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自身抗体穿透活的上皮细胞。

Penetration of autoantibodies into living epithelial cells.

作者信息

Golan T D, Gharavi A E, Elkon K B

机构信息

Hospital for Special Surgery, Cornell University Medical College, New York, New York.

出版信息

J Invest Dermatol. 1993 Mar;100(3):316-22. doi: 10.1111/1523-1747.ep12469994.

Abstract

The ability of autoantibodies to penetrate living cells is controversial. We have identified immunoglobulin G (IgG) antibodies capable of penetrating an epithelial cell line, COLO-16, in five of 36 (14%) antinuclear antibody positive sera from patients with SLE. Thirty minutes following incubation of cells with dilutions of either whole sera, globulin fractions, or F(ab')2 fragments of IgG, approximately 80-90% of cells demonstrated intranuclear IgG by indirect immunofluorescence. Viability of cells prior to assay was > 98% as determined by trypan blue staining and penetration of IgG into the nuclei did not affect viability or DNA synthesis of the cells in short-term culture. Intracellular IgG could not be detected following exposure of the cells to high-titer reference autoantibodies of known specificities (against DNA, Ro, La, Sm, RNP, or ribosomes). Furthermore, absorption of the sera with either DNA or chromatin failed to abolish intranuclear penetration, indicating that the autoantibodies were not directed against DNA receptors or nucleosomes on the cell surface. Antibody uptake was relatively selective for epithelial cell lines, because intranuclear IgG was not detected in cell lines of lymphoid origin exposed to the sera. Two of the five sera immunoprecipitated proteins of molecular weight 88 kD with or without a 68-kD protein from COLO-16 cells labeled with 125I at the cell surface. These findings indicate that a subset of SLE patients have IgG capable of penetrating a cell line of epithelial origin. These antibodies, most likely, bind to cell surface proteins and are translocated into the cell nucleus. Although direct immunofluorescence of a skin biopsy obtained from one of the five patients with "penetrating IgG" also showed intranuclear staining for IgG, the biologic relevance of these findings remains to be determined.

摘要

自身抗体穿透活细胞的能力存在争议。我们在36份系统性红斑狼疮(SLE)患者的抗核抗体阳性血清中,发现有5份(14%)含有能够穿透上皮细胞系COLO - 16的免疫球蛋白G(IgG)抗体。用全血清、球蛋白组分或IgG的F(ab')2片段稀释液孵育细胞30分钟后,通过间接免疫荧光法检测发现,约80 - 90%的细胞细胞核内有IgG。通过台盼蓝染色测定,检测前细胞活力> 98%,IgG进入细胞核并不影响短期培养中细胞的活力或DNA合成。将细胞暴露于已知特异性的高滴度参考自身抗体(针对DNA、Ro、La、Sm、RNP或核糖体)后,未检测到细胞内IgG。此外,用DNA或染色质吸收血清并不能消除细胞核内的穿透现象,这表明自身抗体并非针对细胞表面的DNA受体或核小体。抗体摄取对上皮细胞系具有相对选择性,因为暴露于这些血清的淋巴源性细胞系中未检测到细胞核内IgG。这5份血清中的2份免疫沉淀了COLO - 16细胞表面用125I标记的分子量为88 kD的蛋白质,有的还沉淀了分子量为68 kD的蛋白质。这些发现表明,一部分SLE患者的IgG能够穿透上皮来源的细胞系。这些抗体很可能与细胞表面蛋白结合,并转运至细胞核内。尽管对5例“穿透性IgG”患者之一进行的皮肤活检直接免疫荧光检查也显示细胞核内有IgG染色,但这些发现的生物学意义仍有待确定。

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