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Comparison of the distribution of combined immunological and virological responses in adult HIV positive patients across Antiretroviral Therapy (ART)providers in Tshwane : a multilevel analysisWandai, Elia Muchiri January 2014 (has links)
Background: Immunological and virological responses to ART are important outcome indicators that are mostly used to evaluate the success of an ART program. A comparative performance between ART providers based on the two outcomes can be useful in optimising resources to underperforming providers and advising quality improvement plans.
Aim: To compare immunological and virological responses of ART for adult HIV positive patients between providers in Tshwane District, Gauteng Province, South Africa.
Methodology: This study was an analytical observational study that retrospectively compared patient treatment outcomes on immunological and virological responses between 16 Antiretroviral Therapy (ART) providers. The analysis compared baseline patients’ status on these two outcomes with their statuses after 6 and12 months on ART. Ordinary logistic regression was used to calculate Standardised Incidence Ratios (SIR), while multilevel model analysis was used to calculate specific provider random effects of poor immunological and virological responses.
Results: After 6 months of treatment, the SIR of poor immunological outcome for all clinics under study, as predicted by the unadjusted logistic regression models was 0.29 (95% CI: 0.27-0.31), but varied from a low of 0.14 (95% CI: 0.00-0.40) to a high of 0.66 (95% CI: 0.13-1.20) between the clinics. Two clinics had a Standardised Incidence Ratio (SIR) of poor immunological response that was significantly below 1 (poor immunological rate below average), while three clinics had an SIR above 1 (poor immunological rate above average) under the unadjusted logistic models. After adjusting for the effects of gender, age, drug combination, religion and present virological status, no clinic had a SIR that was significantly below 1, but two clinics had a SIR that was significantly above 1.
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Under the logistic multilevel (MLLR) analysis, the unadjusted model flagged two clinics whose clinic specific effects were below zero (lower rate of poor immunological outcome below that of the total sample) and one clinic whose clinic specific effect was above zero (higher rate of poor immunological outcome below the total sample rate). The adjusted model showed that no clinic had residual effects that were significantly below or above zero. The confidence intervals for MLLR model were found not to be wider than those of the logistic regression (LR) models particularly for clinics with small sample sizes. A number of clinics changed the relative order of their SIR/random effects after case-mix adjustments under both the LR and MLLR modelling.
For poor virological response, both the LRD and MLLR models indicated no clinic specific effects. The predicted poor virological response rate by the case-mix unadjusted LR model was 0.12 (95% CI 0.11 - 0.13). All clinics except one had SIRs that were not significantly different from 1. After adjusting for CD4 count and age, no clinic had an SIR that was significantly different from 1.
Conclusions: Case-mix or patients baseline characteristics explained much of the variation in the Standardised Incidence Ratios (SIR) of poor immunological outcome after 6 months of patient treatment, while provider (clinic) specific effects explained much of the variation after 12 months of treatment. After 6 months of treatment, the results also showed that there were significant differences in the SIR between the clinics before case-mix adjustments, but the differences disappeared after case-mix adjustments. This shows that comparison of treatment outcomes between providers (clinics) can be misleading if no proper adjustment are made for confounding factors.
Differences in the SIRs for poor virological outcome, after 6 months of patient treatment were no longer significant between clinics after taking account of CD4 count and age. / Dissertation (MSc)--University of Pretoria, 2014. / gm2014 / School of Health Systems and Public Health / unrestricted
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Immunological and virological responses in highly active antiretroviral therapy naive patients exposed to isoniazid preventive therapyManda, Robert January 2009 (has links)
This study compare immunological and virological outcomes in antiretroviral therapy naïve patients exposed to Isoniazid prevention treatment.Medical records of antiretroviral naïve patients managed in the public sector from 1st January 2006 to 31st December 2006 were analysed.Multivariate analysis of variance showed that each treatment group achieved statistically significant increases in CD4+ cell count and viral load decay at each follow-up time point. Pairwise post hoc contrast tests showed patients in NVPipt-past group and EFVipt-past group to have superior immunological and virological outcomes respectively. / Health Studies / M.A. (Public health)
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Virological failure among adult HIV positive patients three years after starting antiretroviral treatment at Mankweng Hospital, Limpopo Province, RSALekoloana, Matome Abel January 2014 (has links)
Thesis (MPH.) --Univesity of Limpopo, 2014 / Background: The main goal of HAART is to achieve maximal viral suppression. However, with poor adherence to therapy the chances of achieving and maintaining successful viral suppression are decreased, leading to virological failure. And virological failure has been recognized by WHO as one of the early warning signs of drug resistance. This operational research sought to explore virological failure as a treatment outcome to evaluate program performance at a facility level.
Methods: Purposive sampling as per inclusion and exclusion criteria was used to retrospectively review clinical records of the first 700 adult HIV positive patients (350 males and 350 females) who initiated antiretroviral treatment between April 2004 and December 2007 at this adult HIV clinic, were followed up for at least 3 years and treated according to the South African government’s National Department of Health 2004 HIV treatment guidelines for adults and adolescents.
Major Results: 268 clinical records, 97 (27.71%) male and 171 (58.86%) female records were eligible for inclusion in the study. The proportion of females was higher (63.8%) than males (32.8%) with an average age of 38.95 years. 24 (8.9%) patients in the study sample experienced virological failure during the study period; 11 (11.3%) males and 13 (7.6%) females. Two-thirds (66.6%) of patients who failed to suppress at their first viral load measurement proceeded to develop virological failure. Overall, there was no association of statistical significance between age, sex, baseline CD4 cell count and baseline regimen, and virological failure at various intervals, p> 0.05.
