史蒂文斯-约翰逊综合征的体外药物因果关系评估-淋巴细胞转化试验的替代方法。
In vitro drug causality assessment in Stevens-Johnson syndrome - alternatives for lymphocyte transformation test.
机构信息
ADR-AC GmbH, Bern, Switzerland.
出版信息
Clin Exp Allergy. 2013 Sep;43(9):1027-37. doi: 10.1111/cea.12145.
BACKGROUND
Patients with Stevens-Johnson syndrome (SJS) or toxic epidermal necrolysis (TEN) are often exposed simultaneously to a few potentially culprit drugs. However, both the standard lymphocyte transformation tests (LTT) with proliferation as the assay end-point as well as skin tests, if done, are often negative.
OBJECTIVE
As provocation tests are considered too dangerous, there is an urgent need to identify the relevant drug in SJS/TEN and to improve sensitivity of tests able to identify the causative drug.
METHODS
Fifteen patients with SJS/TEN with the ALDEN score ≥ 6 and 18 drug-exposed controls were included. Peripheral blood mononuclear cells (PBMC) were isolated and cultured under defined conditions with drugs. LTT was compared to the following end-points: cytokine levels in cell culture supernatant, number of granzyme B secreting cells by ELISpot and intracellular staining for granulysin and IFNγ in CD3(+) CD4(+), CD3(+) CD8(+) and NKp46(+) cells. To further enhance sensitivity, the effect of IL-7/IL-15 pre-incubation of PBMC was evaluated.
RESULTS
Lymphocyte transformation tests was positive in only 4/15 patients (sensitivity 27%, CI: 8-55%). Similarly, with granzyme B-ELISpot culprit drugs were positive in 5/15 patients (sensitivity 33%, CI: 12-62%). The expression of granulysin was significantly induced in NKp46(+) and CD3(+) CD4(+) cells (sensitivity 40%, CI: 16-68% and 53%, CI: 27-79% respectively). Cytokine production could be demonstrated in 38%, CI: 14-68% and 43%, CI: 18-71% of patients for IL-2 and IL-5, respectively, and in 55%, CI: 23-83% for IFNγ. Pre-incubation with IL-7/IL-15 enhanced drug-specific response only in a few patients. Specificities of tested assays were in the range of 95 (CI: 80-99%)-100% (CI: 90-100%).
CONCLUSIONS AND CLINICAL RELEVANCE
Granulysin expression in CD3(+) CD4(+) , Granzyme B-ELISpot and IFNγ production considered together provided a sensitivity of 80% (CI: 52-96%) and specificity of 95% (80-99%). Thus, this study demonstrated that combining different assays may be a feasible approach to identify the causative drug of SJS/TEN reactions; however, confirmation on another group of patients is necessary.
背景
史蒂文斯-约翰逊综合征(SJS)或中毒性表皮坏死松解症(TEN)患者通常同时接触几种潜在的罪魁祸首药物。然而,标准的淋巴细胞转化试验(LTT)与增殖作为检测终点以及皮肤试验,如果进行的话,通常都是阴性的。
目的
由于激发试验被认为太危险,因此迫切需要确定 SJS/TEN 中的相关药物,并提高能够识别致病药物的试验的敏感性。
方法
纳入 15 名 SJS/TEN 患者(ALDEN 评分≥6)和 18 名药物暴露对照者。分离外周血单核细胞(PBMC),并在定义的条件下用药物培养。将 LTT 与以下终点进行比较:细胞培养上清液中的细胞因子水平、通过 ELISpot 检测的颗粒酶 B 分泌细胞数量以及 CD3(+)CD4(+)、CD3(+)CD8(+)和 NKp46(+)细胞中颗粒溶素和 IFNγ 的细胞内染色。为了进一步提高敏感性,评估了 IL-7/IL-15 对 PBMC 的预孵育效果。
结果
只有 4/15 名患者的淋巴细胞转化试验呈阳性(敏感性 27%,CI:8-55%)。同样,用颗粒酶 B-ELISpot 检测,有 5/15 名患者的罪魁祸首药物呈阳性(敏感性 33%,CI:12-62%)。NKp46(+)和 CD3(+)CD4(+)细胞中颗粒溶素的表达明显增加(敏感性分别为 40%,CI:16-68%和 53%,CI:27-79%)。分别有 38%(CI:14-68%)和 43%(CI:18-71%)的患者产生了细胞因子 IL-2 和 IL-5,有 55%(CI:23-83%)的患者产生了 IFNγ。用 IL-7/IL-15 预孵育仅增强了少数患者的药物特异性反应。测试方法的特异性在 95%(CI:80-99%)至 100%(CI:90-100%)之间。
结论和临床相关性
CD3(+)CD4(+)中的颗粒溶素表达、颗粒酶 B-ELISpot 和 IFNγ 产生综合考虑,敏感性为 80%(CI:52-96%),特异性为 95%(80-99%)。因此,本研究表明,结合不同的检测方法可能是一种可行的方法来确定 SJS/TEN 反应的致病药物;然而,还需要在另一组患者中进行验证。
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