Malaria treatment in Ethiopia: antimalarian drug efficacy monitoring system and use of evidence for policy

Ambachew Medhin Yohannes

12 September 2013

The purpose of this study was to describe the characteristics and findings of antimalarial drug efficacy studies conducted in Ethiopia and to use the findings to formulate recommendations for antimalarial drug efficacy monitoring and use of evidence to inform antimalarial treatment policy for the Ethiopian setting. This study reviewed 44 antimalarial efficacy studies conducted in Ethiopia from 1974 to 2011. The analysis of results indicated that chloroquine as the first-line antimalarial drug for the treatment of malaria due to Plasmodium falciparum had a 22% therapeutic failure in 1985. Chloroquine was replaced with sulfadoxine-pyrimethamine in 1998, more than 12 years later, when its therapeutic failure had reached 65%. Sulfadoxinepyrimethamine at the time of its introduction had a treatment failure of 7.7%; it was replaced after seven years in 2004 by artemether-lumefantrine; by then its treatment failure had reached 36%. The WHO recommends the replacement of a first-line antimalarial drug when more than 10% of treatment failure is reported. The replacement drug should have a therapeutic efficacy of more than 95%; while the change itself should be completed within two years. The prolonged delay to replace failing antimalarial drugs in Ethiopia seems to have been influenced mainly by the lack of systematic antimalarial drug efficacy data collection and pragmatic use of the data and evidence gathered.Almost eight years after its introduction, isolated studies show that the efficacy of artemether-lumefantrine has decreased from 99% in 2003 to around 96.3% in 2008. Though this decrease is not statistically significant (chi-square 1.5; P=0.22) and has not reached the threshold of 10%, it is plausible that its efficacy may drop further. This is mainly due to regulatory provisions in the country that allow marketing of oral artemisinin mono-therapies that are not recommended for malaria treatment, use of less effective antimalarial combination drugs in the neighboring countries and widespread drug quality problems. The situation calls for and this study recommends the establishment of stringent drug efficacy monitoring and early warning system and alignment of the antimalarial drug regulatory practices with recommendations of the WHO. / Health Studies / D. Litt. et Phil. (Health Studies)

Malaria

Antimalarial drug efficacy

Monitoring

Treatment policy and guideline change

616.936200963

Malaria -- Treatment -- Ethiopia

Malaria -- Chemotherapy -- Ethiopia

Malaria treatment in Ethiopia: antimalarian drug efficacy monitoring system and use of evidence for policy

Ambachew Medhin Yohannes

12 September 2013

The purpose of this study was to describe the characteristics and findings of antimalarial drug efficacy studies conducted in Ethiopia and to use the findings to formulate recommendations for antimalarial drug efficacy monitoring and use of evidence to inform antimalarial treatment policy for the Ethiopian setting. This study reviewed 44 antimalarial efficacy studies conducted in Ethiopia from 1974 to 2011. The analysis of results indicated that chloroquine as the first-line antimalarial drug for the treatment of malaria due to Plasmodium falciparum had a 22% therapeutic failure in 1985. Chloroquine was replaced with sulfadoxine-pyrimethamine in 1998, more than 12 years later, when its therapeutic failure had reached 65%. Sulfadoxinepyrimethamine at the time of its introduction had a treatment failure of 7.7%; it was replaced after seven years in 2004 by artemether-lumefantrine; by then its treatment failure had reached 36%. The WHO recommends the replacement of a first-line antimalarial drug when more than 10% of treatment failure is reported. The replacement drug should have a therapeutic efficacy of more than 95%; while the change itself should be completed within two years. The prolonged delay to replace failing antimalarial drugs in Ethiopia seems to have been influenced mainly by the lack of systematic antimalarial drug efficacy data collection and pragmatic use of the data and evidence gathered.Almost eight years after its introduction, isolated studies show that the efficacy of artemether-lumefantrine has decreased from 99% in 2003 to around 96.3% in 2008. Though this decrease is not statistically significant (chi-square 1.5; P=0.22) and has not reached the threshold of 10%, it is plausible that its efficacy may drop further. This is mainly due to regulatory provisions in the country that allow marketing of oral artemisinin mono-therapies that are not recommended for malaria treatment, use of less effective antimalarial combination drugs in the neighboring countries and widespread drug quality problems. The situation calls for and this study recommends the establishment of stringent drug efficacy monitoring and early warning system and alignment of the antimalarial drug regulatory practices with recommendations of the WHO. / Health Studies / D. Litt. et Phil. (Health Studies)

Malaria

Antimalarial drug efficacy

Monitoring

Treatment policy and guideline change

616.936200963

Malaria -- Treatment -- Ethiopia

Malaria -- Chemotherapy -- Ethiopia

Rational development of novel activity probes for the analysis of human cytochromes P450

Sellars, J.D., Skipsey, M., Sadr-ul-Shaheed, Gravell, Sebastian, Abumansour, Hamza M.A., Kashtl, Ghasaq J., Irfan, Jawaria, Khot, Mohamed, Pors, Klaus, Patterson, Laurence H., Sutton, Chris W.

