46 results on '"Smaill, Fiona"'
Search Results
2. The anti-idiotypic antibody 1F7 selectively inhibits cytotoxic T cells activated in HIV-1 infection.
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Grant, Michael, Smaill, Fiona, Muller, Sybille, Kohler, Heinz, and Rosenthal, Kenneth
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T cells , *ANTI-idiotypic antibodies , *HIV infections - Abstract
SummaryCirculating CD8+ T lymphocyte numbers rise substantially following infection with HIV-1. This expanded CD8+ T cell population includes HIV-specific CTL and CTL that kill activated uninfected CD4+ lymphocytes. Experimental, epidemiological and clinical evidence supports the possibility that expansion of CD8+ CTL contributes to CD4+ T cell depletion and disease progression in human HIV infection. Therefore, modulation of CD8+ T cell numbers or of certain CD8+ CTL activated in HIV-infected individuals may be beneficial. It was found that 1F7, a mAb against an idiotype common to anti-HIV and anti-simian immunodeficiency virus (SIV) antibodies, selectively inhibited both anti-HIV CTL and CTL against uninfected CD4+ T cells. Alloantigen-specific CTL and NK cells from either HIV-infected individuals or controls were unaffected by 1F7. Prolonged incubation of CD8+ T cells from HIV-infected individuals with 1F7 induces apoptosis, which was shown to be reflected functionally in reduced total CTL activity and in especially reduced CTL activity against uninfected CD4+ lymphocytes. The selective reactivity of 1F7 with certain CD8+ CTL could be applied towards the modulation of CD8+ T cell responses involved in AIDS pathogenesis. [ABSTRACT FROM AUTHOR]
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- 2000
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3. Patient characteristics and determinants of CD4 at diagnosis of HIV in Mexico from 2008 to 2017: a 10-year population-based study.
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Azamar-Alonso, Amilcar, Bautista-Arredondo, Sergio A., Smaill, Fiona, Mbuagbaw, Lawrence, Costa, Andrew P., and Tarride, Jean-Eric
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DIAGNOSIS of HIV infections , *DELAYED diagnosis , *HEALTH policy , *CONFIDENCE intervals , *MULTIVARIATE analysis , *AGE distribution , *MEDICAL care , *PATIENTS , *POPULATION geography , *HUMAN services programs , *TREATMENT effectiveness , *SEX distribution , *CD4 lymphocyte count , *DESCRIPTIVE statistics , *PUBLIC hospitals , *STATISTICAL models , *LOGISTIC regression analysis , *ODDS ratio , *RESIDENTIAL patterns - Abstract
Background: In 2007–2012 the Mexican government launched the National HIV program and there was a major change in HIV policies implemented in 2013–2018, when efforts focused on prevention, increase in early diagnosis and timely treatment. Still, late HIV diagnosis is a major concern in Mexico due to its association with the development of AIDS development and mortality. Thus, the objectives of this study were to identify the determinants of late HIV diagnosis (i.e. CD4 count less than 200 cells/mm3) in Mexico from 2008 to 2017 and to evaluate the impact of the 2013–2017 National HIV program. Methods: Using patient level data from the SALVAR database, which includes 64% of the population receiving HIV care in Mexico, an adjusted logistic model was conducted. Main study outcomes were HIV late diagnosis which was defined as CD4 count less than 200 cells/mm3 at diagnosis. Results: The study included 106,830 individuals newly diagnosed with HIV and treated in Mexican public health facilities between 2008 and 2017 (mean age: 33 years old, 80% male). HIV late diagnosis decreased from 45 to 43% (P < 0.001) between 2008 and 2012 and 2013–2017 (i.e. before and after the implementation of the 2013–2017 policy). Multivariable logistic regressions indicated that being diagnosed between 2013 and 2017 (odds ratio [OR] = 0.96 [95% Confidence interval [CI] [0.93, 0.98]) or in health facilities specialized in HIV care (OR = 0.64 [95% CI 0.60, 0.69]) was associated with early diagnosis. Being male, older than 29 years old, diagnosed in Central East, the South region of Mexico or in high-marginalized locality increased the odds of a late diagnosis. Conclusions: The results of this study indicate that the 2013–2017 National HIV program in Mexico has been marginally successful in decreasing the proportion of individuals with late HIV diagnosis in Mexico. We identified several predictors of late diagnosis which could help establishing health policies. The main determinants for late diagnosis were being male, older than 29 years old, and being diagnosed in a Hospital or National Institute. [ABSTRACT FROM AUTHOR]
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- 2021
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4. Medical microbiology.
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Richardson, Harold and Smaill, Fiona
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DIAGNOSTIC microbiology , *IMMUNOASSAY - Abstract
Provides information on several diagnostic procedures used in microbiology. Immunoassays; Automated and semiautomated systems; Applications of the diagnostic methods.
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- 1998
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5. In early HIV infection, immediate vs deferred antiretroviral therapy reduced serious illnesses at 3 years.
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Smaill, Fiona
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HIV infections , *ANTIRETROVIRAL agents , *CD4 antigen , *TUBERCULOSIS prevention , *ISONIAZID , *HIV-positive persons , *HIV seroconversion - Abstract
The article discusses reduction in serious AIDS-related or non-AIDS-related illnesses in early HIV infection by immediate antiretroviral therapy (ART) as compared to deferred ART. Topics discussed include establishing criteria for treatment based delivering HIV care, endorsing treatment regardless of CD4+ count by HIV guidelines and prevention of tuberculosis (TB) by Early Antiretroviral Treatment and/or Early Isoniazid Prophylaxis against Tuberculosis in HIV-infected Adults (TEMPRANO) trials.
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- 2015
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6. Methodological and Reporting Quality of Noninferiority Randomized Controlled Trials Comparing Antiretroviral Therapies: A Systematic Review.
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Lo, Carson K L, Komorowski, Adam S, Hall, Clayton W, Sandstrom, Teslin S, Alamer, Amnah A M, Mourad, Omar, Li, Xena X, Ohaly, Rand Al, Benoit, Marie-Ève, Duncan, D Brody, Fuller, Charlotte A, Shaw, Shazeema, Suresh, Mallika, Smaill, Fiona, Kapoor, Andrew K, Smieja, Marek, Mertz, Dominik, Bai, Anthony D, and Group, for the McMaster Infectious Diseases Fellow Research
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HIV infections , *MEDICAL databases , *RESEARCH , *MEDICAL information storage & retrieval systems , *CONFIDENCE intervals , *SYSTEMATIC reviews , *ANTIRETROVIRAL agents , *ANTI-infective agents , *HIGHLY active antiretroviral therapy , *COMPARATIVE studies , *MEDICAL protocols , *DESCRIPTIVE statistics , *BLIND experiment , *MEDLINE , *RESEARCH bias - Abstract
Background It is unclear whether the reporting quality of antiretroviral (ARV) noninferiority (NI) randomized controlled trials (RCTs) has improved since the CONSORT guideline release in 2006. The primary objective of this systematic review was assessing the methodological and reporting quality of ARV NI-RCTs. We also assessed reporting quality by funding source and publication year. Methods We searched Medline, Embase, and Cochrane Central from inception to 14 November 2022. We included NI-RCTs comparing ≥2 ARV regimens used for human immunodeficiency virus treatment or prophylaxis. We used the Cochrane Risk of Bias 2.0 tool to assess risk of bias. Screening and data extraction were performed blinded and in duplicate. Descriptive statistics were used to summarize data; statistical tests were 2 sided, with significance defined as P <.05. The systematic review was prospectively registered (PROSPERO CRD42022328586), and not funded. Results We included 160 articles reporting 171 trials. Of these articles, 101 (63.1%) did not justify the NI margin used, and 28 (17.5%) did not provide sufficient information for sample size calculation. Eighty-nine of 160 (55.6%) reported both intention-to-treat and per-protocol analyses, while 118 (73.8%) described missing data handling. Ten of 171 trials (5.9%) reported potentially misleading results. Pharmaceutical industry–funded trials were more likely to be double-blinded (28.1% vs 10.3%; P =.03) and to describe missing data handling (78.5% vs 59.0%; P =.02). The overall risk of bias was low in 96 of 160 studies (60.0%). Conclusions ARV NI-RCTs should improve NI margin justification, reporting of intention-to-treat and per-protocol analyses, and missing data handling to increase CONSORT adherence. [ABSTRACT FROM AUTHOR]
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- 2023
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7. In HIV-1, immediate vs deferred antiretroviral therapy and isoniazid vs no isoniazid reduced severe illness at 30 mo.
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Smaill, Fiona
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DRUG therapy for tuberculosis , *ISONIAZID , *ANTIRETROVIRAL agents , *AIDS , *FACTORIAL experiment designs , *HIV , *HIV infections , *LONGITUDINAL method , *MEDICAL protocols , *MORTALITY , *AIDS-related opportunistic infections , *RANDOMIZED controlled trials , *HIGHLY active antiretroviral therapy , *TREATMENT effectiveness , *SEVERITY of illness index , *TREATMENT delay (Medicine) , *THERAPEUTICS - Abstract
Questions: In adults with HIV-1 infection, does immediate antiretroviral therapy (ART) reduce severe illness compared with deferred ART? Does isoniazid preventive therapy (IPT) reduce severe illness compared with no IPT? Methods Design: Randomized, controlled, 2 x 2 factorial trial (TEMPRANO ANRS 12136 trial). ClinicalTrials.gov NCT00495651. Allocation: Concealed.* Blinding: Unblinded.* Follow-up period: 30 months. Setting: 9 centers in Abidjan, Ivory Coast. Patients: 2076 patients ≥ 18 years of age (median age 35 y, 79% women, median CD4+ count 459 to 467 cells/mm[sup 3]) who had HIV-1 infection or dual HIV-1 and HIV-2 infection, CD4+ count < 800 cells/mm[sup 3], and did not meet World Health Organization (WHO) criteria for starting ART. Intervention: ART started immediately (n = 1041) or deferred until WHO criteria for starting ART were reached (n = 1035). Patients were also randomized to IPT, 300 mg/d starting 1 month after randomization and continuing for 6 months (n = 1038), or no IPT (n = 1038). Outcomes: Primary outcome was a composite of all-cause mortality or severe HIV-related illness (AIDS-defining disease, non–AIDS-defining cancer, or non–AIDS-defining invasive bacterial disease). Other outcomes included grade 3 or 4 adverse events (severe or life-threatening events including gastrointestinal, respiratory, cardiovascular, cutaneous, neurologic, or other adverse events, or hematologic or biochemical test abnormalities). Patient follow-up: 85% completed the 30-month visit or died (intention-to-treat analysis). Main results: Immediate ART, with or without IPT, reduced the primary outcome compared with deferred ART, with or without IPT (Table). IPT, with early or deferred ART, reduced the primary outcome compared with no IPT, with early or deferred ART (Table). No interaction was found between treatments and the primary outcome. Immediate ART did not differ from deferred ART and IPT did not differ from no IPT for all-cause mortality (Table). Immediate ART increased grade 3 or 4 adverse events at < 6 months (4.2% vs 1.7%, relative risk increase 154%, 95% CI 46 to 338) and reduced events at 6 to 30 months (2.6% vs 5.6%, relative risk reduction 52%, CI 23 to 69) compared with deferred ART; IPT did not differ from no IPT for grade 3 or 4 adverse events at < 6 months or 6 to 30 months. Conclusion: In adults with HIV-1 infection, immediate vs deferred antiretroviral therapy and isoniazid preventive therapy vs no isoniazid reduced severe illness at 30 months. [ABSTRACT FROM AUTHOR]
