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自身抗体的同种型影响自身免疫性血小板减少性紫癜中抗体包被血小板的吞噬作用。

The isotype of autoantibodies influences the phagocytosis of antibody-coated platelets in autoimmune thrombocytopenic purpura.

机构信息

Institute of Transfusion Medicine and Transplantation Immunology, University Hospital Muenster, Germany.

出版信息

Scand J Immunol. 2011 Nov;74(5):489-95. doi: 10.1111/j.1365-3083.2011.02600.x.

Abstract

Autoimmune thrombocytopenic purpura (AITP) is an acquired autoimmune bleeding disorder, characterized by isolated thrombocytopenia because of destruction of auto-antibody-coated platelets by Fc-receptor-mediated phagocytosis. The destruction of autoantibody-sensitized platelets by FcγR-bearing phagocytic cells and the following antigen presentation are considered to play a key role for the pathophysiology of AITP. Although different isotypes of AITP-mediating autoantibodies, e.g. IgG, IgM and IgA, are frequently found in AITP patients, their role in the pathophysiology of AITP remains unclear. Using a flow cytometric monocyte-based phagocytosis assay, we investigated the impact of disease-associated autoantibody isotype in antibody-mediated phagocytosis of platelets. Platelets, labelled with 5-chloromethyl fluorescein diacetate (CMFDA), were incubated with AITP patients' serum characterized by pure IgG or IgM antiplatelet autoantibodies. Labelled platelets were incubated with monocytes. Phagocytosis was defined as the product of percentage of CMFDA-positive monocytes and mean fluorescence intensity of CMFDA. Adherence of platelets to monocytes was quantified by anti-CD61-PerCp in a CMFDA(+) CD14(+) gate. IgG-coated platelets showed a significantly higher phagocytic index than IgM-coated platelets (mean 796 ± 157 versus 539 ± 78, P < 0.01). There were no significant differences regarding platelet adherence to monocytes. The isotype of autoantibodies influences the quantity of in vitro phagocytosis of autologous platelets by monocytes. Therefore, the AITP-mediating autoantibody isotype should be considered more carefully in pathophysiologic models and furthermore in diagnostic, therapeutic and prognostic approaches in AITP.

摘要

自身免疫性血小板减少性紫癜(AITP)是一种获得性自身免疫性出血性疾病,其特征为孤立性血小板减少症,由于 Fc 受体介导的吞噬作用导致自身抗体包被的血小板被破坏。FcγR 阳性吞噬细胞对自身抗体致敏的血小板的破坏和随后的抗原提呈被认为在 AITP 的病理生理学中发挥关键作用。尽管 AITP 患者中经常发现不同的 AITP 介导的自身抗体同种型,例如 IgG、IgM 和 IgA,但它们在 AITP 的病理生理学中的作用仍不清楚。我们使用基于流式细胞术的单核细胞吞噬测定法,研究了疾病相关自身抗体同种型在抗体介导的血小板吞噬中的作用。用 5-氯甲基荧光素二乙酸酯(CMFDA)标记血小板,与 AITP 患者的血清孵育,该血清特征为纯 IgG 或 IgM 抗血小板自身抗体。标记的血小板与单核细胞孵育。吞噬作用定义为 CMFDA 阳性单核细胞的百分比和 CMFDA 的平均荧光强度的乘积。通过 CMFDA(+)CD14(+)门中的抗 CD61-PerCp 量化血小板与单核细胞的黏附。与 IgM 包被的血小板相比,IgG 包被的血小板表现出明显更高的吞噬指数(平均 796 ± 157 对 539 ± 78,P < 0.01)。血小板与单核细胞的黏附无显著差异。自身抗体的同种型影响单核细胞体外吞噬自身血小板的数量。因此,在病理生理模型中,以及在 AITP 的诊断、治疗和预后方法中,应更仔细地考虑 AITP 介导的自身抗体同种型。

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