Dissertations / Theses on the topic 'Malaria drug treatment][Mefloquine'

Resistance to antimalarial drugs is increasing nearly everywhere in the tropical world, confounding global attempts to "Roll Back Malaria". Antimalarial treatment with artemisinin, artesunate, or artemether has proved rapidly effective in the treatment of non complicated and complicated malaria and remarkably nontoxic. However there is a number of important questions that still need urgent attention: Should artemisinin be deployed alone or in combination with other antimalarial drugs such mefloquine or other compound (s); which is the best regimen (s); can artemisinin and its derivatives (artesunate or artemether) reduce the mortality in severe malaria and which is the best drug(s); are there important neurotoxic side effects in patients treated with this group of antimalarial drugs. In order to answer those questions a series of studies were conducted in Vietnam and these form the basis of this thesis. The conclusion is: 1) Dihydroartemisinin-piperaquine is an inexpensive, safe, highly efficacious fixeddose antimalarial combination treatment that could make an important contribution to the control of multidrug-resistant fa1ciparum malaria for Vietnan1 and other countries. 2) Artemether is a satisfactory alternative to quinine for the treatment of severe malaria in adults. The rectal administration of artemisinin would obviollsly constitute a useful therapeutic advance, in comparing with parenteral drugs such as artemether and artesunate, particularly in areas where parenteral administration is difficult. 3) The artemisinin derivatives have an acceptable safety profile. 4) Viet Nam has shown that it is possible to "Roll Back Malaria" assuming one has access to good drugs and a willingness to implement change. Those studies have helped to confirm that the qinghaosu (artemisinin) group of drugs is the most important new class of antimalarials developed in the last fifty years.

Malaria is currently one of the most imperative parasitic diseases in developing countries. Artesunate has a short half-life, low aqueous solubility and resultant poor and erratic absorption upon oral administration, which translate to low bioavailability. Mefloquine is eliminated slowly with a terminal elimination half-life of approximately 20 days and has neuropsychiatric side effects. Novel drug delivery systems have been utilised to optimise chemotherapy with currently available antimalarial drugs. Pheroid™ technology is a patented drug delivery system which has the ability to capture, transport and deliver pharmaceutical compounds. Pheroid™ technology may play a key role in ensuring effective delivery and enhanced bioavailability of novel antimalarial drugs. The aim of this study was to evaluate the possible efficacy and bioavailability enhancement of the selected antimalarial drugs, artesunate and mefloquine, in combination with Pheroid™ vesicles. The in vitro efficacy of artesunate and mefloquine co-formulated in the oil phase of Pheroid™ vesicles and entrapped in Pheroid™ vesicles 24 hours after manufacturing were investigated against a 3D7 chloroquine-sensitive strain of Plasmodium falciparum. Parasitemia (%) was quantified with flow cytometry after incubation periods of 48 and 72 hours. Drug sensitivity was expressed as 50% inhibitory concentration (IC50) values. An in vivo bioavailability study with artesunate and mefloquine was also conducted in combination with Pheroid™ vesicles, using a mouse model. A sensitive and selective liquid chromatography-tandem mass spectrometry (LC-MS/MS) method was developed to analyse the drug levels. C57 BL6 mice were used during this study. The selected antimalarial drugs were administered at a dose of 20 mg/kg with an oral gavage tube. Blood samples were collected by means of tail bleeding. The in vitro drug sensitivity assays revealed that artesunate, co-formulated in the oil phase of Pheroid™ vesicles and evaluated after a 48 hour incubation period, decreased the IC50 concentration significantly by 90%. Extending the incubation period to 72 hours decreased the IC50 concentration of artesunate, also co-formulated in the oil phase of Pheroid ™ vesicles significantly by 72%. No statistically significant differences between the reference and Pheroid™ vesicle groups were achieved when artesunate was entrapped 24 hours after manufacturing of Pheroid™ vesicles. Mefloquine co-formulated in the oil phase of Pheroid™ vesicles and evaluated after a 48 hour incubation period decreased the IC50 concentration by 36%. Extending the incubation period to 72 hours increased the efficacy of the Pheroid™ vesicles and the IC50 concentration was significantly decreased by 51%. In contrast with the results obtained with artesunate, entrapment of mefloquine in Pheroid™ vesicles 24 hours after manufacturing decreased the IC50 concentration significantly by 66%. The LC-MS/MS method was found to be sensitive, selective and accurate for the determination of artesunate and its active metabolite, dihydroartemisinin (DHA) in mouse plasma and mefloquine in mouse whole blood. Most of the artesunate plasma concentrations were below the limit of quantification in the reference group and relatively high outliers were observed in some of the samples. The mean artesunate levels of the Pheroid™ vesicle group were lower compared to the reference group, but the variation within the Pheroid™ vesicle group lessened significantly. The mean DHA concentrations of the Pheroid™ vesicle group were significantly higher. DHA obtained a higher peak plasma drug concentration with the Pheroid™ vesicle group (173.0 ng/ml) in relation to the reference group (105.0 ng/ml) and at a much faster time (10 minutes in Pheroid™ vesicles in contrast to 30 minutes of the reference group). Pharmacokinetic models could not be constructed due to blood sampling per animal limitation. The incorporation of mefloquine in Pheroid™ vesicles did not seem to have improved results in relation to the reference group. No statistical significant differences were observed in the pharmacokinetic parameters between the two groups. The relative bioavailability (%) of the Pheroid™ vesicle incorporated mefloquine was 7% less bioavailable than the reference group.
Thesis (M.Sc. (Pharmaceutics))--North-West University, Potchefstroom Campus, 2010.

