4 research outputs found
Genotypic tropism testing in proviral DNA to guide maraviroc initiation in aviremic subjects: 48âweek analysis of the PROTEST study
Introduction: In a previous interim 24âweek virological safety analysis of the PROTEST study [1], initiation of Maraviroc (MVC) plus 2 nucleoside reverseâtranscriptase inhibitors (NRTIs) in aviremic subjects based on genotypic tropism testing of proviral HIVâ1 DNA was associated with low rates of virological failure. Here we present the final 48âweek analysis of the study.
Methods
PROTEST was a phase 4, prospective, singleâarm clinical trial (ID: NCT01378910) carried on in 24 HIV care centres in Spain. MaravirocânaĂŻve HIVâ1âpositive adults with HIVâ1 RNA (VL) 10% in a singleton), initiated MVC with 2 NRTIs and were followed for 48 weeks. Virological failure was defined as two consecutive VL>50 c/mL. Recent adherence was calculated as: (# pills taken/# pills prescribed during the previous week)*100.
Results
Tropism results were available from 141/175 (80.6%) subjects screened: 87/141 (60%) were R5 and 74/87 (85%) were finally included in the study. Their median age was 48 years, 16% were women, 31% were MSM, 36% had CDC category C at study entry, 62% were HCV+ and 10% were HBV+. Median CD4+ counts were 616 cells/mm3 at screening, and median nadir CD4+ counts were 143 cells/mm3. Previous ART included PIs in 46 (62%) subjects, NNRTIs in 27 (36%) and integrase inhibitors (INIs) in 1 (2%). The main reasons for treatment change were dyslipidemia (42%), gastrointestinal symptoms (22%), and liver toxicity (15%). MVC was given alongside TDF/FTC in 40 (54%) subjects, ABC/3TC in 30 (40%), AZT/3TC in 2 (3%) and ABC/TDF in 2 (3%). Sixtyâtwo (84%) subjects maintained VL<50 c/mL through week 48, whereas 12 (16%) discontinued treatment: two (3%) withdrew informed consent, one (1%) had a R5âX4 shift in HIV tropism between the screening and baseline visits, one (1%) was lost to followâup, one (1%) developed an ARTârelated adverse event (rash), two (3%) died due to nonâstudyârelated causes (1 myocardial infarction at week 0 and 1 lung cancer at week 36), and five (7%) developed protocolâdefined virological failure, although two of them regained VL<50 c/mL with the same MVC regimen (Table 1).
Conclusions
Initiation of MVC plus 2 NRTIs in aviremic subjects based on genotypic tropism testing of proviral HIVâ1 DNA is associated with low rates of virological failure up to one year
Genotypic tropism testing in proviral DNA to guide maraviroc initiation in aviremic subjects: 48âweek analysis of the PROTEST study
Introduction: In a previous interim 24âweek virological safety analysis of the PROTEST study [1], initiation of Maraviroc (MVC) plus 2 nucleoside reverseâtranscriptase inhibitors (NRTIs) in aviremic subjects based on genotypic tropism testing of proviral HIVâ1 DNA was associated with low rates of virological failure. Here we present the final 48âweek analysis of the study.
Methods
PROTEST was a phase 4, prospective, singleâarm clinical trial (ID: NCT01378910) carried on in 24 HIV care centres in Spain. MaravirocânaĂŻve HIVâ1âpositive adults with HIVâ1 RNA (VL) 10% in a singleton), initiated MVC with 2 NRTIs and were followed for 48 weeks. Virological failure was defined as two consecutive VL>50 c/mL. Recent adherence was calculated as: (# pills taken/# pills prescribed during the previous week)*100.
Results
Tropism results were available from 141/175 (80.6%) subjects screened: 87/141 (60%) were R5 and 74/87 (85%) were finally included in the study. Their median age was 48 years, 16% were women, 31% were MSM, 36% had CDC category C at study entry, 62% were HCV+ and 10% were HBV+. Median CD4+ counts were 616 cells/mm3 at screening, and median nadir CD4+ counts were 143 cells/mm3. Previous ART included PIs in 46 (62%) subjects, NNRTIs in 27 (36%) and integrase inhibitors (INIs) in 1 (2%). The main reasons for treatment change were dyslipidemia (42%), gastrointestinal symptoms (22%), and liver toxicity (15%). MVC was given alongside TDF/FTC in 40 (54%) subjects, ABC/3TC in 30 (40%), AZT/3TC in 2 (3%) and ABC/TDF in 2 (3%). Sixtyâtwo (84%) subjects maintained VL<50 c/mL through week 48, whereas 12 (16%) discontinued treatment: two (3%) withdrew informed consent, one (1%) had a R5âX4 shift in HIV tropism between the screening and baseline visits, one (1%) was lost to followâup, one (1%) developed an ARTârelated adverse event (rash), two (3%) died due to nonâstudyârelated causes (1 myocardial infarction at week 0 and 1 lung cancer at week 36), and five (7%) developed protocolâdefined virological failure, although two of them regained VL<50 c/mL with the same MVC regimen (Table 1).
Conclusions
Initiation of MVC plus 2 NRTIs in aviremic subjects based on genotypic tropism testing of proviral HIVâ1 DNA is associated with low rates of virological failure up to one year
How do women living with HIV experience menopause? Menopausal symptoms, anxiety and depression according to reproductive age in a multicenter cohort
CatedresBackground: To estimate the prevalence and severity of menopausal symptoms and anxiety/depression and to assess the differences according to menopausal status among women living with HIV aged 45-60 years from the cohort of Spanish HIV/AIDS Research Network (CoRIS). Methods: Women were interviewed by phone between September 2017 and December 2018 to determine whether they had experienced menopausal symptoms and anxiety/depression. The Menopause Rating Scale was used to evaluate the prevalence and severity of symptoms related to menopause in three subscales: somatic, psychologic and urogenital; and the 4-item Patient Health Questionnaire was used for anxiety/depression. Logistic regression models were used to estimate odds ratios (ORs) of association between menopausal status, and other potential risk factors, the presence and severity of somatic, psychological and urogenital symptoms and of anxiety/depression. Results: Of 251 women included, 137 (54.6%) were post-, 70 (27.9%) peri- and 44 (17.5%) pre-menopausal, respectively. Median age of onset menopause was 48 years (IQR 45-50). The proportions of pre-, peri- and post-menopausal women who had experienced any menopausal symptoms were 45.5%, 60.0% and 66.4%, respectively. Both peri- and post-menopause were associated with a higher likelihood of having somatic symptoms (aOR 3.01; 95% CI 1.38-6.55 and 2.63; 1.44-4.81, respectively), while post-menopause increased the likelihood of having psychological (2.16; 1.13-4.14) and urogenital symptoms (2.54; 1.42-4.85). By other hand, post-menopausal women had a statistically significant five-fold increase in the likelihood of presenting severe urogenital symptoms than pre-menopausal women (4.90; 1.74-13.84). No significant differences by menopausal status were found for anxiety/depression. Joint/muscle problems, exhaustion and sleeping disorders were the most commonly reported symptoms among all women. Differences in the prevalences of vaginal dryness (p = 0.002), joint/muscle complaints (p = 0.032), and sweating/flush (p = 0.032) were found among the three groups. Conclusions: Women living with HIV experienced a wide variety of menopausal symptoms, some of them initiated before women had any menstrual irregularity. We found a higher likelihood of somatic symptoms in peri- and post-menopausal women, while a higher likelihood of psychological and urogenital symptoms was found in post-menopausal women. Most somatic symptoms were of low or moderate severity, probably due to the good clinical and immunological situation of these women