Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children

Patrick Tumwebaze; Melissa D. Conrad; Andrew Walakira; Norbert LeClair; Oswald Byaruhanga; Christine Nakazibwe; Benjamin Kozak; Jessica Bloome; Jaffer Okiring; Abel Kakuru; Victor Bigira; James Kapisi; Jennifer Legac; Jiri Gut; Roland A. Cooper; Moses R. Kamya; Diane V. Havlir; Grant Dorsey; Bryan Greenhouse; Samuel L. Nsobya; Philip J. Rosenthal

Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children

Patrick Tumwebaze
, Melissa D. Conrad
, Andrew Walakira
, Norbert LeClair
, Oswald Byaruhanga
, Christine Nakazibwe
, Benjamin Kozak
, Jessica Bloome
, Jaffer Okiring
, Abel Kakuru
, Victor Bigira
, James Kapisi
, Jennifer Legac
, Jiri Gut
, Roland A. Cooper
, Moses R. Kamya
, Diane V. Havlir
, Grant Dorsey
, Bryan Greenhouse
, Samuel L. Nsobya

Philip J. Rosenthal

Department of Natural Sciences and Mathematics

Research output: Contribution to journal › Article › peer-review

Abstract

Changing treatment practices may be selecting for changes in the drug sensitivity of malaria parasites. We characterized ex vivo drug sensitivity and parasite polymorphisms associated with sensitivity in 459 Plasmodium falciparum samples obtained from subjects enrolled in two clinical trials in Tororo, Uganda, from 2010 to 2013. Sensitivities to chloroquine and monodesethylamodiaquine varied widely; sensitivities to quinine, dihydroartemisinin, lumefantrine, and piperaquine were generally good. Associations between ex vivo drug sensitivity and parasite polymorphisms included decreased chloroquine and monodesethylamodiaquine sensitivity and increased lumefantrine and piperaquine sensitivity with pfcrt 76T, as well as increased lumefantrine sensitivity with pfmdr1 86Y, Y184, and 1246Y. Over time, ex vivo sensitivity decreased for lumefantrine and piperaquine and increased for chloroquine, the prevalences of pfcrt K76 and pfmdr1 N86 and D1246 increased, and the prevalences of pfdhfr and pfdhps polymorphisms associated with antifolate resistance were unchanged. In recurrent infections, recent prior treatment with artemether-lumefantrine was associated with decreased ex vivo lumefantrine sensitivity and increased prevalence of pfcrt K76 and pfmdr1 N86, 184F, and D1246. In children assigned chemoprevention with monthly dihydroartemisinin-piperaquine with documented circulating piperaquine, breakthrough infections had increased the prevalence of pfmdr1 86Y and 1246Y compared to untreated controls. The noted impacts of therapy and chemoprevention on parasite polymorphisms remained significant in multivariate analysis correcting for calendar time. Overall, changes in parasite sensitivity were consistent with altered selective pressures due to changing treatment practices in Uganda. These changes may threaten the antimalarial treatment and preventive efficacies of artemether-lumefantrine and dihydroartemisinin-piperaquine, respectively.

Original language	American English
Pages (from-to)	3018-3030
Number of pages	13
Journal	Antimicrobial Agents and Chemotherapy
Volume	59
Issue number	6
State	Published - Mar 9 2015

Funding

This work was supported by grants from the National Institutes of Health (AI075045, HD059454, AI089674, and TW007375) and the Doris Duke Charitable Foundation.

Funders	Funder number
National Institutes of Health	AI089674, HD059454, TW007375
National Institute of Allergy and Infectious Diseases	R01AI075045
Doris Duke Charitable Foundation

ASJC Scopus Subject Areas

Pharmacology
Pharmacology (medical)
Infectious Diseases

Keywords

malaria
Plasmodium falciparum
Uganda

Disciplines

Medicinal Chemistry and Pharmaceutics
Parasitic Diseases
Pharmacology, Toxicology and Environmental Health

Access to Document

Impact of Antimalarial Treatment and Chemoprevention on the DrugFinal published version, 978 KBLicense: Unspecified

OpenUrl availability

Full text

Cite this

Tumwebaze, P., Conrad, M. D., Walakira, A., LeClair, N., Byaruhanga, O., Nakazibwe, C., Kozak, B., Bloome, J., Okiring, J., Kakuru, A., Bigira, V., Kapisi, J., Legac, J., Gut, J., Cooper, R. A., Kamya, M. R., Havlir, D. V., Dorsey, G., Greenhouse, B., ... Rosenthal, P. J. (2015). Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children. Antimicrobial Agents and Chemotherapy, 59(6), 3018-3030.