Drug resistance is a serious problem in health care in general, and in malaria treatment in particular, rendering many of our previously considered ‘wonder drugs’ useless. Recently, large sums of money have been allocated for the continuous development of new drugs to replace the failing ones. We seem to be one step behind the evolution of antimalarial resistance; is it possible to get one step ahead? Are interventions which slow down the evolution and spread of drug-resistant malaria parasites achievable? In this thesis, I address these issues with experimental data, using the well-established rodent malaria model Plasmodium chabaudi to understand the selective advantages and disadvantages drug-resistant parasites endure within a vertebrate host and the selective pressures various drug treatment regimes exert on these parasites. Competitive interactions between drug-resistant and drug-sensitive parasites were observed within the host, with resistant parasites having a competitive disadvantage in the absence of drug treatment. The frequency of resistant parasites at the start of the infection was an important determinant of the strength of selection: the lower their frequency, the stronger the competitive suppression in non-treated hosts and the greater their competitive release following drug treatment. Genetically similar genotypes, one resistant and one sensitive, showed similar dynamics following drug treatment. Multiplicity of infection did not have an effect on the within-host dynamics: a larger number of co-infecting susceptible genotypes did not lead to greater competitive suppression or release of resistant parasites. Lastly, various drug treatment regimes were compared. Conventional drug treatment resulted in the greatest selective advantage for drug-resistant parasites, while less aggressive treatments were equally as effective, or even better, at improving host health and reducing overall infectiousness. These studies demonstrate that altering the within-host ecology of drug-resistant parasites by administering drugs and hence removing the drug-sensitive competitors has a large influence on the transmission potential of drug-resistant parasites. Furthermore, this thesis provides proof of principle that other drug treatment regimes different from those currently in use could better control drug-resistant parasites, without compromising other treatment goals. In the case of malaria, less drugs may mean extending the useful lifespan of that drug.

Tuberculosis (TB) and malaria continue to be major public health concerns, globally claiming 2-3 million deaths every year. A number of efficacious drugs are available for the treatment of TB and malaria, which, through various combination therapies, are fully effective in treating these diseases. However, the wide spread resistance in M. tuberculosis (Mtb) and P. falciparum, the causative agents of TB and malaria, respectively, has made the existing therapies less effective. Thus novel agents able to circumvent drug resistance and other challenges associated with existing TB and malaria treatments are urgently needed. The development of a new drug is a lengthy and costly process; therefore, approaches that can save both time and money need to be emphasised. Drug repositioning is one such approach that has been applied in this project. Drug repositioning basically involves a situation where a drug active in one disease is derivatised or used as a template for the synthesis of derivatives active in another disease. This approach has the potential to significantly shorten the drug discovery process. This study focused on the repositioning of two drugs, the antibacterial agent fusidic acid and the antipsychotic agent metergoline, in TB and/or malaria via medicinal chemistry approaches. New semisynthetic derivatives of fusidic acid and metergoline were synthesized and evaluated for antimycobacterial activity against the H37Rv strain of Mtb and antiplasmodial activity against the NF54 strain of P. falciparum.

