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先天性克氏锥虫病:一种基于特异性 IgM 捕获的诊断传播的检测方法的建立与评估。

Congenital chagas disease: Development and assessment of a specific IgM capture-based assay for diagnosis of transmission.

机构信息

Laboratorio de Tecnología Inmunológica (Facultad de Bioquímica y Ciencias Biológicas Universidad Nacional del Litoral)- Santa Fe - Argentina.

Centro de Estudios en Salud Global (Facultad de Ciencias Médicas - Universidad Nacional del Litoral)-Santa Fe- Argentina.

出版信息

Acta Trop. 2021 Jan;213:105738. doi: 10.1016/j.actatropica.2020.105738. Epub 2020 Nov 4.

Abstract

Transplacental transmission by Trypanosoma cruzi (T. cruzi) infection can be effectively treated if parasiticide drugs are administered as early as possible during childhood. Furthermore, an ideal situation would be to diagnose the infection near birth in order to avoid the loss of patients during the subsequent follow-up. These situation are desirable due to the maximum benefit of drugs in early stages which, consequently, implies a relevant contribution to eliminate mother-to-child transmission. However, available techniques for that purpose have limitations as being operator-dependent (microhematocrit), require several months follow-up (IgG detection) or specialized laboratories (PCR). In this study we propose to detect specific IgM antibodies (Ab) by developing a capture-based ELISA employing an improved antigen (Ag) to diagnose the transplacental transmission of T. cruzi, and in consequence, to enhance access to effective treatment. Firstly, a new chimera Ag (CP4) was obtained from the fusion of CP1 and CP3 protein, carrying FRA, SAPA, MAP, TSSAII/V/VI and TcD Ag from T. cruzi. Then, we optimized the assay by capturing IgM Ab with a polyclonal anti-IgM Ab and evaluating three Ag formulations to detect specific IgM bound. The formulations were formed as follows: i) F1: CP1 and CP3; ii) F2: CP1, CP3, B13 and P2β; iii) F3: by CP4. Detection of Ab-binding Ag was carried out using an anti-His Ab since all Ag were expressed with a His-tag. The evaluation panel consisted of sera from vertically infected children under 1-year-old (6 younger than 15 days, 7 older) and samples from non-infected children of women with chronic Chagas Disease. The ELISA assay employing CP4 showed better performance with notable high sensitivity and specificity (92.3% and 93.9%, respectively). Positive and negative likelihood ratios of the test (15.2 and 0.082) suggest its potential clinical relevance in term of post-test probability of infection. In conclution, we developed a standardized and non-operator dependent test to detect specific anti-T. cruzi IgM Ab. Although increased sample size is needed for its validation, our results indicate that this capture-based technique employing CP4 Ag can certainly improve the diagnosis of connatal infection.

摘要

如果在儿童时期尽早使用寄生虫药物进行治疗,可有效治疗通过克氏锥虫(Trypanosoma cruzi,T. cruzi)感染的胎盘传播。此外,在出生时诊断感染是理想的情况,以避免在随后的随访中失去患者。由于早期药物的最大效益,这些情况是可取的,这意味着对消除母婴传播有重要贡献。然而,目前为此目的而采用的技术具有一些局限性,例如:操作人员依赖性(微量血球容积计),需要数月的随访(IgG 检测)或专业实验室(PCR)。在这项研究中,我们通过开发一种基于捕获的 ELISA 来检测特异性 IgM 抗体(Ab),该 ELISA 采用改良的抗原(Ag)来诊断克氏锥虫的胎盘传播,从而提高获得有效治疗的机会。首先,通过融合 CP1 和 CP3 蛋白获得了一种新的嵌合 Ag(CP4),该蛋白携带来自克氏锥虫的 FRA、SAPA、MAP、TSSAII/V/VI 和 TcD Ag。然后,我们通过使用多克隆抗 IgM Ab 捕获 IgM Ab 并评估三种用于检测特异性 IgM 结合的 Ag 制剂来优化该测定法。制剂的形成方式如下:i)F1:CP1 和 CP3;ii)F2:CP1、CP3、B13 和 P2β;iii)F3:CP4。使用抗 His Ab 进行 Ab-结合 Ag 的检测,因为所有 Ag 均带有 His 标签。评估小组由 1 岁以下(6 名小于 15 天,7 名大于 15 天)的垂直感染儿童的血清和患有慢性恰加斯病的妇女的未感染儿童的样本组成。使用 CP4 的 ELISA 检测显示出更好的性能,具有很高的灵敏度和特异性(分别为 92.3%和 93.9%)。该测试的阳性和阴性似然比(15.2 和 0.082)表明,其在感染后的后测试概率方面具有潜在的临床相关性。总之,我们开发了一种标准化的、非操作人员依赖的检测方法来检测特异性抗克氏锥虫 IgM Ab。尽管需要增加样本量进行验证,但我们的结果表明,该基于捕获的技术使用 CP4 Ag 可以提高先天性感染的诊断。

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