Factors influencing adherence to antiretroviral therapy in adolescents at Botswana-Baylor Children's Clinical Centre of Excellence : a qualitative study

Marukutira, Tafireyi

11 1900

The aim of the study was to determine the factors that influence adherence to ART among adolescents who contracted HIV through vertical transmission. Qualitative research using descriptive phenomenology was conducted at Botswana-Baylor Children’s Clinical Centre of Excellence. Data was collected using in-depth individual semi-structured interviews. Eight (8) adolescents between 14 and 19 years who had been on ART for minimum of 4 years were interviewed. Thematic analysis of data was done and five (5) themes emerged from the participants' description of the experience of taking ART over a long period of time. The themes that emerged indicated the factors that influence adherence to ART, and they included knowledge and positive beliefs about ART, need for support, ART difficult treatment regimen, having a regular doctor and psychosocial emotional needs. The findings suggested that the adolescents who contracted HIV through vertical transmission require support while continuing on a simplified long-term ART regimen after an assessment of their psychological well beings and periodic checks. / Health Studies / M.A. (Public Health)

Factors influencing adherence

Adolescents

Antiretroviral therapy

Vertical transmission

Human immunodeficiency virus

616.9792

HIV infections -- Treatment -- Botswana

Teenagers -- Diseases -- Botswana

Virus diseases -- Treatment -- Botswana

Antiretroviral agents -- Botswana

HIV and AIDS in the workplace : the role of the employee assistant practitioners

Matarose-Molehe, Martha Mpuseng

12 January 2015

The purpose of this study is to explore the EAP environment and provide a better understanding of the related roles of the Employee Assistant Practitioners/Professionals (EAPs) in respect of their treatment of various forms of illnesses in the workplace – particularly HIV and AIDS. The EAP role is not aligned to any individual profession, as it is designed to match employees’ holistic needs. It is in this context that the repertoire of EAP roles would include caring, psycho-social, therapeutic and technical skills. The EAP role is therefore endowed with the potential to meet a range of inter-departmental and multi-disciplinary needs – such as Nursing, Allied Health Professions, and Healthcare Sciences. A generic Assistant Practitioners Performance Management system (scorecard) had to be developed and agreed to with the City of Johannesburg’s (CoJ) Management in order to maintain consistency when developing APE programmes and roles. Notwithstanding the fact that the Employee Assistant Practitioners do also address the growing HIV/AIDS concerns in the workplace – including psycho-social problems of employees and their families – there is minimal acknowledgment of the EAPs’ roles, and little recognition of their welfare and well-being programmes. Drawing eclectically from various inter-related disciplinary terrains, the study centripetally explores the roles of EAPs as well as HIV/AIDS frameworks in the workplace. Quantitative and qualitative descriptive research methods were employed to assess challenges encountered by the City of Johannesburg (C.o.J) employees and their dependants. Questionnaires were used for the data collection of this study. The repertoire of participants in the study (n=55) comprised of doctors, social workers, nurses, HR officers, and other CoJ employees themselves. vi The questionnaire became the pivotal quantitative data analysis reference point ias it focused on numbers or quantities, and less on the qualitative analysis, which focused on differences in quality. The results of the study are based on numeric analysis and statistics to quantify the qualitative analysis. The prevalence of fewer participants was largely influenced by the depth of the data collection process, which did not allow for large numbers of research participants. The findings of the study revealed, amongst other factors, that there was an unsurpassed need to integrate different HIV/AIDS frameworks in order that the roles of EAPs becomes more effectively and efficiently defined and executed. The roles of EAPs were hitherto not well defined, resulting in duplication and confusion of service delivery to some employees utilising the EAP services. However, some of the EAP roles are highly appreciated and increasingly supported by managers and employees. Based on the findings of the study, recommendations were made for clarifying and extending the criticality of EAP roles and functions. / Health Studies / Ph. D. (Health Studies)

Employee assistance programme

Employee service delivery

Legal aspects

Psycho-social aspects

Quality of work life

Human Immunodeficiency Virus

Acquired Immune Deficiency Syndrome

362.106

HIV infections -- Treatment

AIDS (Disease) -- Treatment

Occupational health services

Work environment

Prevalence and predictors of immunologic failure among HIV patients on HAART in southern Ethiopia