A thesis presented on a clinical trial of amodiaquine (AQ) and sulphadoxine-pyrimethamine (SP) used singly and in combination (AQ+SP) compared with chloroquine (CQ) for the treatment of 900 pregnant women who had falciparum malaria infection detected by a screening programme using OptiMAL antigen dipsticks during routine antenatal clinic sessions at the St. Theresa's hospital. Enrolment into the study began in March 2003 and ended in September 2004 but follow up of treated women continued to March 2005.

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New antimalarial drugs are urgently needed to combat emerging multidrug resistant strains of malaria parasites. This Highlight focuses on plant-derived natural products that are of interest as potential leads towards new antimalarial drugs including synthetic analogues of natural compounds, with the exception of artemisinin derivatives, which are not included due to limited space. Since effective antimalarial treatment is often unavailable or unaffordable to many of those who need it, there is increasing interest in the development of locally produced herbal medicines; recent progress in this area will also be reviewed in this Highlight.

Malaria is more prevalent today and the death toll is on the increase annually. It is one of the leading causes of morbidity and mortality worldwide and most of these deaths are in the poorest regions of the world. About 500 million cases are reported annually with more than 2 million deaths, and most are children. It is the major killer in the tropics and a major public health problem in developing countries and Papua New Guinea (PNG) is no exception. Resistant strains have been reported. This may be enhanced by inappropriate human behaviour in the use of anti-malarial drugs. Human factors include inappropriate prescribing and patient behaviour in using anti-malarial drugs. Despite the establishment of the standard treatment guidelines for malaria in PNG, three out of every four patients have chloroquine-resistant falciparum malaria and malaria remains a major health problem. The aim of this study was to evaluate the influence of an education program on patients carers' understanding and effective use of anti-malarial drugs for the treatment of uncomplicated malaria in children in general health clinics in PNG. The trial design involved a pre-post intervention study with a control group. The study was undertaken in the National Capital District. Papua New Guinea using one Clinic as the intervention site and another as the control site. The two clinics were similar in characteristics as confirmed in the study by demographic data where there were no significant differences observed. The data collection took placed over the period February to April 2002. It included observation of drug provision at study sites and interviews of patient carers on the first day at the clinic and a follow up seven days later. Three questionnaires were developed to evaluate the process and outcomes of malaria drug treatment in the above health facilities.
Prescribing data were collected from prescriptions and patient carers' interviewed prior to the intervention program. Following the provision of drug information to patient carers. similar drug information and compliance questioning was undertaken. Differences in the pre-post elements of the study and in the control group over the study period were evaluated using Chi-Squared, Kruskal-Wallis, Fisher's Exact or Student's t-tests as appropriate. In excess of 100 patients in the pre- and in the post intervention phases were evaluated for their understanding and effective use of the anti-malarial drugs. In addition, 100 clients were in the control group at another clinic. Patients had attended the clinic up to 8 times in the previous year with a median of 2 visits. Amodiaquine, Fansidar, albendazole and paracetamol made up a total of 60% of the drugs prescribed. The use of medicines was strongly supported with 94.4% indicating no problems with the medication. Only 3% of patients received herbal or local remedies for malaria treatment. 1n patients 10 years or less or their carers, it was found, there was a significant improvement in the carers understanding of the medications. There was a statistically significant improvement in patient outcomes from 57.9% to 92.3% reported as cured following the intervention program. The study has also identified low levels of appropriate administration of antibiotic suspensions in children by patient carers.
For example, incorrect responses recorded for amoxycillin suspension were 80.8% (143). Septrim tablets 92% (23), Septrim suspension 86% (123), erythromycin suspension 100% (26), and chloramphenicol suspension 84.4% (38). In this study the face to face (one-to-one) education program was used to influence patient carers understanding and effective use of drugs. The intervention program involved advising, informing, encouraging, and counselling the patient carers verbally on the appropriate and effective use of medicines. The verbal message was reinforced by a suitable label typed in English and Pidgin-English where instructions were clear, simple and unambiguous. The label was then attached to the envelopes or containers containing the drugs. On feedback, the information on the understanding and effective use of drugs was re-emphasized to the carers to reinforce their understanding for future references. Results showed that the intervention program made an impact in improved patient carers understanding and effective use of drugs and children's health outcomes. In conclusion, it is evident that a patient intervention program designed to improve the dosages and frequency of administration of anti-malarial drugs in PNG had no statistically significant outcome. This may be because the current level of understanding was quite high (>70%) and the study experienced a ceiling effect. However, as shown in the results, the patient carers understanding on the appropriate and effective use of drugs was lower during the pre-intervention and control group.
When compared clinic-pre with clinic-post, there was a significant difference (P < 0.05) in the cured group and the improved cure rate increases from 57.9% to 92.3%. When compared control pre with control post groups, there was no significant difference (P > 0.05) in the cured group. Therefore, the study identified an improvement in patient outcomes with respect to malaria. Hence. the simple intervention program in influencing patient carers understanding of the appropriate and effective use of medications led to a marked improvement in patient outcomes.