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- 2015
8. In early HIV infection, immediate vs deferred antiretroviral therapy reduced serious illnesses at 3 years.
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Smaill, Fiona
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HIV prevention , *HIV infection transmission , *AIDS , *AIDS-related complex , *MEDICAL protocols , *MORTALITY , *TIME , *RANDOMIZED controlled trials , *HIGHLY active antiretroviral therapy , *TREATMENT effectiveness , *HIV seroconversion , *CD4 lymphocyte count , *TREATMENT delay (Medicine) ,PREVENTION of disease progression - Abstract
Question: In adults with HIV infection and CD4+ count > 500 cells/mm[sup 3], does immediate antiretroviral therapy (ART) reduce serious AIDS-related or non–AIDS-related illnesses compared with deferred ART? Methods Design: Randomized controlled trial (Strategic Timing of Antiretroviral Therapy [START] study). ClinicalTrials.gov NCT00867048. Allocation: Concealed.* Blinding: Blinded* (outcome adjudicators). Follow-up period: Mean 3 years. Setting: 215 centers in 35 countries. Patients: 4685 generally healthy patients ≥ 18 years of age (median age 36 y, 73% men, median CD4+ count 651 cells/mm[sup 3]) who were HIV positive, had 2 CD4+ counts > 500 cells/mm[sup 3]≥ 2 weeks apart ≤ 60 days before enrollment, and had not started ART. Exclusion criteria included pregnancy, breastfeeding, or history of AIDS. Intervention: ART started immediately (n = 2326) or deferred until CD4+ count reached ≤ 350 cells/mm[sup 3] or an AIDS-related event or other condition requiring ART occurred (n = 2359). Outcomes: Primary outcome was a composite of serious AIDS-related events (death due to AIDS or any AIDS-defining event other than nonfatal herpes simples virus infection or esophageal candidiasis) or serious non–AIDS-related events (death not related to AIDS, cardiovascular disease, end-stage renal disease, decompensated liver disease, or non–AIDS-defining cancer other than basal cell or squamous cell skin cancer). Other outcomes included components of the composite outcome, all-cause mortality, grade 4 events (symptomatic, non–AIDS-related, potentially life-threatening events requiring medical intervention), and unscheduled non–AIDS-related hospitalization. Patient follow-up: 95% (intention-to-treat analysis). Main results: Immediate ART reduced serious AIDS-related and non–AIDS-related events compared with deferred ART; groups did not differ for all-cause mortality, grade 4 events, or unscheduled non–AIDS-related hospitalizations (Table). Conclusion: In adults with HIV infection and CD4+ count > 500 cells/mm[sup 3], immediate antiretroviral therapy reduced serious illnesses compared with deferred therapy. [ABSTRACT FROM AUTHOR]
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- 2015
9. In HIV-1, immediate vs deferred antiretroviral therapy and isoniazid vs no isoniazid reduced severe illness at 30 mo.
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Smaill, Fiona
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ANTIRETROVIRAL agents , *HIV seroconversion - Published
- 2015
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10. Commentary: Single daily dose of aminoglycoside is the preferred mode of administration.
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Smaill, Fiona
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AMINOGLYCOSIDES - Abstract
Opinion. Focuses on the preference for single daily dose of aminoglycoside. Benefits from one single dosing.
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- 1996
11. Factors partitioning physical frailty in people aging with HIV: A classification and regression tree approach.
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Inceer, Mehmet, Brouillette, Marie‐J., Fellows, Lesley K., Morais, José A., Harris, Marianne, Smaill, Fiona, Smith, Graham, Thomas, Réjean, and Mayo, Nancy E.
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HIV-positive persons , *LIFESTYLES , *FRAIL elderly , *CONFIDENCE intervals , *HYPOTHYROIDISM , *CANNABIS (Genus) , *CROSS-sectional method , *REGRESSION analysis , *AGING , *ODDS ratio , *COMORBIDITY , *PHENOTYPES , *TOBACCO - Abstract
Objective: To estimate the extent to which comorbidity and lifestyle factors were associated with physical frailty in middle‐aged and older Canadians living with HIV. Design: Cross‐sectional analysis of 856 participants from the Canadian Positive Brain Health Now cohort. Methods: The frailty indicator phenotype was adapted from Fried's criteria using self‐report items. Univariate logistic regression and classification and regression tree (CaRT) models were used to identify the most relevant independent contributors to frailty. Results: In all, 100 men (14.0%) and 26 women (19.7%) were identified as frail (≥ 3/5 criteria) for an overall prevalence of 15.2%. Nine comorbidities showed an influential association with frailty. The most influential comorbidities were hypothyroidism [odds ratio (OR) = 2.55, 95% confidence interval (CI): 1.29–5.03] and arthritis (OR = 2.54, 95% CI: 1.58–4.09). Additionally, tobacco (OR = 1.79, 95% CI: 1.05–3.04) showed an association. Any level of alcohol consumption showed a protective effect for frailty. The CaRT model showed nine pathways that led to frailty. Arthritis was the most discriminatory variable followed by alcohol, hypothyroidism, tobacco, cancer, cannabis, liver disease, kidney disease, osteoporosis, lung disease and peripheral vascular disease. The prevalence of physical frailty for people with arthritis was 27.4%; with additional cancer or tobacco and alcohol the prevalence rates were 47.1% and 46.1%, respectively. The protective effect of alcohol consumption evident in the univariate model appeared again in the CaRT model, but this effect varied. Cognitive frailty (19.5% overall) and emotional frailty (37.9% overall) were higher than the prevalence of physical frailty. Conclusions: Specific comorbidities and tobacco use were implicated in frailty, suggesting that it is comorbidities causing frailty. However, some frailty still appears to be HIV‐related. The higher prevalence of cognitive and emotional frailty highlights the fact that physical frailty should not be the only focus in HIV. [ABSTRACT FROM AUTHOR]
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- 2022
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12. New Approaches to TB Vaccination.
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Zhou Xing, Jeyanathan, Mangalakumari, and Smaill, Fiona
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TUBERCULOSIS vaccines , *MYCOBACTERIUM tuberculosis , *IMMUNOLOGY , *INFANT diseases , *ANTIGENS , *T helper cells - Abstract
The article offers information on novel approaches for the development and delivery of tuberculosis (TB) vaccines with a thorough understanding of pathogenicity of Mycobacterium (M) and immunology. Topics covered include the M bovis-based Bacille Calmette-Guérin (BCG) vaccine for infants and the M tuberculosis immunodominant antigen with activator adjutant T helper cell type 1 (Th1). Also discussed are antigen-preventing cells (APCs) and respiratory mucosal (RM) or intradermal vaccination.
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- 2014
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13. A longitudinal view of successful aging with HIV: role of resilience and environmental factors.
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Mayo, Nancy E., Brouillette, Marie-Josée, Nadeau, Lyne, Dendukuri, Nandini, Harris, Marianne, Smaill, Fiona, Smith, Graham, Thomas, Réjean, and Fellows, Lesley K.
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HIV , *SUCCESSFUL aging , *QUALITY of life , *REGRESSION trees , *LONELINESS , *HIV-positive persons - Abstract
Purpose: The purpose of this study is to estimate the extent to which people aging with HIV meet criteria for successful aging as operationalized through HRQL and maintain this status over time. A second objective is to identify factors that place people at promise for continued successful aging, including environmental and resilience factors. Methods: Participants were members of the Positive Brain Health Now (BHN) cohort. People ≥ 50 years (n = 513) were classified as aging successfully if they were at or above norms on 7 or 8 of 8 health-related quality of life domains from the RAND-36. Group-based trajectory analysis, regression tree analysis, a form of machine learning, and logistic regression were applied to identify factors predicting successful aging. Results: 73 (14·2%) met criteria for successful aging at entry and did not change status over time. The most influential factor was loneliness which split the sample into two groups with the prevalence of successful aging 28·4% in the "almost never" lonely compared to 4·6% in the "sometimes/often" lonely group. Other influential factors were feeling safe, social network, motivation, stigma, and socioeconomic status. These factors identified 17 sub-groups with at least 30 members with the proportions classified as aging successfully ranging from 0 to 79·4%. The nine variables important to classifying successful aging had a predictive accuracy of 0.862. Self-reported cognition but not cognitive test performance improved this accuracy to 0.895. The two groups defined by successful aging status did not differ on age, sex or viral load, nadir and current. Conclusion: The results indicate the important role of social determinants of health in successful aging among people living with HIV. [ABSTRACT FROM AUTHOR]
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- 2022
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14. Factors Contributing to the Lack of Human Immunodeficiency Virus Type 1 (HIV-1) Transmission...
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Bienzle, Dorothee, MacDonald, Kelly S., Smaill, Fiona M., Kovacs, Colin, Baqi, Mahin, Courssaris, Barbaram, Luscher, Mark A., Walmsley, Sharon L., and Rosenthal, Kenneth L.
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HIV infections , *HIV antibodies - Abstract
Evaluates couples discordant in their HIV-1 infection status for the presence of protective factors. Infectivity of phytohemagglutinin-stimulated CD4 blasts; Risk factors for HIV infection in seronegative subjects; Lysis of infected CD4 cells and B cell lines by autologous cytotoxic T lymphocytes.
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- 2000
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15. The impact of routine HIV drug resistance testing in Ontario: A controlled interrupted time series study.
