Your search keyword '"Cahn, Pedro"' showing total 16 results

1. Opening the door on entry inhibitors in HIV: Redefining the use of entry inhibitors in heavily treatment experienced and treatment‐limited individuals living with HIV.

Author

Orkin, Chloe, Cahn, Pedro, Castagna, Antonella, Emu, Brinda, Harrigan, P Richard, Kuritzkes, Daniel R., Nelson, Mark, and Schapiro, Jonathan

Subjects

*HIV infections, *HIV-positive persons, *ANTIRETROVIRAL agents, *PATIENTS' attitudes, *MULTIDRUG resistance, *MEDICAL needs assessment

Abstract

Introduction: Entry inhibitors are a relatively new class of antiretroviral therapy and are typically indicated in heavily treatment experienced individuals living with HIV. Despite this, there is no formal definition of 'heavily treatment experienced'. Interpretation of this term generally includes acknowledgement of multidrug resistance and reflects the fact that patients in need of further treatment options may have experienced multiple lines of therapy. However, it fails to recognize treatment limiting factors including contraindications, age‐associated comorbidities, and difficulty adhering to regimens. Methods: This manuscript follows a roundtable discussion and aims to identify the unmet needs of those living with HIV who are in need of further treatment options, to broaden the definition of heavily treatment experienced and to clarify the use of newer agents, with an emphasis on the potential role of entry inhibitors, in this population. Results/Conclusions: Within the entry inhibitor class, mechanisms of action differ between agents; resistance to one subclass does not confer resistance to others. Combinations of entry inhibitors should be considered in the same regimen, and if lack of response is seen to one entry inhibitor another can be tried. When selecting an entry inhibitor, physicians should account for patient preferences and needs as well as agent‐specific clinical characteristics. Absence of documented multidrug resistance should not exclude an individual from treatment with an entry inhibitor; entry inhibitors are a valuable treatment option for all individuals who are treatment limited or treatment exhausted. We should advocate for additional clinical trials that help define the role of entry inhibitors in people with exhausted/limited ART options other than drug resistance. [ABSTRACT FROM AUTHOR]

Published

2022

2. The HIV epidemic in Latin America: a time to reflect on the history of success and the challenges ahead.

Author

Crabtree‐Ramírez, Brenda, Belaunzarán‐Zamudio, Pablo F, Cortes, Claudia P, Morales, Miguel, Sued, Omar, Sierra‐Madero, Juan, Cahn, Pedro, Pozniak, Anton, and Grinsztejn, Beatriz

Subjects

PRE-exposure prophylaxis, NEEDLE exchange programs, HIV, EPIDEMICS, SEXUALLY transmitted diseases

Abstract

Keywords: Latin America; HIV epidemic; migration; HIV; PrEP in Latin America; ART; HIV testing EN Latin America HIV epidemic migration HIV PrEP in Latin America ART HIV testing 1 4 4 04/01/20 20200301 NES 200301 According to Joint United Nations Programme on HIV/AIDS (UNAIDS) data, 1,900,000 adults and children were living with HIV in Latin America and the Caribbean in 2018 [1], where overall prevalence was 0.5%. Finally, the consequences of migration for the HIV epidemic in our region have rarely been considered in relation to the implementation of HIV prevention, treatment and care programmes. Latin America, HIV epidemic, migration, HIV, PrEP in Latin America, ART, HIV testing. [Extracted from the article]

Published

2020

3. Expert consensus statement on the science of HIV in the context of criminal law.

Author

Barré‐Sinoussi, Françoise, Abdool Karim, Salim S., Albert, Jan, Bekker, Linda‐Gail, Beyrer, Chris, Cahn, Pedro, Calmy, Alexandra, Grinsztejn, Beatriz, Grulich, Andrew, Kamarulzaman, Adeeba, Kumarasamy, Nagalingeswaran, Loutfy, Mona R., El Filali, Kamal M., Mboup, Souleymane, Montaner, Julio S. G., Munderi, Paula, Pokrovsky, Vadim, Vandamme, Anne‐Mieke, Young, Benjamin, and Godfrey‐Faussett, Peter

Subjects

HIV infection transmission, SEXUAL intercourse, CRIMINAL justice system, HIGHLY active antiretroviral therapy, PHYLOGENY