Includes bibliographical references (leaves 57-62).
Changes in Antimalarial Drug Policies are intended to improve case management and reduce both social and financial burden associated with malaria. To achieve this providers have to translate the policy into practice since they have the privilege of being the primary contact to those affected by malaria. The main aim of this study is to examine the extent of implementation of the change in antimalarial drug policy in Uganda, from chloroquine monotherapy to combination therapy of CQ+SP for management of uncomplicated malaria. Prescribing practice of health personnel in selected health facilities in Rakai and Kampala Districts is used as a measure of level of adherence to the change in policy.

Malaria is a health, social and economic burden in Nigeria and consistently ranks amongst the four most common causes of childhood deaths. Treatment of malaria is usually started at home
care is only sought from the health facility when the treatment is ineffective (McCombie, 1996). Patent medicine vendors (PMVs) have been identified as a widely patronized source for drugs used in the home treatment of malaria (Breiger et al, 2001
Goodman, et al, 2007
Salako et al, 2001). Inadequate or poor knowledge and practices in the use of anti-malaria drugs (AMDs) increases morbidity and mortality, undermines therapeutic efficacy, and promotes the emergence and spread of drugresistant malaria. Aim: The aim of the study was to describe and quantify the knowledge and self-reported practices of PMVs in the use of antimalarials, particularly artemisinin-based combination therapies (ACTs), in a poor urban community in Lagos state, Nigeria.

Deuxième pays le plus endémique pour le paludisme au monde, la république démocratique du Congo (RDC) a adopté officiellement l’initiative Faire Reculer le Paludisme en 2001 et depuis, aligne sa politique de lutte contre le paludisme sur les directives de l’OMS dont les orientations les plus récentes consistent en 3 stratégies :[1] assurer aux malades un accès rapide à un traitement efficace et abordable, [2] assurer aux personnes exposées au risque, notamment les jeunes enfants et les femmes enceintes, l’association la plus adaptée de mesures de protection au niveau personnel et communautaire et [3] donner l’accès, aux femmes enceintes exposées au risque, à des traitements préventifs.

Afin de contribuer à l’amélioration de la lutte antipaludique en RDC, le travail a été réalisé en 3 parties :une portant sur la pertinence du traitement préventif intermittent à la Sulfadoxine-Pyriméthamine (TPI-SP) chez la femme enceinte en contexte d’augmentation de la résistance du parasite, une 2e sur les facteurs déterminants l’adhésion des prestataires de soins, des vendeurs des médicaments et des patients à association Artesunate-Amodiaquine (AS-AQ) et une 3e décrivant le paludisme sévère chez l’enfant.

La 1ère partie du travail portant sur le TPI-SP a été réalisée en 2 temps. La première approche a consisté en une analyse rétrospective des poids de naissance des nouveau-nés en fonction de la prise du TPI-SP par les mères dans 3 maternités en 2007 où les niveaux de résistance à la SP étaient différents. La deuxième approche, comparait l’effet du traitement préventif intermittent à la Sulfadoxine-Pyriméthamine en 1998/1999 et en 2007 à la prophylaxie à base de chloroquine en 1998/1999 à l’Est de la RDC dans un milieu où la résistance à la Sulfadoxine-Pyriméthamine avait accru considérablement.

