Bell L M, Solomon K R, Gold J P, Tan K N
Division of Pediatric Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts 02115.
J Biol Chem. 1994 Sep 9;269(36):22758-63.
Surface expression of the T cell antigen receptor (TCR) in mature T cells requires the association of a variable heterodimer (alpha.beta or gamma.delta) with six invariant CD3 polypeptides (gamma, delta, epsilon-epsilon, zeta-zeta, or zeta-eta). We described here that deletion of the cytoplasmic tail polypeptide sequence (Lys-Lys-Lys-Asn-Ser) of TCR beta-chain (beta CT) results in expression of the truncated beta-chain on the surface of a mature T cell hybridoma line, in the absence of TCR-alpha, as a glycophosphatidylinositol (GPI)-anchored monomeric polypeptide. The GPI-anchored TCR-beta CT is not associated with CD3-epsilon and is incapable of conventional signal transduction. Association with TCR-alpha prevents beta CT from GPI-linkage formation. The alpha beta CT heterodimer binds the CD3 polypeptides, and the resultant TCR alpha beta CT/CD3 complex is capable of signal transduction. Our data show that a signal sequence for GPI-linkage formation is present in TCR-beta, and this alternative membrane anchoring mechanism can be utilized by beta-chain polypeptide lacking the CT sequence. We conclude therefore that in the absence of TCR-alpha expression, the beta-chain CT sequence plays an essential function in hindering GPI-linkage formation, thereby preventing escape of incompletely assembled TCR beta-chain to the cell surface of mature T cells.
成熟T细胞中T细胞抗原受体(TCR)的表面表达需要一个可变异二聚体(αβ或γδ)与六种恒定的CD3多肽(γ、δ、ε-ε、ζ-ζ或ζ-η)结合。我们在此描述,TCRβ链(βCT)的胞质尾多肽序列(Lys-Lys-Lys-Asn-Ser)缺失导致截短的β链在成熟T细胞杂交瘤细胞系表面表达,在没有TCR-α的情况下,作为糖磷脂酰肌醇(GPI)锚定的单体多肽。GPI锚定的TCR-βCT不与CD3-ε结合,并且不能进行传统的信号转导。与TCR-α结合可防止βCT形成GPI连接。αβCT异二聚体结合CD3多肽,并且产生的TCRαβCT/CD3复合物能够进行信号转导。我们的数据表明,TCR-β中存在用于形成GPI连接的信号序列,并且这种替代的膜锚定机制可被缺乏CT序列的β链多肽利用。因此,我们得出结论,在没有TCR-α表达的情况下,β链CT序列在阻碍GPI连接形成中起重要作用,从而防止未完全组装的TCRβ链逃逸到成熟T细胞的细胞表面。
