活化和增强人类t淋巴细胞与自体红细胞的接触是它们在37度下稳定粘附的必要条件。

T Khavkin, M Kuchler, M Carl, J R Murphy, S Baqar, R E Triemer, M J Liao, D Testa
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引用次数: 1

摘要

人红细胞(RBC)与自体t细胞的粘附在体内并不发生,在体外是在4度下诱导的。37度的自体e - rotting以前没有被描述过。在这项工作中,淋巴细胞-红细胞粘附研究了混合白细胞-红细胞培养和来自健康献血者的全血。重要的细胞化学和电镜研究表明,t细胞可以在37度时与自体红细胞形成稳定的e -莲座。正如之前报道的冷依赖性可逆结瘤一样,稳定结瘤是由红细胞LFA3和淋巴细胞CD2分子介导的。独特的是,这种现象需要t细胞激活和t细胞与红细胞膜之间增强的接触。这些要求是通过将细胞培养物暴露于:(1)PHAP的红细胞凝集成分PHAE,或(2)非红细胞凝集的有丝分裂原PHAL, Con A, OKT3或SEA,或斑疹伤寒群立克次体或沙门氏菌抗原来满足的,前提是红细胞膜被分离。当培养基中存在神经氨酸酶时,立克次体血清阳性个体或接种沙门氏菌的培养物在抗原暴露后表现出粘附现象。这里描述的系统2可以作为一种诊断工具,用于定义具有抗原记忆的活化t细胞和t细胞克隆,能够诱导细胞介导的免疫。
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Activation and enhanced contact of human T-lymphocytes with autologous red blood cells are required for their stable adherence at 37 degrees.

The adherence of human red blood cells (RBC) to autologous T-cells does not occur in the body, and in vitro is elicited at 4 degrees. Autologous E-rosetting at 37 degrees has not previously been described. In this work, lymphocyte-RBC adherence has been studied in mixed leukocyte-RBC cultures and in whole blood from healthy donors. Vital, cytochemical and electron microscopic studies have shown that T-cells may form stable E-rosettes with autologous RBC at 37 degrees. As in the previously reported cold-dependent reversible rosetting, stable rosetting is mediated by the erythrocyte LFA3 and lymphocyte CD2 molecules. Uniquely, this phenomenon requires both T-cell activation and an enhanced contact between the T-cell and RBC membranes. These requirements were met by exposure of cell cultures to: (1) PHAE, the erythroagglutinating component of PHAP, or (2) to either non-erythroagglutinating mitogens, PHAL, Con A, OKT3 or SEA, or to antigens of typhus group rickettsiae or salmonellae, provided that the RBC membrane was desialyted. Cultures derived from individuals seropositive to rickettsiae or vaccinated with salmonellae demonstrated the adherence phenomenon after antigen exposure when neuraminidase was present in the culture medium. The system 2 described here can be used as a diagnostic tool for defining activated T-cells and T-cell clones with the memory to antigens capable of inducing cell-mediated immunity.

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