17 results on '"Lara-Aguilar, Violeta"'
Search Results
2. Development and validation of a new and rapid molecular diagnostic tool based on RT-LAMP for Hepatitis C virus detection at point-of-care
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Arca-Lafuente, Sonia, Yépez-Notario, Cristina, Cea-Callejo, Pablo, Lara-Aguilar, Violeta, Crespo-Bermejo, Celia, Martín-Carbonero, Luz, de los Santos, Ignacio, Briz, Verónica, and Madrid, Ricardo
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- 2024
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3. Dynamics of cellular senescence markers after HCV elimination spontaneously or by DAAs in people living with HIV
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Lara-Aguilar, Violeta, Valle-Millares, Daniel, Crespo-Bermejo, Celia, Grande-García, Sergio, Llamas-Adán, Manuel, Cortijo-Alfonso, María Engracia, Martín-Carbonero, Luz, Domínguez, Lourdes, Ryan, Pablo, de los Santos, Ignacio, Bartolomé-Sánchez, Sofía, Vidal-Alcántara, Erick Joan, Jiménez-Sousa, María Angeles, Fernández-Rodríguez, Amanda, and Briz, Verónica
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- 2023
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4. 903 Protein Saver cards: the best alternative for dried blood spot storage at room temperature for HCV RNA
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Arca-Lafuente, Sonia, Casanueva-Benítez, Cristina, Crespo-Bermejo, Celia, Lara-Aguilar, Violeta, Martín-Carbonero, Luz, de los Santos, Ignacio, Madrid, Ricardo, and Briz, Verónica
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- 2022
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5. Changes in the senescence profile and immune checkpoints in HIV-infected individuals after COVID-19
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Crespo-Bermejo, Celia, primary, Brochado-Kith, Oscar, additional, Grande-Garcia, Sergio, additional, Lara-Aguilar, Violeta, additional, Llamas-Adan, Manuel, additional, Arca-Lafuente, Sonia, additional, Martin-Carbonero, Luz, additional, de los Santos, Ignacio, additional, Jimenez Sousa, M Angeles, additional, Resino, Salvador, additional, Berenguer, Juan, additional, Madrid, Ricardo, additional, Fernandez-Rodriguez, Amanda, additional, and Briz, Veronica, additional
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- 2024
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6. Dynamics of HIV Reservoir and HIV-1 Viral Splicing in HCV-Exposed Individuals after Elimination with DAAs or Spontaneous Clearance
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Instituto de Salud Carlos III, European Commission, National Institutes of Health (US), Fundação para a Ciência e a Tecnologia (Portugal), Lara-Aguilar, Violeta [0000-0003-0015-5961], Martín-Carbonero, Luz [0000-0001-8102-4079], Ryan, Pablo [0000-0002-4212-7419], De Los Santos, Ignacio [0000-0001-7073-5211], Fernández-Rodríguez, Amanda [0000-0002-5110-2213], Briz, Verónica [0000-0003-2297-5098], Martínez-Román, Paula, Crespo-Bermejo, Celia, Valle-Millares, Daniel, Lara-Aguilar, Violeta, Arca-Lafuente, Sonia, Martín-Carbonero, Luz, Ryan, Pablo, De Los Santos, Ignacio, López-Huertas, María Rosa, Palladino, Claudia, Muñoz Muñoz, María, Fernández-Rodríguez, Amanda, Coiras, Mayte, Briz, Verónica, Instituto de Salud Carlos III, European Commission, National Institutes of Health (US), Fundação para a Ciência e a Tecnologia (Portugal), Lara-Aguilar, Violeta [0000-0003-0015-5961], Martín-Carbonero, Luz [0000-0001-8102-4079], Ryan, Pablo [0000-0002-4212-7419], De Los Santos, Ignacio [0000-0001-7073-5211], Fernández-Rodríguez, Amanda [0000-0002-5110-2213], Briz, Verónica [0000-0003-2297-5098], Martínez-Román, Paula, Crespo-Bermejo, Celia, Valle-Millares, Daniel, Lara-Aguilar, Violeta, Arca-Lafuente, Sonia, Martín-Carbonero, Luz, Ryan, Pablo, De Los Santos, Ignacio, López-Huertas, María Rosa, Palladino, Claudia, Muñoz Muñoz, María, Fernández-Rodríguez, Amanda, Coiras, Mayte, and Briz, Verónica