Abstract

Abstract: Introduction: Globally, prosecutions for non‐disclosure, exposure or transmission of HIV frequently relate to sexual activity, biting, or spitting. This includes instances in which no harm was intended, HIV transmission did not occur, and HIV transmission was extremely unlikely or not possible. This suggests prosecutions are not always guided by the best available scientific and medical evidence. Discussion: Twenty scientists from regions across the world developed this Expert Consensus Statement to address the use of HIV science by the criminal justice system. A detailed analysis of the best available scientific and medical research data on HIV transmission, treatment effectiveness and forensic phylogenetic evidence was performed and described so it may be better understood in criminal law contexts. Description of the possibility of HIV transmission was limited to acts most often at issue in criminal cases. The possibility of HIV transmission during a single, specific act was positioned along a continuum of risk, noting that the possibility of HIV transmission varies according to a range of intersecting factors including viral load, condom use, and other risk reduction practices. Current evidence suggests the possibility of HIV transmission during a single episode of sex, biting or spitting ranges from no possibility to low possibility. Further research considered the positive health impact of modern antiretroviral therapies that have improved the life expectancy of most people living with HIV to a point similar to their HIV‐negative counterparts, transforming HIV infection into a chronic, manageable health condition. Lastly, consideration of the use of scientific evidence in court found that phylogenetic analysis alone cannot prove beyond reasonable doubt that one person infected another although it can be used to exonerate a defendant. Conclusions: The application of up‐to‐date scientific evidence in criminal cases has the potential to limit unjust prosecutions and convictions. The authors recommend that caution be exercised when considering prosecution, and encourage governments and those working in legal and judicial systems to pay close attention to the significant advances in HIV science that have occurred over the last three decades to ensure current scientific knowledge informs application of the law in cases related to HIV. [ABSTRACT FROM AUTHOR]

Published

2018

4. Virologic failure and mortality in older ART initiators in a multisite Latin American and Caribbean Cohort.

Author

Carriquiry, Gabriela, Giganti, Mark J., Castilho, Jessica L., Jayathilake, Karu, Cahn, Pedro, Grinsztejn, Beatriz, Cortes, Claudia, Pape, Jean W., Padgett, Denis, Sierra‐Madero, Juan, McGowan, Catherine C., Shepherd, Bryan E., and Gotuzzo, Eduardo

Subjects

HIV infections, THERAPEUTICS, ANTIVIRAL agents, MORTALITY, VIRAL load, CARIBBEAN people, HEALTH

Abstract

Abstract: Introduction: The “greying” of the HIV epidemic necessitates a better understanding of the healthcare needs of older HIV‐positive adults. As these individuals age, it is unclear whether comorbidities and their associated therapies or the ageing process itself alter the response to antiretroviral therapy (ART). In this study, HIV treatment outcomes and corresponding risk factors were compared between older ART initiators and those who were younger using data from the Caribbean, Central and South America Network for HIV Epidemiology (CCASAnet). Methods: HIV‐positive adults (≥18 years) initiating ART at nine sites in Argentina, Brazil, Chile, Haiti, Honduras, Mexico and Peru were included. Patients were classified as older (≥50 years) or younger (<50 years) based on age at ART initiation. ART effectiveness was measured using three outcomes: death, virologic failure and ART treatment modification. Cox regression models for each outcome compared risk between older and younger patients, adjusting for other covariates. Results: Among 26,311 patients initiating ART between 1996 and 2016, 3389 (13%) were ≥50 years. The majority of patients in both ≥50 and <50 age groups received a non‐nucleoside reverse transcriptase inhibitor‐based regimen (89% vs. 87%), did not have AIDS at baseline (63% vs. 62%), and were male (59% vs. 58%). Older patients had a higher risk of death (adjusted hazard ratio (aHR) 1.64; 95% confidence intervals (CI): 1.48 to 1.83) and a lower risk of virologic failure (aHR: 0.73; 95% CI: 0.63 to 0.84). There was no difference in risk of ART modification (aHR: 1.00; 95% CI: 0.94 to 1.06). Risk factors for death, virologic failure and treatment modification were similar for each group. Conclusions: Older age at ART initiation was associated with increased mortality and decreased risk of virologic failure in our cohort of more than 26,000 ART initiators in Latin America and the Caribbean. To the best of our knowledge this is the first study from the region to evaluate ART outcomes in this growing and important population. Given the complexity of issues related to ageing with HIV, a greater understanding is needed in order to properly respond to this shifting epidemic. [ABSTRACT FROM AUTHOR]

Published

2018

5. Dolutegravir-lamivudine as initial therapy in HIV-1 infected, ARV-naive patients, 48-week results of the PADDLE (Pilot Antiretroviral Design with Dolutegravir LamivudinE) study.

