首页> 外文OA文献 >Human T-cell heterogeneity as delineated with a specific human thymus lymphocyte antiserum. In vitro effects on mitogen response mixed leukocyte culture, cell-mediated lymphocytotoxicity, and lymphokine production.
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Human T-cell heterogeneity as delineated with a specific human thymus lymphocyte antiserum. In vitro effects on mitogen response mixed leukocyte culture, cell-mediated lymphocytotoxicity, and lymphokine production.

机译:用特定的人胸腺淋巴细胞抗血清描述的人T细胞异质性。体外对有丝分裂原反应的影响混合了白细胞培养,细胞介导的淋巴细胞毒性和淋巴因子的产生。

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摘要

Human peripheral blood lymphocytes (PBL) were evaluated by their responses to phytohemmagglutinin (PHA-P), concanavallin A (con-A), and pokeweed mitogen (PWM), both before and after treatment with an antiserum against human thymic lymphocyte antigens (HTLA) that had been made T-cell-specific by multiple absorptions with immunoglobulin EAC-positive lymphoblast cell lines (B cells). Cells treated with HTLA were examined for their ability to react in a mixed lymphocyte culture (MLC) and to form killer cells in a cell-mediated lymphocytotoxicity (CML) system. Sensitized cells were also examined for their ability to respond to purified protein derivative (PPD) by blastogenesis, migration inhibitory factor release (MIP), and lymphotoxin (LT) production, both before and after treatment with HTLA and complement. The HTLA was in itself highly stimulatory to PBL. However, with the addition of complement and subsequent cell destruction, a marked decrease in its stimulatory response was noted. PBL treated with HTLA and complement exhibited marked inhibition of responsiveness to con-A with little decrease in PHA-P -OR PWM stimulation except at very high concentration of HTLA. MLC reaction was inhibited only when responder cells were treated with HTLA + C'. Treatment of stimulator cells with HTLA + C' did not significantly alter the MLC response. The HTLA + C'-treated cells failed to form killer cells in the CML reaction and inhibited PPD-induced blasto-genesis from PPD-sensitized individuals; however, treatment of sensitized cells with HTLA + C' had little effects on the release of MIF and LT. It is suggested that subpopulations of T-cells carry surface antigens that bind with this specific antisera, and that the con-A-responsive cells, the responder cells in the MLC, and killer T-cells comprise a separate subset from cells responding to PHA-P or PWM, OR THE MIF-and LT-producing cells.
机译:在用针对人胸腺淋巴细胞抗原(HTLA)的抗血清治疗之前和之后,通过对植物血凝素(PHA-P),伴刀豆球蛋白A(con-A)和商陆有丝分裂原(PWM)的反应来评估人外周血淋巴细胞(PBL)免疫球蛋白EAC阳性淋巴母细胞细胞系(B细胞)经多次吸收后已成为T细胞特异性。检查了用HTLA处理的细胞在混合淋巴细胞培养(MLC)中反应的能力以及在细胞介导的淋巴细胞毒性(CML)系统中形成杀伤细胞的能力。还用HTLA和补体处理前后,通过成纤维细胞生成,迁移抑制因子释放(MIP)和淋巴毒素(LT)产生来检测致敏细胞对纯化蛋白衍生物(PPD)的反应能力。 HTLA本身对PBL非常有促进作用。然而,随着补体的添加和随后的细胞破坏,注意到其刺激反应显着降低。用HTLA和补体处理的PBL表现出对con-A的显着抑制,PHA-P -OR PWM刺激几乎没有降低,除非HTLA浓度很高。仅当响应细胞用HTLA + C'处理时,MLC反应才被抑制。用HTLA + C'处理刺激细胞并未显着改变MLC反应。 HTLA + C'处理的细胞未能在CML反应中形成杀伤细胞,并抑制了PPD致敏的人的PPD诱导的胚发生。但是,用HTLA + C'处理致敏细胞对MIF和LT的释放几乎没有影响。提示T细胞亚群携带与该特异性抗血清结合的表面抗原,并且con-A应答细胞,MLC中的应答细胞和杀伤性T细胞包含与对PHA应答的细胞不同的子集-P或PWM,或产生MIF和LT的单元。

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