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溶菌酶特异性抑制的免疫调节。III. 单克隆抑制性T细胞产物诱导的免疫抑制的表位特异性扩增。

Immunoregulation of lysozyme-specific suppression. III. Epitope-specific amplification of immunosuppression induced by monoclonal suppressor-T-cell products.

作者信息

Adorini L, Colizzi V, Pini C, Appella E, Doria G

出版信息

Cell Immunol. 1986 Sep;101(2):502-11. doi: 10.1016/0008-8749(86)90161-9.

Abstract

The hen egg-white lysozyme (HEL)-specific suppression induced by soluble molecules produced by a monoclonal T-cell lymphoma line (LH8-105) obtained from HEL-specific suppressor T lymphocytes has been examined. Injection of I-J+ molecules from LH8-105 cell culture supernatant (TsFa) in HEL-primed mice during the afferent phase of the response induced Lyt-2+ second order suppressor T (Ts) cells which, upon transfer into HEL-CFA-primed syngeneic recipients, inhibit the delayed-type hypersensitivity (DTH) response to HEL. Transfer of spleen cells from TsFa-injected mice primed with HEL or human lysozyme suppresses the DTH response to HEL in recipient mice whereas this response is not affected by cell transfer from ring-necked pheasant egg-white lysozyme (REL)-primed and TsFa-injected mice, indicating that induction of second order Ts by TsFa is specific for a lysozyme epitope including phenylalanine at position 3. Fine antigenic specificity of second order Ts-cell induction is confirmed by similar results obtained upon injection of TsFa in mice primed with HEL N-terminal synthetic peptide or with an analog in which, as in REL, phenylalanine has been substituted by tyrosine at position 3. The same fine antigenic specificity observed in the induction of second order Ts cells is also present in the expression of TsFe suppressive activity. The similar antigenic specificity of Tsa and Tse suggests that Tse cells could result from amplification of the Tsa cell population or these two cell subsets could reflect different maturation stages of the same cell type rather than distinct T-cell populations activated in cascade.

摘要

对由从溶菌酶特异性抑制性T淋巴细胞获得的单克隆T细胞淋巴瘤系(LH8 - 105)产生的可溶性分子所诱导的鸡卵清溶菌酶(HEL)特异性抑制作用进行了研究。在反应的传入阶段,将LH8 - 105细胞培养上清液中的I - J⁺分子(TsFa)注射到用HEL致敏的小鼠体内,诱导产生了Lyt - 2⁺二级抑制性T(Ts)细胞,将这些细胞转移到用HEL - CFA致敏的同基因受体小鼠中时,可抑制对HEL的迟发型超敏反应(DTH)。用HEL或人溶菌酶致敏并注射了TsFa的小鼠的脾细胞转移,可抑制受体小鼠对HEL的DTH反应,而环颈雉卵清溶菌酶(REL)致敏并注射了TsFa的小鼠的细胞转移对该反应没有影响,这表明TsFa诱导二级Ts细胞对包括第3位苯丙氨酸的溶菌酶表位具有特异性。在用HEL N末端合成肽或第3位苯丙氨酸被酪氨酸取代(如同在REL中)的类似物致敏的小鼠中注射TsFa后获得的相似结果,证实了二级Ts细胞诱导作用的精细抗原特异性。在二级Ts细胞诱导过程中观察到的相同精细抗原特异性,也存在于TsFe抑制活性的表达中。Tsa和Tse的相似抗原特异性表明,Tse细胞可能是Tsa细胞群体扩增的结果,或者这两个细胞亚群可能反映了同一细胞类型的不同成熟阶段,而不是级联激活的不同T细胞群体。

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