Author

Cahn, Pedro, Rolón, María José, Figueroa, María Inés, Gun, Ana, Patterson, Patricia, and Sued, Omar

Subjects

*THERAPEUTICS, *HIV infections, *LAMIVUDINE, *HIGHLY active antiretroviral therapy, *DRUG tolerance, *INTEGRASE inhibitors

Abstract

Introduction: A proof-of-concept study was designed to evaluate the antiviral efficacy, safety and tolerability of a two-drug regimen with dolutegravir 50 mg once daily (QD) plus lamivudine 300 mg once daily as initial highly active antiretroviral therapy (HAART) among antiretroviral (ARV)-naive patients. Methods: PADDLE is a pilot study including 20 treatment-naive adults. To be selected, participants had no IAS-USA-defined resistance, HIV-1 RNA =100,000 copies/mL at screening and negative HBsAg. Plasma viral load (pVL) was measured at baseline; days 2, 4, 7, 10, 14, 21 and 28; weeks 6, 8 and 12; and thereafter every 12 weeks up to 96 weeks. Primary endpoint was the proportion of patients with HIV-1 RNA <50 copies/mL in an intention to treat (ITT)-exposed analysis at 48 weeks (the FDA snapshot algorithm). Results: Median HIV-1 RNA at entry was 24,128 copies/mL (interquartile range (IQR): 11,686-36,794). Albeit as per protocol, all patients had pVL =100,000 copies/mL at screening as required by inclusion criteria, four patients had =100,000 copies/mL at baseline. Median baseline CD4+ T-cell count was 507 per cubic millimetre (IQR: 296-517). A rapid decline in pVL was observed (median VL decay from baseline to week 12 was 2.74 logs). All patients were suppressed at week 8 onwards up to week 24. At week 48, 90% (18/20) reached the primary endpoint of a pVL <50 copies/mL. Median change in CD4 cell count between baseline and week 48 was 267 cells/mm³ (IQR: 180-462). No major tolerability/toxicity issues were observed. Nineteen patients completed 48 weeks of the study, and one patient (with undetectable VL at last visit) committed suicide. One patient presented a low-level protocol-defined confirmed virological failure at week 36, being the only observed failure. This patient had pVL <50 copies/mL at the end-of-study visit without having changed the two-drug regimen. Observed failure rate was 5%. This is the first report of integrase strand transfer inhibitor/lamivudine dual regimen in ARV-naive patients. Conclusions: This novel dual regimen of dolutegravir and lamivudine warrants further clinical research and consideration as a potential therapeutic option for ARV-therapy-naive patients. [ABSTRACT FROM AUTHOR]

Published

2017

6. Assessing the HIV Care Continuum in Latin America: progress in clinical retention, cART use and viral suppression.

Author

Rebeiro, Peter F, Cesar, Carina, Shepherd, Bryan E, De Boni, Raquel B, Cortés, Claudia P, Rodriguez, Fernanda, Belaunzarán‐Zamudio, Pablo, Pape, Jean W, Padgett, Denis, Hoces, Daniel, McGowan, Catherine C, and Cahn, Pedro

Subjects

THERAPEUTICS, HIV infections, ANTIRETROVIRAL agents, COHORT analysis, IMMUNOSUPPRESSION, VIRAL disease treatment, MEDICAL care

Abstract

Introduction: We assessed trends in HIV Care Continuum outcomes associated with delayed disease progression and reduced transmission within a large Latin American cohort over a decade: clinical retention, combination antiretroviral therapy (cART) use and viral suppression (VS). Methods: Adults from Caribbean, Central and South America network for HIV epidemiology clinical cohorts in seven countries contributed data between 2003 and 2012. Retention was defined as two or more HIV care visits annually, >90 days apart. cART was defined as prescription of three or more antiretroviral agents annually. VS was defined as HIV-1 RNA <200 copies/mL at last measurement annually. cART and VS denominators were subjects with at least one visit annually. Multivariable modified Poisson regression was used to assess temporal trends and examine associations between age, sex, HIV transmission mode, cohort, calendar year and time in care. Results: Among 18,799 individuals in retention analyses, 14,380 in cART analyses and 13,330 in VS analyses, differences existed between those meeting indicator definitions versus those not by most characteristics. Retention, cART and VS significantly improved from 2003 to 2012 (63 to 77%, 74 to 91% and 53 to 82%, respectively; p<0.05, each). Female sex (risk ratio (RR)=0.97 vs. males) and injection drug use as HIV transmission mode (RR=0.83 vs. male sexual contact with males (MSM)) were significantly associated with lower retention, but unrelated with cART or VS. MSM (RR=0.96) significantly decreased the probability of cART compared with heterosexual transmission. Conclusions: HIV Care Continuum outcomes improved over time in Latin America, though disparities for vulnerable groups remain. Efforts must be made to increase retention, cART and VS, while engaging in additional research to sustain progress in these settings. [ABSTRACT FROM AUTHOR]

