通过 Chagas-Flow ATE IgG1 评估慢性南美锥虫病苯并咪唑病因治疗后不同南美锥虫基因型特异性血清学特征

IF 3.8 2区 医学 Q1 Medicine PLoS Neglected Tropical Diseases Pub Date : 2024-09-13 DOI:10.1371/journal.pntd.0012487
Glaucia Diniz Alessio, Carolina Malheiros Araújo Silvestrini, Silvana Maria Elói-Santos, Eliane Dias Gontijo, Policarpo Ademar Sales Júnior, Danielle Marchetti Vitelli-Avelar, Renato Sathler-Avelar, Ana Paula Barbosa Wendling, Andréa Teixeira-Carvalho, Marta de Lana, Olindo Assis Martins-Filho
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引用次数: 0

摘要

本研究旨在利用恰加斯-弗洛 ATE IgG1 方法验证病原学治疗对慢性恰加斯病患者(CH)基因型特异性血清学诊断的影响。为此,研究人员在研究基线和 5 年随访期间检测了共计 92 份南美锥虫病患者血清样本,分为未接受治疗(NT,n = 32)和苯并咪唑治疗(Bz-T,n = 60)两类。在研究基线,所有患者都通过 Chagas-Flow ATE IgG1 确诊为恰加斯病,并使用一组属性("抗原/血清稀释/截止值";"EVI/250/30%")。研究基线的基因型特异性血清诊断表明,96% 的患者(44/46)的血清学特征与 TcII 基因型感染相符。在 5 年的随访监测中,NT 和 Bz-T 的抗 EVI IgG1 反应性没有变化。然而,在 Bz-T 基因型特异性 IgG1 反应性中发现了明显的差异。最明显的变化包括抗母细胞 TcVI/(AVI)、抗母细胞 TcII/(AII)和抗表母细胞 TcVI/(EVI)反应性。尽管 NT 的基因型特异性血清学没有变化(TcI = 6%;TcII = 94%),但与基线(TcII = 97%;TcVI = 3%)相比,5 年随访(TcII = 100%)时发现 Bz-T 样本的 T. cruzi 基因型特异性血清分类非常明显。抗原虫 TcI/(TI)是导致基因型特异性血清分类发生变化的原因。总之,我们在 Bz 治疗后发现了不同的 T. cruzi 基因型特异性血清学,这再次强调了在对慢性南美锥虫病患者进行临床前治疗期间完成基因型特异性血清诊断的重要性。
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Dissimilar Trypanosoma cruzi genotype-specific serological profile assessed by Chagas-Flow ATE IgG1 upon benznidazole etiological treatment of chronic Chagas disease
The present study aimed to verify the impact of etiological treatment on the genotype-specific serological diagnosis of chronic Chagas disease patients (CH), using the Chagas-Flow ATE IgG1 methodology. For this purpose, a total of 92 serum samples from CH, categorized as Not Treated (NT, n = 32) and Benznidazole-Treated (Bz-T, n = 60), were tested at Study Baseline and 5Years Follow-up. At Study Baseline, all patients have the diagnosis of Chagas disease confirmed by Chagas-Flow ATE IgG1, using the set of attributes (“antigen/serum dilution/cut-off”; “EVI/250/30%”). The genotype-specific serodiagnosis at Study Baseline demonstrated that 96% of patients (44/46) presented a serological profile compatible with TcII genotype infection. At 5Years Follow-up monitoring, NT and Bz-T presented no changes in anti-EVI IgG1 reactivity. However, significant differences were detected in the genotype-specific IgG1 reactivity for Bz-T. The most outstanding shift comprised the anti-amastigote TcVI/(AVI), anti-amastigote TcII/(AII) and anti-epimastigote TcVI/(EVI) reactivities. Regardless no changes in the genotype-specific serology of NT (TcI = 6%; TcII = 94%), distinct T. cruzi genotype-specific sero-classification was detected for Bz-T samples at 5Years Follow-up (TcII = 100%) as compared to Baseline (TcII = 97%; TcVI = 3%). The anti-trypomastigote TcI/(TI) was the attribute accountable for the change in genotype-specific sero-classification. In conclusion, our findings of dissimilar T. cruzi genotype-specific serology upon Bz-treatment re-emphasize the relevance of accomplishing the genotype-specific serodiagnosis during clinical pos-therapeutic management of chronic Chagas disease patients.
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来源期刊
PLoS Neglected Tropical Diseases
PLoS Neglected Tropical Diseases Medicine-Infectious Diseases
CiteScore
7.40
自引率
10.50%
发文量
723
审稿时长
2-3 weeks
期刊介绍: PLOS Neglected Tropical Diseases publishes research devoted to the pathology, epidemiology, prevention, treatment and control of the neglected tropical diseases (NTDs), as well as relevant public policy. The NTDs are defined as a group of poverty-promoting chronic infectious diseases, which primarily occur in rural areas and poor urban areas of low-income and middle-income countries. Their impact on child health and development, pregnancy, and worker productivity, as well as their stigmatizing features limit economic stability. All aspects of these diseases are considered, including: Pathogenesis Clinical features Pharmacology and treatment Diagnosis Epidemiology Vector biology Vaccinology and prevention Demographic, ecological and social determinants Public health and policy aspects (including cost-effectiveness analyses).
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