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Mbuagbaw, Lawrence, Logie, Carmen H., Thabane, Lehana, Smaill, Fiona, Smieja, Marek, Burchell, Ann N., Rachlis, Beth, Tarride, Jean-Eric, Kroch, Abigail, Mazzulli, Tony, Alvarez, Elizabeth, Lawson, Daeria O., Nguyen, Francis, Perez, Richard, and Seow, Hsien
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ANTI-HIV agents , *DRUG resistance , *TIME series analysis , *CLINICAL drug trials - Abstract
Background: Knowledge of HIV drug resistance informs the choice of regimens and ensures that the most efficacious options are selected. In January 2014, a policy change to routine resistance testing was implemented in Ontario, Canada. The objective of this study was to investigate the policy change impact of routine resistance testing in people with HIV in Ontario, Canada since January 2014. Methods: We used data on people with HIV living in Ontario from administrative databases of the Institute for Clinical Evaluative Sciences (ICES) and Public Health Ontario (PHO), and ran ordinary least squares (OLS) models of interrupted time series to measure the levels and trends of 2-year mortality, 2-year hospitalizations and 2-year emergency department visits before (2005–2013) and after the policy change (2014–2017). Outcomes were collected in biannual periods, generating 18 periods before the intervention and 8 periods after. We included a control series of people who did not receive a resistance test within 3 months of HIV diagnosis. Results: Data included 12,996 people with HIV, of which 8881 (68.3%) were diagnosed between 2005 and 2013, and 4115 (31.7%) were diagnosed between 2014 and 2017. Policy change to routine resistance testing within 3 months of HIV diagnosis led to a decreasing trend in 2-year mortality of 0.8% every six months compared to the control group. No significant differences in hospitalizations or emergency department visits were noted. Interpretation: The policy of routine resistance testing within three months of diagnosis is beneficial at the population level. [ABSTRACT FROM AUTHOR]
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- 2021
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16. Urinary symptoms and quality of life in women living with HIV: a cross-sectional study.
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Larouche, Maryse, Albert, Arianne Y. K., Lipsky, Nancy, Walmsley, Sharon, Loutfy, Mona, Smaill, Fiona, Trottier, Sylvie, Bitnun, Ari, Yudin, Mark H., Cundiff, Geoffrey W., and Money, Deborah M.
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HIV-positive women , *QUALITY of life , *SYMPTOMS , *CROSS-sectional method , *PSYCHOLOGICAL distress , *GENITAL warts - Abstract
Introduction and hypothesis: To determine prevalence and quality of life impact of lower urinary tract symptoms (LUTS) in women living with HIV (WLWH). Methods: Cross-sectional urinary questionnaires were included in a multicenter national prospective study of the HPV vaccine in WLWH. Demographic and clinical information was abstracted from the parent study. The Urinary Distress Inventory (UDI-6) and Urinary Impact Questionnaire (UIQ-7) were administered. Wilcoxon rank sum, two-sample chi-square or Fisher's exact tests were used as appropriate to compare women with UDI-6 score ≥ 25 to those with lower UDI-6 scores on demographic and HIV-related factors. Significant categorical variables were followed up with logistic regression to estimate odds ratios (OR). Results: One hundred seventy-seven women completed urinary questionnaires (85.5% of cohort). Median age was 44.1 (37.2–50.6). Mean CD4 count was 621 (410–785), and 132 women (74.6%) were virologically suppressed. Median UDI-6 score was 4.2 (0–25). Fifty-one women (28.8%) had a UIQ-7 score > 0. Among those with a UDI-6 score of at least 25, median UIQ-7 was 9.5 (0–47.6). UDI-6 ≥ 25 was significantly associated with increasing age, higher BMI, Canada as country of origin, peri-/postmenopausal status (OR 3.37, 95% CI = 1.71 to 6.75) and being parous (OR 2.92, 95% CI = 1.27 to 7.59) (all p < 0.05). HIV-related factors were not associated with UDI-6 ≥ 25. Conclusions: LUTS were common, but we did not demonstrate a negative impact on quality of life in this sample of WLWH. Large comparative studies are needed to determine whether HIV is a risk factor for bothersome LUTS in women. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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17. Impact of Loneliness on Brain Health and Quality of Life Among Adults Living With HIV in Canada.
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Harris, Marianne, Brouillette, Marie-Josée, Scott, Susan C., Smaill, Fiona, Smith, Graham, Thomas, Réjean, Fellows, Lesley K., and Mayo, Nancy E.
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Background: People aging with HIV are at risk for loneliness, with stigmatization and economic marginalization added to the health challenges arising from chronic infection. This study provides evidence for the extent, contributors, and consequences of loneliness in people living with HIV, focusing on brain health and quality of life. Setting: Cross-sectional data from 856 middle-aged and older adults living with HIV recruited from 5 urban specialty clinics in Canada were drawn from the inaugural visit of the Positive Brain Health Now cohort study. Methods: Participants completed an extensive assessment of biopsychosocial variables. The prevalence, severity, and quality of life impact of self-reported loneliness were described. Clinical and environmental factors hypothesized as contributing to loneliness, and the consequences of loneliness on health and function were identified using logistic, ordinal, and linear regression. Results: Eighteen percent reported being "quite often" and 46% "sometimes" lonely. Those with more loneliness were younger, less mobile, suffered more financial hardship, and were more likely to use opioids. HIV symptoms, pain, fatigue, low motivation, stigma, and unemployment were related to loneliness. Loneliness increased the odds of cognitive impairment, low mood, stress, and poor physical health. Those who were "quite often" lonely were over 4 times more likely to report poor or very poor quality of life than those who were "almost never" lonely. Conclusion: Loneliness is common in middle-aged and older people living with HIV in Canada. Many of the associated factors are modifiable, offering novel targets for improving brain health, general health, and quality of life in HIV. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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18. Prevalent and persistent oncogenic HPV types in a cohort of women living with HIV prior to HPV vaccination.
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McClymont, Elisabeth, Lee, Marette, Raboud, Janet, Coutlée, François, Walmsley, Sharon, Lipsky, Nancy, Loutfy, Mona, Trottier, Sylvie, Smaill, Fiona, Klein, Marina B., Harris, Marianne, Cohen, Jeffrey, Yudin, Mark H., Wobeser, Wendy, and Money, Deborah
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HIV-positive women , *HUMAN papillomavirus vaccines , *PAPILLOMAVIRUSES , *CERVICAL cancer , *HIV infection complications , *HIV infections , *IMMUNIZATION , *CERVICAL intraepithelial neoplasia , *PAPILLOMAVIRUS diseases , *RESEARCH funding , *LONGITUDINAL method , *DISEASE complications ,CERVIX uteri tumors - Abstract
Objective: To describe prevalent and persistent oncogenic human papillomavirus (HPV) types detected in women living with HIV (WLWH) in Canada, including women with cervical dyskaryosis, and to determine predictors of type-specific HPV persistence.Methods: Women and girls living with HIV, recruited from 14 sites of HIV care across Canada, were included in a sub-analysis of a prospective vaccine immunogenicity cohort study (two HPV DNA results, at least one cervical cytology result pre-vaccination). Demographic and clinical data were collected alongside cervical samples for cytology and HPV DNA typing between November 25, 2008, and May 19, 2015.Results: Pre-vaccination, HPV16 and HPV52 were the most prevalent oncogenic HPV types. Of the 252 women and girls who met the eligibility criteria, 45% were infected with at least one oncogenic HPV type and one-third of participants had a persistent oncogenic infection. HPV16, 45, and 52 were the most frequently persistent types. Seventeen percent of women had persistent infections with oncogenic HPV types not within currently available vaccines (HPV35/39/51/56/59/68/82). Lower CD4 count significantly predicted HPV persistence (P=0.024). Cervical cytology results were normal for 82.9% of participants, atypical squamous cells of undetermined significance for 2.4%, low-grade squamous intraepithelial lesions for 11.5%, and high-grade squamous intraepithelial lesions for 2.8%.Conclusion: Unvaccinated WLWH were infected with a wide range of oncogenic HPV types. The findings highlighted the importance of optimal treatment of HIV and continued cervical cancer screening as key steps toward the global elimination of cervical cancer. [ABSTRACT FROM AUTHOR]- Published
- 2020
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19. Impact of quadrivalent HPV vaccine dose spacing on immunologic response in women living with HIV.
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McClymont, Elisabeth, Ogilvie, Gina, Albert, Arianne, Johnston, Angela, Raboud, Janet, Walmsley, Sharon, Lipsky, Nancy, Loutfy, Mona, Trottier, Sylvie, Smaill, Fiona, Yudin, Mark H., Klein, Marina B., Harris, Marianne, Wobeser, Wendy, Bitnun, Ari, Kakkar, Fatima, Samson, Lindy, Brophy, Jason, Karatzios, Christos, and Money, Deborah
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PAPILLOMAVIRUSES , *HIV-positive women , *VACCINES , *CD4 lymphocyte count , *HUMAN papillomavirus vaccines , *VIRAL load - Abstract
HPV vaccination schedules have changed as evidence has supported reduced dosing and extended intervals. Women living with HIV (WLWH) represent an important population with no data on alternative dosing. Girls and WLWH received quadrivalent HPV (qHPV) vaccine in a pan-Canadian study of immunogenicity and efficacy. Serology was performed at months 0/2/7/12/18/24. Medical and sexual history was collected throughout. Linear regression was used to determine if spacing of doses was associated with peak antibody titer. Multivariable analyses demonstrated significant relationships between peak antibody titer and time to blood draw post last vaccine dose, naivety to the relevant HPV type, and HIV viral load for all qHPV types. There was a significant relationship between peak HPV16/18 antibody titer and age. Taking age, time to serology, CD4 cell count, CD4 nadir, HIV viral load, and HPV naivety into account, spacing of the three qHPV vaccine doses did not significantly impact peak antibody titers. [ABSTRACT FROM AUTHOR]
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- 2020
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20. Persistence of Non-Vaccine Oncogenic HPV Genotypes in Quadrivalent HPV-Vaccinated Women Living With HIV.
