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3. HCV-coinfection is related to an increased HIV-1 reservoir size in cART-treated HIV patients: a cross-sectional study

Author

López-Huertas, Maria Rosa, Palladino, Claudia, Garrido-Arquero, Marta, Esteban-Cartelle, Beatriz, Sánchez-Carrillo, Marta, Martínez-Román, Paula, Martín-Carbonero, Luz, Ryan, Pablo, Domínguez-Domínguez, Lourdes, Santos, Ignacio De Los, Moral, Sara De La Fuente, Benito, José Miguel, Rallón, Norma, Alcamí, José, Resino, Salvador, Fernández-Rodríguez, Amanda, Coiras, Mayte, Briz, Verónica, and on behalf of the Multidisciplinary Group of viral coinfection HIV/Hepatitis (COVIHEP)

Published
2019
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4. Dynamics of HIV Reservoir and HIV-1 Viral Splicing in HCV-Exposed Individuals after Elimination with DAAs or Spontaneous Clearance

Author

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.

Published
2022

5. T cell maturation and senescence after HCV cure in HIV-HCV coinfected patients: a prospective study

Author

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

Published
2022
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6. HCV eradication with DAAs differently affects HIV males and females: A whole miRNA sequencing characterization

Author

Valle-Millares, Daniel, primary, Brochado-Kith, Óscar, additional, Gómez-Sanz, Alicia, additional, Martín-Carbonero, Luz, additional, Ryan, Pablo, additional, De los Santos, Ignacio, additional, Castro, Juan M., additional, Troya, Jesús, additional, Mayoral-Muñoz, Mario, additional, Cuevas, Guillermo, additional, Martínez-Román, Paula, additional, Sanz-Sanz, Jesús, additional, Muñoz-Muñoz, María, additional, Jiménez-Sousa, María Á, additional, Resino, Salvador, additional, Briz, Verónica, additional, and Fernández-Rodríguez, Amanda, additional

Published
2022
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7. Different HCV exposure drives specific miRNA profile in PBMCS of HIV patients

Author

Valle-Millares, Daniel, Brochado-Kith, Óscar, Martín-Carbonero, Luz, Domínguez-Domínguez, Lourdes, Ryan, Pablo, De los Santos, Ignacio, De la Fuente, Sara, Castro, Juan M., Lagarde, María, Cuevas, Guillermo, Mayoral-Muñoz, Mario, Matarranz, Mariano, Díez, Victorino, Gómez-Sanz, Alicia, Martínez-Román, Paula, Crespo-Bermejo, Celia, Palladino, Claudia, Muñoz-Muñoz, María, Jiménez-Sousa, María A., Resino, Salvador, Briz, Verónica, Fernández-Rodríguez, Amanda, Multidisciplinary Group of Viral Coinfection HIV/Hepatitis, UAM. Departamento de Medicina, Instituto de Salud Carlos III, Fundación Universidad Alfonso X el Sabio, Fundación Banco Santander, Red de Investigación Cooperativa en Investigación en Sida, Centro de Investigación Biomédica en Red - CIBERINFEC (Enfermedades Infecciosas), Repositório da Universidade de Lisboa, Universidad Alfonso X El Sabio, Red Española de Investigación en SIDA, Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (España), Valle-Millares, Daniel, Brochado-Kith, Óscar, Martín-Carbonero, Luz, Domínguez-Domínguez, Lourdes, Ryan, Pablo, De Los Santos, Ignacio, Lagarde, María, Cuevas, Guillermo, Matarranz, Mariano, Díez, Victorino, Gómez-Sanz, Alicia, Crespo-Bermejo, Celia, Palladino, Claudia, Muñoz-Muñoz, María, Jiménez-Sousa, María A, Resino, Salvador, Briz, Verónica, and Fernández-Rodríguez, Amanda

