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急性登革热感染中T细胞增殖受损。

Impaired T cell proliferation in acute dengue infection.

作者信息

Mathew A, Kurane I, Green S, Vaughn D W, Kalayanarooj S, Suntayakorn S, Ennis F A, Rothman A L

机构信息

Center for Infectious Disease and Vaccine Research, University of Massachusetts Medical Center, Worcester 01655, USA.

出版信息

J Immunol. 1999 May 1;162(9):5609-15.

Abstract

Decreased proliferative responses to mitogens and recall Ags have been observed in PBMC obtained during several acute human viral infections. To determine whether cell-mediated responses are altered during acute dengue infection, we examined the proliferative responses of PBMC from children enrolled in a prospective study of dengue infections in Thailand. All responses of PBMC during acute illness were compared with the same patients' PBMC obtained at least 6 mo after their infection. Proliferative responses to PHA, anti-CD3, tetanus toxoid, and dengue Ags were decreased significantly in PBMC obtained during the acute infection. The proliferative responses to PHA were restored by the addition of gamma-irradiated autologous convalescent or allogeneic PBMC. Cell contact with the irradiated PBMC was necessary to restore proliferation. Non-T cells from the acute PBMC of dengue patients did not support proliferation of T cells from control donors in response to PHA, but T cells from the PBMC of patients with acute dengue proliferated if accessory cells from a control donor were present. Addition of anti-CD28 Abs restored anti-CD3-induced proliferation of the PBMC of some patients. The percentage of monocytes was reduced in the acute sample of PBMC of the dengue patients. Addition of IL-2 or IL-7, but not IL-4 or IL-12, also restored proliferation of acute PBMC stimulated with anti-CD3. The results demonstrate that both quantitative and qualitative defects in the accessory cell population during acute dengue illness result in a depression of in vitro T cell proliferation.

摘要

在几种人类急性病毒感染期间获得的外周血单个核细胞(PBMC)中,已观察到对有丝分裂原和回忆抗原的增殖反应降低。为了确定急性登革热感染期间细胞介导的反应是否改变,我们检测了参与泰国登革热感染前瞻性研究的儿童PBMC的增殖反应。将急性疾病期间PBMC的所有反应与感染后至少6个月获得的同一患者的PBMC进行比较。急性感染期间获得的PBMC对PHA、抗CD3、破伤风类毒素和登革热抗原的增殖反应显著降低。添加γ射线照射的自体恢复期或同种异体PBMC可恢复对PHA的增殖反应。与照射后的PBMC进行细胞接触对于恢复增殖是必要的。登革热患者急性PBMC中的非T细胞不支持对照供体T细胞对PHA的增殖反应,但如果存在对照供体的辅助细胞,急性登革热患者PBMC中的T细胞会增殖。添加抗CD28抗体可恢复一些患者PBMC的抗CD3诱导的增殖。登革热患者PBMC急性样本中的单核细胞百分比降低。添加IL-2或IL-7,但不添加IL-4或IL-12,也可恢复抗CD3刺激的急性PBMC的增殖。结果表明,急性登革热疾病期间辅助细胞群体的数量和质量缺陷导致体外T细胞增殖受到抑制。

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