Therapy, Highly Active, Humans, Immunology and Allergy, Medicine, Potency, Tenofovir, Polymorphism, Genetic, business.industry, virus diseases, Middle Aged, Settore MED/07 - Microbiologia e Microbiologia Clinica, Resistance mutation, 030112 virology, Virology, HIV Reverse Transcriptase, In vitro, 030104 developmental biology, Female, business, medicine.drug

Abstract

The impact of baseline HIV-1 reverse transcriptase (RT) polymorphisms on response to first-line modern HAART containing tenofovir disoproxil fumarate (TDF) and emtricitabine (FTC) was evaluated. The impact of each RT polymorphism on virological success (VS) was evaluated in 604 HIV-1 subtype B-infected patients starting TDF+FTC-containing HAART. TDF and FTC antiviral activity was also tested in PBMCs infected by mutagenised HIV. Structural analysis based on docking simulations was performed. A98S was the only mutation significantly correlated with an increased proportion of patients achieving VS at 24 weeks (94.0% vs. 84.3%; P=0.03). Multivariate regression and Cox model analyses confirmed this result. At concentrations close to the minimal concentration achieved in patient plasma, TDF and FTC exhibited higher potency in the presence of A98S-mutated virus compared with wild-type (IC90,TDF, 8.6±1.1 vs. 19.3±3.5nM; and IC90,FTC, 12.4±7.7 vs. 16.8±9.8nM, respectively). The efficacy of FTC, abrogated by M184V, was partially restored by A98S (IC90,FTC, 5169±5931nM for A98S+M184V vs. 18477±12478nM for M184V alone). Docking analysis showed the higher potency of TDF and FTC in the presence of A98S-mutated virus was mainly due to higher binding affinity between drugs and mutated RT compared with wild-type. In the presence of FTC, A98S also partially restored the RT binding affinity impaired by M184V alone. A98S polymorphism improves virological response to TDF+FTC-containing HAART. This may help clinicians in the choice of the optimal NRTI backbone aimed at achieving maximal virological inhibition.

Published

2016

3. Different kinetics of viral replication and DNA integration in the main HIV-1 cellular reservoirs in the presence and absence of integrase inhibitors

Author

Francesca Ceccherini-Silberstein, Stefano Aquaro, Carlo Federico Perno, Chiara Orlandi, Matteo Surdo, Fabiola Di Santo, Mauro Magnani, Maria Francesca Cortese, and Anna Casabianca

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, Cell type, 2-LTR, Virus Integration, Proviral HIV-DNA, 030106 microbiology, HIV Core Protein p24, Integrase inhibitor, Virus Replication, Peripheral blood mononuclear cell, 03 medical and health sciences, chemistry.chemical_compound, CD4(+) T-cells, HIV-1 reservoir, Integrase inhibitors, Macrophages, Virology, medicine, Humans, HIV Integrase Inhibitors, DNA Integration, Cells, Cultured, Pharmacology, virus diseases, Settore MED/07 - Microbiologia e Microbiologia Clinica, Raltegravir, In vitro, 030104 developmental biology, chemistry, Viral replication, DNA, Viral, Dolutegravir, HIV-1, medicine.drug

Abstract

To compare the kinetics of integration, p24 production and equilibrium of the different HIV-DNA forms in human primary cells in the presence/absence of integrase-inhibitors (INIs) in vitro. Monocyte-derived-macrophages (MDMs), CD4+ T-cells and peripheral blood mononuclear cells (PBMCs) were infected with HIV-1 in the presence/absence of raltegravir and dolutegravir. HIV-DNA levels and p24 production were measured by qPCR and ELISA assays, respectively. In the absence of INIs, levels of HIV-DNA forms were initially very low, with an increase in the integration process starting at 3 dpi. HIV-DNA increased more slowly in MDMs than it did in CD4+ T-cells and PMBCs peaking at 21 dpi with a mean of 1580 (±890) and 615 (±37) copies/103 cells for proviral and unintegrated HIV-DNA, and 455,972 (±213,255) pg/mL of p24 at the same time point. In CD4+ T-cells the proviral HIV-DNA increased together with unintegrated HIV-DNA peaking at 7 dpi (583 ± 261 and 338 ± 254 copies/103 cells) when the p24 was 218,000 (±75,600) pg/mL. A similar trend was observed in PBMCs (494 ± 361 and 350 ± 123 copies/103 cells for proviral and unintegrated HIV-DNA, and p24 production of 149,400 ± 131,800 pg/mL). Both INIs inhibited viral replication and integration in all the cell types that were tested, especially starting at 3 dpi. However, a small but measurable amount of HIV-DNA ( In conclusion, our study showed differences in HIV-DNA kinetic integration between CD4+ T-cells and MDMs, which could explain the divergent kinetics of viral-replication. Both INIs inhibited HIV-1 integration and replication with no difference found between CD4+ T-cells and MDMs. However, residual HIV-DNA remained detectable up to 30 dpi in INI-treated MDMs although complete inhibition of HIV replication was achieved. The clinical significance of this minor DNA persistence deserves further investigation considering the role of macrophages as reservoirs.