Kesetebirhan Delele Yirdaw

20 August 2015

Immunologic monitoring is part of the standard care for patients on antiretroviral treatment. Yet, little is known about the routine implementation of immunologic monitoring in Ethiopia. This study assessed the pattern of immunologic monitoring, immunologic response, level of immunologic treatment failure and factors related to it among patients on antiretroviral therapy in selected hospitals in southern Ethiopia. A retrospective longitudinal analytic study was conducted using documents of patients started on antiretroviral therapy. A total of 1,321 documents of patients reviewed revealed timely immunologic monitoring were inadequate. Despite overall adequate immunologic response, the prevalence of immunologic failure was 11.5% (n=147). Having WHO Stage III/IV of the disease and a higher CD4 (cluster differentiation 4) cell count at baseline were identified as risks for immunologic failure. These findings highlight the magnitude of the problem of immunologic failure. Prioritizing monitoring for high risk patients may help in effective utilisation of meager resources / Health Studies / M.A. (Public Health)

Human Immunodeficiency Virus

CD4 cell

Adherence

Immunologic treatment failure

Antiretroviral treatment failure

Prevalence

Patient

Predict

615.79240963

Highly active antiretroviral therapy

Addressing Adherence to Antiretroviral Therapy in Ouagadougou, Burkina Faso: Insights from hospital ethnography

Munro, Kimberly

08 1900

L'épidémie de l'infection au virus de l'immunodéficience humaine (VIH) constitue une crise majeure en santé publique de nos jours. Les efforts de la communauté internationale visent à rendre les traitements antirétroviraux (TARV) plus accessibles aux personnes vivant avec le VIH, particulièrement dans les contextes à ressources limitées. Une observance quasi-parfaite aux TARV est requise pour tirer le maximum de bénéfices thérapeutiques à l'échelle individuelle et à l'échelle populationnelle. Cependant, l’accroissement de la disponibilité des TARV s'effectue dans des pays africains qui disposent de systèmes de santé fragiles et sous-financés. Ceux-ci souffrent également d'une pénurie de personnel de santé, lequel joue un rôle central dans la mise en oeuvre et la pérennité des interventions, notamment celle du soutien à l'observance thérapeutique. La présente étude ethnographique relate l'expérience de personnel de santé dans la fourniture des services de soutien à l'observance dans un contexte de ressources limitées et d'accroissement de l'accès aux TARV. L'étude a été menée dans deux centres hospitaliers de la capitale du Burkina Faso, Ouagadougou. Trois conclusions principales sont mises au jour. Tout d'abord, une bonne organisation – tant logistique que matérielle – dans la provision de services de soutien à l'observance est capitale. L’infrastructure d’observance doit aller au-delà des unités de prise en charge et s’intégrer au sein du système de santé pour assurer un impact durable. De plus, la provision des TARV dans le cadre d'une prise en charge médicale exhaustive est essentielle pour un soutien à l'observance efficace. Ceci implique la présence de professionnelles de santé en nombre suffisant et disposant d‘outils pour soutenir leur pratique clinique (tests de laboratoire, traitements pour infections opportunistes), ainsi que des mécanismes pour leur permettre d’aider les patients à gérer la vie quotidienne (gratuité des services, programmes d’alphabétisation et soutien psychosociale). Enfin, une amélioration de la coordination des programmes VIH au niveau national et international est nécessaire pour assurer une prise en charge cohérente au niveau local. La programmation conçue dans les pays étrangers qui est incomplète et de courte durée a un impact majeur sur la disponibilité de ressources humaines et matérielles à long terme, ainsi que sur les conditions de travail et de prestation de services dans les unités de soins. / The human immunodeficiency virus (HIV) epidemic is the most pressing public health crisis of modern times. Present international focus targets expanding access to life-saving antiretroviral treatment (ART) for people living with HIV/AIDS – referred to as treatment scale-up- in contexts with limited resources. Near perfect adherence to ART regimens is required to maximize individual and public health outcomes. ART is being scaled-up in African countries with under-funded, fragile health systems. These health systems are further plagued by a shortage of health professionals who play a critical role in the implementation and sustainability of ART programmes, including the provision of adherence support. This ethnographic study sought to explore the experience of health providers in addressing adherence to ART in settings of limited resources where ART is being scaled-up. The study took place in two hospital centres in the capital city of Burkina Faso; Ouagadougou. The study led to three broad conclusions. First, good organization is imperative in the delivery of adherence support services, both in terms of logistics and materiality. This infrastructure must extend beyond the level of the hospital ward, to the level of the health sector in order to ensure a sustainable impact. Second, the provision of ART within a comprehensive package of care is an essential component of effective adherence support. This involves equipping providers with tools to assist them in their clinical practice (laboratory monitoring, treatment for opportunistic infections, and additional staff) as well as mechanisms for them to help patients negotiate the trials of daily life (gratuity of care, literacy support, psychosocial support). Third, there is a need for improved coordination of nationally and internationally-led HIV programming for coherent service provision at the local level. Limited and short-term external funding affects the long-term availability of material and human resources, as well as working conditions and service provision on the wards. The results of the study contribute to the existing academic literature on ART adherence, to the design of future research projects, and to the organization of adherence support services.