Published

2016

7. HIV-TB coinfection impairs CD8+ T-cell differentiation and function while dehydroepiandrosterone improves cytotoxic antitubercular immune responses.

Author

Suarez, Guadalupe V., Angerami, Matías T., Vecchione, María B., Laufer, Natalia, Turk, Gabriela, Ruiz, Maria J., Mesch, Viviana, Fabre, Bibiana, Maidana, Patricia, Ameri, Diego, Cahn, Pedro, Sued, Omar, Salomón, Horacio, Bottasso, Oscar A., and Quiroga, María F.

Abstract

Tuberculosis (TB) is the leading cause of death among HIV-positive patients. The decreasing frequencies of terminal effector (TTE) CD8+T cells may increase reactivation risk in persons latently infected with Mycobacterium tuberculosis (Mtb). We have previously shown that dehydroepiandrosterone (DHEA) increases the protective antitubercular immune responses in HIV-TB patients. Here, we aimed to study Mtb-specific cytotoxicity, IFN-γ secretion, memory status of CD8+T cells, and their modulation by DHEA during HIV-TB coinfection. CD8+T cells from HIV-TB patients showed a more differentiated phenotype with diminished naïve and higher effector memory and TTE T-cell frequencies compared to healthy donors both in total and Mtb-specific CD8+T cells. Notably, CD8+T cells from HIV-TB patients displayed higher Terminal Effector (TTE) CD45RAdim proportions with lower CD45RA expression levels, suggesting a not fully differentiated phenotype. Also, PD-1 expression levels on CD8+T cells from HIV-TB patients increased although restricted to the CD27+ population. Interestingly, DHEA plasma levels positively correlated with TTE in CD8+T cells and in vitro DHEA treatment enhanced Mtb-specific cytotoxic responses and terminal differentiation in CD8+T cells from HIV-TB patients. Our data suggest that HIV-TB coinfection promotes a deficient CD8+ T-cell differentiation, whereas DHEA may contribute to improving antitubercular immunity by enhancing CD8+T-cell functions during HIV-TB coinfection. [ABSTRACT FROM AUTHOR]

Published

2015

8. Mortality and loss to follow-up among HIV-infected persons on long-term antiretroviral therapy in Latin America and the Caribbean.

Author

Carriquiry, Gabriela, Fink, Valeria, Koethe, John Robert, Giganti, Mark Joseph, Jayathilake, Karu, Blevins, Meridith, Cahn, Pedro, Grinsztejn, Beatriz, Wolff, Marcelo, Pape, Jean William, Padgett, Denis, Madero, Juan Sierra, Gotuzzo, Eduardo, McGowan, Catherine Carey, and Shepherd, Bryan Earl

Subjects

HIV prevention, HIV infections, THERAPEUTICS, MEDICAL care of HIV-positive persons, ANTI-HIV agents, HIV protease inhibitors