Published

2018

4. Incomplete APOBEC3G/F Neutralization by HIV-1 Vif Mutants Facilitates the Genetic Evolution from CCR5 to CXCR4 Usage

Author

Valentina Svicher, Carlo Federico Perno, Valentina Fedele, Fabio Continenza, Maria Concetta Bellocchi, Daniele Armenia, Fabiola Di Santo, Patrizia Saccomandi, Anne-Geneviève Marcelin, Slim Fourati, Lucia Parrotta, Giosuè Costa, Emanuela Balestra, Claudia Alteri, Francesca Ceccherini-Silberstein, Vincent Calvez, Silvia Barbaliscia, Rossana Scutari, Anna Artese, Stefano Alcaro, Stefania Carta, L. Carioti, and Matteo Surdo

Subjects

Nonsynonymous substitution, Receptors, CXCR4, Receptors, CCR5, viruses, Mutant, HIV Infections, V3 loop, Biology, medicine.disease_cause, Antiviral Agents, Neutralization, Virus, Cell Line, Cytosine Deaminase, Evolution, Molecular, Cytidine Deaminase, medicine, Humans, Pharmacology (medical), APOBEC Deaminases, Amino Acid Sequence, APOBEC3G, Pharmacology, chemistry.chemical_classification, Mutation, Base Sequence, virus diseases, Settore MED/07 - Microbiologia e Microbiologia Clinica, Virology, Amino acid, HEK293 Cells, Infectious Diseases, Amino Acid Substitution, chemistry, HIV-1, Leukocytes, Mononuclear

Abstract

Incomplete APOBEC3G/F neutralization by a defective HIV-1Vif protein can promote genetic diversification by inducing G-to-A mutations in the HIV-1 genome. The HIV-1 Env V3 loop, critical for coreceptor usage, contains several putative APOBEC3G/F target sites. Here, we determined if APOBEC3G/F, in the presence of Vif-defective HIV-1 virus, can induce G-to-A mutations at V3 positions critical to modulation of CXCR4 usage. Peripheral blood mononuclear cells (PBMC) and monocyte-derived macrophages (MDM) from 2 HIV-1-negative donors were infected with CCR5-using 81.A-Vif WT virus (i.e., with wild-type [WT] Vif protein), 81.A-Vif E45G , or 81.A-Vif K22E (known to incompletely/partially neutralize APOBEC3G/F). The rate of G-toA mutations was zero or extremely low in 81.A-Vif WT - and 81.A-Vif E45G -infected PBMC from both donors. Conversely, G-to-A enrichment was detected in 81.A-Vif K22E -infected PBMC (prevalence ranging from 2.18% at 7 days postinfection [dpi] to 3.07% at 21 dpi in donor 1 and from 10.49% at 7 dpi to 8.69% at 21 dpi in donor 2). A similar scenario was found in MDM. G-to-A mutations occurred at 8 V3 positions, resulting in nonsynonymous amino acid substitutions. Of them, G24E and E25K strongly correlated with phenotypically/genotypically defined CXCR4-using viruses ( P = 0.04 and 5.5e−7, respectively) and increased the CXCR4 N-terminal binding affinity for V3 (WT, −40.1 kcal/mol; G24E, −510 kcal/mol; E25K, −522 kcal/mol). The analysis of paired V3 and Vif DNA sequences from 84 HIV-1-infected patients showed that the presence of a Vif-defective virus correlated with CXCR4 usage in proviral DNA ( P = 0.04). In conclusion, incomplete APOBEC3G/F neutralization by a single Vif amino acid substitution seeds a CXCR4-using proviral reservoir. This can have implications for the success of CCR5 antagonist-based therapy, as well as for the risk of disease progression.