- Abstract
Background: Although human immunodeficiency virus type 1 (HIV-1) reservoir size is very stable under antiretroviral therapy (ART), individuals exposed to the Hepatitis C virus (HCV) (chronically coinfected and spontaneous clarifiers) show an increase in HIV reservoir size and in spliced viral RNA, which could indicate that the viral protein regulator Tat is being more actively synthesized and, thus, could lead to a higher yield of new HIV. However, it is still unknown whether the effect of HCV elimination with direct-acting antivirals (DAAs) could modify the HIV reservoir and splicing. Methods: This longitudinal study (48 weeks’ follow-up after sustained virological response) involves 22 HIV+-monoinfected individuals, 17 HIV+/HCV- spontaneous clarifiers, and 24 HIV+/HCV+ chronically infected subjects who eliminated HCV with DAAs (all of them aviremic, viral load < 50). Viral-spliced RNA transcripts and proviral DNA copies were quantified by qPCR. Paired samples were analyzed using a mixed generalized linear model. Results: A decrease in HIV proviral DNA was observed in HIV+/HCV- subjects, but no significant differences were found for the other study groups. An increased production of multiple spliced transcripts was found in HIV+ and HIV+/HCV+ individuals. Conclusions: We conclude that elimination of HCV by DAAs was unable to revert the consequences derived from chronic HCV infection for the reservoir size and viral splicing, which could indicate an increased risk of rapid HIV-reservoir reactivation. Moreover, spontaneous clarifiers showed a significant decrease in the HIV reservoir, likely due to an enhanced immune response in these individuals.
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- 2022
7. Dynamics of HIV Reservoir and HIV-1 Viral Splicing in HCV-Exposed Individuals after Elimination with DAAs or Spontaneous Clearance
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Martinez-Roman, Paula, Crespo-Bermejo, Celia, Valle-Millares, Daniel, Lara-Aguilar, Violeta, Arca de Lafuente, Sonia, Martín-Carbonero, Luz, Ryan, Pablo, de Los Santos, Ignacio, Lopez-Huertas, Maria Rosa, Palladino, Claudia, Muñoz-Muñoz, María, Fernandez-Rodriguez, Amanda, Coiras, Mayte, Briz, Veronica, COVIHEP network, Instituto de Salud Carlos III, Red de Investigación Cooperativa en Investigación en Sida (España), Unión Europea. Fondo Europeo de Desarrollo Regional (FEDER/ERDF), Fundação para a Ciência e Tecnologia (Portugal), National Institutes of Health (Estados Unidos), European Commission, National Institutes of Health (US), Fundação para a Ciência e a Tecnologia (Portugal), Lara-Aguilar, Violeta, Martín-Carbonero, Luz, Ryan, Pablo, de Los Santos, Ignacio, Fernández-Rodríguez, Amanda, and Briz, Verónica
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HIV/HCV ,HIV reservoir ,viral splicing ,dynamics ,coinfection ,DAAs ,spontaneous HCV clearance ,Coinfection ,virus diseases ,Spontaneous HCV clearance ,Viral splicing ,General Medicine ,Dynamics - Abstract