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McClymont, Elisabeth, Coutlée, François, Lee, Marette, Albert, Arianne, Raboud, Janet, Walmsley, Sharon, Lipsky, Nancy, Loutfy, Mona, Trottier, Sylvie, Smaill, Fiona, Klein, Marina B., Yudin, Mark H., Harris, Marianne, Wobeser, Wendy, Bitnun, Ari, Samson, Lindy, and Money, Deborah
- Abstract
Background: Human papillomavirus (HPV) vaccines have promising safety and immunogenicity data in women living with HIV (WLWH). However, it is critical to understand the residual burden of oncogenic HPV within WLWH to inform postvaccination cervical screening needs. We assessed rates of persistent infection with nonquadrivalent HPV (qHPV) oncogenic types in a cohort of qHPV-vaccinated WLWH. Setting: Multicentre, longitudinal cohort across Canada. Methods: WLWH were scheduled to receive 3 doses of qHPV vaccine. Participants provided health data and HPV DNA samples. Persistent cases of HPV were defined as new HPV in samples from ≥2 consecutive visits or as HPV present in the last sample. HPV31/ 33/35/39/45/51/52/56/58/59/68/82 were considered to have oncogenic potential. Median follow-up time was 4 years after initial vaccine dose. Results: A total of 284 participants were eligible for this analysis with 1205 person-years (PY) of follow-up (≥1 dose of vaccine, ≥1 HPV DNA result after vaccination). The highest incidence of persistent infection was with HPV51 (1.38/100 PY), followed by HPV52 (1.18/100 PY), and HPV39 (1.06/100 PY). The incidence of persistent infection with pooled HPV types added in the nonavalent vaccine (HPV31/33/45/52/58) was lower than the incidence of persistent oncogenic HPV types not contained within available vaccines (HPV35/39/51/56/59/68) (2.4/100 PY versus 3.6/100 PY, respectively). Conclusions: qHPV-vaccinated WLWH continue to face a burden of persistent oncogenic HPV infection. Although the nonavalent vaccine could alleviate some of this burden, 2 of the top 3 persistent oncogenic HPVs in this cohort are not contained within any available vaccine. This highlights the need for ongoing cervical screening in HPV-vaccinated WLWH. [ABSTRACT FROM AUTHOR]
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- 2020
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21. Relationships between cognition, function, and quality of life among HIV+ Canadian men.
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Mayo, Nancy E., Brouillette, Marie-Josée, Scott, Susan C., Harris, Marianne, Smaill, Fiona, Smith, Graham, Thomas, Réjean, Fellows, Lesley K., and and investigators from the Positive Brain Health Now Study
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QUALITY of life , *STRUCTURAL equation modeling , *COGNITION , *BIOPSYCHOSOCIAL model , *OLDER men - Abstract
Objective: To estimate the extent to which HIV-related variables, cognition, and other brain health factors interrelate with other HIV-associated symptoms to influence function, health perception, and QOL in older HIV+ men in Canada.Design: Cross-sectional structural equation modelling (SEM) of data from the inaugural visit to the Positive Brain Health Now Cohort.Setting: HIV clinics at 5 Canadian sites.Subjects: 707 men, age ≥ 35 years, HIV+ for at least one year, without clinically diagnosed dementia.Main Outcome Measures: Five latent and 21 observed variables from the World Health Organization's biopsychosocial model for functioning and disability and the Wilson-Cleary Model were analysed. SEM was used to link disease factors to symptoms, impairments, function, health perception, and QOL with a focus on cognition.Results: QOL was explained directly by depression, social role, health perception, social support, and quality of the environment. Measured cognitive performance had direct effects on activity/function and indirect effects on participation, HP and QOL, acting through self-reported cognitive difficulties and meaningful activities.Conclusion: The biopsychosocial model showed good fit, with RMSEA < 0.05. This is the first time the full model has been tested in HIV. All of the domains included in the model are theoretically amenable to intervention and many have evidence-based interventions that could be harnessed to improve QOL. [ABSTRACT FROM AUTHOR]- Published
- 2020
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22. Efficacy of the Quadrivalent Human Papillomavirus Vaccine in Girls and Women Living With Human Immunodeficiency Virus.
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McClymont, Elisabeth, Lee, Marette, Raboud, Janet, Coutlée, François, Walmsley, Sharon, Lipsky, Nancy, Loutfy, Mona, Trottier, Sylvie, Smaill, Fiona, Klein, Marina B, Harris, Marianne, Cohen, Jeffrey, Yudin, Mark H, Wobeser, Wendy, and Money, Deborah
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CONFIDENCE intervals , *GENITAL warts , *HIV infections , *MEDICAL protocols , *RISK assessment , *VACCINES , *WOMEN'S health , *HUMAN papillomavirus vaccines , *TREATMENT effectiveness , *VACCINATION , *THERAPEUTICS ,PAPILLOMAVIRUS disease prevention - Abstract
Background Human papillomavirus (HPV) vaccination is safe and efficacious in women without human immunodeficiency virus (HIV). Although good immunogenicity has been observed in women living with HIV (WLWH), efficacy data in this population are needed. Methods We enrolled 420 females aged ≥9 years (range, 9–65) living with HIV. Participants were to receive 3 doses of qHPV vaccine (0/2/6 months). The main endpoint was vaccine failure (ie, incident persistent qHPV infection, cervical intraepithelial neoplasia of grade 2 or higher [CIN2+], or genital warts). We compared these rates to published rates in vaccinated and unvaccinated women without HIV as well as unvaccinated WLWH. Results Among 279 eligible women, median follow-up was 2 years. In the intention-to-treat population, the incidence rate (IR) of persistent qHPV (HPV6/11/16/18) was 2.3 per 100 person-years (/100PY) (95% confidence interval [CI], 1.1–4.1), and IR of genital warts was 2.3/100PY (95% CI, 1.2–4.1). In the per-protocol efficacy population, IR of persistent qHPV was 1.0/100PY (95% CI, 0.3–2.6) and of genital warts was 1.0/100PY (95% CI, 0.3–2.5). No cases of CIN2+ occurred. Reported rates of qHPV-related infection and disease within vaccinated women without HIV, unvaccinated women without HIV, and vaccinated WLWH: 0.1 (95% CI, 0.02–0.03), 1.5 (95% CI, 1.1–2.0), and 1.2 (95% CI, 0.2–3.4) /100PY, respectively. The rate of persistent qHPV among vaccinated WLWH was lower than among unvaccinated WLWH (2.3 vs 6.0/100PY). Conclusions Vaccinated WLWH may be at higher risk for vaccine failure than vaccinated women without HIV. However, overall rates of vaccine failure were low, and rates of persistent qHPV were lower than in unvaccinated WLWH. [ABSTRACT FROM AUTHOR]
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- 2019
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23. New Tuberculosis Vaccine Strategies: Taking Aim at Un-Natural Immunity.
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Jeyanathan, Mangalakumari, Yao, Yushi, Afkhami, Sam, Smaill, Fiona, and Xing, Zhou
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TUBERCULOSIS vaccines , *IMMUNITY , *MYCOBACTERIUM tuberculosis , *VACCINES , *LUNG infections - Abstract
Despite some major progress made in developing tuberculosis (TB) vaccine strategies, with a dozen novel vaccines currently in the clinical pipeline, the world is still missing an effective TB vaccine. This questions whether any major breakthroughs can be achieved without making a drastic departure from the current strategy, which creates a state of ‘near-natural immunity’, imitating the natural immunity developed after Mycobacterium tuberculosis ( Mtb ) infection. Here, we argue instead that mounting evidence suggests an effective strategy ought to induce a state of all-around ‘un-natural’ immunity comprising trained innate immunity (TII), tissue-resident memory T cells (T RM ), and anti- Mtb surface antibodies in the lung. Thus, here we summarize the latest information, thinking, and development in the field of TB and vaccines. [ABSTRACT FROM AUTHOR]
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- 2018
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24. Induction of an Immune-Protective T-Cell Repertoire With Diverse Genetic Coverage by a Novel Viral-Vectored Tuberculosis Vaccine in Humans.
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Jeyanathan, Mangalakumari, Daniela Damjanovic, Yushi Yao, Jonathan Bramson, Fiona Smaill, Zhou Xing, Damjanovic, Daniela, Yao, Yushi, Bramson, Jonathan, Smaill, Fiona, and Xing, Zhou
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TUBERCULOSIS vaccines , *T cells , *EPITOPES , *MYCOBACTERIUM tuberculosis , *CHEST diseases , *THERAPEUTICS - Abstract
Background: Whether a candidate tuberculosis vaccine induces clinically relevant protective T-cell repertoires in humans will not be known until the completion of costly efficacy clinical trials.Methods: We have developed an integrated immunologic approach to investigate the clinical relevance of T cells induced by a novel tuberculosis vaccine in a phase 1 trial. This approach consists of screening for likely dominant T-cell epitopes, establishing antigen-specific memory T-cell lines for identifying CD8+ and CD4+ T-cell epitopes, determining the ability of vaccine-induced T cells to inhibit mycobacterial growth in infected cells, and examining the genetic diversity of HLA recognition and the clinical relevance of identified T-cell epitopes.Results: A single-dose immunization in BCG-primed adults with an adenovirus-based tuberculosis vaccine elicits a repertoire of memory T cells capable of recognizing multiple Ag85A epitopes. These T cells are polyfunctional and cytotoxic and can inhibit mycobacterial growth in infected target cells. Some identified T-cell epitopes are promiscuous and recognizable by the common HLA alleles. These epitopes are clinically relevant to the epitopes identified in people with latent Mycobacterium tuberculosis infection and treated patients with tuberculosis.Conclusions: These data support further clinical development of this candidate vaccine. Our approach helps fill the gap in clinical tuberculosis vaccine development. [ABSTRACT FROM AUTHOR]- Published
- 2016
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25. HIV viral suppression results in higher antibody responses in HIV-positive women vaccinated with the quadrivalent human papillomavirus vaccine.
