Instituto de Investigaciones Biotecnológicas-Instituto Tecnológico de Chascomús (IIB-INTECh), Universidad Nacional de San Martín (UNSAM) and Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Buenos Aires, Argentina.
Servicio de Parasitología-Chagas, Hospital de Niños Dr. Ricardo Gutiérrez, Buenos Aires, Argentina.
J Clin Microbiol. 2017 Dec;55(12):3444-3453. doi: 10.1128/JCM.01317-17. Epub 2017 Oct 4.
Chagas disease is caused by the protozoan parasite Assessment of parasitological cure upon treatment with available drugs relies on achieving consistent negative results in conventional parasitological and serological tests, which may take years to assess. Here, we evaluated the use of a recombinant antigen termed trypomastigote small surface antigen (TSSA) as an early serological marker of drug efficacy in -infected children. A cohort of 78 pediatric patients born to -infected mothers was included in this study. Only 39 of the children were infected with , and they were immediately treated with trypanocidal drugs. Serological responses against TSSA were evaluated in infected and noninfected populations during the follow-up period using an in-house enzyme-linked immunosorbent assay (ELISA) and compared to conventional serological methods. Anti-TSSA antibody titers decreased significantly faster than anti-whole parasite antibodies detected by conventional serology both in -infected patients undergoing effective treatment and in those not infected. The differential kinetics allowed a significant reduction in the required follow-up periods to evaluate therapeutic responses or to rule out maternal-fetal transmission. Finally, we present the case of a congenitally infected patient with an atypical course in whom TSSA provided an early marker for infection. In conclusion, we showed that TSSA was efficacious both for rapid assessment of treatment efficiency and for early negative diagnosis in infants at risk of congenital infection. Based upon these findings we propose the inclusion of TSSA for refining the posttherapeutic cure criterion and other diagnostic needs in pediatric Chagas disease.
恰加斯病由原生动物寄生虫引起。评估用现有药物治疗后的寄生虫治愈情况依赖于在常规寄生虫学和血清学检测中获得持续的阴性结果,这可能需要数年时间进行评估。在这里,我们评估了使用重组抗原(称为锥鞭毛小表面抗原,TSSA)作为药物疗效的早期血清学标志物在感染儿童中的应用。本研究纳入了一组 78 名出生于感染母亲的儿科患者。只有 39 名儿童感染了,他们立即接受了杀锥虫药物治疗。在随访期间,使用内部酶联免疫吸附试验(ELISA)评估了感染和未感染人群针对 TSSA 的血清学反应,并与常规血清学方法进行了比较。在接受有效治疗的感染患者和未感染患者中,抗-TSSA 抗体滴度的下降速度明显快于常规血清学检测到的抗全寄生虫抗体。这种差异动力学允许显著减少评估治疗反应或排除母婴传播所需的随访期。最后,我们介绍了一例先天性感染患者的不典型病程,TSSA 为感染提供了早期标志物。总之,我们表明 TSSA 既可以快速评估治疗效率,也可以在有先天性感染风险的婴儿中进行早期阴性诊断。基于这些发现,我们建议将 TSSA 纳入治疗后治愈标准的细化以及儿科恰加斯病的其他诊断需求。