15 Pág., Background: Although human immunodeficiency virus type 1 (HIV-1) reservoir size is very stable under antiretroviral therapy (ART), individuals exposed to the Hepatitis C virus (HCV) (chronically coinfected and spontaneous clarifiers) show an increase in HIV reservoir size and in spliced viral RNA, which could indicate that the viral protein regulator Tat is being more actively synthesized and, thus, could lead to a higher yield of new HIV. However, it is still unknown whether the effect of HCV elimination with direct-acting antivirals (DAAs) could modify the HIV reservoir and splicing. Methods: This longitudinal study (48 weeks’ follow-up after sustained virological response) involves 22 HIV+-monoinfected individuals, 17 HIV+/HCV- spontaneous clarifiers, and 24 HIV+/HCV+ chronically infected subjects who eliminated HCV with DAAs (all of them aviremic, viral load < 50). Viral-spliced RNA transcripts and proviral DNA copies were quantified by qPCR. Paired samples were analyzed using a mixed generalized linear model. Results: A decrease in HIV proviral DNA was observed in HIV+/HCV- subjects, but no significant differences were found for the other study groups. An increased production of multiple spliced transcripts was found in HIV+ and HIV+/HCV+ individuals. Conclusions: We conclude that elimination of HCV by DAAs was unable to revert the consequences derived from chronic HCV infection for the reservoir size and viral splicing, which could indicate an increased risk of rapid HIV-reservoir reactivation. Moreover, spontaneous clarifiers showed a significant decrease in the HIV reservoir, likely due to an enhanced immune response in these individuals., Financial support was provided by the Instituto de Salud Carlos III to V.B. and A.F.-R. (PI15CIII/00031 and PI18CIII/00020) and the SPANISH AIDS Research Network (RD16CIII/0002/0001 and RD16CIII/0002/0002—ISCIII—FEDER). A.F.-R. is supported by the Miguel Servet program from Fondo de Investigación Sanitaria (ISCIII) (CP14/CIII/00010). Financial support was provided by the National Institutes of Health (NIH) (Grant R01AI143567) for M.C. The work of M.R.L.-H. is financed by the NIH (Grant R01AI143567). C.P. is funded by FCT—Fundação para a Ciência e a Tecnologia, I.P. (national funding), under a contract program as defined by DL No. 57/2016 and Law No. 57/2017.
- Published
- 2022
8. HCV spontaneous clearers showed low senescence profile in people living with HIV
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Lara-Aguilar, Violeta, primary, Valle-Millares, Daniel, additional, Crespo-Bermejo, Celia, additional, Llamás-Adán, Manuel, additional, Grande-García, Sergio, additional, Cortijo-Alfonso, María Engracia, additional, Martín-Carbonero, Luz, additional, Domínguez, Lourdes, additional, Ryan, Pablo, additional, Santos, Ignacio de los, additional, Bartolomé-Sanchez, Sofía, additional, Briz, Verónica, additional, and Fernández-Rodríguez, Amanda, additional
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- 2023
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9. Dynamics of cellular senescence markers after HCV elimination in people living with HIV
- Author
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Lara-Aguilar, Violeta, primary, Valle-Millares, Daniel, additional, Crespo-Bermejo, Celia, additional, Grande-García, Sergio, additional, Llamás-Adán, Manuel, additional, Cortijo-Alfonso, María Engracia, additional, Martín-Carbonero, Luz, additional, Domínguez, Lourdes, additional, Ryan, Pablo, additional, Santos, Ignacio de los, additional, Bartolomé-Sanchez, Sofía, additional, Vidal-Alcantara, Erick Joan, additional, Fernández-Rodríguez, Amanda, additional, and Briz, Verónica, additional
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- 2023
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10. HCV spontaneous clearers showed low senescence profile in people living with HIV under long ART.