Dans les régions où la résistance du parasite était de faible (Mikalayi: 1,6% d’échec thérapeutique chez l’enfant) à modéré (Kisangani: 21,7% d’échec thérapeutique chez l’enfant), le TPI-SP réduit le risque de faible poids à la naissance, à Kisangani (OR ajusté :0,15; IC95%, 0,05-0.46) et à Mikalayi (OR ajusté :0,12; IC95%, 0,01-0,89). Dans ces 2 sites, le poids de naissance moyen des Nouveau-nés était plus élevé pour les mères ayant reçu 2 doses par rapport à celui des Nouveau-nés des mères en ayant reçu une seule ou aucune (P<0.001). A Rutshuru où la résistance était élevée (60,6% d’échec thérapeutique chez l’enfant), l’effet du TPI-SP semble moindre: en 2007 - en comparaison dose-dépendante (2 doses Vs 0-1 dose) du poids à la naissance des nouveau-nés en 2007 pour les mères sous TPI-SP – on observait un effet bénéfique chez les primigestes et non chez les multigestes et une légère régression du gain pondéral [(53,9g ( P=0,027) pour les nouveau-nés des mères sous SP en 2007 Vs 70,2g (P=0,003) pour ceux des mères sous SP en 1998/1999 par rapport à ceux des mères sous chloroquine en 1998/1999. Néanmoins, le TPI-SP reste efficace en 2007 comme en 1998-1999 par rapport à la prophylaxie à base de chloroquine en 1998/1999 (poids moyen supérieur et réduction du risque de PPN pour les 2 groupes sous SP).

La 2e partie, traitait des déterminants de l’adhésion des prestataires et des patients au nouveau médicament recommandé par la politique nationale pour la prise en charge des cas de paludisme simple ( AS-AQ ) en 2 enquêtes transversales :une étude préliminaire qui a été réalisée dans les CS fonctionnels de Kisangani en avril 2008 et une étude étendue à 3 des 10 districts sanitaires de la province Orientale de mars à juin 2009. Ces 2 enquêtes ont ensuite servi à une analyse systémique des facteurs d’adhésion des prestataires de soins à l’AS-AQ basée sur le modèle de diagnostic de Green et Kreuter et les étapes de changement de comportement de PROCHASKA pour la planification des interventions de promotion.

Le recours à l’AS-AQ pour le traitement du paludisme simple progresse (41% et 69% des prescriptions dans les services sanitaires respectivement 3 et 4 ans après le changement de politique national de lutte antipaludique), mais reste inférieur à la cible d’au moins 80% visée par la politique nationale. Malgré la croyance en l’efficacité du nouveau traitement, son utilisation effective rencontre comme principaux obstacles, selon l’avis des prestataires de soins, des vendeurs de médicaments et des patients, sa faible disponibilité, son coût élevé, la présence sur le marché d’antipaludiques retirés du protocole national de traitement et de l’AS-AQ de mauvaise qualité à un coût moindre et la crainte des effets indésirables. Tandis que les facteurs incitatifs à son utilisation sont, l’efficacité thérapeutique perçue de l’AS-AQ, la présence du médicament dans les formations sanitaires, la recommandation de son utilisation par les directives du Ministère de la Santé (notamment sous forme de guides techniques), la formation et la supervision des prestataires, l’intention de prescrire l’AS-AQ aux patients ou d’en prendre soi-même, une plus longue durée de consultation, le fait de fournir des explications aux patients, de travailler dans le milieu rural.

La dernière partie du travail consistait en une étude prospective menée du 1er janvier 2010 au 28 février 2011 décrivant le diagnostic et la prise en charge du paludisme grave chez les enfants admis dans 2 HGR de Kisangani.

Le paludisme constitue un des principaux motifs d’hospitalisation des enfants en RDC (37,0% à Kisangani) dont l’évaluation est souvent incomplète (53,6% avec goutte épaisse négative ou sans, insuffisamment explorés et traités comme paludisme grave) et le traitement parfois inadéquat (outre les affections non palustres probables non traitées, il y avait notamment surutilisation des produits sanguins exposant les enfants aux risques infectieux transfusionnels). Ainsi, les limites du plateau technique des HGR et l’organisation du circuit des malades semblent entraîner une sous-estimation, entre autre, des complications métaboliques du paludisme grave et des autres infections graves du jeune enfant et par conséquent des écarts au protocole de prise en charge préjudiciables aux patients.