Published

2015

5. Comparative antiviral activity of integrase inhibitors in human monocyte-derived macrophages and lymphocytes

Author

Matteo Surdo, Carlo Federico Perno, Fabiola Di Santo, Francesca Ceccherini-Silberstein, Michela Pollicita, Fernanda Scopelliti, and Stefano Aquaro

Subjects

HIV, integrase inhibitors, macrophages, PBMC, lymphocytes, Cell type, Human immunodeficiency virus (HIV), HIV Core Protein p24, Integrase inhibitor, Apoptosis, Microbial Sensitivity Tests, Biology, Pharmacology, medicine.disease_cause, Peripheral blood mononuclear cell, 03 medical and health sciences, Virology, medicine, Humans, HIV Integrase Inhibitors, Inhibitory effect, Cells, Cultured, 030304 developmental biology, 0303 health sciences, 030306 microbiology, Raltegravir, Settore MED/07 - Microbiologia e Microbiologia Clinica, 3. Good health, Monocyte-Derived Macrophages, HIV-1, medicine.drug

Abstract

The activity of raltegravir and 4 other integrase inhibitors (MK-2048, L870,810, IN2, and IN5) was investigated in primary human macrophages, PBMC and C8166-lymphocytic T cells, in order to determine their relative potency and efficacy in different cellular systems of HIV infection. Raltegravir showed better protective efficacy in all cell types; MK-2048, L870,810 and IN5 showed a potent anti-HIV-1 activity in macrophages, while in lymphocytes only MK-2048 and L870,810 showed an inhibitory effect comparable to raltegravir. IN2 was a poorly effective anti-HIV-1 compound in all cellular systems. All effective integrase inhibitors exhibited a potent antiviral activity against both X4 and R5 HIV-1 strains. In general, raltegravir, MK-2048, L870,810 and IN5 showed anti HIV activity similar or slightly higher in macrophages compared to PBMC and C8166 T cells: for MK-2048, the EC(50) was 0.4, 0.9, 11.5 nM in macrophages, in PBMCs and T cells, respectively; for L870,810, the EC(50) was 1.5, 14.3, and 10.6 nM, respectively; for IN5 the EC(50) was 0.5, 13.7, and 5.7 nM, respectively.

Published

2011

6. Hepatitis B surface antigen genetic elements critical for immune escape correlate with hepatitis B virus reactivation upon immunosuppression

Author

Matteo Surdo, L. Carioti, Maria Concetta Bellocchi, Valentina Svicher, Claudio Maria Mastroianni, M. Paoloni, Claudia Alteri, L. Colagrossi, Yoram Louzoun, Romina Salpini, Mariarosaria Esposito, Michela Pollicita, Carlo Federico Perno, Loredana Sarmati, Massimo Andreoni, Mario Angelico, Massimo Marignani, Cesare Sarrecchia, Chiara D'Amore, Marianna Aragri, Christina Becker, Fabiola Di Santo, Aldo Marrone, Miriam Lichtner, A. Ricciardi, Daniele Armenia, Jens Verheyen, Salpini, R, Colagrossi, L, Bellocchi, Mc, Surdo, M, Becker, C, Alteri, C, Aragri, M, Ricciardi, A, Armenia, D, Pollicita, M, Di Santo, F, Carioti, L, Louzoun, Y, Mastroianni, Cm, Lichtner, M, Paoloni, M, Esposito, M, D'Amore, C, Marrone, A, Marignani, M, Sarrecchia, C, Sarmati, L, Andreoni, M, Angelico, M, Verheyen, J, Perno, Cf, Svicher, V, Marrone, Aldo, Verhejen, J, and Svicher, V.