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Money, Deborah M., Moses, Erin, Blitz, Sandra, Vandriel, Shannon M., Lipsky, Nancy, Walmsley, Sharon L., Loutfy, Mona, Trottier, Sylvie, Smaill, Fiona, Yudin, Mark H., Klein, Marina, Harris, Marianne, Cohen, Jeffrey, Wobeser, Wendy, Bitnun, Ari, Lapointe, Normand, Samson, Lindy, Brophy, Jason, Karatzios, Christos, and Ogilvie, Gina
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HIV-positive women , *AIDS vaccines , *HUMAN papillomavirus vaccines , *ANTIBODY formation , *HIV infections , *THERAPEUTICS , *IMMUNOGENETICS , *CD4 lymphocyte count - Abstract
Objective To evaluate the immunogenicity and safety of the quadrivalent HPV (qHPV) vaccine in HIV-positive women over 24 months. Design Between November 2008 and December 2012, 372 women aged 15 and older were enrolled from 14 Canadian HIV outpatient clinics in an open label cohort study. The qHPV vaccine (0.5 mL) was administered intramuscularly at months 0, 2 and 6. The primary study endpoint was seroconversion to any of the HPV types targeted by the qHPV vaccine. Antibody levels were measured at 0, 2, 7, 12, 18, and 24 months. Adverse events were recorded throughout. Results Of 372 participants enrolled, 310 (83%) received at least one dose of the qHPV vaccine and 277 (74%) received all three doses. Ninety-five percent (293/308) were seronegative for at least one vaccine type at baseline. The median age was 38 years (IQR 32–45, range 15–66), 36% were white, 44% black and 13% were of Indigenous origin. Seventy-two percent of participants had a suppressed HIV viral load (VL < 40 c/ml) at baseline, with a median CD4 count of 510 cells/mm 3 (376–695). Month 7 HPV type-specific seroconversion rates were 99.0%, 98.7%, 98.1% and 93.6% for HPV types 6, 11, 16 and 18 respectively in the per-protocol population. Participants with suppressed HIV VL at first vaccine had a 1.74–3.05 fold higher peak antibody response compared to those without ( p from 0.006 to <0.0001). Conclusions This study is the first to examine the qHPV vaccine in HIV-positive women out to 24 months and the first to include HIV-positive women through to age 66. The qHPV vaccine was well tolerated, and highly immunogenic. As women with suppressed viral load had higher antibody responses, planning HPV vaccination to occur when persons are virologically suppressed would be optimal for maximizing immune response. Findings provide strong evidence that older HIV-positive women can still benefit from HPV vaccination. Clinical trial registration: http://www.isrctn.com/ISRCTN33674451 [ABSTRACT FROM AUTHOR]
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- 2016
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26. The effects of HIV-1 subtype and ethnicity on the rate of CD4 cell count decline in patients naive to antiretroviral therapy: a Canadian-European collaborative retrospective cohort study.
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Klein, Marina B., Young, Jim, Dunn, David, Ledergerber, Bruno, Sabin, Caroline, Cozzi-Lepri, Alessandro, Dabis, Francois, Harrigan, Richard, Tan, Darrell H., Walmsley, Sharon, Gill, John, Cooper, Curtis, Scherrer, Alexandra U., Mocroft, Amanda, Hogg, Robert S., and Smaill, Fiona
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HIV , *CD4 lymphocyte count , *ANTIRETROVIRAL agents , *RETROSPECTIVE studies , *COHORT analysis , *HIV infection transmission - Abstract
Background: Ethnic differences have the potential to confound associations between HIV-1 subtype and immunologic progression. We compared declines in CD4 cell counts during untreated infection for the most prevalent HIV-1 subtypes, focusing on distinguishing between the effects of viral subtype and ethnicity. Methods: We combined data from 4 European and 6 Canadian cohorts, selecting adults in the stable chronic phase of untreated HIV infection. We estimated the change in square root CD4 cell count over time for subtypes and ethnicities using mixed models, adjusting for covariates selected for their potential effect on initial CD4 cell count or its decline. Results: Data from 9772 patients were analyzed, contributing 79 175 measurements of CD4 cell count and 24 157 person-years of follow-up. Overall, there were no appreciable differences in CD4 cell count decline for viral subtypes A, CRF01_AE, CRF02_AG, C and G compared with viral subtype B; whereas the decline in CD4 cell count in patients of African ancestry was considerably slower than in patients of other ethnicity. When ethnic groups were studied separately, there was evidence for slower declines in CD4 cell count in viral subtypes C, and possibly A and G, compared with viral subtype B in patients of African ancestry but not among patients of other ethnicities, suggesting an interaction between subtype and ethnicity. Interpretation: Ethnicity is a major determinant of CD4 cell count decline; viral subtype differences may have existed but were small compared with the effect of ethnicity and were most apparent in patients of African ancestry. In developing countries, slower CD4 cell count declines among individuals of African descent may translate to a longer asymptomatic phase and increase the opportunity for HIV transmission. [ABSTRACT FROM AUTHOR]
- Published
- 2014
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27. The importance of motherhood in HIV-positive women of reproductive age in Ontario, Canada.
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Kennedy, V. Logan, Serghides, Lena, Raboud, Janet M., Su, DeSheng, Blitz, Sandra, Hart, Trevor A., Walmsley, Sharon L., Angel, Jonathan B., Smaill, Fiona M., Ralph, Edward D., Tharao, Wangari E., and Loutfy, Mona R.
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AGE distribution , *CONFIDENCE intervals , *EPIDEMIOLOGY , *MOTHERHOOD , *PROBABILITY theory , *QUESTIONNAIRES , *PSYCHOLOGY of women , *REPRODUCTIVE health , *LOGISTIC regression analysis , *DATA analysis , *HIV seroconversion , *DATA analysis software , *DESCRIPTIVE statistics - Abstract
Motherhood is personally, culturally, and historically rooted. Recent publications have focused on medical issues related to pregnancy and HIV, with attention on fetal well-being. There is limited literature on the importance of motherhood for HIV-positive women. Our study's purpose was to investigate the importance of motherhood among HIV-positive women of reproductive age in Ontario, Canada and to analyze the correlates thereof. We present our findings using a secondary analysis of cross-sectionally collected data from a study assessing fertility desires and intentions of HIV-positive women. The sub-analysis's outcome of interest was based on the question: “Being a mother is important to me” with a 5-point Likert scale that was dichotomized intostrongly agree/agreevs.neutral/disagree/strongly disagree. Logistic regression models were fit to calculate unadjusted and adjusted odds ratios (ORs) for significant correlates. Of the 497 respondents, median age was 38 (interquartile range [IQR] 32–43), 46% were African, 74% had given birth, and 57% intended to give birth. A total of 452 (91%) agreed (N= 75) or strongly agreed (N= 377) that being a mother was important to them. Age less than 40 years (OR 3.0; 95% confidence interval [CI] 1.6–5.7, African ethnicity (OR 9.2; 95% CI 3.2–26.3), immigration within 10 years (OR 19.6, 95% CI 4.6–83.1), and partner or family desire for a pregnancy (OR 3.3; 95% CI 1.5–7.3) were significant correlates of the importance of motherhood in a univariate analysis. Importance of motherhood was associated with desire (OR 6.2, 95% CI 3.1–12.3) and intention to give birth (OR 6.9, 95% CI 3.1–15.2), and previous birth (OR 8.5, 95% CI 4.2–16.8). In the multivariable model, the significant correlates were of age less than 40 years (OR 3.9; 95% CI 1.8–8.4), immigration within 10 years (OR 14.1; 95% CI 3.2–61.5), and having previously given birth (OR 11.2; 95% CI 5.1–24.4). The majority of women felt strongly that motherhood was important to them particularly among younger women, recent immigrants, and women who were mothers. [ABSTRACT FROM AUTHOR]
- Published
- 2014
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28. Antivirals for influenza: a summary of a systematic review and meta-analysis of observational studies.
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Santesso, Nancy, Hsu, Jonathan, Mustafa, Reem, Brozek, Jan, Chen, Yao Long, Hopkins, Jessica P., Cheung, Adrienne, Hovhannisyan, Gayane, Ivanova, Liudmila, Flottorp, Signe A., Sæterdal, Ingvil, Wong, Arthur D., Tian, Jinhui, Uyeki, Timothy M., Akl, Elie A., Alonso‐Coello, Pablo, Smaill, Fiona, and Schünemann, Holger J.
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INFLUENZA treatment , *ANTIVIRAL agents , *MEDICAL decision making , *SYSTEMATIC reviews , *META-analysis , *SCIENTIFIC observation , *RANDOMIZED controlled trials - Abstract
Despite the use of antivirals to treat patients with severe influenza, questions remain with respect to effects and safety. Although a recent systematic review has provided some indication of benefit, the analysis is limited by the quality of the available evidence from randomized controlled trials. To supplement the existing information, the authors conducted a systematic review of observational studies of antiviral treatment for influenza. This report summarises the findings of that review. Similar to the randomised trials, the confidence in the estimates of the effects for decision-making is low to very low primarily due to the risk of selection and publication bias in the observational studies. From these observational studies, the summary estimates suggest that oseltamivir may reduce mortality, hospitalisation and duration of symptoms compared with no treatment. Inhaled zanamivir may also reduce symptom duration and hospitalisations, but patients may experience more complications compared with no treatment. Earlier treatment with antivirals is generally associated with better outcomes than later treatment. Further high-quality evidence is needed to inform treatment guidelines because of the overall low to very low quality of evidence. [ABSTRACT FROM AUTHOR]
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- 2013
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29. Evaluation of HIV and Highly Active Antiretroviral Therapy on the Natural History of Human Papillomavirus Infection and Cervical Cytopathologic Findings in HIV-Positive and High-Risk HIV-Negative Women.
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Blitz, Sandra, Baxter, Joanna, Raboud, Janet, Walmsley, Sharon, Rachlis, Anita, Smaill, Fiona, Ferenczy, Alex, Coutlée, François, Hankins, Catherine, and Money, Deborah
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HIGHLY active antiretroviral therapy , *THERAPEUTICS , *HIV infections , *PAPILLOMAVIRUS diseases , *CELLULAR pathology , *CERVIX uteri diseases , *DISEASES in women - Abstract
Background. The Canadian Women's HIV Study (CWHS) enrolled human immunodeficiency virus (HIV)–positive and high-risk HIV-negative women in a longitudinal cohort. This analysis considered the effects of HIV and highly active antiretroviral therapy (HAART) on HPV persistence and cervical squamous intraepithelial lesions (SILs).Methods. Longitudinal cytopathologic and HPV DNA results were analyzed using multistate models. States of cervical SIL were defined as absent, present, and treatment; HPV states were defined as negative or positive. Demographic variables and markers of sexual activity were considered predictors. Results were calculated on the basis of transition probabilities and reported as hazard ratios (HRs).Results. The CWHS followed 750 HIV-positive and 323 HIV-negative women during 1993–2002. A total of 467 and 456 women were included in the longitudinal cervical cytopathologic and HPV DNA analyses, respectively. HIV-positive women had increased prevalence (46.6% vs 28.7%; P < .0001), increased acquisition (HR, 2.3; P = .03), and decreased clearance (HR, 0.4; P < .001) of oncogenic HPV as compared to HIV-negative women. Oncogenic HPV infection predicted progression of cervical dysplasia from normal to abnormal SIL (HR, 2.8; P = .002). Among HIV-positive participants, HAART increased the likelihood of regression (from present to absent) of cervical SIL (HR, 3.3; P = .02) and increased the clearance of oncogenic HPV types other than HPV-16 or HPV-18 (HR, 2.2; P = .01).Conclusions. This analysis demonstrated beneficial effects of HAART on cervical SIL in HIV-positive women. [ABSTRACT FROM AUTHOR]
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- 2013
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30. Herpes Simplex Virus Type 2 Coinfection Does Not Accelerate CD4 Count Decline in Untreated HIV Infection.
