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一种基于RD1的内部酶联免疫斑点-γ干扰素检测法,而非结核菌素皮肤试验,用于诊断潜伏性结核分枝杆菌感染。

An in-house RD1-based enzyme-linked immunospot-gamma interferon assay instead of the tuberculin skin test for diagnosis of latent Mycobacterium tuberculosis infection.

作者信息

Codecasa Luigi, Mantegani Paola, Galli Laura, Lazzarin Adriano, Scarpellini Paolo, Fortis Claudio

机构信息

Villa Marelli Institute, Lombardy Regional Reference Centre for Tuberculosis, Niguarda Hospital, Milan, Italy.

出版信息

J Clin Microbiol. 2006 Jun;44(6):1944-50. doi: 10.1128/JCM.02265-05.

Abstract

Identification of individuals infected with Mycobacterium tuberculosis is essential for the control of tuberculosis (TB). The specificity of the currently used tuberculin skin test (TST) is poor because of the broad antigenic cross-reactivity of purified protein derivative (PPD) with BCG vaccine strains and environmental mycobacteria. Both ESAT-6 and CFP-10, two secretory proteins that are highly specific for M. tuberculosis complex, elicit strong T-cell responses in subjects with TB. Using an enzyme-linked immunospot (ELISPOT)-IFN-gamma assay and a restricted pool of peptides derived from ESAT-6 and CFP-10, we have previously demonstrated a high degree of specificity and sensitivity of the test for the diagnosis of TB. Here, 119 contacts of individuals with contagious TB who underwent TST and the ELISPOT-IFN-gamma assay were consecutively recruited. We compared the efficacy of the two tests in detecting latent TB infection and defined a more appropriate TST cutoff point. There was little agreement between the tests (k = 0.33, P < 0.0001): 53% of the contacts with a positive TST were ELISPOT negative, and 7% with a negative TST were ELISPOT positive. Furthermore, respectively 76 and 59% of the ELISPOT-negative contacts responded in vitro to BCG and PPD, suggesting that most of them were BCG vaccinated or infected with nontuberculous mycobacteria. The number of spot-forming cells significantly correlated with TST induration (P < 0.0001). Our in-house ELISPOT assay based on a restricted pool of highly selected peptides is more accurate than TST for identifying individuals with latent TB infection and could improve chemoprophylaxis for the control of TB.

摘要

识别感染结核分枝杆菌的个体对于控制结核病至关重要。由于纯化蛋白衍生物(PPD)与卡介苗菌株及环境分枝杆菌存在广泛的抗原交叉反应,目前使用的结核菌素皮肤试验(TST)特异性较差。ESAT-6和CFP-10这两种对结核分枝杆菌复合群高度特异的分泌蛋白,能在结核病患者体内引发强烈的T细胞反应。我们此前利用酶联免疫斑点(ELISPOT)-γ干扰素检测法以及源自ESAT-6和CFP-10的限定肽库,证明了该检测方法在结核病诊断中具有高度的特异性和敏感性。在此,我们连续招募了119名结核病患者的接触者,他们接受了TST和ELISPOT-γ干扰素检测。我们比较了这两种检测方法在检测潜伏性结核感染方面的效果,并确定了更合适的TST临界值。两种检测方法之间几乎没有一致性(k = 0.33,P < 0.0001):TST呈阳性的接触者中有53%的ELISPOT检测为阴性,而TST呈阴性的接触者中有7%的ELISPOT检测为阳性。此外,分别有76%和59%的ELISPOT检测为阴性的接触者在体外对卡介苗和PPD有反应,这表明他们中的大多数接种过卡介苗或感染了非结核分枝杆菌。斑点形成细胞的数量与TST硬结显著相关(P < 0.0001)。我们基于高度精选的限定肽库的内部ELISPOT检测法在识别潜伏性结核感染个体方面比TST更准确,并且可以改善结核病控制的化学预防措施。

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