Conclusion: It was a challenge to keep patients in care but those that remained in care had good treatment outcomes with only 8.9% developing virological failure. Failure to suppress at first viral load preceded virological failure in the majority of patients.
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Immunological and virological responses in highly active antiretroviral therapy naive patients exposed to isoniazid preventive therapyManda, Robert January 2009 (has links)
This study compare immunological and virological outcomes in antiretroviral therapy naïve patients exposed to Isoniazid prevention treatment.Medical records of antiretroviral naïve patients managed in the public sector from 1st January 2006 to 31st December 2006 were analysed.Multivariate analysis of variance showed that each treatment group achieved statistically significant increases in CD4+ cell count and viral load decay at each follow-up time point. Pairwise post hoc contrast tests showed patients in NVPipt-past group and EFVipt-past group to have superior immunological and virological outcomes respectively. / Health Studies / M.A. (Public health)
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Avaliação da presença de mutações de resistência no gene da NS5B e do prognóstico da infecção pelo HCV através da IL-28B em pacientes monoinfectados com HCV no RJ / Evaluation of resistance mutations presence in the NS5B gene and prognosis of HCV infection throught IL-28B in HCV monoinfected patients of RJMagda Cristina Bernardino Castilho 27 March 2013 (has links)
Estima-se que a prevalência global da população mundial com hepatite C é de 3%. Pouco se sabe sobre a resposta ao tratamento com respeito à resistência viral. Algumas mutações no fragmento de 109 aminoácidos da NS5B são associadas com resistência ao interferon (IFN) e ribavirina (RBV). Estudos moleculares e clínicos identificaram fatores associados com o hospedeiro e vírus relacionados associada com a resposta ao tratamento, tal como o gene que codifica a IL-28B. Este estudo foi dividido em duas fases, cujos objetivos foram caracterizar a frequência de mutações que conferem resistência ao HCV e avaliar a relevância das mutações em pacientes Respondedores (R) ou Não Respondedores (NR) ao tratamento e caracterizar geneticamente as populações sobre polimorfismos genéticos nos SNPs da IL-28B em relação ao prognóstico da resposta ao tratamento. As amostras dos pacientes foram submetidas a testes de genotipagem e carga viral. As sequências geradas foram comparadas no BLAST e no banco de dados Los Alamos HCV. Realizamos o alinhamento das sequências homólogas e as mutações identificadas. Com base no genótipo e carga viral determinamos a classificação dos pacientes de acordo com a resposta à terapia. O DNA genômico foi isolado a partir de sangue periférico para a realização da tipagem de SNPs de IL-28B. A metodologia utilizada foi de PCR em tempo real utilizando sondas TaqMan SNP específico. A análise dos dados foi realizada utilizando GraphPad Prism com qui-quadrado, risco relativo (RR), Odds Ratio (OR) e intervalo de confiança de 95%, com um nível de significância de P <0,05. Foi encontrado na primeira fase deste estudo uma taxa significativa mutações associadas ao tratamento nas amostras estudadas. A prevalência de mutações associadas à resistência ao IFN e RBV bem como a novos medicamentos antivirais localizados no fragmento de 109 aminoácidos da NS5B foi examinado em 69 indivíduos infectados naïve no Rio de Janeiro, Brasil. Na segunda fase, as mutações foram clinicamente relevantes. Desde então, procuramos observar as diferenças entre melhor ou pior prognóstico de acordo com a imunogenética que mostrou diferenciação entre os grupos R e NR ao tratamento em relação ao prognóstico da resposta terapêutica. Quando as diferenças entre as sequências da NS5B e a resposta ao tratamento foram consideradas verificou-se que associada a mutação R254K, estava a C316N que poderia conduzir a uma não resposta à terapia no genótipo 1b. Os nossos dados também suportaram forte associação de IL-28B rs12979860, com elevada probabilidade de resposta à terapia de IFN + RBV. Nossos dados evidenciam a presença de pacientes virgens de tratamento que abrigam mutações de resistência previamente descritas na literatura. A análise dos fatores preditores de resposta virológica mostrou que a predição de boa resposta ou não ao tratamento e ainda da progressão da doença é dependente de uma importante interação entre a genética viral e a do hospedeiro. Fato este importante para que no momento de avaliação de diagnóstico e conduta terapêutica, o médico possa tomar medidas apropriadas para o tratamento de cada paciente individualmente independentemente do genótipo do HCV em questão. / It is estimated that the overall prevalence of the average world population with hepatitis C is 3%. Little is known about the treatment response with respect to viral resistance. Some mutations in the 109-aminoacid fragment of NS5B are associated to Interferon (IFN) and Ribavirin (RBV) resistance. Molecular and clinical studies have identified factors associated with the host and related viruses associated with response to treatment, as the gene encoding IL-28B. This study was divided into two phases whose objectives were to characterize the frequency of mutations conferring resistance to HCV viral evaluating the relevance of these in Responders (R) or Non-Responders (NR) patients to treatment and to characterize genetically the populations regarding genetic polymorphisms SNPs IL-28B in relation to prognosis of response to treatment for HCV. Patient samples were subjected to tests for genotyping and viral load. The sequences generated were compared in the BLAST and the Los Alamos database HCV. We conducted the alignment of homologous sequences and mutations identified. Based on virological parameters genotype and viral load determined the classification of patients according to response to therapy. Genomic DNA was isolated from peripheral blood for carrying out the typing of SNPs of IL-28B. The methodology used was real-time PCR using TaqMan probes specific SNPs. Data analysis was performed using GraphPad Prism with chi-square, relative risk (RR), Odds Ratio (OR) and confidence interval of 95% with a significance level of P <0.05. To study these biological parameters we associated the responsive patients, non-responders, the viral load, genotype, and IL-28B polymorphism to treatment outcome. We found in the first phase of this study a significant rate of treatment-associated mutations in the samples studied. The prevalence of mutations associated to resistance to interferon and ribavirin (IFN/RBV) as well new antiviral drugs located in the 109 aminoacid fragment of NS5B was examined in 69 Hepatitis C Virus drug naïve (HCV)-infected individuals in Rio de Janeiro, Brazil. In the second phase, the mutations revealed clinically relevant from the gene in question. Since then, we seek to observe the differences between better or worse prognosis according to immunogenetic showed that differentiation between the immunogenetics of the groups R and NR to treatment in relation to prognosis of therapeutic response. When the differences between the NS5B sequences at baseline and the treatment response were considered we found that R254K associated with C316N mutations could lead to a non-response to IFN-RBV therapy in genotype 1b. Our data also strong support the association of rs12979860 IL-28B polymorphism with high probability of response to IFN + RBV therapy. Our data highlight the presence of HCV genotypes from drug naïve patients harboring resistance mutations previously described in literature. The analysis of predictors virologic response demonstrated that the prediction of better or worse therapy response and further the disease progression is dependent of a significant interaction between viral and host genetics. This fact is important for diagnosis evaluation and clinical therapeutic, the medico can take appropriate measures to treat each individual patient irrespective of the genotype of HCV in question.
