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白细胞介素-4抑制抗μ链抗体诱导的人B细胞增殖:环磷酸腺苷依赖性抑制途径的参与。

IL-4 counteracts anti-mu-induced human B cell proliferation: involvement of a cAMP-dependent inhibitory pathway.

作者信息

Taieb J, Leca G, Auffredou M T, Galanaud P, Vazquez A

机构信息

Inserm U 131, Clamart, France.

出版信息

Eur Cytokine Netw. 1991 Aug-Sep;2(4):265-72.

PMID:1721849
Abstract

In this report we show that IL-4 inhibits DNA synthesis induced by stimulation of human B cells with mitogenic doses of either soluble anti-mu mAb DA44 or phorbol ester. In contrast, earlier steps of anti-mu-induced B cell stimulation, such as RNA synthesis, CD23 expression and IL-6 production, were not inhibited but rather increased in the presence of IL-4. From these results, IL-4 appears therefore to exert two opposite effects on DA44 anti-mu mAb-induced human B cell activation: early steps are stimulated, and later steps inhibited. The results of kinetic analysis were consistent with this model. The inhibitory activity of IL-4 required an active cAMP-dependent pathway since IL-4-mediated inhibition of anti-mu-induced B cell proliferation was abolished in the presence of two specific inhibitors of the cAMP pathway (H8 and 2',5'-dideoxyadenosine which are specific for cAMP-dependent protein kinase and adenylate cyclase respectively). Furthermore, IL-4 induced a delayed and prolonged increase in intracellular cAMP concentrations (observed between 4 and 48 hours of culture), and this strongly suggests that the late inhibitory effects of IL-4 is cAMP-dependent. Moreover, this delayed IL-4-mediated cAMP production is probably sufficient to prevent anti-mu induced DNA synthesis since addition of the cAMP agonist forskolin on day 1 or 2 of culture also suppresses the anti-mu-mediated B cell proliferation.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在本报告中,我们表明白细胞介素-4(IL-4)可抑制用促有丝分裂剂量的可溶性抗μ单克隆抗体DA44或佛波酯刺激人B细胞所诱导的DNA合成。相反,抗μ诱导的B细胞刺激的早期步骤,如RNA合成、CD23表达和IL-6产生,在IL-4存在的情况下并未受到抑制,反而增加。因此,从这些结果来看,IL-4似乎对DA44抗μ单克隆抗体诱导的人B细胞活化发挥两种相反的作用:早期步骤受到刺激,后期步骤受到抑制。动力学分析结果与该模型一致。IL-4的抑制活性需要一条活跃的cAMP依赖性途径,因为在存在两种cAMP途径的特异性抑制剂(分别对cAMP依赖性蛋白激酶和腺苷酸环化酶具有特异性的H8和2',5'-二脱氧腺苷)的情况下,IL-4介导的抗μ诱导的B细胞增殖抑制作用被消除。此外,IL-4诱导细胞内cAMP浓度延迟且持续升高(在培养4至48小时之间观察到),这强烈表明IL-4的后期抑制作用是cAMP依赖性的。而且,这种延迟的IL-4介导的cAMP产生可能足以阻止抗μ诱导的DNA合成,因为在培养的第1天或第2天添加cAMP激动剂福斯可林也会抑制抗μ介导的B细胞增殖。(摘要截断于250字)

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