Randomized Controlled Trial of Levamisole Hydrochloride as Adjunctive Therapy in Severe Falciparum Malaria With High Parasitemia

Maude, Richard J.; Silamut, Kamolrat; Plewes, Katherine; Charunwatthana, Prakaykaew; Ho, May; Faiz, M. Abul; Rahman, Ridwanur; Hossain, Amir; Hassan, M. Kabir; Yunus, Emran Bin; Hoque, Gofranul; Islam, Faridul; Ghose, Aniruddha; Hanson, Josh; Schlatter, Joël; Lacey, Rachel; Eastaugh, Alison; Tärning, Joel; Lee, Sue J.; White, Nicholas J.; Chotivanich, Kesinee; Day, Nicholas P. J.; Dondorp, Arjen M.

doi:10.1093/infdis/jit410

Cited by 42 publications

(37 citation statements)

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“…In a similar fashion, dichloracetate may be effective at reducing plasma lactate levels [34], however, it seems unlikely to be an effective adjuvant reducing the underlying causes of tissue hypoxia and mortality. Several of the current experimental adjuvant or supporting treatments are aiming at an improvement of the microcirculation in severe malaria, including nitric oxide donors [35, 36], and compounds affecting cytoadhesion and sequestration [15, 37]. Our results suggest that improvement in blood or plasma lactate concentrations over time is an adequate endpoint for trials evaluating these interventions.…”

Section: Discussionmentioning

confidence: 80%

“…Serial GCS (assessed 6 hourly) and lactate (assessed 6 hourly) data from adult patients with severe malaria enrolled in studies at Chittagong Medical College Hospital (CMCH), Chittagong, Bangladesh between 2005 and 2012. The Bangladeshi patients were enrolled in observational and treatment studies including studies on levamisole, timing of enteral feeding, N-acetylcysteine and paracetamol [15, 18, 20, 22]. These randomized clinical trials were monitored internally as well as by an outside monitor.…”

Section: Methodsmentioning

confidence: 99%

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Defining Surrogate Endpoints for Clinical Trials in Severe Falciparum Malaria

et al. 2017

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BackgroundClinical trials in severe falciparum malaria require a large sample size to detect clinically meaningful differences in mortality. This means few interventions can be evaluated at any time. Using a validated surrogate endpoint for mortality would provide a useful alternative allowing a smaller sample size. Here we evaluate changes in coma score and plasma lactate as surrogate endpoints for mortality in severe falciparum malaria.MethodsThree datasets of clinical studies in severe malaria were re-evaluated: studies from Chittagong, Bangladesh (adults), the African ‘AQUAMAT’ trial comparing artesunate and quinine (children), and the Vietnamese ‘AQ’ study (adults) comparing artemether with quinine. The absolute change, relative change, slope of the normalization over time, and time to normalization were derived from sequential measurements of plasma lactate and coma score, and validated for their use as surrogate endpoint, including the proportion of treatment effect on mortality explained (PTE) by these surrogate measures.ResultsImprovements in lactate concentration or coma scores over the first 24 hours of admission, were strongly prognostic for survival in all datasets. In hyperlactataemic patients in the AQ study (n = 173), lower mortality with artemether compared to quinine closely correlated with faster reduction in plasma lactate concentration, with a high PTE of the relative change in plasma lactate at 8 and 12 hours of 0.81 and 0.75, respectively. In paediatric patients enrolled in the ‘AQUAMAT’ study with cerebral malaria (n = 785), mortality was lower with artesunate compared to quinine, but this was not associated with faster coma recovery.ConclusionsThe relative changes in plasma lactate concentration assessed at 8 or 12 hours after admission are valid surrogate endpoints for severe malaria studies on antimalarial drugs or adjuvant treatments aiming at improving the microcirculation. Measures of coma recovery are not valid surrogate endpoints for mortality.

