Mosier D E, Stell K L, Gulizia R J, Torbett B E, Gilmore G L
Division of Immunology, Medical Biology Institute, La Jolla, California 92137.
J Exp Med. 1993 Jan 1;177(1):191-4. doi: 10.1084/jem.177.1.191.
The autosomal recessive scid mutation results in defective immunoglobulin and T cell receptor gene rearrangement. The scid mutation occurred in the allotype congenic C.B-17 line, and up to 25% of C.B-17 scid mice spontaneously produce both T cells and immunoglobulin, a phenotype known as "leaky." Moreover, introduction of neonatal T cells into C.B-17 scid mice leads to immunoglobulin production by 100% of animals. We have produced mice homozygous for both the scid and beige mutations. By contrast with C.B-17 scid mice, BALB/c scid.beige mice have a < 2% incidence of "leakiness." This percentage does not increase with age, and introduction of neonatal T cells fails to rescue immunoglobulin production. This suggests that a gene (or genes) closely linked to the beige locus regulates B and/or T cell development.
常染色体隐性重症联合免疫缺陷(scid)突变导致免疫球蛋白和T细胞受体基因重排缺陷。scid突变发生在同种异型同类系C.B-17品系中,高达25%的C.B-17 scid小鼠会自发产生T细胞和免疫球蛋白,这种表型被称为“渗漏”。此外,将新生T细胞引入C.B-17 scid小鼠会导致100%的动物产生免疫球蛋白。我们培育出了scid和米色突变均为纯合子的小鼠。与C.B-17 scid小鼠相比,BALB/c scid.beige小鼠“渗漏”的发生率<2%。这个百分比不会随着年龄增长而增加,并且引入新生T细胞也无法挽救免疫球蛋白的产生。这表明与米色基因座紧密连锁的一个(或多个)基因调节B和/或T细胞的发育。