human immunodeficiency virus

antiretroviral treatment

adherence

health systems

hospital ethnography

virus de l'immunodéficience humaine

traitement antirétroviral

observance thérapeutique

systèmes de santé

ethnographie hospitalière

Association entre les dérégulations des cellules dendritiques et les altérations des lymphocytes B présentes chez les patients infectés par le VIH

Fontaine, Julie

11 1900

La dérégulation du compartiment B est une conséquence importante de l’infection par le virus de l’immunodéficience humaine (VIH), qui peut mener à des manifestations autoimmunes et ultimement à des lymphomes B. Parmi les premières anomalies détectées, on dénote l’activation polyclonale, reflétée par la présence d’hyperglobulinémie (hyper-Ig) et des titres élevés d’autoanticorps chez les patients. On observe également une altération des dynamiques des populations, notamment une expansion de la population des cellules matures activées. De plus, les patients évoluent vers l’incapacité de générer une réponse humorale efficace, et sont sujets à une perte de la mémoire immunologique en phase chronique, caractérisée par une diminution de la population des cellules mémoires et par l’épuisement cellulaire. Toutefois, on connaît très peu les mécanismes impliqués dans de telles altérations. Les cellules dendritiques (DC) sont parmi les premières populations cellulaires à rencontrer et à propager le VIH lors d’une infection, et s’en trouvent affectées directement et indirectement, par le virus et ses composantes. On retrouve en effet une diminution des fréquences de DC dans le sang, les muqueuses et les organes lymphoïdes de patients infectés par le VIH, ainsi qu’un blocage au niveau de la maturation cellulaire. Toutefois, un débat perdure quant à l’apparition de ces altérations durant la phase aigüe de l’infection, et à la restauration des fréquences et des fonctions des DC chez les patients sous traitement. Cette controverse est due à la rareté des études longitudinales incluant des suivis qui s’échelonnent de la phase aigüe à la phase chronique de l’infection. Les DC jouent un rôle important dans le développement, la survie et l’activation des lymphocytes B, de façon T-dépendante et T-indépendante, notamment via des facteurs de croissance tel que BLyS (B lymphocyte stimulator). Par conséquent, nous formulons l’hypothèse que dans le cadre d’une infection VIH, les altérations observées au niveau des cellules B sont modulées par les DC. L’objectif majeur de cette étude est donc d’évaluer l’implication potentielle des DC dans les altérations des cellules B au cours de l’infection par le VIH. Pour ce faire, nous avons d’abord caractérisé de façon longitudinale le statut des populations de DC du sang périphérique de patients infectés au VIH et présentant différents types de progression de la maladie. Cela nous a permis d’évaluer la présence d’une corrélation entre les dynamiques de DC et le type de progression. Par la suite, nous avons évalué la capacité des DC à exprimer BLyS, puis mesuré sa concentration ainsi que celles d’autres facteurs de croissance des cellules B dans le plasma des patients. Enfin, nous avons caractérisé le statut des lymphocytes B, en fonction du stade de l’infection et du taux de progression clinique des patients. Cette étude démontre une diminution de la fréquence des populations de DC myéloïdes (mDC) dans le sang de patients infectés par le VIH sujets à une progression clinique. Cette diminution est observée dès le stade aigu de l’infection et au-delà du traitement antirétroviral (ART). Des concentrations élevées de MCP-1 (monocyte chemotactic protein), MIP (macrophage inflammatory protein) -3α et MIP-3β suggèrent la possibilité d’un drainage vers des sites périphériques. Nous observons également des niveaux supérieurs à la normale de précurseurs CD11c+CD14+CD16- en phase chronique, possiblement liés à une tendence de régénération des DC. Les patients en phase chronique présentent de hautes concentrations plasmatiques de BLyS, reflétée par un haut taux d’expression de cette cytokine par les mDC et leurs précurseurs. Parallèlement, nous observons une expansion des cellules B matures activées ainsi que des taux élevés d’IgG et IgA dans le sang de ces patients. De plus, nous constatons l’expansion d’une population de cellules B qui présente à la fois des caractéristiques de cellules B immatures transitionnelles (TI, transitional immature), et de cellules B recirculantes activées de la zone marginale (MZ, marginal zone), considérées ici comme des «précurseurs/activées de la MZ». Cette étude démontre aussi, chez les progresseurs lents, une meilleure préservation du compartiment des DC du sang périphérique, accompagnée d’une augmentation de précurseurs des DC de phénotype CD11c+CD14+CD16+, ainsi que des concentrations plasmatiques et niveaux d’expression normaux de BLyS. Conséquemment, nous n’avons pas observé d’augmentation des cellules B matures activées et des cellules B