Tumwebaze, P, Conrad, MD, Walakira, A, LeClair, N, Byaruhanga, O, Nakazibwe, C, Kozak, B, Bloome, J, Okiring, J, Kakuru, A, Bigira, V, Kapisi, J, Legac, J, Gut, J, Cooper, RA, Kamya, MR, Havlir, DV, Dorsey, G, Greenhouse, B, Nsobya, SL & Rosenthal, PJ 2015, 'Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children', Antimicrobial Agents and Chemotherapy, vol. 59, no. 6, pp. 3018-3030.

@article{ff9c3f50c4ce4e98a56a25e3381bcd95,

title = "Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children",

abstract = "Changing treatment practices may be selecting for changes in the drug sensitivity of malaria parasites. We characterized ex vivo drug sensitivity and parasite polymorphisms associated with sensitivity in 459 Plasmodium falciparum samples obtained from subjects enrolled in two clinical trials in Tororo, Uganda, from 2010 to 2013. Sensitivities to chloroquine and monodesethylamodiaquine varied widely; sensitivities to quinine, dihydroartemisinin, lumefantrine, and piperaquine were generally good. Associations between ex vivo drug sensitivity and parasite polymorphisms included decreased chloroquine and monodesethylamodiaquine sensitivity and increased lumefantrine and piperaquine sensitivity with pfcrt 76T, as well as increased lumefantrine sensitivity with pfmdr1 86Y, Y184, and 1246Y. Over time, ex vivo sensitivity decreased for lumefantrine and piperaquine and increased for chloroquine, the prevalences of pfcrt K76 and pfmdr1 N86 and D1246 increased, and the prevalences of pfdhfr and pfdhps polymorphisms associated with antifolate resistance were unchanged. In recurrent infections, recent prior treatment with artemether-lumefantrine was associated with decreased ex vivo lumefantrine sensitivity and increased prevalence of pfcrt K76 and pfmdr1 N86, 184F, and D1246. In children assigned chemoprevention with monthly dihydroartemisinin-piperaquine with documented circulating piperaquine, breakthrough infections had increased the prevalence of pfmdr1 86Y and 1246Y compared to untreated controls. The noted impacts of therapy and chemoprevention on parasite polymorphisms remained significant in multivariate analysis correcting for calendar time. Overall, changes in parasite sensitivity were consistent with altered selective pressures due to changing treatment practices in Uganda. These changes may threaten the antimalarial treatment and preventive efficacies of artemether-lumefantrine and dihydroartemisinin-piperaquine, respectively.",

keywords = "malaria, Plasmodium falciparum, Uganda",

author = "Patrick Tumwebaze and Conrad, \{Melissa D.\} and Andrew Walakira and Norbert LeClair and Oswald Byaruhanga and Christine Nakazibwe and Benjamin Kozak and Jessica Bloome and Jaffer Okiring and Abel Kakuru and Victor Bigira and James Kapisi and Jennifer Legac and Jiri Gut and Cooper, \{Roland A.\} and Kamya, \{Moses R.\} and Havlir, \{Diane V.\} and Grant Dorsey and Bryan Greenhouse and Nsobya, \{Samuel L.\} and Rosenthal, \{Philip J.\}",

year = "2015",

month = mar,

day = "9",

language = "American English",

volume = "59",

pages = "3018--3030",

journal = "Antimicrobial Agents and Chemotherapy",

issn = "1098-6596",

number = "6",

}

TY - JOUR

T1 - Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children

AU - Tumwebaze, Patrick

AU - Conrad, Melissa D.

AU - Walakira, Andrew

AU - LeClair, Norbert

AU - Byaruhanga, Oswald

AU - Nakazibwe, Christine

AU - Kozak, Benjamin

AU - Bloome, Jessica

AU - Okiring, Jaffer

AU - Kakuru, Abel

AU - Bigira, Victor

AU - Kapisi, James

AU - Legac, Jennifer

AU - Gut, Jiri

AU - Cooper, Roland A.

AU - Kamya, Moses R.

AU - Havlir, Diane V.

AU - Dorsey, Grant

AU - Greenhouse, Bryan

AU - Nsobya, Samuel L.

AU - Rosenthal, Philip J.