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Lara‐Aguilar, Violeta, Crespo‐Bermejo, Celia, Llamas‐Adán, Manuel, Grande‐García, Sergio, Cortijo‐Alfonso, María Engracia, Martín‐Carbonero, Luz, Domínguez, Lourdes, Ryan, Pablo, de los Santos, Ignacio, Bartolomé‐Sanchez, Sofía, Valle‐Millares, Daniel, Jiménez‐Sousa, María Ángeles, Briz, Verónica, and Fernández‐Rodríguez, Amanda
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HIV-positive persons ,STEM cell factor ,MACROPHAGE colony-stimulating factor ,GRANULOCYTE-colony stimulating factor ,PLACENTAL growth factor ,HIV status ,IMMUNOSENESCENCE - Abstract
Coinfection with hepatitis C virus (HCV) and human immunodeficiency virus (HIV) increases immune activation, inflammation, and oxidative stress that could lead to premature senescence. Different HCV infections, either acute or chronic infection, could lead to distinct premature cellular senescence in people living with HIV (PLWHIV). Observational study in 116 PLWHIV under antiretroviral treatment with different HCV status: (i) n = 45 chronically infected with HCV (CHC); (ii) n = 36 individuals who spontaneously clarify HCV (SC); (iii) n = 35 HIV controls. Oxidative stress biomarkers were analyzed at lipid, DNA, protein, and nitrates levels, as well as antioxidant capacity and glutathione reductase enzyme. Replicative senescence was evaluated by relative telomere length (RTL) measurement. Additionally, 26 markers of Senescence‐Associated Secretory Phenotype (SASP) were analyzed by multiplex immunoassays (Luminex xMAP technology). Differences were evaluated by generalized linear model (GLMs) adjusted by most significant covariates. The SC group had a senescence signature similar to the HIV control group and slightly lower SASP levels. However, significant differences were observed with respect to the CHC group, where an increase in the nitrate concentration [adjusted arithmetic mean ratio, aAMR = 1.73 (1.27–2.35), p < 0.001, q = 0.009] and the secretion of 13 SASP‐associated factors [granulocyte macrophage colony‐stimulating factor (GM‐CSF), interferon‐β, interleukin (IL)‐1β, IL‐2, IL‐8, IL‐13, tumor necrosis factor (TNF)‐α, IL‐1α, IL‐1RA, IL‐7, IL‐15, C‐X‐C motif chemokine ligand 10 (IP‐10), stem cell factor (SCF); q < 0.1)] was detected. The CHC group also showed higher values of IL‐1α, IP‐10, and placental growth factor 1 (PIGF‐1) than HIV controls. The SC group showed a slightly lower senescence profile than the HIV group, which could indicate a more efficient control of viral‐induced senescence due to their immune strengths. Chronic HCV infection in PLWHIV led to an increase in nitrate and elevated SASP biomarkers favoring the establishment of viral persistence. [ABSTRACT FROM AUTHOR]
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- 2023
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11. 903 Protein Saver cards: the best alternative for dried blood spot storage at room temperature for HCV RNA
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Madrid González, Ricardo, Arca‑Lafuente, Sonia, Casanueva‑Benítez, Cristina, Crespo‑Bermejo, Celia, Lara‑Aguilar, Violeta, Martín‑Carbonero, Luz, Santos, Ignacio de los, Briz, Verónica, Madrid González, Ricardo, Arca‑Lafuente, Sonia, Casanueva‑Benítez, Cristina, Crespo‑Bermejo, Celia, Lara‑Aguilar, Violeta, Martín‑Carbonero, Luz, Santos, Ignacio de los, and Briz, Verónica
- Abstract
Hepatitis C virus (HCV) infection remains a global health problem, detected only in the early stages by molecular tests. Molecular tests detect HCV RNA, which is very prone to degradation by ribonucleases, reason why blood samples must be transported and stored at − 20 °C, or even − 70 °C for long-term storage. Flinders Technology Associates (FTA) cards are a useful sampling collecting device for dry blood spot (DBS) storage, especially for low and middle-income countries (LMIC). In this study, we analyzed viral HCV RNA integrity for long-term storage at room temperature compared to − 20 °C using two diferent types of cards for DBS: FTA Classic and 903 Protein Saver cards. For this purpose, DBS were prepared on these cards using blood or plasma samples from HCV infected patients, and samples were analysed by conventional RT-PCR. Our results showed that 903 Protein Saver cards are the best and cheapest alternative for DBS storage at room temperature. In these conditions, we found that HCV RNA integrity lasted for up to 9 months., Comunidad de Madrid, Depto. de Genética, Fisiología y Microbiología, Fac. de Ciencias Biológicas, TRUE, pub