Subjects

Male, HBsAg, Glycosylation, medicine.medical_treatment, Medizin, medicine.disease_cause, genetic variability, HBV, education.field_of_study, immunosuppression, biology, virus diseases, Immunosuppression, surface antigen, Hepatitis B, Middle Aged, Settore MED/07 - Microbiologia e Microbiologia Clinica, Rituximab, Female, Antibody, medicine.drug, Adult, medicine.medical_specialty, Hepatitis B virus, Settore MED/17 - Malattie Infettive, Population, Hepatitis B, Chronic, Internal medicine, Drug Resistance, Viral, medicine, Humans, Hepatitis B Antibodies, education, Aged, Immune Evasion, Immunosuppression Therapy, Hepatitis B Surface Antigens, Hepatology, business.industry, medicine.disease, Virology, digestive system diseases, Immunology, Mutation, biology.protein, Virus Activation, business

Abstract

Hepatitis B virus (HBV) reactivation during immunosuppression can lead to severe acute hepatitis, fulminant liver failure, and death. Here, we investigated hepatitis B surface antigen (HBsAg) genetic features underlying this phenomenon by analyzing 93 patients: 29 developing HBV reactivation and 64 consecutive patients with chronic HBV infection (as control). HBsAg genetic diversity was analyzed by population-based and ultradeep sequencing (UDS). Before HBV reactivation, 51.7% of patients were isolated hepatitis B core antibody (anti-HBc) positive, 31.0% inactive carriers, 6.9% anti-HBc/anti-HBs (hepatitis B surface antibody) positive, 6.9% isolated anti-HBs positive, and 3.4% had an overt HBV infection. Of HBV-reactivated patients, 51.7% were treated with rituximab, 34.5% with different chemotherapeutics, and 13.8% with corticosteroids only for inflammatory diseases. In total, 75.9% of HBV-reactivated patients (vs. 3.1% of control patients; P

Published

2015

7. HBsAg genetic elements critical for immune escape correlate with HBV-reactivation upon immunosuppression

Author

Romina, Salpini, Luna, Colagrossi, Maria Concetta Bellocchi, Matteo, Surdo, Christina, Becker, Claudia, Alteri, Marianna, Aragri, Alessandra, Ricciardi, Daniele, Armenia, Michela, Pollicita, Fabiola Di Santo, Luca, Carioti, Yoram, Louzoun, Mastroianni, Claudio Maria, Lichtner, Miriam, Maurizio, Paoloni, Mariarosaria, Esposito, Chiara, D'Amore, Aldo, Marrone, Massimo, Marignani, Cesare, Sarrecchia, Loredana, Sarmati, Massimo, Andreoni, Mario, Angelico, Jens, Verhejen, Carlo Federico Perno, and Valentina, Svicher

Subjects

virus reactivation, hepatitis b virus, hepatitis b

Published

2015

8. Comparative replication capacity of raltegravir-resistant strains and antiviral activity of the new-generation integrase inhibitor dolutegravir in human primary macrophages and lymphocytes

Author

Fabiola Di Santo, Anne-Geneviève Marcelin, Maria Francesca Cortese, Isabelle Malet, Carlo Federico Perno, Michela Pollicita, Valentina Svicher, Vincent Calvez, Lavinia Fabeni, Valentina Fedele, Matteo Surdo, and Francesca Ceccherini-Silberstein

Subjects

Microbiology (medical), Pyridones, Cells, Lymphocyte, Mutant, Drug Resistance, Integrase inhibitor, primary cells, HIV Integrase, Microbial Sensitivity Tests, 3-Ring, Virus Replication, Peripheral blood mononuclear cell, Piperazines, chemistry.chemical_compound, Heterocyclic Compounds, Raltegravir Potassium, Drug Resistance, Viral, Oxazines, medicine, Potency, Humans, Pharmacology (medical), Viral, HIV Integrase Inhibitors, Lymphocytes, Cells, Cultured, Pharmacology, Cultured, Chemistry, Macrophages, HIV infection, inhibition of viral replication, HIV-1, Heterocyclic Compounds, 3-Ring, Mutant Proteins, Pyrrolidinones, Settore MED/07 - Microbiologia e Microbiologia Clinica, Raltegravir, Virology, Infectious Diseases, medicine.anatomical_structure, Viral replication, Dolutegravir, medicine.drug