précurseurs/activées de la MZ. Toutefois, la fréquence des cellules B matures de la MZ est diminuée, reflétant possiblement leur recrutement vers des sites périphériques et leur contribution à un mécanisme actif de contrôle de la progression de la maladie. L’ensemble de ce travail suggère que dans le cadre d’une infection au VIH, les altérations observées au niveau des DC modulent les anomalies des cellules B. Par conséquent, le maintien de l’équilibre des fonctions DC, notamment les fonctions noninflammatoires, pourrait avoir un impact important dans la prévention de la progression de maladies associées aux altérations du compartiment des cellules B. / Dysregulations of the B cell compartment are an important consequence of human immunodeficiency (HIV) infection, which can lead to auto-immune manifestations and ultimately to B cell lymphomas. One of the first alterations is polyclonal activation, reflected by hyperglobulinemia (hyper-Ig) and elevated autoantibody titers. We can also observe alterations in population dynamics, namely an expansion of the pool of activated B cells. Furthermore, HIV infected patients evolve towards the incapacity to generate effective humoral responses, and experience a loss of immunological memory in the chronic phase, characterized by a decrease in the memory B cell pool and cell exhaustion. The mechanisms involved in this phenomenon are poorly understood and thus remain to be elucidated. Mucosal dendritic cells (DC) are among the first cell populations to encounter HIV during an infection and are directly and indirectly affected by the virus and viral components. Indeed, HIV infected individuals present decreased DC frequencies in their blood, mucosaeand lymphoid organs, as well as a block in DC maturation process. However, whether these defects appear as soon as the acute phase and persist beyond ART, remains controversial. This is mainly due to the scarcity of longitudinal studies including patients’ visits from the earliest phases of infection and following ART. DC play an important role in T-dependent and T-independent B cell development, survival and activation, namely through the production of growth factors such as B Lymphocyte Stimulator (BLyS). Therefore, we hypothesize that B cell abnormalities in HIVinfected individuals may be modulated by altered DC populations. The main objective of this study is to evaluate DC involvement in the establishment of B cell alterations related to HIV infection. We have thus first characterized the DC status by longitudinally assessing the dynamics of peripheral blood DC populations of HIV infected individuals with different rates of disease progression. This allowed us to evaluate the potential correlation between DC population dynamics and rate of disease progression. We have then evaluated BLyS expression by mDC and their precursors, and measured plasma concentrations of BlyS and other cytokines with B cell growth factor properties. Finally, we have characterized the dynamics of blood B cell populations, with regard to the phase of HIV infection and the rate of clinical progression. We demonstrate a decrease in the frequencies of blood myeloid DC (mDC) in HIV progressors. This drop was observed as early as in the acute phase and following the initiation of ART. Elevated blood concentrations of monocyte chemotactic protein (MCP) -1, macrophage inflammatory protein (MIP) -3α and MIP-3β suggest that the observed decrease is due to recruitment to peripheral sites. However, this hypothesis will be tested in a subsequent projet. We have also observed an increase of monocytic CD11c+CD14+CD16- DC precursors in chronic phases, possibly reflecting the high DC turnover. Furthermore, chronically infected HIV progressors present elevated blood BLyS concentrations, and high BLyS expression by DC and DC precursors. In parallel, these patients present increased frequencies of blood mature activated B cells as well as hyper IgG and IgA. Interestingly, we also observe expansion of a B cell population with features of precursors/activated marginal zone (MZ) B cells. On the other hand, slow progressors show a better preservation of their mDC compartment, accompanied by an increase in DC precursors with a CD11c+CD14+CD16+ phenotype. These patients present normal BLyS plasma concentrations and membrane expression on DC and precursors. In parallel, they have normal frequencies of blood mature activated B cells and precursors/activated MZ B cells. However, we found decreased frequencies of mature MZ B cells, suggesting recruitment to peripheral sites and involvement in active control of disease progression. Our results suggest that, in an HIV infection, alterations observed in the DC compartment contribute to B cell abnormalities. Therefore, it is crucial to maintain the equilibrium of DC fonctions, namely non-inflammatory functions, in order to prevent progression of disease attributable to dysregulation of the B cell compartment.

