Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania

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Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania. / Massaga, J J; Lusingu, J P; Makunde, R; Malebo, H M; Chile, M M; Akida, J A; Lemnge, M M; Rønn, A M; Theander, T G; Bygbjerg, I C; Kitua, A Y.

In: Tanzania Health Research Bulletin, Vol. 10, No. 3, 2008, p. 144-50.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Massaga, JJ, Lusingu, JP, Makunde, R, Malebo, HM, Chile, MM, Akida, JA, Lemnge, MM, Rønn, AM, Theander, TG, Bygbjerg, IC & Kitua, AY 2008, 'Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania', Tanzania Health Research Bulletin, vol. 10, no. 3, pp. 144-50.

APA

Massaga, J. J., Lusingu, J. P., Makunde, R., Malebo, H. M., Chile, M. M., Akida, J. A., Lemnge, M. M., Rønn, A. M., Theander, T. G., Bygbjerg, I. C., & Kitua, A. Y. (2008). Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania. Tanzania Health Research Bulletin, 10(3), 144-50.

Vancouver

Massaga JJ, Lusingu JP, Makunde R, Malebo HM, Chile MM, Akida JA et al. Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania. Tanzania Health Research Bulletin. 2008;10(3):144-50.

Author

Massaga, J J ; Lusingu, J P ; Makunde, R ; Malebo, H M ; Chile, M M ; Akida, J A ; Lemnge, M M ; Rønn, A M ; Theander, T G ; Bygbjerg, I C ; Kitua, A Y. / Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania. In: Tanzania Health Research Bulletin. 2008 ; Vol. 10, No. 3. pp. 144-50.

Bibtex

@article{fd368b40e60811ddbf70000ea68e967b,
title = "Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania",
abstract = "Amodiaquine (AQ), an effective antimalarial drug for uncomplicated malaria, has been greatly restricted after cases of life-threatening agranulocytosis and hepatic toxicity during prophylactic use. We conducted a hospital based open-label randomised clinical trial in 40 indigenous semi-immune healthy adult male volunteers with and without malaria parasites. The objective was to collect data on biological and haematological safety, tolerability, and parasitological efficacy to serve as baseline in the evaluation of the effectiveness of AQ preventive intermittent treatment against malaria morbidity in infants. Volunteers were stratified according to parasitaemia status and randomly assigned 20 participants each arm to three days treatment with either AQ or chloroquine (CQ). The level of difference of selected haematological and hepatological values pre-and post-trial were marginal and within the normal limits. Clinical adverse effects mostly mild and transient were noticed in 33.3% CQ treated-aparasitaemic, 23.8% of CQ treated-parasitaemic, 28.6% ofAQ-treated parasitaemic and 14.3% of aparasitaemic receiving AQ. Amodiaquine attained 100% parasitological clearance rate versus 70% in CQ-treated volunteers. The findings indicate that there was no agranulocytosis or hepatic toxicity suggesting that AQ may pose no public health risk in its wide therapeutic dosage uses. Larger studies are needed to exclude rare adverse effects.",
author = "Massaga, {J J} and Lusingu, {J P} and R Makunde and Malebo, {H M} and Chile, {M M} and Akida, {J A} and Lemnge, {M M} and R{\o}nn, {A M} and Theander, {T G} and Bygbjerg, {I C} and Kitua, {A Y}",
year = "2008",
language = "English",
volume = "10",
pages = "144--50",
journal = "Tanzania health research bulletin",
issn = "0856-6496",
publisher = "National Institute for Medical Research Health Research Users' Trust Fund",
number = "3",

}

RIS

TY - JOUR

T1 - Biological and haematological safety profile of oral amodiaquine and chloroquine in healthy volunteers with or without Plasmodium falciparum infection in northeast Tanzania

AU - Massaga, J J

AU - Lusingu, J P

AU - Makunde, R

AU - Malebo, H M

AU - Chile, M M

AU - Akida, J A

AU - Lemnge, M M

AU - Rønn, A M

AU - Theander, T G

AU - Bygbjerg, I C

AU - Kitua, A Y

PY - 2008

Y1 - 2008

N2 - Amodiaquine (AQ), an effective antimalarial drug for uncomplicated malaria, has been greatly restricted after cases of life-threatening agranulocytosis and hepatic toxicity during prophylactic use. We conducted a hospital based open-label randomised clinical trial in 40 indigenous semi-immune healthy adult male volunteers with and without malaria parasites. The objective was to collect data on biological and haematological safety, tolerability, and parasitological efficacy to serve as baseline in the evaluation of the effectiveness of AQ preventive intermittent treatment against malaria morbidity in infants. Volunteers were stratified according to parasitaemia status and randomly assigned 20 participants each arm to three days treatment with either AQ or chloroquine (CQ). The level of difference of selected haematological and hepatological values pre-and post-trial were marginal and within the normal limits. Clinical adverse effects mostly mild and transient were noticed in 33.3% CQ treated-aparasitaemic, 23.8% of CQ treated-parasitaemic, 28.6% ofAQ-treated parasitaemic and 14.3% of aparasitaemic receiving AQ. Amodiaquine attained 100% parasitological clearance rate versus 70% in CQ-treated volunteers. The findings indicate that there was no agranulocytosis or hepatic toxicity suggesting that AQ may pose no public health risk in its wide therapeutic dosage uses. Larger studies are needed to exclude rare adverse effects.

AB - Amodiaquine (AQ), an effective antimalarial drug for uncomplicated malaria, has been greatly restricted after cases of life-threatening agranulocytosis and hepatic toxicity during prophylactic use. We conducted a hospital based open-label randomised clinical trial in 40 indigenous semi-immune healthy adult male volunteers with and without malaria parasites. The objective was to collect data on biological and haematological safety, tolerability, and parasitological efficacy to serve as baseline in the evaluation of the effectiveness of AQ preventive intermittent treatment against malaria morbidity in infants. Volunteers were stratified according to parasitaemia status and randomly assigned 20 participants each arm to three days treatment with either AQ or chloroquine (CQ). The level of difference of selected haematological and hepatological values pre-and post-trial were marginal and within the normal limits. Clinical adverse effects mostly mild and transient were noticed in 33.3% CQ treated-aparasitaemic, 23.8% of CQ treated-parasitaemic, 28.6% ofAQ-treated parasitaemic and 14.3% of aparasitaemic receiving AQ. Amodiaquine attained 100% parasitological clearance rate versus 70% in CQ-treated volunteers. The findings indicate that there was no agranulocytosis or hepatic toxicity suggesting that AQ may pose no public health risk in its wide therapeutic dosage uses. Larger studies are needed to exclude rare adverse effects.

M3 - Journal article

C2 - 19024339

VL - 10

SP - 144

EP - 150

JO - Tanzania health research bulletin

JF - Tanzania health research bulletin

SN - 0856-6496

IS - 3

ER -

ID: 9829443