Wagner H
J Exp Med. 1973 Dec 1;138(6):1379-97. doi: 10.1084/jem.138.6.1379.
A mouse in vitro allograft system was used to evaluate the concept of T-T interaction in T cell-mediated cellular immunity. In analyzing the responsiveness of thymus-processed lymphocytes as obtained from different tissues, a heretogeneity within T cells was found in regard to their capacity to be immunized in vitro against transplantation antigens. Recirculating T cells were 10-20-fold superior to thymocytes, splenic T cells being intermediate. When few (1.5 x 10(6)) peripheral T cells, in numbers too small to yield good cytotoxic responses, were mixed with 14 x 10(6) thymocytes and the cell mixture immunized in vitro against cell-bound alloantigens, cytotoxic activity was generated exceeding about 10-20-fold the values that could be explained by a pure additive effect. Synergy occurred also in a mixture of responder T cells derived from CBA (H-2(k)) and AKR (H-2(k)) mice. Thus AKR anti-phi C3H serum could be used for discriminating between thymus-derived and peripheral T cell-derived cytotoxic lymphocytes (CL). Cytotoxic activity produced during the synergistic interaction between thymocytes and peripheral T cells was about 70% T cell derived, the remainder being thymus derived. The synoptic interpretation of this finding and "limiting dilution" experiments of the responder cells suggested strongly that peripheral T cells provide the major source for precursor cells of CL, thymocytes acting mainly as helper (amplifier) cells.
利用小鼠体外同种异体移植系统评估T细胞介导的细胞免疫中T-T相互作用的概念。在分析从不同组织获得的经胸腺处理的淋巴细胞的反应性时,发现T细胞在体外针对移植抗原进行免疫的能力方面存在异质性。再循环T细胞比胸腺细胞强10 - 20倍,脾T细胞介于两者之间。当少量(1.5×10⁶)数量太少而无法产生良好细胞毒性反应的外周T细胞与14×10⁶胸腺细胞混合,并且将细胞混合物在体外针对细胞结合的同种异体抗原进行免疫时,产生的细胞毒性活性超过了单纯加性效应所能解释的值的约10 - 20倍。来自CBA(H-2(k))和AKR(H-2(k))小鼠的反应性T细胞混合物中也发生了协同作用。因此,AKR抗-phi C3H血清可用于区分胸腺来源和外周T细胞来源的细胞毒性淋巴细胞(CL)。胸腺细胞和外周T细胞之间协同相互作用期间产生的细胞毒性活性约70%来源于T细胞,其余来源于胸腺。对这一发现的综合解释以及反应细胞的“有限稀释”实验强烈表明,外周T细胞是CL前体细胞的主要来源,胸腺细胞主要起辅助(放大)细胞的作用。