Virus de l'immunodéficience humaine

Cellules dendritiques

Cellules B

BLyS

Progression clinique

Inflammation

Human immunodeficiency virus

Blood

Dendritic cells

B cells

Clinical progression

BLyS

Inflammation

L'impact des cellules dendritiques dans la dérégulation des cellules B dans un contexte d'infection au virus d'immunodéficience humaine

Chagnon-Choquet, Josiane

12 1900

Les cellules dendritiques (DC) sont parmi les premières cellules à rencontrer le virus d’immunodéficience humaine (VIH) au niveau des muqueuses. De plus, le fait que les DC sont, de manière directe ou indirecte par le virus et ses composantes, altérées tant par leur nombre, leur phénotype et leur fonction suggère leur implication dans les dérégulations des cellules B. Selon cette hypothèse, des études longitudinales impliquant des individus infectés au VIH-1 présentant différents profils de progression clinique menées dans notre laboratoire ont démontré que les altérations des cellules B sont concomitantes à une augmentation de l’expression de BLyS/BAFF dans le sang ainsi que par les DC myéloïdes (mDC) sanguines. De plus, lors de travaux antérieurs utilisant le modèle murin VIH-transgénique, les altérations des cellules B ont démontré une implication des DC et d’un excès de BLyS/BAFF, et ce, dépendamment du facteur négatif du VIH (Nef). Dans cette optique, nous investiguons dans cette présente étude l’implication de Nef dans la modulation du phénotype des DC ainsi que dans les dérégulations des cellules B. Chez tous les patients virémiques infectés au VIH-1, nous avons détecté la présence de Nef dans le plasma ainsi qu’au niveau des mDC et de leurs précurseurs d’origine monocytaire, tout au long du suivi de la progression clinique et au-delà de la thérapie antirétrovirale (ART). La surexpression de BLyS/BAFF est associée à la présence de Nef au niveau des mDC et de leur précurseur.. Des essais in vitro ont permis de démontrer l’induction d’un phénotype proinflammatoire par des mDC dérivés de monocytes lorsqu’en présence de Nef soluble, via l’augmentation de l’expression de BLyS/BAFF et de TNF-α, et où cet effet est bloqué par l’ajout de l’acide rétinoïque. Nos résultats suggèrent donc que Nef est impliquée dans le déclenchement et la persistance des dérégulations des cellules B retrouvées chez les individus infectés au VIH-1. Basé sur nos observations, une thérapie adjointe impliquant le blocage de BLyS/BAFF et/ou Nef pourrait contribuer au contrôle de l’inflammation et des altérations des cellules B. De plus, la quantification de Nef post-ART pourrait s’avérer utile dans l’évaluation du statut des réservoirs. Précédemment, nous avons démontré que les dérégulations des cellules B sanguines de ces mêmes individus présentant un profil de progression rapide et classique sont accompagnées par l’augmentation de la fréquence d’une population partageant des caractéristiques des cellules B transitionnelles immatures (TI) et des cellules B de la zone marginale (ZM), que nous avons nommé les cellules B précurseur de la ZM. Toutefois, cette population est préservée chez les contrôleurs élites, chez qui nous avons trouvé une diminution significative de la fréquence des cellules B de la ZM présentant des marqueurs phénotypiques plus matures. Récemment, ces cellules ont été associées à un potentiel de fonction régulatrice (Breg), motivant ainsi notre poursuite, dans cette étude, de la caractérisation de ces cellules B. Comme pour les individus non infectés au VIH-1, nous avons démontré que les cellules B matures de la ZM contrôlent leur capacité de production d’IL-10 chez les contrôleurs élites, contrairement à une augmentation chez les progresseurs rapides et classiques. Aussi, les cellules B précurseur de la ZM des contrôleurs élites fournissent une expression importante de LT-α lorsque comparés aux individus non infectés au VIH-1, alors que cet apport de LT-α est attribué aux cellules B TI chez les progresseurs. Le contrôle de la progression clinique semble associé à un ratio en faveur de LT-α vs IL-10 au niveau des cellules B précurseur de la ZM. Nos résultats suggèrent qu’un maintien de l’intégrité du potentiel régulateur ainsi qu’une expression augmentée de LT-α par les cellules B de première ligne, telles les populations de la ZM, sont impliqués dans le contrôle de