Abstract

Objectives To evaluate the replication capacity and phenotypic susceptibility to dolutegravir and raltegravir of wild-type and raltegravir-resistant HIV-1 strains in several cellular systems. Methods The antiviral activities of dolutegravir and raltegravir were evaluated in human primary monocyte-derived macrophages (MDMs), peripheral blood mononuclear cells (PBMCs) and C8166 T lymphocytic cells. The following raltegravir resistance mutations were analysed: N155H, Y143C, N155H + Y143C and G140S+Q148H. Results In the absence of drug, the replication capacity of raltegravir-resistant viruses was strongly reduced compared with wild-type in all cellular models analysed. In MDMs and PBMCs, a dramatic decrease in viral replication was observed for the double mutants N155H + Y143C and G140S + Q148H (ranging from 0.1% to 2.5% compared with wild-type). In MDMs, dolutegravir exhibited high potency, with EC50 and EC90 values of 1.1 ± 0.9 and 5.5 ± 3.4 nM, respectively (comparable to raltegravir). These values (particularly for EC90) were significantly lower than those observed in PBMCs (EC50: 2.7 ± 1.5 nM; EC90: 14.8 ± 0.9 nM) and C8166 cells (EC50: 5.5 ± 0.8 nM; EC90: 64.8 ± 5.8 nM). In all cellular models analysed, dolutegravir showed full efficacy against N155H and Y143C mutants (dolutegravir fold-change resistance ranging from 0.1 to 1.4; raltegravir fold-change resistance ranging from 0.1 to 10.3). In C8166 (the only cell model in which replication capacity was sufficient to perform the test) dolutegravir showed full efficacy against mutations N155H + Y143C (dolutegravir fold-change resistance: 0.6) and a slightly lower activity against G140S+Q148H (dolutegravir fold-change resistance: 2.1). Conclusions Dolutegravir is effective in different HIV cellular targets and against raltegravir-resistant mutants. The high efficacy of dolutegravir in MDMs (cells with limited metabolism) has relevant clinical implications in light of the role of MDMs in the transmission of HIV infection and dissemination in different body compartments.

Published

2014

9. Potent antiviral activity of amprenavir in primary macrophages infected by human immunodeficiency virus

Author

Raffaele Caliò, Francesconi M, Stefano Aquaro, Fabiola Di Santo, Carlo Federico Perno, and Tania Guenci

Subjects

HAART, CD4-lymphocytes, HIV Infections, In Vitro Techniques, Virus Replication, Virus, Protease inhibitors, Reservoirs, Therapy, Amprenavir, Antigen, Virology, medicine, Humans, Protease inhibitor (pharmacology), Furans, Pharmacology, Sulfonamides, biology, Macrophages, virus diseases, Biological activity, HIV Protease Inhibitors, Settore MED/07 - Microbiologia e Microbiologia Clinica, biology.organism_classification, In vitro, Enzyme inhibitor, Lentivirus, biology.protein, HIV-1, Carbamates, medicine.drug

Abstract

Objective of the present study was then to assess the antiviral activity of the protease inhibitor amprenavir in macrophages (M/M), and to compare it with its efficacy in peripheral blood lymphocytes (PBL). M/M were obtained from blood of sero-negative healthy donors and infected with M-tropic HIV-1 strain (HIV-1(Ba-L)). The stabilized infection was assessed by monitoring the HIV-1 p24 gag antigen production in the supernatants of M/M cultures. In the setting of acute infection (treatment before HIV-1 challenge), amprenavir showed substantial activity both in M/M and PBL at similar concentrations (EC(50): 0.011 and 0.031 microM, respectively); complete inhibition of HIV-1 replication was achieved in both cell types at concentration of about 2 microM. In the setting of chronical infection (i.e. antiviral treatment several days after established infection), an antiviral effect of amprenavir was achieved in M/M, but at concentrations higher than those active in acutely infected M/M (EC(50): 0.72 microM, EC(90): 18.2 microM). The antiviral effect in chronically infected M/M was sustained for at least 2 weeks of continuous treatment. These findings suggest that amprenavir (at relatively high concentrations) has a clinically relevant antiviral effect in persistently infected reservoirs of HIV.

