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抗免疫球蛋白对小鼠淋巴细胞的激活作用。II. B淋巴细胞成熟亚群的非胸腺依赖性反应。

Activation of mouse lymphocytes by anti-immunoglobulin. II. A thymus-independent response by a mature subset of B lymphocytes.

作者信息

Sieckmann D G, Scher I, Asofsky R, Mosier D E, Paul W E

出版信息

J Exp Med. 1978 Dec 1;148(6):1628-43. doi: 10.1084/jem.148.6.1628.

Abstract

Mouse spleen cells can be stimulated to proliferate in vitro by purified anti-mu or anti-gamma,kappa antibodies. These responses can be obtained in cell populations bearing membrane immunoglobulin (Ig), purified by the fluorescence activated cell sorter (FACS), but they are not observed in FACS-purified Ig- cell populations. Furthermore, treatment of spleen cell populations with anti-Thy 1.2 and complement does not impair the response, nor does addition of nylon wool-purified T lymphocytes enhance it. These results indicate that B lymphocytes respond to anti-Ig and that their response does not require T cells. On the other hand, cells from athymic nude (nu/nu) mice respond slightly less well to anti-mu than do cells from heterozygous littermate (nu/+) controls; nu/nu cells are almost unresponsive to anti-gamm,kappa and addition of nylon wool-purified T cells from nu/+ controls does not restore the response. This suggests that T lymphocytes or the thymus may control the appearance of cells responsive to anti-gamma,kappa. Responsiveness of normal mice to anti-mu does not appear until 4 wk of age and does not reach maximum levels until 8 wk of age. Acquisition of full responsiveness to anti-gamma,kappa is even more delayed. This, together with the failure of mice with the CBA/N B-cell defect to respond to anti-Ig, suggests that cells stimulated to proliferate by anti-Ig are a mature subset of B cells. Depletion of adherent cells by Sephadex G-10 treatment or by treatment with carbonyl iron and exposure to a magnetic field does not diminish anti-mu or anti-gamma,kappa responses, suggesting that the responsiveness does not require the presence of macrophages. Thus, activation of B-cell proliferation by anti-Ig appears to be a T-cell independent, macrophage-independent process in which membrane Ig plays a direct role in signal generation.

摘要

纯化的抗μ或抗γ、κ抗体可刺激小鼠脾细胞在体外增殖。在通过荧光激活细胞分选仪(FACS)纯化的带有膜免疫球蛋白(Ig)的细胞群体中可获得这些反应,但在FACS纯化的Ig阴性细胞群体中未观察到这些反应。此外,用抗Thy 1.2和补体处理脾细胞群体不会损害反应,添加尼龙毛纯化的T淋巴细胞也不会增强反应。这些结果表明B淋巴细胞对抗Ig有反应,且它们的反应不需要T细胞。另一方面,无胸腺裸鼠(nu/nu)的细胞对抗μ的反应比杂合子同窝对照(nu/+)的细胞稍差;nu/nu细胞几乎对抗γ、κ无反应,添加来自nu/+对照的尼龙毛纯化T细胞也不能恢复反应。这表明T淋巴细胞或胸腺可能控制对抗γ、κ有反应的细胞的出现。正常小鼠对抗μ的反应直到4周龄才出现,直到8周龄才达到最高水平。对抗γ、κ的完全反应的获得甚至更延迟。这与具有CBA/N B细胞缺陷的小鼠对抗Ig无反应一起,表明被抗Ig刺激增殖的细胞是B细胞的一个成熟亚群。通过Sephadex G - 10处理或用羰基铁处理并暴露于磁场来耗尽黏附细胞,不会减弱对抗μ或抗γ、κ的反应,这表明反应不需要巨噬细胞的存在。因此,抗Ig激活B细胞增殖似乎是一个不依赖T细胞、不依赖巨噬细胞的过程,其中膜Ig在信号产生中起直接作用。

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