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Κλινικοί, γενετικοί και εργαστηριακοί προγνωστικοί παράγοντες σχετιζόμενοι με τη θεραπευτική απάντηση σε ασθενείς με χρόνια ηπατίτιδα C / Therapeutic response to patient with chronic hepatitis C due to clinical genetic and laboratory prognostic factorsΣυροκώστα, Ιουλία 26 June 2007 (has links)
H θεραπεία της χρόνιας ηπατίτιδας C παραμένει πρόκληση ,ιδιαίτερα για κάποιους ασθενείς ,μια και ποικίλοι παράγοντες που αφορούν τόσο τον ιό όσο και τον ξενιστή σχετίζονται με χαμηλότερη ιολογική απάντηση στη θεραπεία .Ο γονότυπος τύπου 1 και το υψηλό ιϊκό φορτίο έναρξης είναι οι κύριοι ιϊκοί παράγοντες που σχετίζονται με χαμηλότερη ιολογική απάντηση στη θεραπεία ,ενώ για τον ασθενή οι παράγοντες που σχετίζονται με χαμηλότερη ιολογική απάντηση στη θεραπεία είναι η μη ανταπόκριση ή η υποτροπή σε προηγούμενη θεραπεία ,η παρουσία κίρρωσης ,η Αφροαμερικανική καταγωγή, η μεγαλύτερη των 40 ετών ηλικία, η μη συμμόρφωση στη θεραπεία και η παχυσαρκία. Τα οβάλ ηπατοκύτταρα είναι πρόδρομα ηπατικά κύτταρα που έχουν συσχετισθεί με την εξέλιξη της ηπατικής νόσου και την ανάπτυξη ηπατοκυτταρικού καρκινώματος σε πειραματικά μοντέλα .Πρόσφατα έχουμε αποδείξει ότι σε περιπτώσεις χρόνιας ηπατίτιδας τύπου Β ή C η παρουσία πρόδρομων ηπατικών κυττάρων σχετίζεται με τη σοβαρότητα της νόσου το βαθμό ίνωσης και το σχετιζόμενο κίνδυνο ανάπτυξης ηπατοκυτταρικού καρκινώματος Αυτή η μελέτη προσπάθησε να εντοπίσει τους παράγοντες που παίζουν καθοριστικό ρόλο στην μακροχρόνια ανταπόκριση στη θεραπεία ασθενών με χρόνια ηπατίτιδα C καθώς και τον ρόλο που μπορεί να έχει σε αυτή τη διαδικασία η ύπαρξη πρόγονων ηπατικών κυττάρων . Στόχος του έργου είναι η διερεύνηση ποικίλων κλινικών γενετικών εργαστηριακών και ιστολογικών παραμέτρων οι οποίες σχετίζονται με τη θεραπεία σε ασθενείς με χρόνια HCV λοίμωξη. Δευτερογενής στόχος της μελέτης είναι ο καθορισμός ομάδων υψηλού κινδύνου για την ανάπτυξη κίρρωσης και ηπατοκυτταρικού καρκίνου. ΣΧΕΔΙΑΣΜΟΣ 135 ενήλικες ασθενείς με θετική PCR και με βιοψία ήπατος που πιστοποιούσε χρόνια ηπατίτιδα εισήχθησαν στη μελέτη και τυχαιοποιήθηκαν να λάβουν είτε μονοθεραπεία με 3 MU ιντερφερόνης a2b τρεις φορές την εβδομάδα για 24 εβδομάδες ή συνδιασμό με ιντερφερόνη ή ή πεγκυλιωμένη ιντερφερόνη a2a (40 KD) μία φορά την εβδομάδα και προσθήκη 1000ή1200 mg ριμπαβιρίνης για 24 ή 48 εβδομάδες ανάλογα τον γονότυπο .Όλοι οι ασθενείς παρακολουθούνταν για την ασφάλεια την αντοχή και την αποτελεσματικότητα στο τέλος της εβδομάδας 2, 4, 8 και κάθε 4 εβδομάδες κατά τη διάρκεια της θεραπείας . Μετά την ολοκλήρωση της θεραπείας οι ασθενείς παρακολουθούνταν στις εβδομάδες 4, 12, 24 . Το πρώιμο τελικό σημείο ήταν η απώλεια του μετρήσιμου RNA του ιού της ηπατίτιδας C (HCV- RNA < 100c/ml) την εβδομάδα 24 μετά το τέλος της θεραπείας . Για να μελετήσουμε τη συσχέτιση των πρόγονων ηπατικών κυττάρων με την ανταπόκριση στη θεραπεία μελετήθηκαν 77 ηπατικές βιοψίες από ισάριθμους ασθενείς με χρόνια ηπατίτιδα C. Σαν μάρτυρες χρησιμοποιήθηκαν 10 φυσιολογικές ηπατικές βιοψίες .29 ασθενείς που ανταποκρίθηκαν στη θεραπεία και είχαν αρνητική PCR στο τέλος της προκαθορισμένης περιόδου αποτέλεσαν την ομάδα (Α) .29 ασθενείς που δεν ανταποκρίθηκαν στη θεραπεία και είχαν θετική PCR στο τέλος της προκαθορισμένης περιόδου αποτέλεσαν την ομάδα (Β) και τέλος 19 ασθενείς που υποτροπίασαν μετά αρχική ανταπόκριση στη θεραπεία αποτέλεσαν την ομάδα (Γ).