Subjects
QH301-705.5, Medicina, Human immunodeficiency virus (HIV), Medicine (miscellaneous), Acute infection, medicine.disease_cause, PI3K signaling, Peripheral blood mononuclear cell, General Biochemistry, Genetics and Molecular Biology, Article, chemistry.chemical_compound, Spontaneous viral clearance, microRNA, medicine, Biology (General), Gene, business.industry, virus diseases, HIV, Virology, digestive system diseases, MicroRNAs, chemistry, High throughput sequence, Antifolate, HCV, Hiv patients, business
Abstract

18 Pág. Departamento de ​Mejora Genética Animal, Micro RNAs (miRNAs) are essential players in HIV and HCV infections, as both viruses modulate cellular miRNAs and interact with the miRNA-mediated host response. We aim to analyze the miRNA profile of HIV patients with different exposure to HCV to explore specific signatures in the miRNA profile of PBMCs for each type of infection. We massively sequenced small RNAs of PBMCs from 117 HIV+ infected patients: 45 HIV+ patients chronically infected with HCV (HIV/HCV+), 36 HIV+ that spontaneously clarified HCV after acute infection (HIV/HCV-) and 36 HIV+ patients without previous HCV infection (HIV). Thirty-two healthy patients were used as healthy controls (HC). Differential expression analysis showed significantly differentially expressed (SDE) miRNAs in HIV/HCV+ (n = 153), HIV/HCV- (n = 169) and HIV (n = 153) patients. We found putative dysregulated pathways, such as infectious-related and PI3K signaling pathways, common in all contrasts. Specifically, putatively targeted genes involved in antifolate resistance (HIV/HV+), cancer-related pathways (HIV/HCV-) and HIF-signaling (HIV) were identified, among others. Our findings revealed that HCV strongly influences the expression profile of PBMCs from HIV patients through the disruption of its miRNome. Thus, different HCV exposure can be identified by specific miRNA signatures in PBMCs., This work has been supported by grants from Institute of Health Carlos III, [PI15CIII/00031 and PI18CIII/00020/ to AFR and VB] and the Foundation Universidad Alfonso X el Sabio-Santander [grant number 1.010.932 to AFR] and the Spanish AIDS Research Network (RD16CIII/0002/0002), and Centro de Investigación Biomédica en Red (CIBER) en Enfermedades Infecciosas (CB21/13/00044). AFR is supported by the Miguel Servet programme from Fondo de Investigación Sanitaria (ISCIII) [CP14/CIII/00010 and CPII20CIII/0001]

Published
2021

8. Provirus reactivation is impaired in HIV-1 infected individuals on treatment with dasatinib and antiretroviral therapy

Author

Vigón, Lorena, primary, Martínez-Román, Paula, additional, Rodríguez-Mora, Sara, additional, Torres, Montserrat, additional, Puertas, María C., additional, Mateos, Elena, additional, Salgado, María, additional, Navarro, Antonio, additional, Sánchez-Conde, Matilde, additional, Ambrosioni, Juan, additional, Cervero, Miguel, additional, Wyen, Christoph, additional, Hoffmann, Christian, additional, Miró, José M, additional, Alcamí, José, additional, Podzamczer, Daniel, additional, García-Gutiérrez, Valentín, additional, Martínez-Picado, Javier, additional, Briz, Verónica, additional, Rosa López-Huertas, María, additional, Planelles, Vicente, additional, Coiras, Mayte, additional, Corona, Magdalena, additional, del Mar Díaz-Goizueta, María, additional, Knops, Elena, additional, Luna de Abia, Alejandro, additional, Martín-Carbonero, Luz, additional, Ryan, Pablo, additional, and Spivak, Adam, additional

Published
2021
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9. Estudio inmuno-virológico del reservorio del Virus de la Inmunodeficiencia Humana tipo 1 en individuos coinfectados por el virus de la hepatitis C. Impacto de la curación del Virus de la Hepatitis C

Author

Martínez Román, Paula, Briz Sebastián, Verónica, Universidad de Alcalá. Departamento de Biología de Sistemas, and Universidad de Alcalá. Programa de Doctorado en Ciencias de la Salud

Subjects
Microbiología Clínica, Biología Molecular de Microorganismos, Virología (VIH/VHC), Microbiología (VIH/VHC), Biology, Biología y Biomedicina
Abstract

