腺苷受体与癌症。
Adenosine receptors and cancer.
作者信息
Fishman P, Bar-Yehuda S, Synowitz M, Powell J D, Klotz K N, Gessi S, Borea P A
机构信息
Can-Fite BioPharma, Kiryat Matalon, Petach Tikva, 49170, Israel.
出版信息
Handb Exp Pharmacol. 2009(193):399-441. doi: 10.1007/978-3-540-89615-9_14.
The A(1), A(2A), A(2B) and A(3) G-protein-coupled cell surface adenosine receptors (ARs) are found to be upregulated in various tumor cells. Activation of the receptors by specific ligands, agonists or antagonists, modulates tumor growth via a range of signaling pathways. The A(1)AR was found to play a role in preventing the development of glioblastomas. This antitumor effect of the A(1)AR is mediated via tumor-associated microglial cells. Activation of the A(2A)AR results in inhibition of the immune response to tumors via suppression of T regulatory cell function and inhibition of natural killer cell cytotoxicity and tumor-specific CD4+/CD8+ activity. Therefore, it is suggested that pharmacological inhibition of A(2A)AR activation by specific antagonists may enhance immunotherapeutics in cancer therapy. Activation of the A(2B)AR plays a role in the development of tumors via upregulation of the expression levels of angiogenic factors in microvascular endothelial cells. In contrast, it was evident that activation of A(2B)AR results in inhibition of ERK1/2 phosphorylation and MAP kinase activity, which are involved in tumor cell growth signals. Finally, A(3)AR was found to be highly expressed in tumor cells and tissues while low expression levels were noted in normal cells or adjacent tissue. Receptor expression in the tumor tissues was directly correlated to disease severity. The high receptor expression in the tumors was attributed to overexpression of NF-kappaB, known to act as an A(3)AR transcription factor. Interestingly, high A(3)AR expression levels were found in peripheral blood mononuclear cells (PBMCs) derived from tumor-bearing animals and cancer patients, reflecting receptor status in the tumors. A(3)AR agonists were found to induce tumor growth inhibition, both in vitro and in vivo, via modulation of the Wnt and the NF-kappaB signaling pathways. Taken together, A(3)ARs that are abundantly expressed in tumor cells may be targeted by specific A(3)AR agonists, leading to tumor growth inhibition. The unique characteristics of these A(3)AR agonists make them attractive as drug candidates.
人们发现,A(1)、A(2A)、A(2B)和A(3) G蛋白偶联细胞表面腺苷受体(ARs)在各种肿瘤细胞中上调。特定配体、激动剂或拮抗剂激活这些受体后,会通过一系列信号通路调节肿瘤生长。人们发现A(1)AR在预防胶质母细胞瘤的发生中发挥作用。A(1)AR的这种抗肿瘤作用是通过肿瘤相关小胶质细胞介导的。激活A(2A)AR会通过抑制调节性T细胞功能以及抑制自然杀伤细胞的细胞毒性和肿瘤特异性CD4+/CD8+活性来抑制对肿瘤的免疫反应。因此,有人提出,用特异性拮抗剂对A(2A)AR激活进行药理抑制可能会增强癌症治疗中的免疫疗法。激活A(2B)AR通过上调微血管内皮细胞中血管生成因子的表达水平在肿瘤发生中起作用。相反,很明显激活A(2B)AR会抑制ERK1/2磷酸化和丝裂原活化蛋白激酶活性,而这些与肿瘤细胞生长信号有关。最后,人们发现A(3)AR在肿瘤细胞和组织中高表达,而在正常细胞或邻近组织中表达水平较低。肿瘤组织中的受体表达与疾病严重程度直接相关。肿瘤中高受体表达归因于NF-κB的过表达,已知NF-κB作为A(3)AR转录因子发挥作用。有趣的是,在来自荷瘤动物和癌症患者的外周血单核细胞(PBMCs)中发现了高A(3)AR表达水平,这反映了肿瘤中的受体状态。已发现A(3)AR激动剂在体外和体内均可通过调节Wnt和NF-κB信号通路诱导肿瘤生长抑制。综上所述,在肿瘤细胞中大量表达的A(3)ARs可能成为特异性A(3)AR激动剂的作用靶点,从而导致肿瘤生长抑制。这些A(3)AR激动剂的独特特性使其成为有吸引力的候选药物。
Zotero 插件