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从成人骨髓中筛选凋亡细胞特异性人源抗体。

Selection of apoptotic cell specific human antibodies from adult bone marrow.

作者信息

Grönwall Caroline, Charles Edgar D, Dustin Lynn B, Rader Christoph, Silverman Gregg J

机构信息

School of Medicine, New York University, New York, New York, United States of America.

Laboratory of Virology and Infectious Disease, Rockefeller University, New York, New York, United States of America.

出版信息

PLoS One. 2014 Apr 23;9(4):e95999. doi: 10.1371/journal.pone.0095999. eCollection 2014.

Abstract

Autoreactive antibodies that recognize neo-determinants on apoptotic cells in mice have been proposed to have protective, homeostatic and immunoregulatory properties, although our knowledge about the equivalent antibodies in humans has been much more limited. In the current study, human monoclonal antibodies with binding specificity for apoptotic cells were isolated from the bone marrow of healthy adults using phage display technology. These antibodies were shown to recognize phosphorylcholine (PC)-associated neo-determinants. Interestingly, three of the four identified apoptotic cell-specific antibody clones were encoded by VH3 region rearrangements with germline or nearly germline configuration without evidence of somatic hypermutation. Importantly, the different identified antibody clones had diverse heavy chain CDR3 and deduced binding surfaces as suggested by structure modeling. This may suggest a potentially great heterogeneity in human antibodies recognizing PC-related epitopes on apoptotic cells. To re-construct the postulated structural format of the parental anti-PC antibody, the dominant clone was also expressed as a recombinant human polymeric IgM, which revealed a substantially increased binding reactivity, with dose-dependent and antigen-inhibitable binding of apoptotic cells. Our findings may have implication for improved prognostic testing and therapeutic interventions in human inflammatory disease.

摘要

有研究提出,识别小鼠凋亡细胞上新抗原决定簇的自身反应性抗体具有保护、稳态和免疫调节特性,不过我们对人类中相应抗体的了解要有限得多。在本研究中,利用噬菌体展示技术从健康成年人的骨髓中分离出了对凋亡细胞具有结合特异性的人单克隆抗体。这些抗体被证明可识别与磷酸胆碱(PC)相关的新抗原决定簇。有趣的是,四个已鉴定的凋亡细胞特异性抗体克隆中有三个由具有种系或近乎种系构型的VH3区域重排编码,且无体细胞超突变的证据。重要的是,如结构建模所示,不同的已鉴定抗体克隆具有不同的重链互补决定区3(CDR3)和推导的结合表面。这可能表明人类识别凋亡细胞上PC相关表位的抗体存在潜在的巨大异质性。为了重建假定的亲本抗PC抗体的结构形式,优势克隆也被表达为重组人聚合IgM,其显示出显著增强的结合反应性,对凋亡细胞的结合呈剂量依赖性且可被抗原抑制。我们的发现可能对改善人类炎症性疾病的预后检测和治疗干预具有启示意义。

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