Ces résultats mettent en lumière la nécessité :

•d’inscrire parmi les priorités du Programme National de Lutte contre le Paludisme, des recherches pour évaluer une option alternative au traitement préventif intermittent avec 2 doses de SP (traitement préventif intermittent avec d’autres antipaludiques) et à l’est du pays le recours préférentiel à la moustiquaire imprégnée à longue durée, en particulier chez la multigeste.

•de retenir, pour la promotion de l’utilisation de l’AS-AQ pour le traitement du paludisme simple, comme priorités :

o mettre à profit les opportunités actuelles de financement dans le domaine de la lutte antipaludique pour améliorer la disponibilité de l’AS-AQ à un coût accessible et à améliorer l’approvisionnement aussi bien des formations sanitaires publiques et privées que des officines pharmaceutiques ;

o assainir le secteur pharmaceutique de manière à endiguer la circulation d’antipaludique de mauvaise qualité à bas prix qui alimente les habitudes d’automédication courante dans les ménages ;

o élaborer des programmes de promotion de l’utilisation de l’AS-AQ, en élargissant la cible des interventions autant aux prestataires de soins du secteur privé qu’aux vendeurs de médicaments ;

o Adapter les programmes de promotion de l’AS-AQ au stade de changement de comportement auquel se trouve les acteurs après analyse des déterminants de leurs comportements notamment, les facteurs prédisposant (aussi bien les connaissances que les croyances et les intentions des prescripteurs), les facteurs potentialisant (notamment la disponibilité de l’AS-AQ de bonne qualité, son accessibilité financière aux patients) et les facteurs renforçant (supervision, contrats de performance).

•de renforcer le plateau technique des HGR et y améliorer le circuit des patients pour leur permettre de jouer pleinement leur rôle dans la prise en charge des formes graves du paludisme. /

Second most endemic country for malaria in the world, the Democratic Republic of Congo (DRC) has officially adopted the Roll Back Malaria (RBM) in 2001, since then aligns its malaria control policy on WHO guidelines which last orientations are based on three major strategies [1] prompt access to effective treatment and affordable for the patients [2] association of the most appropriate measures to protect the persons at risk both at individual and community level, including young children and pregnant women, [3] and access to preventive treatments to pregnant women at risk.

In order to contribute in improving malaria control in DRC, the study was carried out in three parts: the first one on the relevance of IPT with SP in pregnant women in the context of increased parasite resistance, the second one on the determinants of adherence of healthcare providers, drugs sellers and patients to AS-AQ, the last one describing severe malaria in children.

The first part of the study on IPTp-SP was performed in 2 stages. We had firstly carried out a retrospective analysis of birth weight comparing newborns whom mothers had received 2 SP doses to those whom mothers had received one or none, in three maternity hospitals in 2007 where levels of SP resistance were different. Then we evaluated the effect of IPTp-SP in 1998/1999 and 2007 compared to prophylaxis with chloroquine in 1998/1999 in eastern DRC in a region where resistance to SP was significantly increased.

In areas where parasite resistance was low (Mikalayi: 1.6% of therapeutic failure in children) our moderate (Kisangani: 21.7% of therapeutic failure in children), the IPTp-SP reduced the risk of LBW in Kisangani (OR adjusted 0.15, 95% CI, 0.04-0.58) and Mikalayi (adjusted OR, 0.12, 95% CI, 0.01-0.89). In both sites, the average birth weight was higher for mothers having received two rather than one or no SP doses (P<0.001). While in Rutshuru, where resistance was high (60.6% treatment failure), the effect of IPT-SP seems lower. In 2007, IPTp-SP had an effect only in primigravidae (dose-response comparison: 2 doses vs. 0-1dose). It was also observed in a slight decrease in body weight gain [(53.9 g (P = 0.027) for mothers having received SP in 2007 vs. 70.2 g (P = 0.003) for those mothers who had received SP in 1998/1999 compared to mothers who had received chloroquine in 1998/1999.