Εξετάσθηκαν τομές παραφίνης πάχους 4 μm και καταμετρήθηκαν τα κύτταρα με μορφολογία οβάλ ηπατοκυττάρων δηλαδή AFPmRNA(+) και πρωτεΐνες CK19 (+) CK7(+) LCA(-) KAI CD34(-) Τα αποτελέσματα εκφράστηκαν σε ποσοστό επί τις %για τα κύτταρα με τα αντίστοιχα μορφολογικά χαρακτηριστικά και συσχετίστηκαν με τις αντίστοιχες κλινικές παραμέτρους. Ηπατικά προγονικά κύτταρα παρουσιάστηκαν και στις 87 βιοψίες αν και ήταν σημαντικά λιγότερα στις βιοψίες ελέγχου. Σύμφωνα με την έκφραση AFPmRNA η επί της % έκφραση ήταν :Ομάδα Β 53.4+ 1.3 > Ομάδα Γ 49+1.8 > Ομάδα Α 30.7 + 1.9 Οι ασθενείς που έλαβαν ιντερφερόνη ανταποκρίθηκαν καλύτερα στη θεραπεία αν ήταν < 40 είχαν γονότυπος 3,ιστορικό IV Χρήσης ουσιών αρνητική PCR-HCV (-) στην εβδομάδα 24 μετά θεραπεία &είχαν απουσία κίρρωσης ενώ είχαν μικρότερη πιθανότητα ανταπόκρισης αν είχαν ηλικία >40 έτη γονότυπο 1 ιστορικό μετάγγισης, αυξημένη ALT ή παρουσία κίρρωσης. Οι ασθενείς που έλαβαν θεραπεία συνδιασμού είχαν ευνοϊκή πρόγνωση αν εμφάνιζαν γονότυπο 2 ή 3 και μη ευνοϊκή αν είχαν γονότυπο 1,4 παρουσία κίρρωσης& αυξημένη γGt . Οι αυξημένες τρανσαμινάσες δεν αποτελούσαν προγνωστικό δείκτη. Στους ασθενείς που έλαβαν θεραπεία με πεγκυλιωμενη ιντερφερονη η ηλικία ή η απουσία κίρρωσης δεν αποτελούσε ανεξάρτητο προγνωστικό παράγοντα αντίθετα με την παραμονή αυξημένης ALT & γGt στον 6ο μήνα θεραπείας Ανεξάρτητοι προγνωστικοί παράγοντες για οποιαδήποτε θεραπευτικό σχήμα ήταν η Ηλικία (< 40 ετών )και η απουσία κίρρωσης .Οι ασθενείς με Φυσιολογικές τρανσαμινάσες αποτελούσαν το 40% των ασθενών μας στη δική μας μελέτη φάνηκε ότι ανταποκρίνονται καλύτερα στη θεραπεία και Σε μικρότερο ποσοστό εμφανίζουν κίρρωση ( 7% ) ενώ οι ασθενείς με κίρρωση Ανταποκρίνονται λιγότερο καλά σε όλες τις θεραπείες εμφανίζουν μεγαλύτερη διάρκεια λοίμωξης,λιπώδες ήπαρ σε μεγαλύτερο ποσοστό (64%) Έχουν αυξημένα ποσοστά ALT-γGt. Ενώ η παρουσία κίρρωσης είναι ανεξάρτητη από τον γονότυπο Τα ΠΗΚ υπάρχουν συχνά σε βιοψίες ήπατος ασθενών με ΧΗC και εκφράζουν AFPmRNA Υπάρχει σημαντική συσχέτιση με τη σοβαρότητα της νόσου και την ανταπόκριση στη θεραπεία Τα ΠΗΚ μπορεί να αποτελέσουν ανεξάρτητο προγνωστικό παράγοντα για την ανταπόκριση στη θεραπεία σε ασθενείς με χρόνια ηπατίτιδα C. / The treatment of chronic hepatitis C remains a challenge, particularly for certain patients as several virus related and patient related factors are associated with a lower virologic response to therapy. Hepatitis C virus genotype 1and a high baseline viral load are the major viral factors associated with a lower virologic response to therapy .Patient –related factors include previous relapse or non response to treatment, the presence of cirrhosis, the African America ethnicity, older age, contraindications to treatment and obesity. Oval hepatocytes (HK) are liver stem cells which are involved in the progress of liver disease and hepatocellular carcinoma development in experimental models. We have previously shown that in case of chronic hepatitis type B or C the presence of OH is related to the severity of the disease, the grade of fibrosis and the relative risk for HCG development. This study try to determine the factors effect the long term suppression of hepatitis C virus and also investigate the correlation of OH expression with treatment response in patients with chronic hepatitis C. Design 135 patients aged 18 years or more with positive HCV RNA and liver biopsy, were enrolled and randomly allocated to one of three regimens: 