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外泌体制备物中存在的支原体污染物可诱导多克隆B细胞反应。

Mycoplasma contaminants present in exosome preparations induce polyclonal B cell responses.

作者信息

Quah Ben J C, O'Neill Helen C

机构信息

School of Biochemistry and Molecular Biology, Australian National University, Canberra, ACT, Australia.

出版信息

J Leukoc Biol. 2007 Nov;82(5):1070-82. doi: 10.1189/jlb.0507277. Epub 2007 Aug 14.

DOI:10.1189/jlb.0507277
PMID:17698916
Abstract

Exosome fractions of dendritic cells (DC) produced in long-term cultures (LTC) were found to contain Mycoplasma contaminants. In this study, Mycoplasma-infected, -uninfected, and -reinfected cultures of DC and control cell lines have been compared for their capacity to activate lymphocytes. Using differential centrifugation, size fractionation, and inhibition assays, it has been possible to map Mycoplasma to the exosome or vesicle fraction purified from culture supernatant (CSN). Mycoplasma fractions were shown to induce proliferation of B and not T cells. The B cell response was sensitive to mitomycin C and primaquine, both known antibiotics, but resistant to protease and DNase, suggesting a role for lipoproteins. Mycoplasma-contaminated exosome fractions of LTC-DC were potent mitogens for naive B cells and promoted Ig secretion. In contrast to the polyclonal B cell mitogen LPS, they were unable to promote Ig isotype switching. They induced polyclonal activation of all B cell subsets, including naive B cells, the T1 and T2 subsets of transitional B cells, marginal zone (MZ), and follicular (FO) B cells. The B cell proliferative response was not antigen-specific and occurred independently of T cell help. Implications for autoimmune sequelae associated with Mycoplasma infection are discussed along with the possibility that primaquine could be an effective treatment for Mycoplasma infection in humans. This study highlights the close association between exosomes and infectious agents like Mycoplasma and cautions about purification procedures for preparation of exosomes for studies on immunity.

摘要

在长期培养(LTC)中产生的树突状细胞(DC)的外泌体组分被发现含有支原体污染物。在本研究中,对受支原体感染、未感染和再次感染的DC培养物以及对照细胞系激活淋巴细胞的能力进行了比较。通过差速离心、尺寸分级分离和抑制试验,已能够将支原体定位到从培养上清液(CSN)中纯化的外泌体或囊泡组分。结果显示支原体组分可诱导B细胞而非T细胞增殖。B细胞反应对两种已知抗生素丝裂霉素C和伯氨喹敏感,但对蛋白酶和DNA酶有抗性,提示脂蛋白起作用。LTC-DC受支原体污染的外泌体组分是未成熟B细胞的强效有丝分裂原,并促进Ig分泌。与多克隆B细胞有丝分裂原LPS不同,它们无法促进Ig同种型转换。它们诱导所有B细胞亚群的多克隆激活,包括未成熟B细胞、过渡性B细胞的T1和T2亚群、边缘区(MZ)和滤泡(FO)B细胞。B细胞增殖反应不是抗原特异性的,且独立于T细胞辅助发生。文中讨论了与支原体感染相关的自身免疫后遗症,以及伯氨喹可能成为人类支原体感染有效治疗方法的可能性。本研究强调了外泌体与支原体等感染因子之间的密切关联,并对用于免疫研究的外泌体制备纯化程序提出了警示。

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Mycoplasma contaminants present in exosome preparations induce polyclonal B cell responses.外泌体制备物中存在的支原体污染物可诱导多克隆B细胞反应。
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