In the second part of the thesis, two cross-sectional surveys were carried out to identify determinants of the adherence of healthcare providers, drugs sellers and patients to the new drug recommended by the national policy for the treatment of uncomplicated malaria (AS-AQ). A preliminary survey was conducted in functional health centre in Kisangani in April 2008 and a second survey extended to three out of 10 health districts in the Eastern Province from March to June 2009.

The use of AS-AQ for the treatment of uncomplicated malaria progresses (from 41% to 69% prescriptions in health services between 2008 and 2009, 3 and 4 years respectively after the malaria control policy change), but still below the target of at least 80% pursued by national policy. Despite the perceived efficacy of AS-AQ by both healthcare providers and drugs vendors, its use was limited due to its low availability, high cost, mistrust on the quality of the available product, availability of inexpensive antimalarial drugs withdrew from national politicy and the fear for adverse effects. While the incentives for its use were, the therapeutic efficacy, availability, directives of the ministries of health (technical guidelines), training and supervision of healthcare providers, the intention to prescribe AS-AQ to patients or to use oneself, lengthy consultations, providing explanations to patients, working in rural areas.

The last part of the thesis was a prospective study conducted from January 2010 to February 2011 that included all children admitted for severe malaria with at least one of the criteria for severe malaria according to WHO.

Malaria is one of the main reasons for hospitalization of children in the DRC (37.0% in Kisangani) whose evaluation is often uncompleted (53.6% no or negative blood smear that are insufficiently explored and treated as severe malaria) and sometimes inadequately treated (in addition to non-malarial severe diseases treated as severe malaria, there was overuse of blood products conducting probably to exposition of children to risks of infection through transfusion). Thus, poor technical support and inadequate organization of the patient circuit seem to lead to underestimation, among others, of metabolic complications of severe malaria and in the non-recognition of other serious infections early childhood, problems that are detrimental to the patients, even when effective drugs are available.

These results highlight the need:

•to include among the priorities of the National Malaria Control Program, research to evaluate an alternative option to 2 doses IPTp-SP (IPT using other antimalarial drugs) and in the east of the country preferential use of MILD, especially in multigravidae.

•for the use of AS-AQ for the treatment of uncomplicated malaria primarily promote:

o the use of current funding opportunities in the field of malaria control to improve the availability of the AS-AQ at an affordable cost and to improve the supply of both public and private health facilities as well as pharmacies;

o to clean up the pharmaceutical sector in order to stem the flow of poor quality cheapest antimalarial drugs that feeds the habits of self-medication common in households;

o to develop communication programs, training and supervision of healthcare providers to promote the use of AS-AQ, expanding the target of interventions to both healthcare providers in the private sector and drugs sellers;

o To adapt AS-AQ promoting programs to the stage of behavior change after analysis of determinants of actors behavior, in particular, the predisposing factors (knowledge as well as beliefs and intentions of the prescriber), the potentializing factors (including the availability of the good quality AS-AQ, affordability to patients) and reinforcing factors (supervision, performance contracts).

•to strengthen the technical support of general hospitals and to improve the organization of the patient circuit in order to enable them to play their full role in the management of severe malaria.

Doctorat en Sciences de la santé publique
info:eu-repo/semantics/nonPublished

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)

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The aim of this chapter is to illustrate some current developments in natural product-derived antimalarial drugs. Traditional medicines have provided two of our most important antimalarial drugs (quinine and artemisinin) and have the potential to provide many novel antimalarial lead compounds of which several examples will be discussed. In addition, well- known natural antimalarials such as artemisinin continue to be an important focus of research and there is also increasing interest in investigating natural product sources that have not been traditionally used as antimalarials such as marine species of plants and animals. Assays based on specific malaria parasite targets such as thioredoxin reductase and heat shock protein have been employed to screen extracts and/or compounds and these have resulted in the identification of a number of potentially interesting antiplasmodial agents. However, since many victims of malaria are unable to afford antimalarial drugs, another approach adopted by some charities/NGO’s is to encourage people to grow their own medicinal plants such as Artemisia annua; some recent studies on this theme will be discussed.

