Abstract
BackgroundMalaria transmission in Latin America is generally hypoendemic and unstable, with Plasmodium vivax as the most prevalent species. However, only a few studies have been carried out in areas with low and unstable transmission, whereas the clinical profile of malaria has been broadly described in hyperendemic areas. The pattern of clinical manifestations and laboratory findings in low to moderate endemic areas of Colombia is reported here.MethodsA passive surveillance study was conducted between 2011 and 2013 involving 1,328 patients with Plasmodium falciparum, P. vivax or mixed malaria infections attending malaria points-of-care of four malaria endemic-areas with distinct transmission intensities and parasite distribution. Trained physicians recorded clinical symptoms and signs as well as socio-demographic characteristics of study participants. Haematological, biochemical and urine tests were performed at the time of diagnosis.ResultsOut of 1,328 cases, 673 (50.7%) were caused by P. vivax; 650 (48.9%) were due to P. falciparum; and five (0.4%) patients had mixed infections (P. falciparum/P. vivax). Most patients (92.5%) presented with uncomplicated malaria characterized by fever, chills, headache, sweating, myalgia/arthralgia and parasitaemia ≤ 20,000 parasites/μL. Fever, tachycardia, pallor and abdominal pain on palpation were more frequent in P. falciparum patients, whereas mild hepatomegaly and splenomegaly were mostly observed with P. vivax. Non-severe anaemia (Hb 7.0-10.9 g/dL) was observed in 20% of the subjects, whereas severe anaemia (Hb < 7.0 g/dL) was present in four patients. Half of the patients presented thrombocytopaenia regardless of parasite species. Leukopaenia, neutrophilia and monocytosis were frequently observed in patients infected with P. falciparum. Mild-to-moderate biochemical alterations were present in ~25% of the patients, particularly abnormal bilirubin in those with P. falciparum and abnormal transaminases in P. vivax malaria patients. Proteinuria was present in ~50% of the patients regardless of parasite species, whereas haemoglobinuria was more common in P. vivax infections. Only 7.5% of the cases were classified as clinically severe malaria, caused by both P. vivax and P. falciparum.ConclusionsThe high prevalence of uncomplicated malaria associated with moderate parasitaemia suggests the importance of timely diagnosis and effective treatment and encourages new activities to further decrease complicated malaria cases and mortality.
Highlights
Malaria transmission in Latin America is generally hypoendemic and unstable, with Plasmodium vivax as the most prevalent species
This study aimed at prospectively collecting information on the clinical profile of malaria from a large number of subjects acutely infected with P. falciparum and P. vivax residing in some of the highest malaria transmission regions in Colombia
Plasmodium species distribution was statistically different in the study sites; the overall distribution indicated a total of 673 (50.7%) participants presenting with P. vivax malaria, and 650 (48.9%) with P. falciparum infections
Summary
Malaria transmission in Latin America is generally hypoendemic and unstable, with Plasmodium vivax as the most prevalent species. The vast majority of these cases (80%) and deaths (90%) were caused by Plasmodium falciparum infections in sub-Saharan Africa, the region with the highest rates of transmission worldwide. Plasmodium vivax is the second most prevalent species that accounts for 75 to 85 million cases/year, corresponding to >50% of malaria infections outside of Africa [3]. Colombia accounts for ~13% of the malaria cases [1,6], predominantly by P. vivax (>70%), which co-exists with P. falciparum, with a remarkably different regional prevalence [6,7]. Such differences in prevalence are mainly due to the varied Duffy antigen expression in these populations [8,9], and the clinical relapses due to P. vivax hypnozoite activation [10]
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