Bluestone J A, Pardoll D, Sharrow S O, Fowlkes B J
Nature. 1987;326(6108):82-4. doi: 10.1038/326082a0.
The thymus is the major site for T-cell receptor (TCR) gene rearrangement and T-cell maturation. The specific antigen recognition structure (TCR) on murine T cells has been shown to be dependent on a polymorphic set of disulphide-linked heterodimers, containing two integral membrane glycoprotein chains, TCR alpha and TCR beta, expressed in non-covalent association with an invariant complex of proteins, CD3 (T3). Recently, a novel TCR/CD3 complex, that includes the product of the TCR gamma gene, has been identified on a subset of both peripheral cells and thymocytes. Here we examine the expression of TCR/CD3 complexes in fetal ontogeny and in the adult thymus. The results demonstrate that CD3+4-8-(T3+,L3T4-,Lyt2-)cells are detected in day-15 fetal thymi, throughout fetal development and in adult thymus. In situ hybridization studies indicate that these early CD3+ cells express high levels of TCR gamma-specific RNA, low levels of TCR beta-specific RNA and no detectable TCR alpha-specific RNA. Day-16 CD3+,4-,8- fetal thymocytes can be activated to proliferate and demonstrate cytolytic activity when cultured in the presence of anti-CD3 monoclonal antibodies and interleukin-2 (IL-2). These results suggest that CD3-bearing cells, present early in thymic ontogeny, express a functional TCR and may, therefore, be important in repertoire development.
胸腺是T细胞受体(TCR)基因重排和T细胞成熟的主要场所。已证明小鼠T细胞上的特异性抗原识别结构(TCR)依赖于一组多态性的二硫键连接的异二聚体,其包含两条完整的膜糖蛋白链,即TCRα和TCRβ,它们与一种不变的蛋白质复合物CD3(T3)以非共价结合的形式表达。最近,在外周细胞和胸腺细胞的一个亚群上鉴定出了一种新型的TCR/CD3复合物,其中包括TCRγ基因的产物。在此,我们研究了TCR/CD3复合物在胎儿发育过程和成年胸腺中的表达情况。结果表明,在胚胎第15天的胎儿胸腺、整个胎儿发育过程以及成年胸腺中均检测到CD3 + 4 - 8 - (T3 + ,L3T4 - ,Lyt2 - )细胞。原位杂交研究表明,这些早期的CD3 + 细胞高水平表达TCRγ特异性RNA,低水平表达TCRβ特异性RNA,未检测到TCRα特异性RNA。当在抗CD3单克隆抗体和白细胞介素-2(IL - 2)存在的情况下培养时,胚胎第16天的CD3 + 、4 - 、8 - 胎儿胸腺细胞可被激活增殖并表现出细胞溶解活性。这些结果表明,在胸腺发育早期出现的带有CD3的细胞表达功能性TCR,因此可能在T细胞库的发育中起重要作用。