Abstract

Introduction: Long-term survival of HIV patients after initiating highly active antiretroviral therapy (ART) has not been sufficiently described in Latin America and the Caribbean, as compared to other regions. The aim of this study was to describe the incidence of mortality, loss to follow-up (LTFU) and associated risk factors for patients enrolled in the Caribbean, Central and South America Network (CCASAnet). Methods: We assessed time from ART initiation (baseline) to death or LTFU between 2000 and 2014 among ART-naïve adults (≥18 years) from sites in seven countries included in CCASAnet: Argentina, Brazil, Chile, Haiti, Honduras, Mexico and Peru. Kaplan-Meier techniques were used to estimate the probability of mortality over time. Risk factors for death were assessed using Cox regression models stratified by site and adjusted for sex, baseline age, nadir pre-ART CD4 count, calendar year of ART initiation, clinical AIDS at baseline and type of ART regimen. Results: A total of 16,996 ART initiators were followed for a median of 3.5 years (interquartile range (IQR): 1.6-6.2). The median age at ART initiation was 36 years (IQR: 30-44), subjects were predominantly male (63%), median CD4 count was 156 cells/μL (IQR: 60-251) and 26% of subjects had clinical AIDS prior to starting ART. Initial ART regimens were predominantly nonnucleoside reverse transcriptase inhibitor based (86%). The cumulative incidence of LTFU five years after ART initiation was 18.2% (95% confidence interval (CI) 17.5-18.8%). A total of 1582 (9.3%) subjects died; the estimated probability of death one, three and five years after ART initiation was 5.4, 8.3 and 10.3%, respectively. The estimated five-year mortality probability varied substantially across sites, from 3.5 to 14.0%. Risk factors for death were clinical AIDS at baseline (adjusted hazard ratio (HR)-1.65 (95% CI 1.47-1.87); pB0.001), lower baseline CD4 (HR-1.95 (95% CI 1.63-2.32) for 50 vs. 350 cells/μL; p<0.001) and older age (HR-1.47 (95% CI 1.29-1.69) for 50 vs. 30 years at ART initiation; p<0.001). Conclusions: In this large, long-term study of mortality among HIV-positive adults initiating ART in Latin America and the Caribbean, overall estimates of mortality were heterogeneous, generally falling between those reported in high-income countries and sub-Saharan Africa. [ABSTRACT FROM AUTHOR]

Published

2015

9. Preferred antiretroviral drugs for the next decade of scale up.

Author

Andrieux-Meyer, Isabelle, Calmy, Alexandra, Cahn, Pedro, Clayden, Polly, Raguin, Gilles, Katlama, Christine, Vitoria, Marco, Levin, Andrew, Lynch, Sharonann, Goemaere, Eric, and Ford, Nathan

Subjects

HIV infections, THERAPEUTICS, ANTIRETROVIRAL agents, HIV prevention, NANOTECHNOLOGY, DRUG tolerance

Abstract

Global commitments aim to provide antiretroviral therapy (ART) to 15 million people living with HIV by 2015, and recent studies have demonstrated the potential for widespread ART to prevent HIV transmission. Increasingly, countries are adapting their national guidelines to start ART earlier, for both clinical and preventive benefits. To maximize the benefits of ART in resource-limited settings, six key principles need to guide ART choice: simplicity, tolerability and safety, durability, universal applicability, affordability and heat stability. Currently available drugs, combined with those in late-stage clinical development, hold great promise to simplify treatment in the short term. Over the longer term, newer technologies, such as long-acting formulations and nanotechnology, could radically alter the treatment paradigm. This commentary reviews recommendations made in an expert consultation on treatment scale up in resource-limited settings. [ABSTRACT FROM AUTHOR]

Published

2012

10. ICOS, SLAM and PD-1 expression and regulation on T lymphocytes reflect the immune dysregulation in patients with HIV-related illness with pulmonary tuberculosis.

Author

Jurado, Javier Oscar, Pasquinelli, Virginia, Alvarez, Ivana Belén, Martínez, Gustavo Javier, Laufer, Natalia, Sued, Omar, Cahn, Pedro, Musella, Rosa María, Abbate, Eduardo, Salomón, Horacio, and Quiroga, María Florencia

Subjects

MYCOBACTERIUM tuberculosis, HIV infections, T cells, PROGRAMMED cell death 1 receptors, PROTEIN expression, IMMUNOREGULATION

Abstract

Background Tuberculosis (TB) continues to be the most frequent cause of illness and death from an infectious agent globally, and its interaction with HIV is having devastating effects. To investigate how HIV alters the immune response to Mycobacterium tuberculosis ( Mtb), we assessed basal and Mtb-induced proliferation, cytokine production, and expression of signalling lymphocytic activation molecule (SLAM), inducible costimulator (ICOS) and programmed death-1 (PD-1) on T lymphocytes from HIV-positive individuals coinfected with TB, HIV-positive subjects, TB patients and healthy donors (HD). Findings HIV-TB patients showed increased ICOS, SLAM and PD-1 basal levels on T lymphocytes, whereas HIV-positive individuals displayed elevated levels of SLAM and PD-1, TB patients high levels of SLAM, and HD low levels of the three proteins. Mtb-stimulation enhanced ICOS expression in the four groups, but only TB and HD increased SLAM and PD-1 levels. Conclusions These data show the immune deregulation that takes place during the immune response against TB in different study populations. [ABSTRACT FROM AUTHOR]

Published

2012

11. Pharmacokinetics of Two Randomized Trials Evaluating the Safety and Efficacy of Indinavir, Saquinavir and Lopinavir in Combination with Low-Dose Ritonavir: The MaxCmin1 and 2 Trials.