la progression clinique du VIH-1, possiblement par leur contribution à la modulation et l’homéostasie immunitaire. De telles populations doivent être considérées lors de l’élaboration de vaccins, ces derniers cherchant à générer une réponse protectrice de première ligne et adaptative. / In the context of HIV-1 infection, DC are amongst the first cells to encounter the virus at the mucosal surfaces, and are directly and indirectly affected by the virus or its components. The fact that DC are altered in number, phenotype and function in the context of HIV, suggest they may be involved in driving B cell dysregulations, which occur as early as in the acute phase of HIV-infection and are not fully restored by therapy. As such, in recent longitudinal studies involving HIV-infected individuals with different rates of disease progression, we have shown that B cell dysregulations were associated with increased BLyS/BAFF expression in plasma and by blood myeloid DC (mDC). In previous work with HIV-transgenic mice, B cell dysregulations involved DC, excess BLyS/BAFF and were dependant on the HIV negative factor (Nef). We therefore aim to investigate the impact of HIV-Nef in modulating DC phenotype and B cell dysregulations. Blood samples from the same HIV-infected individuals as mentioned above were studied, following the identical longitudinal scheme. HIV-Nef was detected in plasma and beared by blood mDC and mDC precursors of all viremic HIV-infected patients, throughout follow-up and beyond therapy. Detection of HIV-Nef in mDC and their precursors was associated with BLyS/BAFF over-expression. In vitro, soluble HIV-Nef drove monocyte-derived mDC towards a pro-inflammatory phenotype by increasing the expression of BLyS/BAFF and TNF-α. Futhermore, this effect was blocked by the addition of retinoic acid. These data suggest that HIV-Nef is involved in the driving and persistence of B cell dysregulations in HIV-infected individuals. Based on our observations, therapeutic blocking of BLyS/BAFF and/or Nef could help control inflammation and B cell disorders. Moreover, measurement of HIV-Nef post-therapy may be useful in assessing reservoir status. We have previously shown that B cell dysregulations in the blood of HIV-infected rapid and classic progressors were accompanied by the increased frequency of a population presenting characteristics of both transitional immature (TI) and marginal zone (MZ) B cells, which we have termed “MZ-like precursors”. However, this population was unaltered in ELITE controllers (EC), even though we found significantly lower frequencies of more mature MZ-like B cells. These results suggest that such first line B cell populations may be involved in the battle against HIV-1. Interestingly, MZ-like B cell populations have recently been associated with Breg potential. As such, we found that as for HIV negative individuals, mature MZ-like B cells control their capacity of IL-10 production in EC. In contrast, HIV-1-infected rapid and classic progressors presented increased relative frequencies of MZ-like B cells expressing IL-10. Interestingly, in EC, blood MZ-like precursors provided substantial LT-α expression when compared to HIV negative individuals, and in contrast to that found in rapid and classic progressors, where significant LT-α expression was provided by TI B cells. In fact, the degree of control of disease progression seems associated with greater LT-α to IL-10 ratio within the MZ-like precursors population. Our results therefore suggest that maintenance of Breg integrity and increased LT-α expression by first line B cells, such as MZ-like populations, is involved in the control of HIV-1 disease progression, possibly trough contribution to immune modulation and homeostasis. Soliciting such populations should be beared in mind in the design of vaccine strategies aiming at generating both first line and adaptive protective responses.

Virus de l'immunodéficience humaine

Nef

cellules dendritiques

cellules B

BLyS

BAFF

inflammation

progression clinique

contrôle de la progression

zone marginale

Human immunodeficiency virus

dendritic cells

B cells

IL-10

clinical progression

marginal zone

Support programme for facilitating the integration of nutrition and food security with HIV prevention, treatment and care