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Tan, Darrell H. S., Raboud, Janet M., Kaul, Rupert, Brunetta, Jason, Kaushic, Charu, Kovacs, Colin, Lee, Edward, Luetkehoelter, Jonathan, Rachlis, Anita, Smaill, Fiona, Smieja, Marek, and Walmsley, Sharon L.
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HERPES simplex virus , *HIV infections , *GLYCOPROTEINS , *VIRAL load , *DISEASE progression , *COHORT analysis - Abstract
The article discusses research comparing the rates of decline of CD4 white blood cells (WBCs) counts in HIV-infected adults with prior antiretroviral therapy (ART)–untreated follow-up according to their Herpes simplex virus type 2 (HSV-2) status. Topics include the prevalence of HSV-2 in HIV-infected adults, the research methodology used to determine the research subjects' HSV serostatus, and a discussion of the results.
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- 2013
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31. Factors affecting antiretroviral pharmacokinetics in HIV-infected women with virologic suppression on combination antiretroviral therapy: a cross-sectional study.
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Loutfy, Mona Rafik, Walmsley, Sharon Lynn, Klein, Marina Barbara, Janet Raboud, Alice Lin-in Tseng, Blitz, Sandra Lauren, Neora Pick, Brian Conway, Angel, Jonathan Benjamin, Rachlis, Anita Rochelle, Gough, Kevin, Cohen, Jeff, Haase, David, Burdge, David, Smaill, Fiona Mary, de Pokomandy, Alexandra, Loemba, Hugues, Trottier, Sylvie, and la Porte, Charles Jean
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ANTIRETROVIRAL agents , *HIV-positive women , *REVERSE transcriptase , *REGRESSION analysis , *EFAVIRENZ , *THERAPEUTICS - Abstract
Background: Although some studies show higher antiretroviral concentrations in women compared to men, data are limited. We conducted a cross-sectional study of HIV-positive women to determine if protease inhibitor (PI) and non-nucleoside reverse transcriptase inhibitor (NNRTI) Cmin and Cmax values were significantly different than historical general population (predominantly male) averages and to evaluate correlates of higher concentrations. Methods: HIV-positive women with virologic suppression (viral load < 50copies/mL) on their first antiretroviral regimen were enrolled. Timed blood samples for Cmin and Cmax were drawn weekly for 3 weeks. The ratio of each individual's median Cmin and Cmax to the published population mean values for their PI or NNRTI was calculated and assessed using Wilcoxon sign-rank. Intra- and inter-patient variability of antiretroviral drug levels was assessed using coefficient of variation and intra-class correlation. Linear regression was used to identify correlates of the square root-transformed Cmin and Cmax ratios. Results: Data from 82 women were analyzed. Their median age was 41 years (IQR=36-48) and duration of antiretrovirals was 20 months (IQR=9-45). Median antiretroviral Cmin and Cmax ratios were 1.21 (IQR=0.72-1.89, p=0.003) (highest ratios for nevirapine and lopinavir) and 0.82 (IQR=0.59-1.14, p=0.004), respectively. Nevirapine and efavirenz showed the least and unboosted atazanavir showed the most intra- and inter-patient variability. Higher CD4+ count correlated with higher Cmin. No significant correlates for Cmax were found. Conclusions: Compared to historical control data, Cmin in the women enrolled was significantly higher whereas Cmax was significantly lower. Antiretroviral Cmin ratios were highly variable within and between participants. There were no clinically relevant correlates of drug concentrations. [ABSTRACT FROM AUTHOR]
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- 2013
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32. Antivirals for Treatment of Influenza.
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Hsu, Jonathan, Santesso, Nancy, Mustafa, Reem, Brozek, Jan, Yao Long Chen, Hopkins, Jessica P., Cheung, Adrienne, Hovhannisyan, Gayane, Ivanova, Liudmila, Flottorp, Signe A., Sæterdal, Ingvil, Wong, Arthur D., Tian, Jinhui, Uyeki, Timothy M., Akl, Elie A., Alonso-Coello, Pablo, Smaill, Fiona, and Schünemann, Holger J.
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RANDOMIZED controlled trials , *INFLUENZA , *ANTIVIRAL agents , *INFLUENZA treatment , *SCIENTIFIC observation , *DRUGS , *OSELTAMIVIR , *PATIENTS - Abstract
Background: Systematic reviews of randomized, controlled trials in patients with influenza suggest a lack of evidence about the effects of antiviral therapy on several patient-important outcomes of influenza. Purpose: To systematically review observational studies for benefits and harms of oseltamivir, zanamivir, amantadine, or rimantadine in the treatment of influenza. Data Sources: MEDLINE, EMBASE, the Cochrane Central Register of Controlled Trials, CINAHL, SIGLE, the Chinese Biomedical Literature Database, Panteleimon, and LILACS up to November 2010; contact with pharmaceutical companies; and reference lists. Study Selection: Observational studies in any language that compared single antiviral therapy with no therapy or other antiviral therapy, or that had no comparator, for influenza or influenza-like illness. Data Extraction: Two independent investigators extracted data. Confidence in the estimates of the obtained effects (quality of evidence) was assessed by using the Grading of Recommendations Assessment, Development, and Evaluation approach. Data Synthesis: 74 studies fulfilled the inclusion criteria. Metaanalyses of the few studies providing effects with adjustment for confounders suggest that, in high-risk populations, oral oseltamivir may reduce mortality (odds ratio, 0.23 [95% CI, 0.13 to 0.43]; low-quality evidence), hospitalization (odds ratio, 0.75 [CI, 0.66 to 0.89]; low-quality evidence), and duration of symptoms (33 hours [CI, 21 to 45 hours]; very low-quality evidence) compared with no treatment. Earlier treatment with oseltamivir was generally associated with better outcomes. Inhaled zanamivir may lead to shorter symptom duration (23 hours [CI, 17 to 28 hours]; moderate-quality evidence) and fewer hospitalizations (odds ratio, 0.66 [CI, 0.37 to 1.18]) but more complications than no treatment. Direct comparison of oral oseltamivir and inhaled zanamivir suggests no important differences in key outcomes. Data from 1 study suggest that oral amantadine may reduce mortality and pneumonia associated with influenza A. No included study evaluated rimantadine. Limitations: Mortality was assessed in high-risk patients, and generalizability is limited. The overall body of evidence is limited by risk for confounding and selection, reporting, and publication bias. Conclusion: Therapy with oral oseltamivir and inhaled zanamivir may provide a net benefit over no treatment of influenza. However, as with the randomized trials, the confidence in the estimates of the effects for decision making is low to very low. Primary Funding Sources: World Health Organization and Mc- Master University. [ABSTRACT FROM AUTHOR]
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- 2012
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33. Safety and Tolerability of Varenicline Tartrate (Champix®/Chantix®) for Smoking Cessation in HIV-Infected Subjects: A Pilot Open-Label Study.
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Cui, Qu, Robinson, Linda, Elston, Dawn, Smaill, Fiona, Cohen, Jeffrey, Quan, Corinna, McFarland, Nancy, Thabane, Lehana, McIvor, Andrew, Zeidler, Johannes, and Smieja, Marek
- Abstract
The prevalence of smoking in HIV-infected subjects is high. As a smoking cessation aid, varenicline (Champix®, Pfizer, Saint-Laurent, QC, Canada or Chantix®, Pfizer, Mission, KS) has not been previously evaluated in HIV-infected smokers. In this multicenter pilot open label study, varenicline 1.0 mg was used twice daily for 12 weeks with dose titration in the first week. Adverse events (AEs) during the treatment period were recorded. Changes from baseline in laboratory tests, vital signs, daily cigarette consumption, nicotine dependence, and withdrawal were measured through week 24. Self-reported abstinence was validated by serum cotinine at week 12. We enrolled 36 subjects with a mean of 29 pack-years of smoking and a minimum of 4 cigarettes per day. All but 1 were male, 33 (92%) were white. The most frequently reported AEs were nausea (33%), abnormal dreams (31%), affect lability (19%), and insomnia (19%). Six (17%) subjects discontinued varenicline due to AEs. No grade 3/4 laboratory abnormalities or serious AEs occurred during the study. There was no significant change in HIV viral load. CD4 counts increased by 69 cells/mm3 ( p=0.001) at week 24. Serum cotinine-verified 4-week continuous abstinence rate through weeks 9-12 was 42% (95% confidence interval [CI]: 26-58%). AEs and abstinence rates were comparable to those in published randomized controlled trials conducted in generally healthy HIV-negative smokers. Varenicline was safe and appears effective among HIV-infected smokers in this exploratory study, although AEs were common. The most common AE was nausea, with no adverse effect on HIV treatment outcome. Close monitoring of liver enzymes and blood pressure is recommended for HIV-positive smokers taking varenicline. [ABSTRACT FROM AUTHOR]
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- 2012
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34. Safety and Tolerability of Varenicline Tartrate (Champix®/Chantix®) for Smoking Cessation in HIV-Infected Subjects: A Pilot Open-Label Study.