Actualmente existen 2,75 millones de personas coinfectadas con el virus de la inmunodeficiencia humana (VIH) y el virus de la hepatitis C (VHC) en el mundo. Estudios previos han mostrado que la coinfección altera la historia natural de ambas enfermedades, empeorando el pronóstico de los pacientes. Aunque hoy en día es posible eliminar la infección por VHC gracias a los nuevos antivirales de acción directa (AADs), todavía no existe una cura para la infección por VIH debido a la persistencia del virus en reservorios latentes inaccesibles al tratamiento antirretorival. Aumentar el conocimiento sobre las consecuencias de la exposición al VHC y la eliminación del mismo en el contexto de la infección por el VIH-1 es crucial a la hora de desarrollar estrategias para el buen manejo de este tipo de pacientes. El presente trabajo identificó un mayor tamaño del reservorio del VIH-1 en individuos coinfectados con infección crónica, así como en individuos aclaradores espontáneos de la infección por el VHC comparados con sujetos monoinfectados VIH+. Respecto a la actividad transcripcional viral, se observó una mayor expresión de transcritos de ARN mensajero viral single y multiple spliced en pacientes coinfectados con infección crónica dada la activación persistente de su sistema inmunitario. Sin embargo, no se encontraron correlaciones evidentes entre el tamaño del reservorio y el splicing viral del VIH-1 para ninguno de los grupos de estudio, probablemente como consecuencia de la integración de provirus en zonas con baja actividad transcripcional y de la acumulación de provirus defectuosos. De igual modo, se observó que la eliminación del VHC con AADs no logra resolver el impacto que la infección crónica por VHC tiene en el reservorio viral del VIH. La estabilización del reservorio viral en estos pacientes se ve reforzada por el éxito del tratamiento antirretroviral y el incremento en la expresión de transcritos virales multiple spliced en células no quiescentes, lo que podría conducir a un desarrollo temprano de SIDA si la terapia fuese discontinuada. Sin embargo, con el tiempo, los pacientes aclaradores espontáneos del VHC son capaces de disminuir el tamaño del reservorio viral, posiblemente debido a la presencia de una respuesta antiviral potente en su organismo, así como a un sistema inmunitario robusto. Por último, el análisis de la evolución de las poblaciones celulares T de memoria muestra un descenso generalizado de la inmunosenescencia gracias a la disminución de la estimulación antigénica de células específicas frente al VIH-1 y al VHC. Además, el descenso en la proporción de células con fenotipo TH1 en individuos aclaradores espontáneos podría relacionarse con el declive en el tamaño del reservorio de los mismos, probablemente debido a su compartimentalización en células T cooperadoras foliculares con este fenotipo y a la normalización de la respuesta inmune inflamatoria.

Published
2021

10. HCV eradication with DAAs differently affects HIV males and females: A whole miRNA sequencing characterization

Author

Instituto de Salud Carlos III, Fundación Universidad Alfonso X el Sabio, Valle-Millares, Daniel [0000-0002-5205-855X], Muñoz Muñoz, María [0000-0003-3805-2108], Jiménez-Sousa, María Angeles [0000-0002-1945-6169], Valle-Millares, Daniel, Brochado-Kith, Óscar, Gómez-Sanz, Alicia, Martín-Carbonero, Luz, Ryan, Pablo, De Los Santos, Ignacio, Castro, Juan M., Troya, Jesús, Mayoral-Muñoz, Mario, Cuevas, G., Martínez-Román, Paula, Sanz-Sanz, Jesús, Muñoz Muñoz, María, Jiménez-Sousa, María Angeles, Resino, Salvador, Briz, Verónica, Fernández-Rodríguez, Amanda, Instituto de Salud Carlos III, Fundación Universidad Alfonso X el Sabio, Valle-Millares, Daniel [0000-0002-5205-855X], Muñoz Muñoz, María [0000-0003-3805-2108], Jiménez-Sousa, María Angeles [0000-0002-1945-6169], Valle-Millares, Daniel, Brochado-Kith, Óscar, Gómez-Sanz, Alicia, Martín-Carbonero, Luz, Ryan, Pablo, De Los Santos, Ignacio, Castro, Juan M., Troya, Jesús, Mayoral-Muñoz, Mario, Cuevas, G., Martínez-Román, Paula, Sanz-Sanz, Jesús, Muñoz Muñoz, María, Jiménez-Sousa, María Angeles, Resino, Salvador, Briz, Verónica, and Fernández-Rodríguez, Amanda