Published

2003

10. Inhibition of Dual/Mixed Tropic HIV-1 Isolates by CCR5-Inhibitors in Primary Lymphocytes and Macrophages

Author

Valentina Svicher, Carlo Federico Perno, Fabiola Di Santo, Domenico Di Carlo, Stefano Aquaro, Patrizia Saccomandi, Francesca Ceccherini-Silberstein, Massimo Andreoni, Matteo Surdo, Emanuela Balestra, Marco Montano, and Loredana Sarmati

Subjects

viruses, Virus Replication, CXCR4, chemistry.chemical_compound, Immunodeficiency Viruses, Genotype, Receptors, Leukocytes, Viral, Lymphocytes, Infectivity, 0303 health sciences, Multidisciplinary, Viral Replication Complex, virus diseases, Antivirals, Settore MED/07 - Microbiologia e Microbiologia Clinica, Viral Persistence and Latency, 3. Good health, AIDS, Phenotype, CCR5 Receptor Antagonists, Medicine, Infectious diseases, Viral Latency, Coreceptors, Research Article, Gene Expression Regulation, Viral, Receptors, CXCR4, Viral Entry, Infectious Disease Control, Anti-HIV Agents, Science, Mononuclear, Sexually Transmitted Diseases, Retrovirology and HIV immunopathogenesis, Viral diseases, CCR5 receptor antagonist, Biology, Microbiology, Cell Line, 03 medical and health sciences, Virology, Retroviruses, Viral Nucleic Acid, Humans, Tropism, 030304 developmental biology, Maraviroc, Macrophages, Leukocytes, Mononuclear, Viral Tropism, Receptors, CCR5, HIV-1, 030306 microbiology, Host Cells, HIV, Viral Replication, Viral Classification, Viral replication, chemistry, Gene Expression Regulation, Tissue tropism, CCR5, Viral Transmission and Infection

Abstract

BackgroundDual/mixed-tropic HIV-1 strains are predominant in a significant proportion of patients, though little information is available regarding their replication-capacity and susceptibility against CCR5-antagonists in-vitro. The aim of the study was to analyze the replication-capacity and susceptibility to maraviroc of HIV-1 clinical isolates with different tropism characteristics in primary monocyte-derived-macrophages (MDM), peripheral-blood-mononuclear-cells (PBMC), and CD4(+) T-lymphocytes.MethodsTwenty-three HIV-1 isolates were phenotipically and genotipically characterized as R5, X4 or dual (discriminated as R5(+)/X4, R5/X4, R5/X4(+)). Phenotypic-tropism was evaluated by multiple-cycles-assay on U87MG-CD4(+)-CCR5(+)-/CXCR4(+)-expressing cells. Genotypic-tropism prediction was obtained using Geno2Pheno-algorithm (false-positive-rate [FPR] = 10%). Replication-capacity and susceptibility to maraviroc were investigated in human-primary MDM, PBMC and CD4(+) T-cells. AMD3100 was used as CXCR4-inhibitor. Infectivity of R5/Dual/X4-viruses in presence/absence of maraviroc was assessed also by total HIV-DNA, quantified by real-time polymerase-chain-reaction.ResultsAmong 23 HIV-1 clinical isolates, phenotypic-tropism-assay distinguished 4, 17 and 2 viruses with R5-tropic, dual/mixed-, and X4-tropic characteristics, respectively. Overall, viruses defined as R5(+)/X4-tropic were found with the highest prevalence (10/23, 43.5%). The majority of isolates efficiently replicated in both PBMC and CD4(+) T-cells, regardless of their tropism, while MDM mainly sustained replication of R5- or R5(+)/X4-tropic isolates; strong correlation between viral-replication and genotypic-FPR-values was observed in MDM (rho = 0.710;p-value = 1.4e-4). In all primary cells, maraviroc inhibited viral-replication of isolates not only with pure R5- but also with dual/mixed tropism (mainly R5(+)/X4 and, to a lesser extent R5/X4 and R5/X4(+)). Finally, no main differences by comparing the total HIV-DNA with the p24-production in presence/absence of maraviroc were found.ConclusionsMaraviroc is effective in-vitro against viruses with dual-characteristics in both MDM and lymphocytes, despite the potential X4-mediated escape. This suggests that the concept of HIV-entry through one of the two coreceptors "separately" may require revision, and that the use of CCR5-antagonists in patients with dual/mixed-tropic viruses may be a therapeutic-option that deserves further investigations in different clinical settings.

Published

2013