3mega units (MU) interferon a2btree times a week for 24 weeks, 3mega units (MU) interferon a2b tree times a week, plus 1000-12000 mg ribavirine per day for 24 weeks or 48 weeks or peg interferon alfa-2a (40KD) plus ribavirine 1000 or 1200 per day for 24 or 48 weeks because of different genotype. All patients were assessed for safety, tolerance and efficacy and the end of weeks 2, 4, 8and every 4 weeks during treatment. After treatment was completed patients were followed up on weeks 4, 12 and 24.The primary endpoint was loss of detectable HCV-RNA (serum HCV-RNA <100 copies/ml) at week 24 after treatment. The study comprised 77 liver biopsies obtained to an equal number of patients with chronic hepatitis C virus infection. To investigate the correlation of OH expression with treatment response ten normal liver biopsy were used as control. Twenty nine patients were assigned as responders (group A) 29 as non responders (group B) and 19 as releasers (group C). Paraffin sections (4μm thick) were subjected. To OH expretion . Cells with morphologic features of OH that were AFPmRNA or protein +/CK19+/CK7+ and LCA (-) /CD 34(-) were scored. Results were expressed as% of positive cells following morphometric analysis and correlated with the clinical parameters. Findings Sustained virological response at 24 weeks after treatment was found in 18( 22% ) of the 88 patient treated for 24 weeks with 3mega units (MU) interferon a2b three times a week ,35 ( 47%) of the 74 patient treated with the combination regiment, and 28 (60% ) of the 47 treated with peg interferon alfa-2a (40KD) plus ribavirine. Logistic recreation identified five independent factors significantly associated with response to treatment with interferon: genotype 2 or 3 , age forty years or less, minimal fibrosis stage, Ivd users , PCR negative at 6 months. Tree factors associated with the response to combination therapy: genotype 2 or 3, no cirrhosis, and high γgt the only factors significantly associated with response with the pegylated interferon treatment is high levels of γgt and alt to the sixth month of treatment. Oval hepatocyte expression was present in all 87 specimens, being significantly lower in controls compared with cases of chronic hepatitis C. According to the AFPmRNA expression, the grade for % OH expression was: (group B) non responders: 53.4+- 1.3> (Group C ) relapses :49+_1.8>(group A) responders30.7 +_1.9The difference was recorded as follows>(group A) vs. Bp<0.01, group A vs. C p<0.01, group B vs. C p<0.05. Conclusions This study demonstrates that OH are frequently present and expresses AFPmRNA in liver biopsies of patients with chronic hepatitis C. There is a significant association with the severity of disease and with response to treatment and may provide additional prognostic information and predict prognosis in cases of chronic hepatitis c. Age forty years or less and the presence of cirrhosis or no, they are independent factors significantly associated with response to any treatment. Patient with persistently normal or almost normal transaminase levels have higher virological response to therapy and less frequently cirrhosis Patient with cirrhosis exhibit lower response rates to therapy. The presents of cirrhosis is not related to genotype . Patients have frequently high levels of alt and γgt before and six months after therapy and have a worse virological response to any therapy.
