Schwaber J, Koenig N, Girard J
Children's Hospital, Boston, Massachusetts 02115.
J Clin Invest. 1988 Oct;82(4):1471-6. doi: 10.1172/JCI113754.
The X chromosome-linked antibody deficiency disease, X-linked agammaglobulinemia (XLA), results from failure of B lymphoid development. In the minor form of XLA, B lymphoid development terminates at the stage of immature B lymphocytes that produce truncated Ig heavy (H) chains composed of D-J-C(mu/delta), resulting from failure of VH gene rearrangement. Fusion of B cells from a patient with the minor form of XLA with mouse myeloma results in complementation of this defect; hybrid cells produce full-length H chains composed of VH-D-JH-C. The VH gene is of human origin. Complementation occurs independent of retention or loss of the human X (XLA) chromosome in the hybrid cells. These results indicate that the D-JH-C structure of the XLA B cells is fully functional for the subsequent rearrangement of a VH gene element, and that failure of immunoglobulin expression is susceptible to correction.
X染色体连锁抗体缺乏病,即X连锁无丙种球蛋白血症(XLA),是由B淋巴细胞发育失败所致。在XLA的轻度形式中,B淋巴细胞发育在未成熟B淋巴细胞阶段终止,这些未成熟B淋巴细胞产生由D-J-C(μ/δ)组成的截短型免疫球蛋白重链(H链),这是由于VH基因重排失败所致。将轻度形式XLA患者的B细胞与小鼠骨髓瘤细胞融合可弥补这一缺陷;杂交细胞产生由VH-D-JH-C组成的全长H链。VH基因是人源的。互补作用的发生与杂交细胞中人X(XLA)染色体的保留或丢失无关。这些结果表明,XLA B细胞的D-JH-C结构对于VH基因元件的后续重排具有完全功能,并且免疫球蛋白表达的失败易于纠正。