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Section: Discussionmentioning

confidence: 80%

Section: Methodsmentioning

confidence: 99%

Defining Surrogate Endpoints for Clinical Trials in Severe Falciparum Malaria

et al. 2017

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“…Only one patient died (control) arm.Maude et al . [126]Chittagong, Bangladesh>or = 16 years P. falciparum (>2%) plus modified WHO severe malaria criteria N = 60Phase II Controlled RCT Levamisole 150 mg po or ng stat dose immediately vs control plus artesunateComposite: Clinical Death or coma recovery Parasite clearance and lactate Pharmacodynamics Microvascular flowDeath 5/29 (17%) Levamisole vs 9/27 (33%) P = 0.22Levamisole inhibits cytoadherence in vitro and reduces sequestration of late-stage parasites.No differences in proportions of trophozoites, measures of parasite clearance in blood over 30 hours or effects sequestrationSpeculated whether rapid clearance of malaria parasites by artesunate may obscure beneficial effects of levamisole. Seizure prophylaxis White et al [127]ThailandChildren >6 years and adultsCerebral malaria N = 46Double blind RCT: 3.5 mg/kg single dose given IM phenobarbitone (Pb) n = 24 Control (n. saline) n = 241 0 Seizure prevention1 0 Convulsions in Pb arm 3/24 (12-5%), vs 13/24 (54%) placebo ( P = 0-006).Seizures prevention superior2 0 Death2 0 Deaths 8 (33%) in Pb arm 5 (20.8) placebo arm ( P = 0.5)Small numbers in trial not able to assess effect on mortality.Kochar et al [130]Rajasthan, IndiaAdults age 14 to 74 yearsCerebral malaria N = 185Randomly assigned:Not specified3/102 (3%) developed seizures after admission in Pb arm vs 19/83 (22.9%) controlReported as a correspondence not formally reported as a peer reviewed manuscript.10 mg/kg im one dose of phenobabitone (Pb) (n = 102) Control (n = 83)Deaths Pb: 29/102 (28.4% vs control 33/83 (39.8%)PbCrawley et al [128]Kilifi, KenyaChildren 9 months to 13 yearsCerebral malaria N = 340Placebo controlled trial1 0 Seizure prevention1 0 Seizure frequency lower in the Pb arm vs placebo group (18 (11%) vs 46 (27%) children had 3 or more seizures OR: 0.32 (95% CI 0.18 to 0.58)Frequency of respiratory arrest was higher in the phenobarbital arm vs placebo arm170 Pb arm/170 placebo armA single intramuscular dose of phenobarbital (Pb) (20 mg/kg) or identical placebo plus quinine2 0 Death2 0 Mortality higher in phenobarbitone arm (30 (18%) vs 14 (8%) deaths; OR 2.39 (1.28–4.64)).Mortality substantially increased in children who received phenobarbital plus three or more doses of diazepam (OR 31.7 (1.2 to 814))Not recommended in CM.Gwer et al [129]two centres Kilifi and Kisumu hospitals, Kenya…”

Section: Introductionmentioning

confidence: 99%

Management of severe paediatric malaria in resource-limited settings

Maitland

2015

BMC Med

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Over 90% of the world’s severe and fatal Plasmodium falciparum malaria is estimated to affect young children in sub-Sahara Africa, where it remains a common cause of hospital admission and inpatient mortality. Few children will ever be managed on high dependency or intensive care units and, therefore, rely on simple supportive treatments and parenteral anti-malarials. There has been some progress on defining best practice for antimalarial treatment with the publication of the AQUAMAT trial in 2010, involving 5,425 children at 11 centres across 9 African countries, showing that in artesunate-treated children, the relative risk of death was 22.5% (95% confidence interval (CI) 8.1 to 36.9) lower than in those receiving quinine. Human trials of supportive therapies carried out on the basis of pathophysiology studies, have so far made little progress on reducing mortality; despite appearing to reduce morbidity endpoints, more often than not they have led to an excess of adverse outcomes. This review highlights the spectrum of complications in African children with severe malaria, the therapeutic challenges of managing these in resource-poor settings and examines in-depth the results from clinical trials with a view to identifying the treatment priorities and a future research agenda.