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Avaliação da presença de mutações de resistência no gene da NS5B e do prognóstico da infecção pelo HCV através da IL-28B em pacientes monoinfectados com HCV no RJ / Evaluation of resistance mutations presence in the NS5B gene and prognosis of HCV infection throught IL-28B in HCV monoinfected patients of RJMagda Cristina Bernardino Castilho 27 March 2013 (has links)
Estima-se que a prevalência global da população mundial com hepatite C é de 3%. Pouco se sabe sobre a resposta ao tratamento com respeito à resistência viral. Algumas mutações no fragmento de 109 aminoácidos da NS5B são associadas com resistência ao interferon (IFN) e ribavirina (RBV). Estudos moleculares e clínicos identificaram fatores associados com o hospedeiro e vírus relacionados associada com a resposta ao tratamento, tal como o gene que codifica a IL-28B. Este estudo foi dividido em duas fases, cujos objetivos foram caracterizar a frequência de mutações que conferem resistência ao HCV e avaliar a relevância das mutações em pacientes Respondedores (R) ou Não Respondedores (NR) ao tratamento e caracterizar geneticamente as populações sobre polimorfismos genéticos nos SNPs da IL-28B em relação ao prognóstico da resposta ao tratamento. As amostras dos pacientes foram submetidas a testes de genotipagem e carga viral. As sequências geradas foram comparadas no BLAST e no banco de dados Los Alamos HCV. Realizamos o alinhamento das sequências homólogas e as mutações identificadas. Com base no genótipo e carga viral determinamos a classificação dos pacientes de acordo com a resposta à terapia. O DNA genômico foi isolado a partir de sangue periférico para a realização da tipagem de SNPs de IL-28B. A metodologia utilizada foi de PCR em tempo real utilizando sondas TaqMan SNP específico. A análise dos dados foi realizada utilizando GraphPad Prism com qui-quadrado, risco relativo (RR), Odds Ratio (OR) e intervalo de confiança de 95%, com um nível de significância de P <0,05. Foi encontrado na primeira fase deste estudo uma taxa significativa mutações associadas ao tratamento nas amostras estudadas. A prevalência de mutações associadas à resistência ao IFN e RBV bem como a novos medicamentos antivirais localizados no fragmento de 109 aminoácidos da NS5B foi examinado em 69 indivíduos infectados naïve no Rio de Janeiro, Brasil. Na segunda fase, as mutações foram clinicamente relevantes. Desde então, procuramos observar as diferenças entre melhor ou pior prognóstico de acordo com a imunogenética que mostrou diferenciação entre os grupos R e NR ao tratamento em relação ao prognóstico da resposta terapêutica. Quando as diferenças entre as sequências da NS5B e a resposta ao tratamento foram consideradas verificou-se que associada a mutação R254K, estava a C316N que poderia conduzir a uma não resposta à terapia no genótipo 1b. Os nossos dados também suportaram forte associação de IL-28B rs12979860, com elevada probabilidade de resposta à terapia de IFN + RBV. Nossos dados evidenciam a presença de pacientes virgens de tratamento que abrigam mutações de resistência previamente descritas na literatura. A análise dos fatores preditores de resposta virológica mostrou que a predição de boa resposta ou não ao tratamento e ainda da progressão da doença é dependente de uma importante interação entre a genética viral e a do hospedeiro. Fato este importante para que no momento de avaliação de diagnóstico e conduta terapêutica, o médico possa tomar medidas apropriadas para o tratamento de cada paciente individualmente independentemente do genótipo do HCV em questão. / It is estimated that the overall prevalence of the average world population with hepatitis C is 3%. Little is known about the treatment response with respect to viral resistance. Some mutations in the 109-aminoacid fragment of NS5B are associated to Interferon (IFN) and Ribavirin (RBV) resistance. Molecular and clinical studies have identified factors associated with the host and related viruses associated with response to treatment, as the gene encoding IL-28B. This study was divided into two phases whose objectives were to characterize the frequency of mutations conferring resistance to HCV viral evaluating the relevance of these in Responders (R) or Non-Responders (NR) patients to treatment and to characterize genetically the populations regarding genetic polymorphisms SNPs IL-28B in relation to prognosis of response to treatment for HCV. Patient samples were subjected to tests for genotyping and viral load. The sequences generated were compared in the BLAST and the Los Alamos database HCV. We conducted the alignment of homologous sequences and mutations identified. Based on virological parameters genotype and viral load determined the classification of patients according to response to therapy. Genomic DNA was isolated from peripheral blood for carrying out the typing of SNPs of IL-28B. The methodology used was real-time PCR using TaqMan probes specific SNPs. Data analysis was performed using GraphPad Prism with chi-square, relative risk (RR), Odds Ratio (OR) and confidence interval of 95% with a significance level of P <0.05. To study these biological parameters we associated the responsive patients, non-responders, the viral load, genotype, and IL-28B polymorphism to treatment outcome. We found in the first phase of this study a significant rate of treatment-associated mutations in the samples studied. The prevalence of mutations associated to resistance to interferon and ribavirin (IFN/RBV) as well new antiviral drugs located in the 109 aminoacid fragment of NS5B was examined in 69 Hepatitis C Virus drug naïve (HCV)-infected individuals in Rio de Janeiro, Brazil. In the second phase, the mutations revealed clinically relevant from the gene in question. Since then, we seek to observe the differences between better or worse prognosis according to immunogenetic showed that differentiation between the immunogenetics of the groups R and NR to treatment in relation to prognosis of therapeutic response. When the differences between the NS5B sequences at baseline and the treatment response were considered we found that R254K associated with C316N mutations could lead to a non-response to IFN-RBV therapy in genotype 1b. Our data also strong support the association of rs12979860 IL-28B polymorphism with high probability of response to IFN + RBV therapy. Our data highlight the presence of HCV genotypes from drug naïve patients harboring resistance mutations previously described in literature. The analysis of predictors virologic response demonstrated that the prediction of better or worse therapy response and further the disease progression is dependent of a significant interaction between viral and host genetics. This fact is important for diagnosis evaluation and clinical therapeutic, the medico can take appropriate measures to treat each individual patient irrespective of the genotype of HCV in question.