Author

Justesen, Ulrik S., Fox, Zoe, Pedersen, Court, Cahn, Pedro, Gerstoft, Jan, Clumeck, Nathan, Losso, Marcello, Peters, Barry, Obel, Niels, Castagna, Antonella, Dragsted, Ulrik B., and Lundgren, Jens D.

Subjects

PROTEASE inhibitors, CHEMICAL inhibitors, PROTEOLYTIC enzymes, DRUG efficacy, ENZYMES, PHARMACOKINETICS, CLINICAL trials, CHOLESTEROL, TOXICITY testing

Abstract

Our objective was to identify possible differences in protease inhibitor plasma concentrations between and within three protease inhibitor regimens (indinavir, saquinavir and lopinavir all in combination with low-dose ritonavir) and to relate these differences to safety and efficacy. Data originated from pre-defined pharmacokinetic substudies within two randomized 48-week trials evaluating the safety and efficacy of three protease inhibitor regimens. At weeks 4 and 48, plasma was collected and minimum drug plasma concentrations, Cmin, were obtained. Out of 656 randomized patients, 283 patients had available Cmin at week 4. Indinavir, saquinavir and lopinavir Cmin were high when combined with low-dose ritonavir. No significant difference in the proportion of patients experiencing treatment failure could be found according to the Cmin within any treatment arm. A saquinavir Cmin > 2000 ng/ml was associated with an increased risk of gastrointestinal grade 3 or 4 adverse events and higher total cholesterol. Overall, there were no changes in Cmin from week 4 to week 48 in patients who remained on therapy. No association between treatment failure and the Cmin could be demonstrated. Associations between high Cmin and toxicity were identified in the saquinavir arm; therefore, dose reductions may be appropriate in certain patients with Cmin several times above the minimum effective concentration. [ABSTRACT FROM AUTHOR]

Published

2007

12. Cerebral tumor-like American trypanosomiasis in acquired immunodeficiency syndrome.

Author

Pagano, Miguel A., Segura, Martín J., Di Lorenzo, Guillermo A., Garau, María L., Molina, Hugo A., Cahn, Pedro, Perez, Héctor, Vítolo, Fabián, Grondona, Alba, Piedimonte, Fabián C., Giannaula, Rolando, Ramia, Raúl, Miranda, Miguel A., Sierra, Hernán, Sica, Roberto E. P., Pagano, M A, Segura, M J, Di Lorenzo, G A, Garau, M L, and Molina, H A

Published

1999

13. Gender-sensitive reporting in medical research.

Author

Heidari, Shirin, Karim, Quarraisha Abdool, Auerbach, Judith D., Buitendijk, Simone E., Cahn, Pedro, Curno, Mirjam J., Hankins, Catherine, Katabira, Elly, Kippax, Susan, Marlink, Richard, Marsh, Joan, Marusic, Ana, Nass, Heidi M., Montaner, Julio, Pollitzer, Elizabeth, Ruiz-Cantero, Maria Teresa, Sherr, Lorraine, Sow, Papa Salif, Squires, Kathleen, and Wainberg, Mark A.

Subjects

MEDICAL research, CLINICAL trials, GENDER differences (Psychology), CLINICAL medicine, SEXUAL psychology

Abstract

Sex and gender differences influence the health and wellbeing of men and women. Although studies have drawn attention to observed differences between women and men across diseases, remarkably little research has been pursued to systematically investigate these underlying sex differences. Women continue to be underrepresented in clinical trials, and even in studies in which both men and women participate, systematic analysis of data to identify potential sex-based differences is lacking. Standards for reporting of clinical trials have been established to ensure provision of complete, transparent and critical information. An important step in addressing the gender imbalance would be inclusion of a gender perspective in the next Consolidated Standards of Reporting Trials (CONSORT) guideline revision. Uniform Requirements for Manuscripts Submitted to Biomedical Journals, as a set of wellrecognized and widely used guidelines for authors and biomedical journals, should similarly emphasize the ethical obligation of authors to present data analyzed by gender as a matter of routine. Journal editors are also promoters of ethical research and adequate standards of reporting, and requirements for inclusion of gender analyses should be integrated into editorial policies as a matter of urgency. [ABSTRACT FROM AUTHOR]

Published

2012

14. Liver cirrhosis in HIV/HCV‐coinfected individuals is related to NK cell dysfunction and exhaustion, but not to an impaired NK cell modulation by CD4+ T‐cells.