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- 2022
12. T cell maturation and senescence after HCV cure in HIV-HCV coinfected patients: a prospective study
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Martínez-Román, Paula, primary, Cortegano, Isabel, additional, Millares, Daniel Valle, additional, Crespo-Bermejo, Celia, additional, Rallón, Norma, additional, Benito, José Miguel, additional, Lara-Aguilar, Violeta, additional, Arca-Lafuente, Sonia, additional, Martín-Carbonero, Luz, additional, Domínguez-Domínguez, Lourdes, additional, Ryan, Pablo, additional, Santos, Ignacio de los, additional, Coiras, Mayte, additional, Palladino, Claudia, additional, Gaspar, María Luisa, additional, Fernández-Rodríguez, Amanda, additional, and Briz, Verónica, additional
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- 2022
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13. 903 Protein Saver cards: the best alternative for dried blood spot storage at room temperature for HCV RNA
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Arca de Lafuente, Sonia, Casanueva-Benítez, Cristina, Crespo-Bermejo, Celia, Lara-Aguilar, Violeta, Martín-Carbonero, Luz, de los Santos, Ignacio, Madrid, Ricardo, Briz, Veronica, and Comunidad de Madrid
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Multidisciplinary ,Temperature ,RNA, Viral ,Humans ,Dried Blood Spot Testing ,Hepacivirus ,Microbiología ,Hepatitis C ,Sensitivity and Specificity ,Genética ,Specimen Handling - Abstract
Hepatitis C virus (HCV) infection remains a global health problem, detected only in the early stages by molecular tests. Molecular tests detect HCV RNA, which is very prone to degradation by ribonucleases, reason why blood samples must be transported and stored at − 20 °C, or even − 70 °C for long-term storage. Flinders Technology Associates (FTA) cards are a useful sampling collecting device for dry blood spot (DBS) storage, especially for low and middle-income countries (LMIC). In this study, we analyzed viral HCV RNA integrity for long-term storage at room temperature compared to − 20 °C using two diferent types of cards for DBS: FTA Classic and 903 Protein Saver cards. For this purpose, DBS were prepared on these cards using blood or plasma samples from HCV infected patients, and samples were analysed by conventional RT-PCR. Our results showed that 903 Protein Saver cards are the best and cheapest alternative for DBS storage at room temperature. In these conditions, we found that HCV RNA integrity lasted for up to 9 months. This work was supported by the Community of Madrid, call for grants for the completion of Industrial PhD to VB and RM (IND2017/BMD-7683) Sí
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- 2022
14. Persistent low-Level viremia in persons living with HIV undertreatment: An unresolved status
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Crespo-Bermejo, Celia, primary, de Arellano, Eva Ramírez, additional, Lara-Aguilar, Violeta, additional, Valle-Millares, Daniel, additional, Gómez-Lus, Mª Luisa, additional, Madrid, Ricardo, additional, Martín-Carbonero, Luz, additional, and Briz, Verónica, additional
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- 2021
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15. Adaptation of the emerging pathogenic yeast Candida auris to high caspofungin concentrations correlates with cell wall changes
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Lara-Aguilar, Violeta, primary, Rueda, Cristina, additional, García-Barbazán, Irene, additional, Varona, Sarai, additional, Monzón, Sara, additional, Jiménez, Pilar, additional, Cuesta, Isabel, additional, Zaballos, Ángel, additional, and Zaragoza, Óscar, additional
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- 2021
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16. Adaptation of the emerging pathogenic yeast Candida auristo high caspofungin concentrations correlates with cell wall changes