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Infection par le VIH-1 groupe O : étude des caractéristiques épidémiologiques et de la réponse immuno-virologique aux antirétroviraux / HIV-1 group O infection : the study of the epidemiological characteristic of this infection and the immune-virological response to ART.Unal, Guillemette 28 May 2018 (has links)
Le VIH-1 groupe O (VIH-1/O) est un groupe divergent de VIH-1, endémique au Cameroun, 140 cas ont été identifiés en France depuis 1990. L’objectif de ce travail était d’évaluer l’impact de la diversité du VIH-1/O sur les caractéristiques épidémiologiques, l’évolution naturelle de l’infection et sur la réponse immuno-virologique aux traitements.En France, le recueil de données de suivi uniques portant sur 101 patients ont permis de mettre en évidence que l’évolution naturelle des VIH-1/O était intermédiaire entre celle des VIH-1/M et celle des VIH-2. La résistance aux INNTI des patients VIH-1/O a été confirmée in vivo. La réponse immuno-virologique aux traitements a été comparée entre les VIH-1/O et les VIH-1/M suivis dans des cohortes en France et dans le cadre d’un essai clinique au Cameroun.Une des caractéristiques des VIH-1/O est une CVp significativement plus faible que celle des VIH-1/M avant l’initiation du traitement. Cela n’a pas d’impact sur la survenue de l’indétectabilité, qui est similaire dans les deux groupes après un an de traitement. La réponse immunologique des patients VIH-1/O est globalement proche de celle des patients VIH-1/M en France. Cependant, la comparaison entre deux populations appariés suivis au Cameroun a montré une réponse immuno-virologique plus faible des patients VIH-1/O, sans que cela ait d’impact clinique.La prise en charge des patients VIH-1/O suivant les recommandations mises en place pour les VIH-1/M est donc efficace si elle ne comporte pas d’INNTI. / HIV-1 group O (HIV-1/O) is genetically distinct from HIV-1/M and is endemic in Cameroon while in France 140 HIV-1/O were diagnoses since 1990. The aim of this work was to characterize HIV-1/O epidemiological characteristics, infection natural evolution and immuno-virological response to treatment.In France, based on a large series of 101 HIV-1/O patients, we demonstrated that the natural evolution of HIV-1/O was in between the evolution of HIV-2 and HIV-1/M, but closer to HIV-1/M. We also confirmed in vivo HIV-1/O natural resistance to INNTI treatment. Then, we compared HIV-1/O and HIV-1/M immune-virological response to ARV treatment. In France, we compared data from two cohorts and a clinical trial was performed in Cameroun. One of the HIV-1/O characteristic is the lower CVp before treatment compared to HIV-1/M in naïve patient. This difference had no impact on the virological responses to cART. The proportion of patients with an undetectable pVL was similar between the two groups one year after the beginning of the treatment. Immunological response was close between HIV-1/O and HIV-1/M in France. But when the two populations were compared in Cameroon, the immunological response to cART was lower for HIV-1/O patients than for HIV-1/M patients, although this diffence didn’t had clinical consequences.HIV-1/O medical care based on HIV-1/M guidelines is highly efficient if the treatment doesn’t include NNRTI treatment.
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Outcomes of paediatric art patients down-referred from a tertiary and a regional hospital to primary care facilities in Buffalo City Municipality, Eastern CapeMaughan, Samantha Jane January 2020 (has links)
Master of Public Health - MPH / Background: According to the Joint United Nations Programme on HIV/AIDS (UNAIDS) 340 000 children between 0-14years of age are living with HIV in South Africa as of 2019. Decentralization of HIV services was included in South Africa’s paediatric guidelines since 2010 in a bid to improve access to care. The current study sought to address the paucity of Eastern Cape (EC) data on the outcomes of down-referred paediatric antiretroviral therapy (ART) patients. These outcomes included retention in care (RIC) and virological suppression after 12 months Methodology: This retrospective analysis was conducted in the Buffalo City Municipality (BCM) district of the EC. The study population included HIV positive males and females, 0-14 years of age at transfer, who were initiated on ART at a tertiary or a regional hospital and subsequently down-referred, between June 2013 and June 2017. Data were collected from electronic databases at the facilities (Tier.net), patient files and patient registers. A descriptive analysis was performed using SPSS Statistics software version 26. Results: In total, 80.1% of patients successfully down-referred to a primary healthcare (PHC) facility, in a median of 42 days. Of those, 95.4% of patients were retained in care at 6 months and 93.1% at 12 months after arrival, with a median of 4 scheduled monthly visits missed. For those with results, virological suppression was maintained in 96.7% of patients at 6 months, 92.2% at 12 months and 96.2% for the entire post-transfer period of 2-14 months. In the 2-14 months post down-referral only 76.9% of patients had at least one viral load (VL) result and 50.3% had one CD4 result. For those with results, immune response (IR) to ART was maintained in 100% of patients at 6 months, 94.3% at 12 months and 97.7% in the 2-14 month period post successful down-referral. Conclusions: This study confirmed that loss to follow-up (LTFU) and treatment interruption at the point of transfer are significant risk factors for paediatric ART patients. This study also demonstrated high levels of RIC once patients had successfully down-referred. However, missed clinic visits suggest possible treatment interruptions for many patients post down-referral. While good virological and immunological responses to ART were maintained at the PHC facilities, suboptimal VL and CD4 monitoring was highlighted by the low proportion of available results. Therefore, while there are a number of issues to address, this study confirms that down-referral is a feasible option for up-scaling paediatric HIV care in the EC.