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Cui, Qu, Robinson, Linda, Elston, Dawn, Smaill, Fiona, Cohen, Jeffrey, Quan, Corinna, McFarland, Nancy, Thabane, Lehana, McIvor, Andrew, Zeidler, Johannes, and Smieja, Marek
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BLOOD cell count , *CONFIDENCE intervals , *HIV infections , *INTERVIEWING , *MEDICAL cooperation , *HEALTH outcome assessment , *QUESTIONNAIRES , *RESEARCH , *RESEARCH funding , *SELF-evaluation , *SMOKING cessation , *T cells , *T-test (Statistics) , *PILOT projects , *VIRAL load , *COTININE , *TREATMENT effectiveness , *REPEATED measures design , *DATA analysis software , *NICOTINIC agonists , *DESCRIPTIVE statistics , *THERAPEUTICS - Abstract
The prevalence of smoking in HIV-infected subjects is high. As a smoking cessation aid, varenicline (Champix®, Pfizer, Saint-Laurent, QC, Canada or Chantix®, Pfizer, Mission, KS) has not been previously evaluated in HIV-infected smokers. In this multicenter pilot open label study, varenicline 1.0 mg was used twice daily for 12 weeks with dose titration in the first week. Adverse events (AEs) during the treatment period were recorded. Changes from baseline in laboratory tests, vital signs, daily cigarette consumption, nicotine dependence, and withdrawal were measured through week 24. Self-reported abstinence was validated by serum cotinine at week 12. We enrolled 36 subjects with a mean of 29 pack-years of smoking and a minimum of 4 cigarettes per day. All but 1 were male, 33 (92%) were white. The most frequently reported AEs were nausea (33%), abnormal dreams (31%), affect lability (19%), and insomnia (19%). Six (17%) subjects discontinued varenicline due to AEs. No grade 3/4 laboratory abnormalities or serious AEs occurred during the study. There was no significant change in HIV viral load. CD4 counts increased by 69 cells/mm3 ( p=0.001) at week 24. Serum cotinine-verified 4-week continuous abstinence rate through weeks 9-12 was 42% (95% confidence interval [CI]: 26-58%). AEs and abstinence rates were comparable to those in published randomized controlled trials conducted in generally healthy HIV-negative smokers. Varenicline was safe and appears effective among HIV-infected smokers in this exploratory study, although AEs were common. The most common AE was nausea, with no adverse effect on HIV treatment outcome. Close monitoring of liver enzymes and blood pressure is recommended for HIV-positive smokers taking varenicline. [ABSTRACT FROM AUTHOR]
- Published
- 2012
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35. A comparison of the MOS-HIV and SF-12v2 for measuring health-related quality of life of men and women living with HIV/AIDS.
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Ion, Allyson, Wenjie Cai, Elston, Dawn, Pullenayegum, Eleanor, Smaill, Fiona, and Smieja, Marek
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HIV-positive women , *HEALTH surveys , *HEALTH status indicators , *PATHOLOGICAL psychology , *MENTAL health - Abstract
Background: The purpose of this study was to examine the relationship between the Medical Outcomes Study-HIV Health Survey (MOS-HIV) and the SF-12v2 to determine if the latter is adequate to assess the health-related quality of life (HRQoL) of men and women living with HIV/AIDS. 112 men and women living with HIV/AIDS who access care at a tertiary HIV clinic in Hamilton, Ontario were included in this cross-sectional analysis. Correlation coefficients of the MOS-HIV physical and mental health summary scores (PHS and MHS) and the SF-12v2 physical and mental component summary scales (PCS and MCS) were calculated along with common sub-domains of the measures including physical functioning (PF), bodily pain (BP), general health perceptions (GH), vitality (VT), social functioning (SF) and mental health (MH) to explore the relationship between these two HRQoL measures. The sub-domains role physical (RP) and role emotional (RE) of the SF-12v2 were compared separately to the sub-domain role functioning (RF) of the MOS-HIV. Weighted kappa scores were calculated to determine agreement beyond chance between the MOS-HIV and SF-12v2 in assigning a HRQoL state (i.e. low, moderate, good, very good). Results: The MOS-HIV had mean PHS and MHS summary scores of 47.3 (SD = 11.5) and 49.2 (SD = 10.7) respectively. The mean SF-12v2 PCS and MCS scores were 47.7 (SD = 11.0) and 44.0 (SD = 10.4). The MOS-HIV and SF-12v2 physical and mental health summary scores were positively correlated (r = 0.84, p < 0.001 and r = 0.76, p < 0.001). All common sub-domains were significantly correlated at p values from < 0.001 to 0.034. Substantial agreement was observed in assigning a HRQoL state (Physical: κ = 0.788, SE = 0.095; Mental: κ = 0.707, SE = 0.095). Conclusions: This analysis validates the SF-12v2 for measuring HRQoL in adult men and women living with HIV/AIDS. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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36. Effect of smoking on lung function, respiratory symptoms and respiratory diseases amongst HIV-positive subjects: a cross-sectional study.
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Qu Cui, Carruthers, Sue, McIvor, Andrew, Smaill, Fiona, Thabane, Lehana, and Smieja, Marek
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SMOKING , *LUNG diseases , *HIV-positive persons , *PULMONARY function tests , *DYSPNEA - Abstract
Background: Smoking prevalence in human immunodeficiency virus (HIV) positive subjects is about three times of that in the general population. However, whether the extremely high smoking prevalence in HIV-positive subjects affects their lung function is unclear, particularly whether smoking decreases lung function more in HIV-positive subjects, compared to the general population. We conducted this study to determine the association between smoking and lung function, respiratory symptoms and diseases amongst HIV-positive subjects. Results: Of 120 enrolled HIV-positive subjects, 119 had an acceptable spirogram. Ninety-four (79%) subjects were men, and 96 (81%) were white. Mean (standard deviation [SD]) age was 43.4 (8.4) years. Mean (SD) of forced expiratory volume in one second (FEV1) percent of age, gender, race and height predicted value (%FEV1) was 93.1% (15.7%). Seventy-five (63%) subjects had smoked 24.0 (18.0) pack-years. For every ten pack-years of smoking increment, %FEV1 decreased by 2.1% (95% confidence interval [CI]: -3.6%, -0.6%), after controlling for gender, race and restrictive lung function (R2 = 0.210). The loss of %FEV1 in our subjects was comparable to the general population. Compared to non-smokers, current smokers had higher odds of cough, sputum or breathlessness, after adjusting for highly active anti-retroviral therapy (HAART) use, odds ratio OR = 4.9 (95% CI: 2.0, 11.8). However respiratory symptom presence was similar between non-smokers and former smokers, OR = 1.0 (95% CI: 0.3, 2.8). All four cases of COPD (chronic obstructive pulmonary disease) had smoked. Four of ten cases of restrictive lung disease had smoked (p = 0.170), and three of five asthmatic subjects had smoked (p = 1.000). Conclusions: Cumulative cigarette consumption was associated with worse lung function; however the loss of % FEV1 did not accelerate in HIV-positive population compared to the general population. Current smokers had higher odds of respiratory symptoms than non-smokers, while former smokers had the same odds of respiratory symptoms as non-smokers. Cigarette consumption was likely associated with more COPD cases in HIV-positive population; however more participants and longer follow up would be needed to estimate the effect of smoking on COPD development. Effective smoking cessation strategies are required for HIV-positive subjects. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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37. Fertility Desires and Intentions of HIV-Positive Women of Reproductive Age in Ontario, Canada: A Cross-Sectional Study.
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Loutfy, Mona R., Hart, Trevor A., Mohammed, Saira S., DeSheng Su, Ralph, Edward D., Walmsley, Sharon L., Soje, Lena C., Muchenje, Marvelous, Rachlis, Anita R., Smaill, Fiona M., Angel, Jonathan B., Raboud, Janet M., Silverman, Michael S., Tharao, Wangari E., Gough, Kevin, and Yudin, Mark H.
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SURVEYS , *CROSS-sectional method , *HIV-positive women , *HUMAN fertility , *LOGISTIC regression analysis , *LIFE expectancy , *VERTICAL transmission (Communicable diseases) , *HIGHLY active antiretroviral therapy - Abstract
Background: Improvements in life expectancy and quality of life for HIV-positive women coupled with reduced vertical transmission will likely lead numerous HIV-positive women to consider becoming pregnant. In order to clarify the demand, and aid with appropriate health services planning for this population, our study aims to assess the fertility desires and intentions of HIV-positive women of reproductive age living in Ontario, Canada. Methodology/Principal Findings: A cross-sectional study with recruitment stratified to match the geographic distribution of HIV-positive women of reproductive age (18-52) living in Ontario was carried out. Women were recruited from 38 sites between October 2007 and April 2009 and invited to complete a 189-item self-administered survey entitled ''The HIV Pregnancy Planning Questionnaire'' designed to assess fertility desires, intentions and actions. Logistic regression models were fit to calculate unadjusted and adjusted odds ratios of significant predictors of fertility intentions. The median age of the 490 participating HIV-positive women was 38 (IQR, 32-43) and 61%, 52%, 47% and 74% were born outside of Canada, living in Toronto, of African ethnicity and currently on antiretroviral therapy, respectively. Of total respondents, 69% (95% CI, 64%-73%) desired to give birth and 57% (95% CI, 53%-62%) intended to give birth in the future. In the multivariable model, the significant predictors of fertility intentions were: younger age (age,40) (p,0.0001), African ethnicity (p,0.0001), living in Toronto (p = 0.002), and a lower number of lifetime births (p = 0.02). Conclusions/Significance: The proportions of HIV-positive women of reproductive age living in Ontario desiring and intending pregnancy were higher than reported in earlier North American studies. Proportions were more similar to those reported from African populations. Healthcare providers and policy makers need to consider increasing services and support for pregnancy planning for HIV-positive women. This may be particularly significant in jurisdictions with high levels of African immigration. [ABSTRACT FROM AUTHOR]
- Published
- 2009
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38. Pathogen inactivation: making decisions about new technologies.
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Klein, Harvey G., Anderson, David, Bernardi, Marie-Josée, Cable, Ritchard, Carey, William, Hoch, Jeffrey S., Robitaille, Nancy, Sivilotti, Marco L. A., and Smaill, Fiona
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CONFERENCES & conventions , *BLOOD transfusion , *SURGERY -- Congresses , *TOXICOLOGY conferences , *MEDICAL conferences - Abstract
Information about several papers discussed at a consensus conference titled "Pathogen Inactivation: Making Decisions About New Technologies" in Toronto, Ontario is presented. Topics include transfusion risks, inactivation technology, toxicology, regulatory approaches, risk analysis, and cost-benefit considerations. The conference also invited experts which made formal presentations.
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- 2007
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39. Prospective, Randomized Inpatient Study of Oral Metronidazole versus Oral Metronidazole and Rifampin for Treatment of Primary Episode of Clostridium difficile--Associated Diarrhea.