Abstract

Gender-specific consequences after HCV eradication are unexplored. MicroRNAs (miRNAs) play a crucial role in the immune response against viral infections. However, few have highlighted miRNA role in sex-biased disease or therapy response. We aim to assess gender differences reflected in the miRNA expression of HIV/HCV-coinfected patients who achieve sustained virological response (SVR) with direct acting antivirals (DAAs). We conducted a prospective study of miRNA expression in PBMCs from 28 chronic HIV/HCV-coinfected patients (HIV/HCV) at baseline and after achieving SVR with DAAs. Sixteen HIV-monoinfected patients (HIV) and 36 healthy controls (HC) were used as controls. Identification of significant differentially expressed (SDE) miRNAs was performed with generalized linear model and mixed GLMs. We also explored putative dysregulated biological pathways. At baseline, the HIV/HCV patients showed differences in the miRNA profile concerning the HIV group (165 and 102 SDE miRNAs for males and females, respectively). Gender-stratified analysis of HIV/HCV group at baseline versus at SVR achievement showed higher differences in males (80 SDE miRNAs) than in females (55 SDE miRNAs). After SVR, HIV/HCV group showed similar values to HIV individuals, especially in females (1 SDE miRNA). However, ten miRNAs in males remained dysregulated, which were mainly involved in cancer, fatty acid, and inflammatory pathways. Taken together, our results show gender-biased dysregulation in the miRNA expression profile of PBMCs after HCV eradication with DAAs. These differences were normalized in females, while miRNA profile and their target-related pathways in males lack of normalization, which may be related to a high-risk of developing liver-related complications.

