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正常淋巴细胞与SJL淋巴瘤(网状细胞肉瘤)的Ia限制相互作用导致淋巴因子产生。II. 抗体增强因子、白细胞介素2和免疫干扰素的快速产生。

Ia-restricted interaction of normal lymphoid cells and SJL lymphoma (reticulum cell sarcoma) leading to lymphokine production. II. Rapid production of antibody-enhancing factor, interleukin 2, and immune interferon.

作者信息

Ponzio N M, Hayama T, Nagler C, Katz I R, Hoffmann M K, Gilbert K, Vilcek J, Thorbecke G J

出版信息

J Natl Cancer Inst. 1984 Feb;72(2):311-20.

PMID:6420599
Abstract

Mixed cell cultures of syngeneic lymph node (LN), spleen, or thymus and gamma-irradiated, syngeneic lymphoma cells of transplantable reticulum cell sarcomas (gamma-RCS) produced within 24 hours high titers of interleukin 2 (IL-2) and immune interferon in their supernatant (SN). These lymphokine titers were much higher than those seen after stimulation with allogeneic cells. SN also had marked enhancing activity for antibody production by anti-T-cell serum plus complement-treated spleen cells to trinitrophenylated polyacrylamide in vitro. This activity could be removed by absorption with cells of an IL-2-dependent cytotoxic cell line. Mixtures of gamma-RCS and LN cells from SJL/J F1 hybrid mice produced these lymphokines only when the non-SJL parent contributed H-2s or H-2b, but not H-2k or H-2d, in the I-region. These I-region restrictions were similar to those observed previously with respect to the ability of T-cells from SJL F1 hybrids to give proliferative responses to gamma-RCS in vitro and of these mice to support tumor growth in vivo. gamma-RCS also induced rapid interferon production in vivo, but serum titers 24 hours after injection consisted primarily of interferon resistant to pH 2 and neutralized by antibody to virally induced interferon (IFN-alpha/beta), and the production of IFN-alpha/beta was not subject to the same genetic restrictions. Although reticulum cell sarcoma cell extracts had no detectable effect in vitro, they were capable of inducing transient IFN production in vivo.

摘要

同基因淋巴结(LN)、脾脏或胸腺与经γ射线照射的可移植性网状细胞肉瘤(γ-RCS)的同基因淋巴瘤细胞的混合细胞培养物,在24小时内其培养上清液(SN)中产生了高滴度的白细胞介素2(IL-2)和免疫干扰素。这些淋巴因子滴度远高于用异基因细胞刺激后所见的滴度。SN对经抗T细胞血清加补体处理的脾细胞针对三硝基苯基化聚丙烯酰胺的体外抗体产生也具有显著的增强活性。这种活性可通过用IL-2依赖性细胞毒性细胞系的细胞吸附而去除。来自SJL/J F1杂种小鼠的γ-RCS和LN细胞的混合物仅在非SJL亲本在I区贡献H-2s或H-2b而非H-2k或H-2d时才产生这些淋巴因子。这些I区限制与先前观察到的关于SJL F1杂种的T细胞在体外对γ-RCS产生增殖反应以及这些小鼠在体内支持肿瘤生长的能力的限制相似。γ-RCS在体内也诱导快速的干扰素产生,但注射后24小时的血清滴度主要由对pH 2有抗性且被病毒诱导的干扰素(IFN-α/β)抗体中和的干扰素组成,并且IFN-α/β的产生不受相同的遗传限制。尽管网状细胞肉瘤细胞提取物在体外没有可检测到的作用,但它们能够在体内诱导短暂的干扰素产生。

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