Nigusso, Fikadu Tadesse

01 1900

The purpose of this study was to develop a support programme for facilitating the integration of nutrition and food security with HIV prevention, treatment and care. The study was organised in three phases. Phase one was a quantitative cross-sectional survey that employed a structured interview with people living with HIV among selected two public hospitals and three health centres. The second phase employed focus group discussion with senior health experts to explore their perspective and experience in integrating nutrition and food security with HIV prevention, treatment, and care. The findings indicated that malnutrition and food insecurity were highly prevalent and significantly affected the treatment outcome and quality of life of PLWHA in the region. Socio-economic, clinical features and structural factors, such as educational status, place of residence, household income, source of drinking water, kind of toilet facility, inadequate dietary diversity, poor asset possession, opportunistic infections, duration on ART, CD4 cell count, and health system-related factors such as lack of viral and CD4 analysis laboratories and inconsistent antiretroviral medication supply were found as predictors of malnutrition and food insecurity. To cope up with the dire impact of malnutrition and food insecurity, short term, erosive and unsustainable food consumption coping strategies were employed. Based on the findings, the researcher developed a support programme for facilitating the integration of nutrition and food security with HIV prevention, treatment and care as phase three of the study. The developed programme is holistic and focuses on multi- and intersectoral collaboration to improve the treatment outcome, quality of life and overall wellbeing people living with HIV. / Health Studies / D. Litt. et Phil. (Health Studies)

Acquired immune deficiency syndrome

Food security

Human immunodeficiency virus

Integration

Nutrition

Programme

Support

616.97920654

AIDS (Disease) -- Prevention

AIDS (Disease) -- Diet therapy

AIDS (Disease) -- Nutritional aspects

HIV infections -- Diet therapy

HIV infections -- Nutritional aspects

Prevalence and predictors of immunologic failure among HIV patients on HAART in southern Ethiopia

Kesetebirhan Delele Yirdaw

20 August 2015

Immunologic monitoring is part of the standard care for patients on antiretroviral treatment. Yet, little is known about the routine implementation of immunologic monitoring in Ethiopia. This study assessed the pattern of immunologic monitoring, immunologic response, level of immunologic treatment failure and factors related to it among patients on antiretroviral therapy in selected hospitals in southern Ethiopia. A retrospective longitudinal analytic study was conducted using documents of patients started on antiretroviral therapy. A total of 1,321 documents of patients reviewed revealed timely immunologic monitoring were inadequate. Despite overall adequate immunologic response, the prevalence of immunologic failure was 11.5% (n=147). Having WHO Stage III/IV of the disease and a higher CD4 (cluster differentiation 4) cell count at baseline were identified as risks for immunologic failure. These findings highlight the magnitude of the problem of immunologic failure. Prioritizing monitoring for high risk patients may help in effective utilisation of meager resources / Health Studies / M. A. (Public Health)

Human Immunodeficiency Virus

CD4 cell

Adherence

Immunologic treatment failure

Antiretroviral treatment failure

Prevalence

Patient

Predict

615.79240963

Highly active antiretroviral therapy

Estado da vitamina D e sua relação com doenças cardiovasculares em indivíduos com HIV/AIDS em tratamento com antirretrovirais: uma revisão sistemática. / Vitamin D status and its relationship with cardiovascular diseases in patients with HIV/AIDS in treatment with antiretroviral: a systematic review.