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“…Although the manifestations of this phenomenon have been described extensively, the underlying mechanisms are not fully elucidated, and therefore, efficient therapeutic interventions have not yet been developed. The host scavenger receptor CD36 is thought to play a central role in malaria-induced ALI/ARDS [2], and the targeting of this molecule has been proposed as an adjunctive therapy for severe malaria [3]. The study by Lagassé et al [4] in this issue of the Journal of Leukocyte Biology shows why, despite its importance in ALI/ARDS, CD36 may not be a good therapeutic target.…”

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confidence: 99%

“…The effect of CD36-blocking therapies on malariainduced lung injuries would thus be uncertain. In fact, they have been shown to induce no improvement when used as adjunctive therapy for severe P. falciparum malaria [3]. Therefore, the use of CD36-blocking molecules for therapeutic intervention in malaria should be reconsidered.…”

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confidence: 99%

Editorial: CD36: Russian roulette of host and parasites during malaria infection

Brugat

2016

Journal of Leukocyte Biology

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Pulmonary complications occur in a significant percentage of adults and children during the course of severe malaria. The cellular and molecular innate immune mechanisms that limit the extent of pulmonary inflammation and preserve lung function during severe Plasmodium infections remain unclear. In particular, the contributions to pulmonary complications by parasitized erythrocyte sequestration and subsequent clearance from the lung microvasculature by immune cells have not been clearly defined. We used the Plasmodium berghei ANKA-C57BL/6 mouse model of severe malaria to investigate the mechanisms governing the nature and extent of malaria-associated lung injury. We have demonstrated that sequestration of infected erythrocytes on postcapillary endothelial surfaces results in acute lung injury and the rapid recruitment of CCR2 + CD11b + Ly6C hi monocytes from the circulation. These recruited cells remain in the lungs as monocyte-derived macrophages and are instrumental in the phagocytic clearance of adherent Plasmodium bergheiinfected erythrocytes. In contrast, alveolar macrophages do not play a significant role in the clearance of malariainfected cells. Furthermore, the results obtained from Ccr2 2/2 , Cd36 2/2 , and CD36 bone marrow chimeric mice showed that sequestration in the absence of CD36mediated phagocytic clearance by monocytes leads to exaggerated lung pathologic features. In summary, our data indicate that the intensity of malaria-induced lung pathologic features is proportional to the steady-state levels of Plasmodium-infected erythrocytes adhering to the pulmonary vasculature. Moreover, the present work has defined a major role of recruited monocytes in clearing infected erythrocytes from the pulmonary interstitium, thus minimizing lung damage. J. Leukoc. Biol. 99: 659-671; 2016.Abbreviations: AMs = alveolar macrophages, ALI = acute lung injury, BAL = bronchoalveolar lavage, DF CO = diffusion factor for carbon monoxide, MDMs = monocyte-derived macrophages, MHCII = major histocompatibility II, tdTPbA = Plasmodium berghei ANKA transgenic for tdTomato, WT = wild typeThe online version of this paper, found at www.jleukbio.org, includes supplemental information. 0741-5400/16/0099-659A 19-gauge gavage tube was inserted into the trachea, and the lungs were inflated with zinc-buffered formalin (Anatech Ltd., Battle Creek, MI, USA) at 30 cm H 2 O. The lungs were removed, incubated in zinc-buffered formalin for

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Randomized Controlled Trial of Levamisole Hydrochloride as Adjunctive Therapy in Severe Falciparum Malaria With High Parasitemia

Cited by 42 publications

References 46 publications

Defining Surrogate Endpoints for Clinical Trials in Severe Falciparum Malaria

Defining Surrogate Endpoints for Clinical Trials in Severe Falciparum Malaria

Management of severe paediatric malaria in resource-limited settings

Editorial: CD36: Russian roulette of host and parasites during malaria infection

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