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大鼠巨噬细胞辅助细胞功能不佳可能反映出它们无法与T细胞形成簇。

The poor accessory cell function of macrophages in the rat may reflect their inability to form clusters with T cells.

作者信息

Kradin R L, McCarthy K M, Dailey C I, Burdeshaw A, Kurnick J T, Schneeberger E E

出版信息

Clin Immunol Immunopathol. 1987 Sep;44(3):348-63. doi: 10.1016/0090-1229(87)90079-1.

Abstract

The accessory cell functions of Ia+ alveolar and peritoneal macrophages were compared to those of splenic cells in the rat. Whereas splenic mononuclear cells and dendritic cells were excellent supporters of both MHC-restricted and nonrestricted T-cell mitogenic responses, Ia+ macrophages were inefficient antigen-presenting cells and poor supporters of lectin mitogenic responses. Binding of antigen-primed T-cell blasts by splenic cells in the presence of Con A or antigen occurred within 30 min and subsequently led to the formation of nonadherent clusters of "dendritic-like cells" and proliferating T-cell blasts. Unstimulated Ia- macrophages failed to bind T cells during 30 min of coculture but formed conjugates with T-cell blasts within 24 hr. Delayed binding did not require the presence of antigen or lectin, or the expression of Ia antigens by the macrophage, and did not lead to T-cell proliferation. Antigen-specific binding and antigen presentation, but not lectin mitogenesis, were enhanced by treating antigen-pulsed Ia+ macrophages with neuraminidase for 30 min at 37 degrees C. Neuraminidase did not augment splenic accessory cell function. Antigen-specific binding of T cells to Ia+ macrophages and accessory cell function may be enhanced by desialation of glycoproteins on the cell surface membrane.

摘要

将大鼠肺泡和腹腔Ia⁺巨噬细胞的辅助细胞功能与脾细胞的辅助细胞功能进行了比较。脾单核细胞和树突状细胞是MHC限制性和非限制性T细胞促有丝分裂反应的优秀支持者,而Ia⁺巨噬细胞是低效的抗原呈递细胞,对凝集素促有丝分裂反应的支持能力较差。在存在刀豆蛋白A或抗原的情况下,脾细胞在30分钟内即可结合抗原致敏的T细胞母细胞,随后形成“树突状样细胞”和增殖的T细胞母细胞的非黏附簇。未受刺激的Ia⁻巨噬细胞在共培养30分钟期间未能结合T细胞,但在24小时内与T细胞母细胞形成结合物。延迟结合不需要抗原或凝集素的存在,也不需要巨噬细胞表达Ia抗原,且不会导致T细胞增殖。通过在37℃用神经氨酸酶处理抗原脉冲的Ia⁺巨噬细胞30分钟,可增强抗原特异性结合和抗原呈递,但不会增强凝集素促有丝分裂作用。神经氨酸酶不会增强脾辅助细胞功能。细胞表面膜上糖蛋白的去唾液酸化可能会增强T细胞与Ia⁺巨噬细胞的抗原特异性结合及辅助细胞功能。

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