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解决人类恰加斯病的挑战:慢性期治疗策略的综合综述和新兴治疗方法。

Tackling the challenges of human Chagas disease: A comprehensive review of treatment strategies in the chronic phase and emerging therapeutic approaches.

机构信息

Laboratorio de Sintese de Farmacos -LASFAR, Instituto de Tecnologia em Farmacos - Farmanguinhos, Fundação Oswaldo Cruz, Rio de Janeiro, RJ 21041-250, Brazil; Laboratório de Físico-Química de Materiais, Seção de Engenharia Química, Instituto Militar de Engenharia, Praça General Tibúrcio 80, Rio de Janeiro, RJ 22290-270, Brazil.

Laboratório de Físico-Química de Materiais, Seção de Engenharia Química, Instituto Militar de Engenharia, Praça General Tibúrcio 80, Rio de Janeiro, RJ 22290-270, Brazil.

出版信息

Acta Trop. 2024 Aug;256:107264. doi: 10.1016/j.actatropica.2024.107264. Epub 2024 May 26.

DOI:10.1016/j.actatropica.2024.107264
PMID:38806090
Abstract

Chagas disease (CD), caused by the flagellated protozoan Trypanosoma cruzi (T. cruzi), affects approximately 7 million people worldwide and is endemic in Latin America, especially among socioeconomically disadvantaged populations. Since the 1960s, only two drugs have been commercially available for treating this illness: nifurtimox (NFX) and benznidazole (BZN). Although these drugs are effective in the acute phase (AP) of the disease, in which parasitemia is usually high, their cure rates in the chronic phase (CP) are low and often associated with several side effects. The CP is characterized by a subpatent parasitaemia and absence of clinical symptoms in the great majority of infected individuals. However, at least 30 % of the individuals will develop potentially lethal symptomatic forms, including cardiac and digestive manifestations. For such reason, in the CP the treatment is usually symptomatic and typically focuses on managing complications such as arrhythmias, heart failure, or digestive problems. Therefore, the need for new drugs or therapeutic approaches using BZN or NFX is extremely urgent. This review presents the main clinical trials, especially in the CP, which involve BZN and NFX in different treatment regimens. Additionally, other therapies using combinations of these drugs with other substances such as allopurinol, itraconazole, ravuconazole, ketoconazole, posaconazole and amiodarone are also reported. The importance of early diagnosis, especially in pediatric patients, is also discussed, emphasizing the need to identify the disease in its early stages to improve the chances of successful treatment.

摘要

恰加斯病(CD)由鞭毛原生动物克氏锥虫(T. cruzi)引起,影响全球约 700 万人,在拉丁美洲流行,尤其是在社会经济地位较低的人群中。自 20 世纪 60 年代以来,仅有两种药物可用于治疗这种疾病:硝呋莫司(NFX)和苯硝唑(BZN)。尽管这些药物在寄生虫血症通常较高的疾病急性期(AP)有效,但在慢性期(CP)的治愈率较低,且常伴有多种副作用。CP 的特征是亚寄生虫血症和绝大多数感染者无临床症状。然而,至少有 30%的感染者会发展为潜在致命的有症状形式,包括心脏和消化系统表现。因此,CP 中的治疗通常是对症治疗,通常侧重于管理心律失常、心力衰竭或消化系统问题等并发症。因此,急需使用 BZN 或 NFX 的新药或治疗方法。本文综述了主要的临床试验,特别是在 CP 中,涉及 BZN 和 NFX 的不同治疗方案。此外,还报告了使用这些药物与别嘌醇、伊曲康唑、拉夫康唑、酮康唑、泊沙康唑和胺碘酮等其他物质联合治疗的其他疗法。早期诊断的重要性,特别是在儿科患者中,也进行了讨论,强调需要在疾病早期识别,以提高成功治疗的机会。

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