5 research outputs found
The complex relationship of exposure to new Plasmodium infections and incidence of clinical malaria in Papua New Guinea
The molecular force of blood-stage infection (molFOB) is a
quantitative surrogate metric for malaria transmission at
population level and for exposure at individual level.
Relationships between molFOB, parasite prevalence and clinical
incidence were assessed in a treatment-to-reinfection cohort,
where P.vivax (Pv) hypnozoites were eliminated in half the
children by primaquine (PQ). Discounting relapses, children
acquired equal numbers of new P. falciparum (Pf) and Pv
blood-stage infections/year (Pf-molFOB = 0-18, Pv-molFOB = 0-23)
resulting in comparable spatial and temporal patterns in
incidence and prevalence of infections. Including relapses,
Pv-molFOB increased >3 fold (relative to PQ-treated children)
showing greater heterogeneity at individual (Pv-molFOB = 0-36)
and village levels. Pf- and Pv-molFOB were strongly associated
with clinical episode risk. Yearly Pf clinical incidence rate
(IR = 0.28) was higher than for Pv (IR = 0.12) despite lower
Pf-molFOB. These relationships between molFOB, clinical
incidence and parasite prevalence reveal a comparable decline in
Pf and Pv transmission that is normally hidden by the high
burden of Pv relapses. CLINICAL TRIAL REGISTRATION:
ClinicalTrials.gov NCT02143934
Efficacy of artemether-lumefantrine and dihydroartemisinin-piperaquine for the treatment of uncomplicated malaria in Papua New Guinea
In 2009, the Papua New Guinea (PNG) Department of Health adopted artemether-lumefantrine (AL) and dihydroartemisinin-piperaquine (DHA-PPQ) as the first- and second-line treatments for uncomplicated malaria, respectively. This study was conducted to assess the efficacy of both drugs following adoption of the new policy.; Between June 2012 and September 2014, a therapeutic efficacy study was conducted in East Sepik and Milne Bay Provinces of PNG in accordance with the standard World Health Organization (WHO) protocol for surveillance of anti-malarial drug efficacy. Patients ≥ 6 months of age with microscopy confirmed Plasmodium falciparum or Plasmodium vivax mono-infections were enrolled, treated with AL or DHA-PPQ, and followed up for 42 days. Study endpoints were adequate clinical and parasitological response (ACPR) on days 28 and 42. The in vitro efficacy of anti-malarials and the prevalence of selected molecular markers of resistance were also determined.; A total of 274 P. falciparum and 70 P. vivax cases were enrolled. The day-42 PCR-corrected ACPR for P. falciparum was 98.1% (104/106) for AL and 100% (135/135) for DHA-PPQ. The day-42 PCR-corrected ACPR for P. vivax was 79.0% (15/19) for AL and 92.3% (36/39) for DHA-PPQ. Day 3 parasite clearance of P. falciparum was 99.2% with AL and 100% with DHA-PPQ. In vitro testing of 96 samples revealed low susceptibility to chloroquine (34% of samples above IC; 50; threshold) but not to lumefantrine (0%). Molecular markers assessed in a sub-set of the study population indicated high rates of chloroquine resistance in P. falciparum (pfcrt SVMNT: 94.2%, n = 104) and in P. vivax (pvmdr1 Y976F: 64.8%, n = 54).; AL and DHA-PPQ were efficacious as first- and second-line treatments for uncomplicated malaria in PNG. Continued in vivo efficacy monitoring is warranted considering the threat of resistance to artemisinin and partner drugs in the region and scale-up of artemisinin-based combination therapy in PNG
The complex relationship of exposure to new Plasmodium infections and incidence of clinical malaria in Papua New Guinea
The molecular force of blood-stage infection (molFOB) is a
quantitative surrogate metric for malaria transmission at
population level and for exposure at individual level.
Relationships between molFOB, parasite prevalence and clinical
incidence were assessed in a treatment-to-reinfection cohort,
where P.vivax (Pv) hypnozoites were eliminated in half the
children by primaquine (PQ). Discounting relapses, children
acquired equal numbers of new P. falciparum (Pf) and Pv
blood-stage infections/year (Pf-molFOB = 0-18, Pv-molFOB = 0-23)
resulting in comparable spatial and temporal patterns in
incidence and prevalence of infections. Including relapses,
Pv-molFOB increased >3 fold (relative to PQ-treated children)
showing greater heterogeneity at individual (Pv-molFOB = 0-36)
and village levels. Pf- and Pv-molFOB were strongly associated
with clinical episode risk. Yearly Pf clinical incidence rate
(IR = 0.28) was higher than for Pv (IR = 0.12) despite lower
Pf-molFOB. These relationships between molFOB, clinical
incidence and parasite prevalence reveal a comparable decline in
Pf and Pv transmission that is normally hidden by the high
burden of Pv relapses. CLINICAL TRIAL REGISTRATION:
ClinicalTrials.gov NCT02143934
Albinama_eLife_Database
Data from: The complex relationship of exposure to new Plasmodium infections and incidence of clinical malaria in Papua New Guinea