Published
2021

11. Different HCV Exposure Drives Specific miRNA Profile in PBMCs of HIV Patients

Author

Instituto de Salud Carlos III, Universidad Alfonso X El Sabio, Red Española de Investigación en SIDA, Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (España), Valle-Millares, Daniel [0000-0002-5205-855X], Brochado-Kith, Óscar [0000-0001-8372-2604], Martín-Carbonero, Luz [0000-0001-8102-4079], Domínguez-Domínguez, Lourdes [0000-0001-6018-9026], Ryan, Pablo [0000-0002-4212-7419], De Los Santos, Ignacio [0000-0001-7073-5211], Lagarde, María [0000-0002-7712-6977], Cuevas, G. [0000-0001-7875-6359], Matarranz, Mariano [0000-0002-6120-7545], Díez, Victorino [0000-0003-1679-133X], Gómez-Sanz, Alicia [0000-0003-4674-3005], Crespo-Bermejo, Celia [0000-0002-2813-2481], Palladino, Claudia [0000-0002-8148-0928], Muñoz Muñoz, María [0000-0001-7875-6359], Jiménez-Sousa, María Angeles [0000-0002-1945-6169], Resino, Salvador [0000-0001-8783-0450], Briz, Verónica [0000-0003-2297-5098], Fernández-Rodríguez, Amanda [0000-0002-5110-2213], Valle-Millares, Daniel, Brochado-Kith, Óscar, Martín-Carbonero, Luz, Domínguez-Domínguez, Lourdes, Ryan, Pablo, De Los Santos, Ignacio, De la Fuente, Sara, Castro, Juan M., Lagarde, María, Cuevas, G., Mayoral-Muñoz, Mario, Matarranz, Mariano, Díez, Victorino, Gómez-Sanz, Alicia, Martínez-Román, Paula, Crespo-Bermejo, Celia, Palladino, Claudia, Muñoz Muñoz, María, Jiménez-Sousa, María Angeles, Resino, Salvador, Briz, Verónica, Fernández-Rodríguez, Amanda, Instituto de Salud Carlos III, Universidad Alfonso X El Sabio, Red Española de Investigación en SIDA, Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (España), Valle-Millares, Daniel [0000-0002-5205-855X], Brochado-Kith, Óscar [0000-0001-8372-2604], Martín-Carbonero, Luz [0000-0001-8102-4079], Domínguez-Domínguez, Lourdes [0000-0001-6018-9026], Ryan, Pablo [0000-0002-4212-7419], De Los Santos, Ignacio [0000-0001-7073-5211], Lagarde, María [0000-0002-7712-6977], Cuevas, G. [0000-0001-7875-6359], Matarranz, Mariano [0000-0002-6120-7545], Díez, Victorino [0000-0003-1679-133X], Gómez-Sanz, Alicia [0000-0003-4674-3005], Crespo-Bermejo, Celia [0000-0002-2813-2481], Palladino, Claudia [0000-0002-8148-0928], Muñoz Muñoz, María [0000-0001-7875-6359], Jiménez-Sousa, María Angeles [0000-0002-1945-6169], Resino, Salvador [0000-0001-8783-0450], Briz, Verónica [0000-0003-2297-5098], Fernández-Rodríguez, Amanda [0000-0002-5110-2213], Valle-Millares, Daniel, Brochado-Kith, Óscar, Martín-Carbonero, Luz, Domínguez-Domínguez, Lourdes, Ryan, Pablo, De Los Santos, Ignacio, De la Fuente, Sara, Castro, Juan M., Lagarde, María, Cuevas, G., Mayoral-Muñoz, Mario, Matarranz, Mariano, Díez, Victorino, Gómez-Sanz, Alicia, Martínez-Román, Paula, Crespo-Bermejo, Celia, Palladino, Claudia, Muñoz Muñoz, María, Jiménez-Sousa, María Angeles, Resino, Salvador, Briz, Verónica, and Fernández-Rodríguez, Amanda

Abstract

Micro RNAs (miRNAs) are essential players in HIV and HCV infections, as both viruses modulate cellular miRNAs and interact with the miRNA-mediated host response. We aim to analyze the miRNA profile of HIV patients with different exposure to HCV to explore specific signatures in the miRNA profile of PBMCs for each type of infection. We massively sequenced small RNAs of PBMCs from 117 HIV+ infected patients: 45 HIV+ patients chronically infected with HCV (HIV/HCV+), 36 HIV+ that spontaneously clarified HCV after acute infection (HIV/HCV-) and 36 HIV+ patients without previous HCV infection (HIV). Thirty-two healthy patients were used as healthy controls (HC). Differential expression analysis showed significantly differentially expressed (SDE) miRNAs in HIV/HCV+ (n = 153), HIV/HCV- (n = 169) and HIV (n = 153) patients. We found putative dysregulated pathways, such as infectious-related and PI3K signaling pathways, common in all contrasts. Specifically, putatively targeted genes involved in antifolate resistance (HIV/HV+), cancer-related pathways (HIV/HCV-) and HIF-signaling (HIV) were identified, among others. Our findings revealed that HCV strongly influences the expression profile of PBMCs from HIV patients through the disruption of its miRNome. Thus, different HCV exposure can be identified by specific miRNA signatures in PBMCs.

Published
2021

12. Dynamics of HIV Reservoir and HIV-1 Viral Splicing in HCV-Exposed Individuals after Elimination with DAAs or Spontaneous Clearance.