Malaria affects about forty percent of the world’s population. Annually more than 1.5 million fatalities due to malaria occur and parasite resistance to existing antimalarial drugs such as mefloquine has already reached disturbingly high levels in South-East Asia and on the African continent. Consequently, there is a dire need for new drugs or formulations in the prophylaxis and treatment of malaria. Artesunate, an artemisinin derivative, represents a new category of antimalarials that is effective against drug-resistant Plasmodium falciparum strains and is of significance in the current antimalarial campaign. As formulating an ACT double fixed-dose combination is technically difficult, it is essential that fixed-dose combinations are shown to have satisfactory ingredient compatibility, stability, and dissolution rates similar to the separate oral dosage forms. Since the general deployment of a combination of artesunate and mefloquine in 1994, the cure rate increased again to almost 100% from 1998 onwards, and there has been a sustained decline in the incidence of Plasmodium falciparum malaria in the experimental studies (Nosten et al., 2000:297; WHO, 2010:17). However, the successful formulation of a solid oral dosage form and fixed dosage combination of artesunate and mefloquine remains both a market opportunity and a challenge. Artesunate and mefloquine both exhibited poor flow properties. Furthermore, different elimination half-lives, treatment dosages as well as solubility properties of artesunate and mefloquine required different formulation approaches. To substantiate the FDA’s pharmaceutical quality by design concept, the double fixed-dose combination of artesunate and mefloquine required strict preliminary formulation considerations regarding compatibility between excipients and between the APIs. Materials and process methods were only considered if theoretically and experimentally proved safe. Infrared absorption spectroscopy (IR) and X-ray powder diffraction (XRPD) data proved compatibility between ingredients and stability during the complete manufacturing process by a peak by peak correlation. Scanning Electron Micrographs (SEM) provided explanations for the inferior flow properties exhibited by the investigated APIs. Particle size analysis and SEM micrographs confirmed that the larger, rounder and more consistently sized particles of the granulated APIs contributed to improved flow under the specified testing conditions. A compressible mixture containing 615 mg of the APIs in accordance with the WHO recommendation of 25 mg/kg of mefloquine taken in two or three divided dosages, and 4 mg/kg/day for 3 days of artesunate for uncomplicated falciparum malaria was developed. Mini-tablets of artesunate and mefloquine were compressed separately and successfully with the required therapeutic dosages and complied with pharmacopoeial standards. Preformulation studies eventually led to a formula for a double fixed-dose combination and with the specific aim of delaying the release of artesunate due to its short half-life. A factorial design revealed the predominant factors contributing to the successful wet granulation of artesunate and mefloquine. A fractional factorial design identified the optimum factors and factor levels. The application of the granulation fluid (20% w/w) proved to be sufficient by a spraying method for both artesunate and mefloquine. A compatible acrylic polymer and coating agent for artesunate, Eudragit® L100 was employed to delay the release of approximately half of the artesunate dose from the double fixed-dose combination tablet until a pH of 6.8. A compressible mixture was identified and formulated to contain 200 mg of artesunate and 415 mg of mefloquine per tablet. The physical properties of the tablets complied with BP standards. An HPLC method from available literature was adapted and validated for analytical procedures. Dissolution studies according to a USP method were conducted to verify and quantify the release of the APIs in the double fixed-dose combination. The initial dissolution rate (DRi) of artesunate and mefloquine in the acidic dissolution medium was rapid as required. The enteric coated fraction of the artesunate exhibited no release in an acidic environment after 2 hours, but rapid release in a medium with a pH of 6.8. The structure of the granulated particles of mefloquine may have contributed to its first order release profile in the dissolution mediums. A linear correlation was present between the rate of mefloquine release and the percentage of mefloquine dissolved (R2 = 0.9484). Additionally, a linear relationship was found between the logarithm of the percentage mefloquine remaining against time (R2 = 0.9908). First order drug release is the dominant release profile found in the pharmaceutical industry today and is coherent with the kinetics of release obtained for mefloquine. A concept pre-clinical phase, double fixed-dose combination solid oral dosage form for artesunate and mefloquine was developed. The double fixed-dose combination was designed in accordance with the WHO’s recommendation for an oral dosage regimen of artesunate and mefloquine for the treatment of uncomplicated falciparum malaria. The specifications of the double fixed-dose combination were developed in close accordance with the FDA’s quality by design concept and WHO recommendations. An HPLC analytical procedure was developed to verify the presence of artesunate and mefloquine. The dissolution profiles of artesunate and mefloquine were investigated during the dissolution studies.
PhD (Pharmaceutics), North-West University, Potchefstroom Campus, 2014