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阐明负责四氯二苯并对二恶英(TCDD)诱导的抗体反应抑制的细胞靶点:II. T淋巴细胞的作用。

Elucidation of cellular targets responsible for tetrachlorodibenzo-p-dioxin (TCDD)-induced suppression of antibody responses: II. The role of the T-lymphocyte.

作者信息

Dooley R K, Morris D L, Holsapple M P

机构信息

Department of Pharmacology and Toxicology, Medical College of Virginia, Virginia Commonwealth University, Richmond 23298.

出版信息

Immunopharmacology. 1990 Jan-Feb;19(1):47-58. doi: 10.1016/0162-3109(90)90026-b.

Abstract

Various immunological assays have been applied by our laboratory in an attempt to assess the role of the T-cell in the TCDD-induced suppression of the antibody response by murine B6C3F1 splenic lymphocytes. Animals were treated in vivo (via gavage) with 1.0 microgram/kg TCDD in corn oil for 5 days before in vitro analysis of splenocyte immunocompetence and T-cell function. To study the effects on T-helper cell function, alterations in the proliferative responses of T-cells following TCDD exposure were investigated. Results show no significant difference in [3H]thymidine uptake between vehicle- and TCDD-treated whole splenocytes 24 h after in vitro stimulation with the T-cell mitogen Con A. This is consistent with the finding that IL-2 production at either 24 or 48 h after Con A stimulation of TCDD-treated lymphocytes was not significantly different from that of vehicle-treated controls. The possibility of the induction of a suppressor T-cell by TCDD was also investigated. Titration of T-cells from TCDD-treated mice into naive splenocyte cultures did not suppress the humoral response to either a T-dependent (SRBC) or a T-independent (DNP-Ficoll) antigen. In contrast, titration of cells stimulated in vitro with Con A for 48 h (a positive control for the induction of a suppressor T-cell) inhibited humoral responses of naive cells to both types of antigen. Likewise, T-cells plus macrophages from TCDD-treated mice did not suppress the in vitro humoral responsiveness of naive B-cells plus macrophages to a T-independent antigen (DNP-Ficoll). These results would indicate that an alteration in T-cell function following TCDD exposure does not play a role in the suppression of the antibody response elicited by antigen stimulation of murine B6C3F1 splenocytes.

摘要

我们实验室应用了各种免疫测定法,试图评估T细胞在2,3,7,8-四氯二苯并对二恶英(TCDD)诱导的小鼠B6C3F1脾淋巴细胞抗体反应抑制中的作用。在对脾细胞免疫能力和T细胞功能进行体外分析之前,动物在体内(通过灌胃)用1.0微克/千克TCDD的玉米油处理5天。为了研究对辅助性T细胞功能的影响,研究了TCDD暴露后T细胞增殖反应的变化。结果显示,在用T细胞有丝分裂原刀豆蛋白A(Con A)进行体外刺激24小时后,载体处理组和TCDD处理组的全脾细胞中[3H]胸腺嘧啶核苷摄取量没有显著差异。这与以下发现一致:在Con A刺激TCDD处理的淋巴细胞后24小时或48小时,白细胞介素-2(IL-2)的产生与载体处理的对照组没有显著差异。还研究了TCDD诱导抑制性T细胞的可能性。将TCDD处理小鼠的T细胞滴定到未致敏的脾细胞培养物中,并未抑制对T依赖性(绵羊红细胞,SRBC)或T非依赖性(二硝基苯-Ficoll,DNP-Ficoll)抗原的体液反应。相比之下,用Con A体外刺激48小时的细胞(诱导抑制性T细胞的阳性对照)滴定抑制了未致敏细胞对两种抗原的体液反应。同样,TCDD处理小鼠的T细胞加巨噬细胞并未抑制未致敏B细胞加巨噬细胞对T非依赖性抗原(DNP-Ficoll)的体外体液反应性。这些结果表明,TCDD暴露后T细胞功能的改变在抑制小鼠B6C3F1脾细胞抗原刺激引发的抗体反应中不起作用。

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