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Lagrotteria, Danny, Holmes, Serena, Smieja, Marek, Smaill, Fiona, and Lee, Christine
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METRONIDAZOLE , *ANTIPARASITIC agents , *NITROIMIDAZOLES , *ANTITUBERCULAR agents , *RIFAMPIN , *CLOSTRIDIOIDES difficile , *CLOSTRIDIUM - Abstract
Background. To date, no randomized trial to address the use of adjunctive rifampin in addition to metronidazole for the treatment of Clostridium difficile-associated diarrhea has been reported. Rifampin has excellent in vitro activity against C. difficile and penetrates into cellular materials where the organisms may persist. Methods. This was a prospective, randomized, single-blinded study of 39 patients that compared therapy with metronidazole alone versus therapy with metronidazole and rifampin for 10 days to treat laboratory-confirmed primary episode C. difficile-associated diarrhea. Twenty patients were randomly assigned to the metronidazole group, and 19 were randomly assigned to the metronidazole and rifampin group. Data were analyzed by intention-to-treat analysis using the 2-tailed Kaplan-Meier method and the log-rank test. Results. Adjunctive rifampin treatment for 10 days, compared with treatment with metronidazole alone for 10 days, was associated with a similar median time to symptom improvement (9.0 days vs. 6.5 days; P = .74), a similar median time to first relapse (26 days vs. 16 days; P = .23), a similar proportion of patients with relapse by study day 40 (42% vs. 38%; P = 1.0), and a similar proportion of patients experiencing nonfatal adverse events (37% vs. 40%; P = .55). There were a significantly higher number of deaths in the metronidazole and rifampin group, compared with the metronidazole group (6 of 19 patients vs. 1 of 20 patients; P = .04), but there were fewer laboratory-confirmed relapses by study day 40 (2 vs. 4; P = .66). Conclusions. We conclude that there is no role for routine rifampin as an adjunct to treatment with metronidazole for hospitalized patients with C. difficile-associated diarrhea. The cure rates for both treatment groups remain unacceptably low, and better treatments are urgently needed. [ABSTRACT FROM AUTHOR]
- Published
- 2006
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40. Canadian consensus guidelines for the care of HIV-positive pregnant women: putting recommendations into practice.
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Burdge, David R., Money, Deborah M., Forbes, John C., Walmsley, Sharon L., Smaill, Fiona M., Boucher, Marc, Samson, Lindy M., and Steben, Marc
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HIV-positive women , *HIV infections , *PREGNANCY , *MOTHERS , *WOMEN'S health - Abstract
Describes several scenarios for the implementation of the Canadian consensus guidelines for the care of HIV-positive pregnant women. Introduction to the guidelines; Case of an HIV-infected pregnant woman who is not receiving antiretroviral therapy when pregnancy is confirmed; HIV-infected pregnant woman receiving combination antiretroviral therapy when pregnancy is confirmed; Treatment of a woman diagnosed with HIV infection, who presents or is referred for care within 1 month of term.
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- 2003
41. Canadian consensus guidelines for the management of pregnancy, labour and delivery and for postpartum care in HIV-positive pregnant women and their offspring (summary of 2002 guidelines).
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Burdge, David R., Money, Deborah M., Forbes, John C., Walmsley, Sharon L., Smaill, Fiona M., Boucher, Marc, Samson, Lindy M., and Steben, Marc
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HIV-positive women , *PREGNANT women , *HEALTH counseling , *CONCEPTION , *AIDS - Abstract
Presents a summary of consensus guidelines for the care of HIV-positive pregnant women and their offspring, which were developed by the Canadian HIV Trials Network Working Group on Vertical HIV Transmission. General principles on the use of antiretroviral drugs in pregnancy; Discussion on preconception counselling and care; Postpartum care of the woman and the neonate.
- Published
- 2003
42. Successful discontinuation of therapy for disseminated Mycobacterium avium complex infection after effective antiretroviral therapy.
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Shafran, Stephen D., Mashinter, Laura D., Phillips, Peter, Lalonde, Richard G., Gill, John, Walsley, Sharon L., Toma, Emil, Conway, Brian, Fong, Ignatius W., Rachlis, Anita R., Williams, Kurt E., Garber, Gary E., Schlech III, Walter F., Smaill, Fiona, Gill, M John, Walmsley, Sharon L, Schlech, Walter F, and Pradier, C
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MYCOBACTERIAL disease treatment , *MYCOBACTERIUM avium - Abstract
Background: Highly active antiretroviral therapy (HAART) is associated with improvement or resolution of several HIV-associated opportunistic infections. Although prophylaxis against disseminated Mycobacterium avium complex infection may be successfully discontinued after a favorable response to HAART, the 1999 guidelines from the U.S. Public Health Service/Infectious Diseases Society of America recommend continuing therapy for disseminated M. avium complex infection, regardless of the response to HAART.Objective: To examine the outcome among patients with disseminated M. avium complex infection whose antimycobacterial therapy was discontinued after a favorable response to HAART.Design: Retrospective chart review between May 2000 and May 2001.Setting: 13 Canadian HIV clinics.Patients: 52 HIV-infected adults (43 men; mean age, 37.3 years) in whom successful antimycobacterial therapy for disseminated M. avium complex infection was discontinued after a favorable virologic response to HAART.Measurements: Survival, survival free of disseminated M. avium complex infection, and CD4(+) cell count responses.Results: At the time of diagnosis of disseminated M. avium complex infection, the median CD4(+) cell count was 0.016 x 10(9) cells/L, and the median plasma HIV RNA level was 90 000 copies/mL (plasma HIV RNA levels were available for only 21 patients). The patients received a median of 32 months of antimycobacterial therapy that included ethambutol plus either clarithromycin or azithromycin. When antimycobacterial therapy was discontinued, the median CD4(+) cell count was 0.23 x 10(9) cells/L and the median plasma HIV RNA level was less than 50 copies/mL. A median of 20 months after discontinuation of antimycobacterial therapy, only 1 patient had developed recurrent M. avium complex disease (37 months after stopping antimycobacterial therapy). This patient had stopped HAART 2 months earlier because of uncontrolled HIV viremia. Twenty months after stopping antimycobacterial therapy, the other 51 patients had a median CD4(+) cell count of 0.288 x 10(9) cells/L; 34 (67%) had undetectable plasma HIV RNA levels, and 8 (15%) had plasma HIV RNA levels of 50 to 1000 copies/mL.Conclusions: Discontinuation of successful disseminated M. avium complex therapy after a successful response to HAART is safe and reduces patients' pill burdens, potential drug adverse effects, drug interactions, and costs of therapy. [ABSTRACT FROM AUTHOR]- Published
- 2002
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43. RANTES Production by T Cells and CD8-Mediated Inhibition of Human Immunodeficiency Virus Gene Expression before Initiation of Potent Antiretroviral Therapy Predict Sustained Suppression of Viral Replication.
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Fransen, Signe, Copeland, Karen F.T., Smieja, Marek, Smaill, Fiona, and Rosenthal, Kenneth L.
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CHEMOKINES , *HIV infections , *THERAPEUTICS , *VIRAL replication - Abstract
Reports that beta-chemokine RANTES production by T cells and CD8-mediated inhibition of human immunodeficiency virus gene expression before initiation of potent antiretroviral therapy predict sustained suppression of viral replication. Effect of the introduction of potent combinations of antiretroviral drugs or highly active antiretroviral therapy in the treatment of human immunodeficiency virus infection.
- Published
- 2000
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44. CORRESPONDENCE.
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Cameron, S.O., Carrington, D., Patterson, W., McDonald, C.J., Court, M., Miller, A.J., Jones, Roger, Hinton, Anthony, Wilkinson, Simon R., Rogstad, K.E., Ahmed-Jushuf, I.H., Tesfa, L., Abdullah, M.S., Streefland, P.H., Matondo, Patrick, Liu, D.T.Y., Smaill, Fiona, and Fleming, Charlotte
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MEDICINE , *POLIO - Abstract
Comments on several issues related to medicine in Great Britain. Opinion on the possibility of an outbreak of poliomyelitis; Views on the relation among plasma concentrations of theophylline, control of symptoms of asthma and peak flow measurements; Reasons of the resistance to using condoms.
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- 1992
45. Factors affecting antiretroviral pharmacokinetics in HIV-infected women with virologic suppression on combination antiretroviral therapy: a cross-sectional study.
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Loutfy, Mona Rafik, Walmsley, Sharon Lynn, Klein, Marina Barbara, Raboud, Janet, Tseng, Alice Lin-In, Blitz, Sandra Lauren, Pick, Neora, Conway, Brian, Angel, Jonathan Benjamin, Rachlis, Anita Rochelle, Gough, Kevin, Cohen, Jeff, Haase, David, Burdge, David, Smaill, Fiona Mary, de Pokomandy, Alexandra, Loemba, Hugues, Trottier, Sylvie, and la Porte, Charles Jean
- Abstract
Background: Although some studies show higher antiretroviral concentrations in women compared to men, data are limited. We conducted a cross-sectional study of HIV-positive women to determine if protease inhibitor (PI) and non-nucleoside reverse transcriptase inhibitor (NNRTI) C(min) and Cmax values were significantly different than historical general population (predominantly male) averages and to evaluate correlates of higher concentrations.Methods: HIV-positive women with virologic suppression (viral load < 50copies/mL) on their first antiretroviral regimen were enrolled. Timed blood samples for C(min) and Cmax were drawn weekly for 3 weeks. The ratio of each individual's median C(min) and Cmax to the published population mean values for their PI or NNRTI was calculated and assessed using Wilcoxon sign-rank. Intra- and inter-patient variability of antiretroviral drug levels was assessed using coefficient of variation and intra-class correlation. Linear regression was used to identify correlates of the square root-transformed C(min) and Cmax ratios.Results: Data from 82 women were analyzed. Their median age was 41 years (IQR=36-48) and duration of antiretrovirals was 20 months (IQR=9-45). Median antiretroviral C(min) and Cmax ratios were 1.21 (IQR=0.72-1.89, p=0.003) (highest ratios for nevirapine and lopinavir) and 0.82 (IQR=0.59-1.14, p=0.004), respectively. Nevirapine and efavirenz showed the least and unboosted atazanavir showed the most intra- and inter-patient variability. Higher CD4+ count correlated with higher C(min). No significant correlates for Cmax were found.Conclusions: Compared to historical control data, C(min) in the women enrolled was significantly higher whereas Cmax was significantly lower. Antiretroviral C(min) ratios were highly variable within and between participants. There were no clinically relevant correlates of drug concentrations.Trial Registration: NCT00433979. [ABSTRACT FROM AUTHOR]- Published
- 2013
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46. Potent Inhibition of Viral Entry and Replication of SARS-CoV by siRNAs Targeting the Genes Encoding the Cellular ACE2 Receptor or the Viral Nucleocapsid Protein
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Yan, Xin, Shen, Hua, Feng, Yan, Wang, Jun, Lou, Shiwen, Wang, Liping, Wong, Gillian, Yang, Zhaoxiong, Jiang, Hongjian, Wu, Xinqi, Hu, Dan, Guan, Yi, Smaill, Fiona, and Zhang, Chengsheng
- Published
- 2007
- Full Text
- View/download PDF
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