Author

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

Subjects
*HIV, *VIRAL load, *HEPATITIS C virus, *TAT protein, *VIRAL proteins
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. [ABSTRACT FROM AUTHOR]

Published
2022
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13. Hepatitis C Virus Influences HIV-1 Viral Splicing in Coinfected Patients

Author

Martínez-Román, Paula, primary, López-Huertas, María Rosa, additional, Crespo-Bermejo, Celia, additional, Arca-Lafuente, Sonia, additional, Cortegano, Isabel, additional, Valle-Millares, Daniel, additional, Gaspar, María Luisa, additional, Martín-Carbonero, Luz, additional, Domínguez-Domínguez, Lourdes, additional, Ryan, Pablo, additional, de los Santos, Ignacio, additional, de la Fuente-Moral, Sara, additional, Fernández-Rodríguez, Amanda, additional, Coiras, Mayte, additional, and Briz, Verónica, additional

Published
2020
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15. Nanotechnology: A reality for diagnosis of HCV infectious disease

Author

Arca-Lafuente, Sonia, Martínez-Román, Paula, Mate-Cano, Irene, Ricardo Madrid, Briz, Verónica, Madrid González, Ricardo, Arca-Lafuente, Sonia, Martínez-Román, Paula, Mate-Cano, Irene, Ricardo Madrid, Briz, Verónica, and Madrid González, Ricardo

Abstract

Hepatitis C virus (HCV) is the primary etiologic agent of liver cirrhosis or hepatocellular carcinoma. HCV elevated infection rates are mostly due to the lack of an accurate and accessible screening and diagno- sis, especially in low- and middle-income countries. Conventional HCV diagnostic algorithm consists of a serological test followed by a nucleic acid test. This sequence of tests is time consuming and not af- fordable for low-resource settings. Nanotechnology have introduced new promising tests for the diagnose of infectious diseases. Based on the employment of nanoparticles and other nanomaterials which lead to highly sensitive and specific nanoscale tests, most of them target pathogen genome. Implementation of nanoscale tests, which are affordable, portable and easy to use by non-specialized personal, would im- prove HCV diagnosis algorithm. In this review, we have summed up the current emerging nanotechnology tools, which will improve actual screening and treatment programs, and help to reach HCV elimination proposal., Depto. de Genética, Fisiología y Microbiología, Fac. de Ciencias Biológicas, TRUE, pub

Published
2019

17. Different HCV Exposure Drives Specific miRNA Profile in PBMCs of HIV Patients.

Author

Valle-Millares D, Brochado-Kith Ó, Martín-Carbonero L, Domínguez-Domínguez L, Ryan P, De Los Santos I, De la Fuente S, Castro JM, Lagarde M, Cuevas G, Mayoral-Muñoz M, Matarranz M, Díez V, Gómez-Sanz A, Martínez-Román P, Crespo-Bermejo C, Palladino C, Muñoz-Muñoz M, Jiménez-Sousa MA, Resino S, Briz V, Fernández-Rodríguez A, and On Behalf Of Multidisciplinary Group Of Viral Coinfection Hiv/Hepatitis Covihep

Abstract

Micro RNAs (miRNAs) are essential players in HIV and HCV infections, as both viruses modulate cellular miRNAs and interact with the miRNA-mediated host response. We aim to analyze the miRNA profile of HIV patients with different exposure to HCV to explore specific signatures in the miRNA profile of PBMCs for each type of infection. We massively sequenced small RNAs of PBMCs from 117 HIV+ infected patients: 45 HIV+ patients chronically infected with HCV (HIV/HCV+), 36 HIV+ that spontaneously clarified HCV after acute infection (HIV/HCV-) and 36 HIV+ patients without previous HCV infection (HIV). Thirty-two healthy patients were used as healthy controls (HC). Differential expression analysis showed significantly differentially expressed (SDE) miRNAs in HIV/HCV+ ( n = 153), HIV/HCV- ( n = 169) and HIV ( n = 153) patients. We found putative dysregulated pathways, such as infectious-related and PI3K signaling pathways, common in all contrasts. Specifically, putatively targeted genes involved in antifolate resistance (HIV/HV+), cancer-related pathways (HIV/HCV-) and HIF-signaling (HIV) were identified, among others. Our findings revealed that HCV strongly influences the expression profile of PBMCs from HIV patients through the disruption of its miRNome. Thus, different HCV exposure can be identified by specific miRNA signatures in PBMCs.

Published
2021
Full Text
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