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免疫与免疫病理学中的长寿浆细胞。

Long-lived plasma cells in immunity and immunopathology.

作者信息

Moser Katrin, Muehlinghaus Gwendolin, Manz Rudi, Mei Henrik, Voigt Caroline, Yoshida Taketoshi, Dörner Thomas, Hiepe Falk, Radbruch Andreas

机构信息

German Arthritis Research Center Berlin, Schumannstrasse 20/21, 10117 Berlin, Germany.

出版信息

Immunol Lett. 2006 Mar 15;103(2):83-5. doi: 10.1016/j.imlet.2005.09.009. Epub 2005 Oct 21.

Abstract

Following tetanus vaccination, a wave of antibody-secreting cells appear in the peripheral blood composed of vaccine-specific, migratory plasmablasts and plasma cells secreting antibodies specific for other antigens. The latter probably were tissue resident plasma cells formed in earlier immune responses that are mobilized due to competition with the newly formed tetanus-specific plasmablasts. Newly formed plasma cells secreting antibodies specific for a particular antigen/vaccine are accommodated in the bone marrow likely at the global expense of the pre-existing long-lived plasma cell population providing humoral memory for other antigens. Plasmablasts but not mature plasma cells are attracted by the ligands for the chemokine receptors CXCR4 and CXCR3. While CXCR4 and its cognate ligand is important for plasma cell homing to the bone marrow, CXCR3 and its ligand IP10 are likely to be involved in attracting them to inflamed tissue. In NZB/W mice, a model for systemic lupus, long-lived autoreactive plasma cells are present not only in bone marrow, but also in inflamed tissues and spleen. Autoreactive plasma cells in the spleen are present long before the onset of the disease, suggesting that these cells contribute to induction of immunopathology.

摘要

破伤风疫苗接种后,外周血中会出现一波分泌抗体的细胞,它们由疫苗特异性的、迁移性的浆母细胞和分泌针对其他抗原的抗体的浆细胞组成。后者可能是在早期免疫反应中形成的组织驻留浆细胞,由于与新形成的破伤风特异性浆母细胞竞争而被动员起来。分泌针对特定抗原/疫苗的抗体的新形成的浆细胞可能会被骨髓容纳,这可能是以牺牲预先存在的为其他抗原提供体液记忆的长寿浆细胞群体为代价的。趋化因子受体CXCR4和CXCR3的配体可吸引浆母细胞,但不能吸引成熟浆细胞。虽然CXCR4及其同源配体对浆细胞归巢至骨髓很重要,但CXCR3及其配体IP10可能参与将它们吸引至炎症组织。在系统性红斑狼疮模型NZB/W小鼠中,长寿的自身反应性浆细胞不仅存在于骨髓中,也存在于炎症组织和脾脏中。脾脏中的自身反应性浆细胞在疾病发作前很久就已存在,这表明这些细胞有助于免疫病理学的诱导。

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