Freitas, Alexandre Magnus Mourao e

06 March 2015

Este estudo faz uma revisão sobre a relação das concentrações de vitamina D e doenças cardiovasculares (DVC) em indivíduos com vírus da imunodeficiência humana e/ou síndrome da imunodeficiência adquirida (HIV/AIDS) em tratamento com terapia antirretroviral (TARV). Um total de 1.288 artigos foram recuperados dos bancos de dados do PubMed, EMBASE, OVID, Cochrane Central, ERIC, SIBi, SciELO, LILACS e Grey literature. Nove deles preencheram os critérios de seleção e foram inclusos nesta revisão sistemática. Existe uma alta prevalência da deficiência de vitamina D em indivíduos HIV-positivo, independentemente da região climática que vivem. Tanto a infecção pelo HIV-1 como a TARV podem interferir no metabolismo da vitamina D. Essa vitamina mostrou uma tendência a decrescer do momento antes da TARV ao depois da iniciação da TARV, sua deficiência foi mais prevalente em pacientes que fazem utilização da TARV do que aqueles que nunca a utilizaram e suas concentrações no organismo mostraram significantes associações com medidores da elasticidade arterial, como Espessamento Média-Íntima (EMI) e Dilatação Mediada por Fluxo (DMF). Essas alterações nos vasos e sistema circulatório predispõem doenças cardiovasculares, tais como, aterosclerose, trombose, infarto do miocárdio e acidente vascular cerebral. Portanto, apesar de existirem controvérsias, indivíduos HIV-positivo podem estar mais propensos ao desenvolvimento de DCV, não apenas pelos efeitos colaterais comuns da TARV e da infecção pelo HIV-1, mas também por estarem mais predispostos a terem hipovitaminose D, e as alterações causadas por este quadro em seu organismo. / This study reviewed the relationship of vitamin D levels and cardiovascular disease (CVD) in individuals with human immunodeficiency virus and/or acquired immunodeficiency syndrome (HIV/AIDS) in treatment with antiretroviral therapy (ART). A total of 1,288 articles were retrieved from the PubMed, EMBASE, Ovid, Cochrane Central, ERIC, SIBi, SciELO, LILACS and Grey literature databases. Nine of them met the selection criteria and were included in this systematic review. There is a high vitamin D deficiency prevalence in HIV positive individuals, regardless of climate area where they live. Both, HIV-1 infection and ART can interfere with the metabolism of vitamin D. This vitamin has shown a tendency to decrease from the moment before ART to the one after the initiation of ART. Its deficiency was more prevalent in patients who use ART than those who are ART-naïve. Vitamin D concentrations showed significant associations with markers of arterial dysfunction, such as carotid artery intima-media thickness (cIMT) and flow-mediated dilatation (FMD). These changes in vessels and circulatory system predispose CVD, such as atherosclerosis, thrombosis, myocardial infarction and stroke. Therefore, although there are controversies, HIV positive individuals may be more prone to the development of CVD, not just for the common side effects of ART and HIV- 1 infection, but also because they are predisposed to have vitamin D deficiency, and all the metabolic changes caused by this situation in his organism. Key-

Antiretroviral Theraphy (ART)

Cardiovascular diseases

Doenças cardiovasculares

Human Immunodeficiency Virus (HIV)

Terapia Antirretroviral (TARV)

Vírus da Imunodeficiência Humana (HIV)

Vitamin D

Vitamina D

Rôle des polymorphismes dans la région C-Terminale de l'enveloppe du VIH dans l'infection de cellules primaires / Impact of polymorphisms in the C-terminal region of the HIV envelope on infection of primary cells

Santos da Silva, Eveline

12 December 2013

Le virus de l'immunodéficience humaine (VIH) est responsable du syndrome d'immunodéficience humaine acquise (SIDA). Le virus est très variable et est classé en divers sous-types dont le sous-type B qui est le plus étudié et le C qui est le plus répandu. L'enveloppe (Env) à la surface du virus lui permet d'infecter des cellules du système immunitaire, parmi lesquelles les lymphocytes T CD4 (LT CD4) et les macrophages sont des cibles privilégiées. Nous avons étudié le rôle de variations de séquences dans la partie de Env qui n'est pas exposée à la surface du virus (la queue intravirale (gp41CT)). Nos résultats montrent que ce domaine contribue à la réplication du virus dans les LT CD4 et que des variations dans ce domaine entravent l'assemblage des protéines de structure du virus, diminuant la production de nouveaux virus. Ce défaut n'est pas observé dans les macrophages, suggérant qu'un facteur cellulaire est impliqué. Identifier ce facteur pourrait fournir de nouvelles cibles antivirales / The human immunodeficiency virus (HIV) is responsible for the pandemic of acquired immunodeficiency syndrome (AIDS). Being highly variable, the virus has been subdivided into viral subtypes. Subtype B is the most studied, while subtype C is the most spread. The envelope (Env) expressed at the surface of the virion enables infection of cells involved in the immune system, like CD4 cells (CD4 TL) and macrophages. We studied the Env region not exposed at the viral surface (intraviral tail, gp41CT), which also harbors sequence characteristics linked to viral subtype. Viruses with subtype C gp41CT had lower replication capacities in CD4 TL. Microscopy analysis showed a defect in clustering of the viral structural protein Gag, revealing that changes in gp41CT affect assembly of all viral components. This defect was seen in CD4 TL but not in macrophages, suggesting the involvement of a cellular factor. Identifying this factor could open new therapeutic leads

Virus de l'immunodéficience humaine

Sous-type non-B

Lymphocytes CD4+

Transmission virale

Queue intracytoplasmique de gp41

Macrophages

Human immunodeficiency virus

Non-B subtype

CD4 T cells

Viral transmission

Gp41 cytoplasmic tail

Macrophages

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