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胸腺肽α1的免疫药理学与细胞因子协同作用

Immunopharmacology of thymosin alpha1 and cytokine synergy.

作者信息

Naylor Paul H, Quadrini Karen, Garaci Enrico, Rasi Guido, Hadden John W

机构信息

IRX Therapeutics Inc., 1 BioScience Park Drive, Farmingdale, NY 11735, USA.

出版信息

Ann N Y Acad Sci. 2007 Sep;1112:235-44. doi: 10.1196/annals.1415.036. Epub 2007 Jun 13.

DOI:10.1196/annals.1415.036
PMID:17567942
Abstract

Thymosin alpha1 (Talpha1) is a 28 amino acid biologically active protein cleaved from positions 2-29 of a precursor protein, prothymosin alpha. Since its discovery, Talpha1 has been administered to animals and humans in a wide variety of settings and its pharmacologic effects are to enhance cellular immunity. Talpha1 administration is highly effective in settings where irradiation, chemotherapy, tumor burden, or immune senescence have caused a reduction of T cell number and/or function. Recent in vitro studies, including the one reported here, suggest that Talpha1 may act via pathways commonly used by various cytokines. This raises the possibility that Talpha1 and cytokines may have synergistic activity through potentiation of cytokine activity by Talpha1. Improved control of tumor growth when tumor-bearing mice were treated with Talpha1 and high doses of IL-2 has been previously reported. We extended those studies with the Lewis lung carcinoma mouse model using IRX-2, a natural well-defined biologic containing multiple cytokines, in combination with Talpha1 (IRX-3). Although IRX-2 was effective alone (using doses that contain significantly less IL-2 than in most typical studies), adding Talpha1 led to significant improvement in survival of the tumor-bearing mice. Based on these observations, the immunopharmacology of Talpha1 predicts an important clinical role for Talpha1 in the restoration of cellular immune activity when used in combination with cytokines. Patients who experience immune suppression due to the presence of tumor, irradiation, and/or chemotherapy or aging of the host would most benefit from this treatment combination.

摘要

胸腺肽α1(Tα1)是一种由前体蛋白原胸腺肽α在2-29位切割产生的含28个氨基酸的生物活性蛋白。自发现以来,Tα1已在多种情况下应用于动物和人类,其药理作用是增强细胞免疫。在因辐射、化疗、肿瘤负荷或免疫衰老导致T细胞数量和/或功能减少的情况下,给予Tα1非常有效。包括本文报道的一项研究在内的近期体外研究表明,Tα1可能通过各种细胞因子常用的途径发挥作用。这增加了Tα1和细胞因子可能通过Tα1增强细胞因子活性而具有协同活性的可能性。先前有报道称,用Tα1和高剂量白细胞介素-2治疗荷瘤小鼠时,肿瘤生长得到了更好的控制。我们使用IRX-2(一种含有多种细胞因子的天然明确生物制剂)与Tα1(IRX-3)联合,在Lewis肺癌小鼠模型中扩展了这些研究。尽管单独使用IRX-2是有效的(使用的剂量比大多数典型研究中的白细胞介素-2含量显著少),但添加Tα1可显著提高荷瘤小鼠的生存率。基于这些观察结果,Tα1的免疫药理学预测,当与细胞因子联合使用时,Tα1在恢复细胞免疫活性方面具有重要的临床作用。因肿瘤存在、辐射和/或化疗或宿主衰老而经历免疫抑制的患者将从这种治疗组合中获益最大。

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