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巨噬细胞在免疫T细胞对可溶性抗原的增殖反应中作为调节者而非自主辅助细胞的作用。

Role of macrophages as modulators but not as autonomous accessory cells in the proliferative response of immune T cells to soluble antigen.

作者信息

Kawai J, Inaba K, Komatsubara S, Hirayama Y, Naito K, Muramatsu S

机构信息

Department of Zoology, Faculty of Science, Kyoto University, Japan.

出版信息

Cell Immunol. 1987 Oct 1;109(1):1-11. doi: 10.1016/0008-8749(87)90287-5.

Abstract

The role of murine macrophages (M phi) and that of splenic dendritic cells (DC) were investigated in the antigen-specific proliferative response of memory T cells of mice primed with key-hole limpet hemocyanin (KLH) 6 weeks or more before. Peritoneal M phi, whether expressing Ia antigens or not, did not function as autonomous accessory cells (A cells). A-cell activity of the spleen adherent cell population, which comprised M phi in the majority and DC in the minority, was abolished by eliminating DC with a DC-specific monoclonal antibody and complement, and regained by the addition of a small number of DC. Though M phi did not function as autonomous A cells, they augmented the proliferative response in the presence of a small number of DC. This occurred not only in the presence of free antigen, but also when DC and/or M phi were pulsed with antigen. A culture supernatant of M phi having interleukin-1 activity was effective in enhancing the proliferation of T cells which responded to antigen-pulsed DC. On the other hand, interleukin-2 did not replace DC even in the presence of antigen-pulsed Ia+ M phi. We also investigated recently primed T cells, but no evidence was obtained in favor of the competence of M phi as autonomous A cells.

摘要

研究了小鼠巨噬细胞(M phi)和脾树突状细胞(DC)在6周或更早之前用钥孔戚血蓝蛋白(KLH)免疫的小鼠记忆T细胞抗原特异性增殖反应中的作用。腹膜M phi,无论是否表达Ia抗原,都不能作为自主辅助细胞(A细胞)发挥作用。脾脏黏附细胞群体的A细胞活性,其中大多数为M phi,少数为DC,通过用DC特异性单克隆抗体和补体消除DC而被消除,并通过添加少量DC而恢复。尽管M phi不能作为自主A细胞发挥作用,但它们在存在少量DC的情况下增强了增殖反应。这不仅在存在游离抗原时发生,而且当DC和/或M phi用抗原脉冲时也会发生。具有白细胞介素-1活性的M phi培养上清液在增强对抗原脉冲DC作出反应的T细胞增殖方面是有效的。另一方面,即使在存在抗原脉冲的Ia + M phi的情况下,白细胞介素-2也不能替代DC。我们还研究了近期免疫的T细胞,但没有获得证据支持M phi作为自主A细胞的能力。

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