首页> 外文期刊>Transfusion: The Journal of the American Association of Blood Banks >Detection of antibodies to Trypanosoma cruzi among blood donors in the southwestern and western United States. II. Evaluation of a supplemental enzyme immunoassay and radioimmunoprecipitation assay for confirmation of seroreactivity.
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Detection of antibodies to Trypanosoma cruzi among blood donors in the southwestern and western United States. II. Evaluation of a supplemental enzyme immunoassay and radioimmunoprecipitation assay for confirmation of seroreactivity.

机译:在美国西南部和西部的献血者中检测到克氏锥虫抗体。二。评价补充酶免疫测定和放射免疫沉淀测定以确认血清反应性。

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BACKGROUND: Chagas' disease, caused by the protozoan parasite Trypanosoma cruzi, is endemic to Latin America and may be transmitted in the United States via blood donated by infected immigrants. Blood-borne pathogens such as T. cruzi require supplemental testing for confirmation of seroreactivity. STUDY DESIGN AND METHODS: A study was undertaken to determine an optimal scheme for confirmation of seroreactivity in repeatedly reactive samples identified by the Chagas antibody enzyme immunoassay (EIA). The procedure for initial confirmation involves three purified antigens coated onto three separate polystyrene beads and uses an EIA format. If the sample is reactive with two of three or three of three antigens, it is confirmed as seroreactive. If none or one of three beads is reactive, the sample is indeterminate and subjected to a radioimmunoprecipitation assay (RIPA). The RIPA must demonstrate characteristic bands at 32, 34, and 90 kDa. RESULTS: When tested with sera from persons with potentially cross-reactive diseases (n = 39) or against a presumed negative population from southeast Wisconsin (n = 289), the confirmatory EIA had a specificity of 100 percent. Sensitivity was 100 percent (28/28) with xenodiagnosis-positive sera and 97.6 percent (80/82) with chagasic sera from Latin America. The RIPA showed a specificity of 100 percent in EIA-nonreactive samples (n = 100) and a sensitivity of 100 percent with both xenodiagnosis-positive (28/28) and chagasic (82/82) sera. CONCLUSION: The confirmatory EIA and the RIPA together provide a highly specific and sensitive means of confirming seroreactivity for antibodies to T. cruzi.
机译:背景:恰加斯氏病由原生动物寄生虫克鲁斯锥虫引起,是拉丁美洲的特有疾病,可能在美国通过受感染移民捐赠的血液传播。血源性病原体(例如克鲁氏锥虫)需要补充测试以确认血清反应。研究设计和方法:进行了一项研究,以确定用于确认由Chagas抗体酶免疫测定(EIA)鉴定的反复反应的样品中血清反应的最佳方案。初步确认程序涉及将三种纯化的抗原包被在三个单独的聚苯乙烯珠上,并使用EIA格式。如果样品与三种抗原中的两种或三种抗原中的三种反应,则确认为血清反应活性。如果三个珠子中没有一个或其中一个具有反应性,则该样品不确定,并进行放射免疫沉淀测定(RIPA)。 RIPA必须显示32、34和90 kDa的特征带。结果:当用具有潜在交叉反应性疾病的血清(n = 39)或针对威斯康星州东南部的阴性人群(n = 289)进行血清测试时,确认的EIA特异性为100%。异种诊断阳性血清的敏感性为100%(28/28),拉丁美洲拉丁裔患者的敏感性为97.6%(80/82)。 RIPA在EIA非反应性样品(n = 100)中显示100%的特异性,异种诊断阳性(28/28)和恰加斯(82/82)血清的敏感性均为100%。结论:验证性EIA和RIPA共同提供了一种高度特异性和灵敏的方法,用于确认针对克鲁氏锥虫的抗体的血清反应活性。

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