Thymosin enhances the production of IL-1 alpha by human peripheral blood monocytes.

Lymphokine research Pub Date : 1989-01-01
S K Hu, M Badamchian, Y L Mitcho, A L Goldstein
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Abstract

Incubation of human peripheral blood monocytes (PBM) with a partially purified thymic preparation, thymosin fraction (TF5), results in a dose dependent production of an interleukin-1 (IL-1)-like factor. The biological activity of this factor can be blocked by anti-IL-1 alpha, but not by anti-IL-1 beta which neutralizes bacterial induced IL-1 activity. Studies with further purified TF5 fractions show that this activity is not due to the well-characterized peptide, thymosin alpha 1 (T alpha 1), but rather a new thymosin peptide(s) isolated from a more basic fraction. Intraperitoneal injection of TF5 also induces the expression of a membrane-bound IL-1 (mIL-1) on mouse peritoneal cells. This study provides the first evidence that TF5 can influence macrophage activity directly by enhancing IL-1 production. This observation may help explain the mechanism by which TF5 modulates immune responses. These results also point to a more selective role for thymic hormones, growth factors and cytokines which may trigger macrophages to secrete different forms of IL-1, which can then regulate either immune and/or inflammatory processes.

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胸腺苷增强人外周血单核细胞IL-1 α的产生。
人外周血单核细胞(PBM)与部分纯化的胸腺制剂胸腺素组分(TF5)孵育,可产生剂量依赖性的白细胞介素-1 (IL-1)样因子。该因子的生物活性可被抗IL-1阻断,但不能被抗IL-1阻断,后者可中和细菌诱导的IL-1活性。对进一步纯化的TF5馏分的研究表明,这种活性不是由于已被充分表征的肽,胸腺素α 1 (T α 1),而是从更基本的馏分中分离出的一种新的胸腺素肽。腹腔注射TF5还可诱导膜结合IL-1 (mIL-1)在小鼠腹膜细胞上的表达。本研究首次证明TF5可以通过促进IL-1的产生直接影响巨噬细胞活性。这一观察结果可能有助于解释TF5调节免疫反应的机制。这些结果还指出,胸腺激素、生长因子和细胞因子的选择性作用更强,它们可能会触发巨噬细胞分泌不同形式的IL-1,从而调节免疫和/或炎症过程。
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