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Traitement antirétroviral précoce des nourrissons infectés par le VIH-1 : évaluation de la réponse virologique à court et moyen termes dans un pays d’Afrique sub-saharienne (Cameroun) / Early antiretroviral treatment in HIV-1-infected infants : Assessment of short- and long-terms virological response in a sub-Saharan country (Cameroon)Ateba Ndongo, Francis 05 October 2017 (has links)
Introduction : Depuis 2015, l’OMS recommande la mise sous traitement antirétroviral systématique de tous les enfants infectés par le VIH pour réduire la mortalité précoce liée au VIH chez les nourrissons en l’absence de traitement. Cependant, malgré la disponibilité des tests de dépistage et des médicaments antirétroviraux, l’initiation précoce de ces traitements reste un défi majeur dans les pays à ressources limitées. L’étude ANRS 12140-PEDIACAM est mise en place pour évaluer la faisabilité, l’efficacité et la tolérance en routine du traitement précoce des enfants infectés par le VIH au Cameroun. Objectifs : Les objectifs de cette thèse visaient à étudier la mortalité et la réponse virologique à deux et quatre ans après l’initiation précoce d’un traitement antirétroviral chez les nourrissons infectés par le VIH, et à identifier les facteurs associés à l’obtention et au maintien d’un succès virologique.Méthodes : Les analyses ont porté sur les 190 enfants infectés par le VIH traités avant l’âge de 1 an (médiane=4 mois), inclus dans les trois sites cliniques du Cameroun participant à la cohorte prospective ANRS PEDIACAM initiée en 2007. La première étude a évalué les performances d’un critère basé sur le nombre de doses manquées de traitement rapporté dans un questionnaire d’observance pour dépister un échec virologique chez les nourrissons. La seconde étude portait sur l’estimation de la fréquence et des facteurs associés à l’obtention d’un succès virologique et à la mortalité à deux ans du traitement, utilisant un modèle de survie à risque compétitif. La troisième concernait l’évolution de la réponse virologique entre 2 et 4 ans du traitement selon le statut virologique obtenu à deux ans.Résultats : Les performances du questionnaire d’observance administré à l’accompagnant du nourrisson s’avèrent limitées, avec une valeur prédictive positive trop faible pour dépister un échec virologique en l’absence de charge virale disponible. La mortalité reste élevée à un an du traitement précoce (18,0% [IC95% : 13,0 - 24,0]). Elle est de 3,3% [IC95% : 0,4 - 6,2] entre 2 et 4 ans de traitement. La probabilité d’atteindre au moins un succès virologique avant 2 ans de traitement est de 80% environ, mais celle d’obtenir une suppression virologique maintenue sur au moins 6 mois n’est que de 67% au seuil de 1000 copies/mL, et de 60% au seuil de 400 copies/mL. A 4 ans du traitement initial, la proportion de charge virale contrôlée (<400 copies/mL) est de 75,2% [68,3-82,1]) chez les 144 enfants toujours vivants et suivis, mais pour 12% la charge virale n’a pas été mesurée. Le seul facteur associé significativement au succès virologique dans les 2 ans du traitement initial est la bonne observance rapportée par l’accompagnant. Et seuls un succès virologique obtenu à 2 ans et l’initiation plus récente du traitement antirétroviral sont associés à un charge virale contrôlée à 4 ans.Conclusion : Même si l’intérêt du traitement précoce des nourrissons infectés par le VIH est démontré, le succès virologique à moyen et long terme passe par des stratégies favorisant l’administration quotidienne soutenue des médicaments et une surveillance régulière de la réponse virologique. L’évaluation de l’observance par questionnaire présente une trop faible performance pour dépister précocement un échec virologique. Il est urgent de donner un accès large à la mesure de la charge virale en routine dans les pays à ressources limitées pour dépister rapidement les échecs virologiques chez les enfants recevant un traitement antirétroviral. / Introduction: Since 2015, the WHO recommends to start antiretroviral treatment promptly in all HIV-infected children in order to reduce HIV related mortality. Despite increasing availability of screening tests and antiretroviral drugs, early initiation of antiretroviral treatment (ART) remains challenging in resource-limited countries. The ANRS 12140-Pediacam study assesses feasibility, effectiveness and tolerability in routine practice of early treatment of HIV-infected children in Cameroon. Objectives: The objectives of this thesis are to study mortality and virologic response at 2 and 4 years of early initiation of ART in HIV-infected infants and identify factors associated with virologic success. Methods: The analysis concerned the 190 HIV-infected infants who have initiated ART no later than 1 year (median=4 months) and were enrolled in the 3 Cameroon clinical sites involved in the PEDIACAM prospective cohort study since 2007. The first study evaluated adherence criterium based on the number of missed doses as reported through an adherence questionnaire in oerder to detect virologic failure in infants. The second study concerned the evaluation of the frequency and the factors associated with virologic success and mortality at 2 years of ART initiation, using competing risk regression. The third study concerned the evolution of virologic response between 2 and 4 years of QRT initiation depending on virologic status achieved at 2 years of ART initiation. Results: The performances of adherence questionnaire administered to the infant's caregiver are limited; the positive predictive value is low for detecting virologic failure in the absence of viral load exam. The mortality is high at 1 year after early ART initiation (18.0% [95% CI: 13.0 – 24.0]). The mortality is 3.3% [95%CI: 0.4 – 6.2] between 2 and 4 years of ART initiation. The probability of achieving at least once virologic success within the first 2 years of ART is around 80.0% but the probability of maintaining virologic success for at least 6 months was 67% for threshold=1000 copies/mL and 60% for threshold=400 copies/mL. At 4 years of ART initiation, the proportion of virologic success (viral load<400 copies/mL) is 75.2% [68.3-82.1]) in the 144 children still alive among whom viral load exam was not performed. The only factor associated with virologic success at 2 years of ART initiation is good adherence as reported by the caregiver. Et seuls un succès virologique obtenu à 2 ans et l’initiation plus récente du traitement antirétroviral sont associés à un charge virale contrôlée à 4 ans.Conclusion: Although the interest of early ART in HIV-infected infants is demonstrated, the mid and long term virologic success pass through strategies enhancing supporting steady and daily administration of drugs and regular monitoring of virologic response. The steady evaluation of adherence as reported by questionnaire has a very low performance for early detecting virologic failure. It is urgent to widely get access to routine viral load exam in resource-limited countries for quickly detecting virologic failures in children receiving antiretroviral treatment.
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