Author

Polo, María L, Ghiglione, Yanina A, Salido, Jimena P, Urioste, Alejandra, Poblete, Gabriela, Sisto, Alicia E, Martinez, Ana, Rolón, María J, Ojeda, Diego S, Cahn, Pedro E, Turk, Gabriela J, and Laufer, Natalia L

Subjects

KILLER cells, CIRRHOSIS of the liver, CELLULAR control mechanisms, CELL physiology

Abstract

Introduction: HIV worsens HCV‐related liver disease by accelerating fibrosis progression; however, progression rates are extremely variable among HIV/HCV‐coinfected individuals. NK cells are associated with modulation of liver fibrosis and are profoundly altered during HCV and HIV infections. CD4+ T‐cells modulate NK cell function, and are also affected by HIV infection. Here, we aim to characterize the association of hepatic fibrosis with both the phenotype and function of peripheral NK cells and their regulation by CD4+ T‐cells, in HIV/HCV‐coinfected individuals. Methods: Thirty‐four HIV/HCV‐coinfected individuals with minimal (n = 16) and advanced (n = 18) fibrosis (METAVIR F0/F1 and F4 scores respectively) and 20 healthy volunteers were enrolled. PBMC were obtained from peripheral blood samples and NK and CD4+ T‐cells were isolated and analysed. NK cell phenotype (CD25, CD69, Nkp46, NKG2D, PD‐1), degranulation (CD107a) and IFN‐γ and TNF‐α production, as well as CD4+ T‐cell activation (CD69, CD25 and CD38) were measured by flow cytometry. CD4+ T‐cell conditioned medium (CM) derived from F0/F1 or F4 individuals was assessed for IL‐2 levels by ELISA. Modulation of NK cell functionality by these CMs was also analysed. Results: When comparing to NK cells from individuals with minimal fibrosis, degranulation and cytokine secretion by NK cells from subjects with F4 scores was significantly impaired, while PD‐1 expression was augmented. On the one hand, neither the expression of activation markers nor IL‐2 secretion was distinctly induced in CD4+ T‐cells from subjects with F0/F1 or F4 METAVIR scores. Finally, NK cell degranulation and cytokine secretion were not differentially modulated by CD4+ T‐cell CM, whether CD4+ T‐cells derived from subjects with minimal or advanced fibrosis. Conclusions: Low levels of NK and CD4+ T‐cells in HIV/HCV‐coinfected individuals with advanced liver fibrosis have been previously described. Here, we show that advanced liver fibrosis in coinfected individuals is associated to a defective function of NK cells and an increased expression of the exhaustion/senescence marker PD‐1. This NK signature could not be attributed to changes in the ability of CD4+ T‐cells to modulate NK cell function. [ABSTRACT FROM AUTHOR]

Published

2019

15. Changes in lipid levels after 48 weeks of dual versus triple therapy observed in the GARDEL study.

Author

Cahn, Pedro, Andrade Villanueva, Jaime, Arribas, Jose, Gatell, Jose, Lama, Javier, Norton, Michel, Patterson, Patricia, Sierra Madero, Juan, Sued, Omar, Ines Figueroa, Maria, and Jose Rolón, Maria

Subjects

*LIPIDS, *RITONAVIR, *THERAPEUTIC use of protease inhibitors, *HIV infections, *THERAPEUTICS, *POLYPHARMACY, *HIV-positive persons