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Lara-Aguilar, Violeta, Rueda, Cristina, García-Barbazán, Irene, Varona, Sarai, Monzón, Sara, Jiménez, Pilar, Cuesta, Isabel, Zaballos, Ángel, and Zaragoza, Óscar
- Abstract
ABSTRACTCandida aurishas emerged as a fungal pathogen that causes nosocomial outbreaks worldwide. Diseases caused by this fungus are of concern, due to its reduced susceptibility to several antifungals. C. aurisexhibits paradoxical growth (PG; defined as growth at high, but not intermediate antifungal concentrations) in the presence of caspofungin (CPF). We have characterized the cellular changes associated with adaptation to CPF. Using EUCAST AFST protocols, all C. aurisisolates tested showed PG to CPF, although in some isolates it was more prominent. Most isolates also showed a trailing effect (TE) to micafungin and anidulafungin. We identified two FKSgenes in C. auristhat encode the echinocandins target, namely β-1,3-glucan synthase. FKS1contained the consensus hot-spot (HS) 1 and HS2 sequences. FKS2only contained the HS1 region which had a change (F635Y), that has been shown to confer resistance to echinocandins in C. glabrata. PG has been characterized in other species, mainly C. albicans, where high CPF concentrations induced an increase in chitin, cell volume and aggregation. In C. aurisCPF only induced a slight accumulation of chitin, and none of the other phenomena. RNAseq experiments demonstrated that CPF induced the expression of genes encoding several GPI-anchored cell wall proteins, membrane proteins required for the stability of the cell wall, chitin synthase and mitogen-activated protein kinases (MAPKs) involved in cell integrity, such as BCK2, HOG1and MKC1(SLT2). Our work highlights some of the processes induced in C. auristo adapt to echinocandins.
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- 2021
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17. Dynamics of HIV Reservoir and HIV-1 Viral Splicing in HCV-Exposed Individuals after Elimination with DAAs or Spontaneous Clearance.
- Author
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Martínez-Román P, Crespo-Bermejo C, Valle-Millares D, Lara-Aguilar V, Arca-Lafuente S, Martín-Carbonero L, Ryan P, de Los Santos I, López-Huertas MR, Palladino C, Muñoz-Muñoz M, Fernández-Rodríguez A, Coiras M, Briz V, and On Behalf Of The Covihep Network
- Abstract
Background: Although human immunodeficiency virus type 1 (HIV-1) reservoir size is very stable under antiretroviral therapy (ART), individuals exposed to the Hepatitis C virus (HCV) (chronically coinfected and spontaneous clarifiers) show an increase in HIV reservoir size and in spliced viral RNA, which could indicate that the viral protein regulator Tat is being more actively synthesized and, thus, could lead to a higher yield of new HIV. However, it is still unknown whether the effect of HCV elimination with direct-acting antivirals (DAAs) could modify the HIV reservoir and splicing. Methods: This longitudinal study (48 weeks’ follow-up after sustained virological response) involves 22 HIV+-monoinfected individuals, 17 HIV+/HCV- spontaneous clarifiers, and 24 HIV+/HCV+ chronically infected subjects who eliminated HCV with DAAs (all of them aviremic, viral load < 50). Viral-spliced RNA transcripts and proviral DNA copies were quantified by qPCR. Paired samples were analyzed using a mixed generalized linear model. Results: A decrease in HIV proviral DNA was observed in HIV+/HCV- subjects, but no significant differences were found for the other study groups. An increased production of multiple spliced transcripts was found in HIV+ and HIV+/HCV+ individuals. Conclusions: We conclude that elimination of HCV by DAAs was unable to revert the consequences derived from chronic HCV infection for the reservoir size and viral splicing, which could indicate an increased risk of rapid HIV-reservoir reactivation. Moreover, spontaneous clarifiers showed a significant decrease in the HIV reservoir, likely due to an enhanced immune response in these individuals.
- Published
- 2022
- Full Text
- View/download PDF
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