PY - 2015/3/9

Y1 - 2015/3/9

N2 - Changing treatment practices may be selecting for changes in the drug sensitivity of malaria parasites. We characterized ex vivo drug sensitivity and parasite polymorphisms associated with sensitivity in 459 Plasmodium falciparum samples obtained from subjects enrolled in two clinical trials in Tororo, Uganda, from 2010 to 2013. Sensitivities to chloroquine and monodesethylamodiaquine varied widely; sensitivities to quinine, dihydroartemisinin, lumefantrine, and piperaquine were generally good. Associations between ex vivo drug sensitivity and parasite polymorphisms included decreased chloroquine and monodesethylamodiaquine sensitivity and increased lumefantrine and piperaquine sensitivity with pfcrt 76T, as well as increased lumefantrine sensitivity with pfmdr1 86Y, Y184, and 1246Y. Over time, ex vivo sensitivity decreased for lumefantrine and piperaquine and increased for chloroquine, the prevalences of pfcrt K76 and pfmdr1 N86 and D1246 increased, and the prevalences of pfdhfr and pfdhps polymorphisms associated with antifolate resistance were unchanged. In recurrent infections, recent prior treatment with artemether-lumefantrine was associated with decreased ex vivo lumefantrine sensitivity and increased prevalence of pfcrt K76 and pfmdr1 N86, 184F, and D1246. In children assigned chemoprevention with monthly dihydroartemisinin-piperaquine with documented circulating piperaquine, breakthrough infections had increased the prevalence of pfmdr1 86Y and 1246Y compared to untreated controls. The noted impacts of therapy and chemoprevention on parasite polymorphisms remained significant in multivariate analysis correcting for calendar time. Overall, changes in parasite sensitivity were consistent with altered selective pressures due to changing treatment practices in Uganda. These changes may threaten the antimalarial treatment and preventive efficacies of artemether-lumefantrine and dihydroartemisinin-piperaquine, respectively.

AB - Changing treatment practices may be selecting for changes in the drug sensitivity of malaria parasites. We characterized ex vivo drug sensitivity and parasite polymorphisms associated with sensitivity in 459 Plasmodium falciparum samples obtained from subjects enrolled in two clinical trials in Tororo, Uganda, from 2010 to 2013. Sensitivities to chloroquine and monodesethylamodiaquine varied widely; sensitivities to quinine, dihydroartemisinin, lumefantrine, and piperaquine were generally good. Associations between ex vivo drug sensitivity and parasite polymorphisms included decreased chloroquine and monodesethylamodiaquine sensitivity and increased lumefantrine and piperaquine sensitivity with pfcrt 76T, as well as increased lumefantrine sensitivity with pfmdr1 86Y, Y184, and 1246Y. Over time, ex vivo sensitivity decreased for lumefantrine and piperaquine and increased for chloroquine, the prevalences of pfcrt K76 and pfmdr1 N86 and D1246 increased, and the prevalences of pfdhfr and pfdhps polymorphisms associated with antifolate resistance were unchanged. In recurrent infections, recent prior treatment with artemether-lumefantrine was associated with decreased ex vivo lumefantrine sensitivity and increased prevalence of pfcrt K76 and pfmdr1 N86, 184F, and D1246. In children assigned chemoprevention with monthly dihydroartemisinin-piperaquine with documented circulating piperaquine, breakthrough infections had increased the prevalence of pfmdr1 86Y and 1246Y compared to untreated controls. The noted impacts of therapy and chemoprevention on parasite polymorphisms remained significant in multivariate analysis correcting for calendar time. Overall, changes in parasite sensitivity were consistent with altered selective pressures due to changing treatment practices in Uganda. These changes may threaten the antimalarial treatment and preventive efficacies of artemether-lumefantrine and dihydroartemisinin-piperaquine, respectively.

KW - malaria

KW - Plasmodium falciparum

KW - Uganda

UR - https://scholar.dominican.edu/all-faculty/152

M3 - Article

C2 - 25753626

SN - 1098-6596

VL - 59

SP - 3018

EP - 3030

JO - Antimicrobial Agents and Chemotherapy

JF - Antimicrobial Agents and Chemotherapy

IS - 6

ER -

Impact of Antimalarial Treatment and Chemoprevention on the Drug Sensitivity of Malaria Parasites Isolated from Ugandan Children

Abstract

Funding

ASJC Scopus Subject Areas

Keywords

Disciplines

Access to Document

OpenUrl availability

Other files and links

Cite this