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一小部分鼠单克隆抗脱氧核糖核酸抗体以时间和温度依赖性方式穿过细胞质并进入细胞核。

A subgroup of murine monoclonal anti-deoxyribonucleic acid antibodies traverse the cytoplasm and enter the nucleus in a time-and temperature- dependent manner.

作者信息

Yanase K, Smith R M, Cĭzman B, Foster M H, Peachey L D, Jarett L, Madaio M P

机构信息

Department of Medicine, University of Pennsylvania School of Medicine, Philadelphia.

出版信息

Lab Invest. 1994 Jul;71(1):52-60.

PMID:8041118
Abstract

BACKGROUND

The capacity of lupus autoantibodies to enter living cells and bind to molecules for which they have intrinsic affinity is not well appreciated. In previous studies, we identified a subgroup of three murine monoclonal IgG anti-DNA antibodies, derived from lupus-prone MRL-lpr/lpr mice, that localized within nuclei of cells in multiple organs and induced functional perturbations, in vivo, after passive transfer to normal mice. To examine the mechanisms of this phenomenon, we now extend these observations, using the same monoclonal anti-DNA antibodies and cultured cell lines.

EXPERIMENTAL DESIGN

Multiple experimental approaches were utilized to track nuclear localization of anti-DNA antibodies, including direct immunofluorescence, confocal microscopy and immunoelectron microscopy. The requirements for nuclear localization were further evaluated quantitatively, in nuclei isolated from co-cultures of cells and 125I-Ig, under varying experimental conditions.

RESULTS

Nuclear localization was observed with the same subset of anti-DNA antibodies that localized within nuclei in vivo; it was dependent on the antigen-binding region of the molecule; and it was not found with other anti-DNA antibodies. At progressive intervals, the Ig were observed: at the cell surface, within the cytoplasm, clustered at the nuclear pore, and within the nucleus. Nuclear localization of Ig was found to be a time- and temperature- dependent process, specific for a subset of anti-DNA antibodies and dependent on the antigen binding region of the Ig.

CONCLUSIONS

This is the first demonstration that monoclonal autoantibodies can traverse both the cell and nuclear membranes to localize within the nuclei of cultured cells. Furthermore, nuclear localization of Ig was regulated in a manner analogous to that of other large cytoplasmic proteins that enter the nucleus. This confirms and extends our results using the same antibodies in whole animals, and it provides the basis to further examine the underlying mechanisms and consequences of this phenomenon.

摘要

背景

狼疮自身抗体进入活细胞并与它们具有内在亲和力的分子结合的能力尚未得到充分认识。在先前的研究中,我们从易患狼疮的MRL-lpr/lpr小鼠中鉴定出一组三种鼠单克隆IgG抗DNA抗体,这些抗体在被动转移到正常小鼠体内后,定位于多个器官细胞的细胞核内,并在体内诱导功能紊乱。为了研究这一现象的机制,我们现在使用相同的单克隆抗DNA抗体和培养细胞系来扩展这些观察结果。

实验设计

采用多种实验方法追踪抗DNA抗体的核定位,包括直接免疫荧光、共聚焦显微镜和免疫电子显微镜。在不同实验条件下,从细胞与125I-Ig共培养物中分离的细胞核中,进一步定量评估核定位的要求。

结果

观察到与在体内定位于细胞核内的相同抗DNA抗体亚组的核定位;它依赖于分子的抗原结合区域;而其他抗DNA抗体未观察到这种情况。随着时间的推移,观察到Ig依次位于:细胞表面、细胞质内、聚集在核孔处以及细胞核内。发现Ig的核定位是一个时间和温度依赖性过程,对抗DNA抗体的一个亚组具有特异性,并依赖于Ig的抗原结合区域。

结论

这是首次证明单克隆自身抗体能够穿过细胞膜和核膜定位于培养细胞的细胞核内。此外,Ig的核定位是以类似于其他进入细胞核的大细胞质蛋白的方式进行调节的。这证实并扩展了我们在全动物中使用相同抗体的结果,并为进一步研究这一现象的潜在机制和后果提供了基础。

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