Abstract
BackgroundChagas disease (CD) has become an emerging global health problem in association with the immigration of individuals from endemic areas (in LatinAmerica) to other countries.Spain is the country in Europe with the highest number of CD cases. Concerning pediatric CD, treatment is not only better tolerated by younger children but also has greater cure possibilities. The aim of this study was to describe clinical and epidemiological aspects of CD in a pediatric population diagnosed of 10 hospitals in the Community of Madrid during the 2004–2018 period, as well as the safety and efficacy of CD treatment on this population.Methodology/Principal findingsA multicenter, retrospective, descriptive study was conducted. The studied population included all identified children under the age of 18 with a diagnosis of CD. Diagnosis was performed with a positive parasitological test (with subsequent confirmation) or confirmed persistence of positive serology beyond 9 months, for children younger than one year-old, and with two different positive serological tests, for children older than one.Fifty-one children were included (59% male; 50.9% born in Spain). All mothers were from Latin America. The median age at diagnosis was 0.7 months for those under one year of age, and 11.08 years for those older than one year-old. Only one case presented a symptomatic course (hydrops faetalis, haemodynamic instability at birth, ascites, anaemia). For 94% treatment was completed. Considering patients who received benznidazole (47), AE were recorded in 48,9%. Among the 32 patients older than one year-old treated with benznidazole, 18 (56.25%) had adverse events whereas in the 15 under one year, 5(33,3%) did. Eigtheen (78.2%) of the patients with benznidazole AE were older than one year-old(median age 11.4 years). Of the patients treated with nifurtimox (9), AE were reported in 3 cases (33,3%).Cure was confirmed in 80% of the children under one year-old vs 4.3% in those older (p<0.001). Loss to follow- up occurred in 35.3% of patients.Conclusions/SignificancesScreening programs of CD since birth allow early diagnosis and treatment, with a significantly higher cure rate in children treated before one year of age, with lower incidence of adverse events. The high proportion of patients lost to follow-up in this vulnerable population is of concern.
Highlights
Chagas disease (CD), caused by the protozoan parasite Trypanosoma cruzi, was listed in 2010 by the World Health Organization (WHO) [1] as one of the neglected tropical diseases (NTDs).6 to7 million people are estimated to be infected around the world [2]
In this paper we describe the epidemiological and clinical characteristics of 51 children diagnosed with pediatric CD in a non-endemic area, as well as the the safety and efficacy of treatment in this patient population
We present one of the largest pediatric CD series diagnosed, treated and followed in a non-endemic area, regardless of their origin
Summary
Chagas disease (CD), caused by the protozoan parasite Trypanosoma cruzi, was listed in 2010 by the World Health Organization (WHO) [1] as one of the neglected tropical diseases (NTDs).6 to million people are estimated to be infected around the world [2]. Due to migratory flows in recent decades, CD has shifted from being confined to endemic areas in Latin America, to being a disease that can be diagnosed worldwide. In endemic areas, infection occured mainly through vector-transmission. Successful results were obtained through the action taken by countries to control vector and transfusion transmission of the parasite. These initiatives led to substantial reductions in these ways of transmission [2]. Chagas disease (CD) has become an emerging global health problem in association with the immigration of individuals from endemic areas (in LatinAmerica) to other countries. The aim of this study was to describe clinical and epidemiological aspects of CD in a pediatric population diagnosed of 10 hospitals in the Community of Madrid during the 2004–2018 period, as well as the safety and efficacy of CD treatment on this population
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