05 June 2016

Yes / The identification and quantification of functional cytochromes P450 (CYPs) in biological samples is proving important for robust analyses of drug efficacy and metabolic disposition. In this study, a novel CYP activity-based probe was rationally designed and synthesised, demonstrating selective binding of CYP isoforms. The dependence of probe binding upon the presence of NADPH permits the selective detection of functionally active CYP. This allows the detection and analysis of these enzymes using biochemical and proteomic methodologies and approaches. / Engineering and Physical Sciences Research Council (EPSRC) and Yorkshire Cancer Research

Human cytochromes P450

Functional cytochromes

CYPs

Drug efficacy

Probe binding

NADPH

Validation préclinique d'un test de prédiction d'efficacité de médicaments anti-cancéreux : application au glioblastome, cancer colorectal et cancer de la prostate / Prediction of cancer drug efficacy using a tumor specific ranking procedure of therapeutic targets : preclinical validation in glioblastoma, colorectal and prostate cancer models

Fritz, Justine

26 September 2016

Nous avons développé un nouveau test de prédiction de l’efficacité de thérapies anti-cancéreuses. Ce concept se base sur la détermination d’une signature moléculaire tumorale par RT-qPCR. Cette signature est issue d’un algorithme de normalisation innovant de comparaison des données d’expression relative des cibles de la tumeur avec celles de tissus de référence. Cette normalisation offre à chaque cible de la signature un rang et un score spécifique permettant de hiérarchiser les voies pro-tumorales afin de trouver la ou les cibles dominantes responsables du développement de la tumeur. La signature comprend des cibles donnant des informations générales sur le statut et l’hétérogénéité de la tumeur, sur l’angiogenèse et la lymphangiogenèse, sur le microenvironnement tumoral et enfin sur l’activité migratoire. Une validation préclinique dans les modèles du cancer colorectal, de la prostate et du glioblastome, a montré que le test est prédictif de l’efficacité thérapeutique. / We developed a new tool for prediction of cancer treatment efficacy. Our process is based on the determination of the molecular signature which is intended to provide a clinician’s decision tool helping to select which tumor signaling pathway(s) has/have to be targeted for best therapeutic effect. This signature representing a scoring obtained by RT-qPCR through a sequential normalization process of the expression level of target genes in the tumor compared to cancer type-specific references. These genes were selected because of a good knowledge of related biological functions, a correlation between expression level and aggressiveness of the tumor, the existence of a therapeutic arsenal already in clinical use. This signature is validated in a preclinical model of colorectal cancer and prostate cancer and glioblastoma. The results obtained show that the test we developed allows to identify the most important signaling pathway implicated in the disease and to choose the best drug.

Médecine personnalisée

Cancer

Signature moléculaire tumorale

Normalisation

RT-qPCR

Cancer colorectal

Cancer de la prostate

Glioblastome

Personalize medicine

Cancer

Tumor molecular signature

Prediction of drug efficacy

Normalization

RT-qPCR

Colorectal cancer

Prostate cancer

Glioblastoma

615.1

616.9

Effet des antirétroviraux sur la pathogénèse du VIH : une étude par modélisation mathématique intégrant la cinétique du virus, de l’immunité, du médicament, et le comportement d’adhésion avec leurs variabilités interindividuelles

Sanche, Steven

08 1900

No description available.

adhésion aux traitements

cellules latentes

contrôle post-traitement

distribution des médicaments

échecs virologiques

efficacité des traitements

extrapolation in vitro à in vivo

modélisation mathématique

persistance du VIH

pharmacologie quantitative des systèmes

rebonds virologiques

résistance aux traitements

variabilité interindividuelle

VIH

drug adherence

drug distribution

drug efficacy

drug individualization

drug resistance

HIV

HIV persistence

in vitro to in vivo extrapolation

interindividual variability

latent cells

mathematical modeling

post-treatment control

quantitative systems pharmacology (QSP)

viral rebound

virologic failure