Abstract

Introduction Treatment with ritonavir-boosted protease inhibitors and nucleoside analogues frequently leads to rises in lipids, which might increase the cardiovascular risk. The aim of this study was to describe changes in lipid levels among HIV positive patients participating in the GARDEL study. Materials and Methods The GARDEL study compared the efficacy and safety of a dual therapy (DT) combination of LPV/r 400/100 mg BID+3TC 150 mg BID to a triple therapy (TT) with LPV/r 400/100 mg BID+3TC or FTC and a third investigator-selected NRTI in fixed-dose combination among HIV+ treatment naïve patients. We compared changes in lipid levels from baseline to week 48 in both arms. Results Patient's characteristics were well balanced regarding mean baseline total cholesterol (157 mg/dL DT, 154 mg/dL TT), triglycerides (142 mg/dL DT, 139 mg/Dl TT), LDL-C (94 mg/dL DT, 91 mg/dL TT) and HDL-C (36 mg/dL DT, 35 mg/dL TT). Changes in total cholesterol, LDL-C and HDL-C were higher in DT arm, compared to TT (32% DT vs 26% TT for cholesterol; 25% DT vs 16% TT for LDL and 33% DT vs 28% TT for HDL). Increase in triglycerides was higher in TT compared to DT (55% DT vs 92% TT) (Table 1). In TT arm LDL-C and total cholesterol elevations were lower among patients receiving TDF compared to those treated with ZDV or ABC. Conclusion Changes in lipid parameters were observed in both arms. Albeit the increase was numerically higher for cholesterol (total and LDL-C) in DT arm while TT arm had higher increases in TG; no difference was observed when week 48 values were compared with the NCEP ATP III goals for cardiovascular risk reduction []. So, the DT strategy, even missing the lipid-lowering effect observed with tenofovir, does not seem to add significant risk to patients treated with this novel strategy. [ABSTRACT FROM AUTHOR]

Published

2014

16. Switching to nevirapine-based regimens after undetectable viral load is not associated with increased risk of discontinuation due to toxicity.

Author

Patterson, Patricia, Socías, Eugenia, Pryluka, Daniel, Lapadula, Pablo, Pérez, Héctor, and Cahn, Pedro

Subjects

HIV infections, THERAPEUTICS, NEVIRAPINE, VIRAL load, CD4 lymphocyte count, VIREMIA, TOXICITY testing

Abstract

Introduction Due to its good tolerability, favourable cardiovascular risk-profile, low-pill burden and cost, nevirapine-based regimens are an attractive simplification strategy for patients with suppressed viral load (VL). However, current guidelines recommend caution if nevirapine (NVP) is prescribed in males and females with CD4 counts above 400 or 250 cells/µL, respectively. The aim of this study is to determine the prevalence and risk factors associated with development of toxicity or treatment discontinuation in patients switching to NVP-based regimens. Materials and Methods Retrospective chart review of HIV-infected patients with suppressed VL who switched from a PI-based regimen to a NVP-based regimen in four HIV clinics in Argentina, between 1997 and 2013. Bivariate and multivariate analyses were performed to explore factors associated with treatment discontinuation. High CD4 count was defined as CD4-cell count ≥400 or 250 cells/µL in males and females, respectively. Results Of 218 patients included, 165 (75.7%) were male; 21 (9.6%) were co-infected with HCV and/or HBV. Median baseline (BSL) CD4 count: 138 cells/µL (IQR: 64-276). At switch, patients had a median age of 38 years (IQR: 33.4-43.8) and had been suppressed for a median of 1.4 years (IQR: 0.6-2.2); 138 patients (63.3%) had high CD4-cell counts: among females, median CD4 count at switch was 462 (IQR: 330-709) cells/µL; among males, 433 (IQR: 305-595) cells/µL. Thirty-six patients (13.5%) presented NVP-related toxicity (30 skin toxicity, 6 hepatic toxicity), 29 (13.3%) discontinued NVP. Median time to development to toxicity: 32 days (IQR: 15-75). In bivariate analysis, chronic hepatitis was the only variable associated with development of toxicity (OR: 2.90, 95% CI 1.08-7.78). In multivariate analysis, no statistical significant associations were observed between either development of toxicity or treatment discontinuation and gender, chronic hepatitis, age or CD4-cell count at BSL or at switch (all p>0.05). Conclusions In our study, switching to a NVP-based regimen in patients with undetectable VL was associated with a low incidence of skin or liver toxicity, and treatment discontinuation. Moreover, these were unrelated to the CD4-cell count. Our findings suggest that, in contrast with ART-naïve patients, switching to NVP-based regimens could be a safe strategy for patients with suppressed viremia regardless of the CD4-cell count. [ABSTRACT FROM AUTHOR]

Published

2014