Menon S, Rahman M A, Ravirajan C T, Kandiah D, Longhurst C M, McNally T, Williams W M, Latchman D S, Isenberg D A
Bloomsbury Rheumatology Unit/Division of Rheumatology, Department of Medicine, University College, London.
J Autoimmun. 1997 Feb;10(1):43-57. doi: 10.1006/jaut.1996.0106.
Antiphospholid antibodies (APL) have a notable association with recurrent miscarriages, arterial and venous thrombosis and thrombocytopenia. Analysis of the potential pathogenic effects of such human antibodies has been hampered by the considerable difficulty in producing IgG as opposed to IgM monoclonal immunoglobulins. We have developed four human monoclonal IgG APL (LJ1, AH2, DA3 and UK4) by fusing the peripheral blood lymphocytes of three patients with SLE with a mouse human heteromyeloma cell line, CB-F7. These antibodies bind to a variety of anionic phospholipids, two (LJ1 and AH2) bind total histones but none binds to ssDNA or dsDNA. Binding to beta 2 GPI is non-specific. UK4 alone demonstrates lupus anticoagulant activity. All four have lambda light chains, two are IgG1 (AH2 and UK4) and two are IgG3 (LJ1 and DA3). These APL utilize VH genes present in the fetally restricted repertoire and multiple somatic mutations in the CDR suggest an antigen-driven process. In contrast, there is no restriction in V lambda gene usage and only one lambda chain is extensively mutated. Two clonally related hybridomas were isolated from a single patients. This supports the theory that clonal expansion is the mechanism whereby antigen selects high affinity mutations.
抗磷脂抗体(APL)与复发性流产、动静脉血栓形成及血小板减少症有着显著关联。与IgM单克隆免疫球蛋白相比,生产IgG存在相当大的困难,这阻碍了对这类人类抗体潜在致病作用的分析。我们通过将三名系统性红斑狼疮患者的外周血淋巴细胞与小鼠-人异源骨髓瘤细胞系CB-F7融合,制备了四种人类单克隆IgG APL(LJ1、AH2、DA3和UK4)。这些抗体可与多种阴离子磷脂结合,其中两种(LJ1和AH2)可与总组蛋白结合,但均不与单链DNA或双链DNA结合。与β2糖蛋白I的结合是非特异性的。仅UK4表现出狼疮抗凝活性。这四种抗体均具有λ轻链,两种为IgG1(AH2和UK4),两种为IgG3(LJ1和DA3)。这些APL利用胎儿受限库中存在的VH基因,互补决定区中的多个体细胞突变提示存在抗原驱动过程。相比之下,Vλ基因的使用没有限制,只有一条λ链发生广泛突变。从一名患者中分离出两个克隆相关的杂交瘤。这支持了克隆扩增是抗原选择高亲和力突变的机制这一理论。
