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Hydrolysis of 2′3′-cGAMP by ENPP 1 and design of nonhydrolyzable analogs

机译:ENPP 1水解2'3'-cGAMP的方法及不可水解类似物的设计

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Agonists of mouse STING (TMEM173) shrink and even cure solid tumors by activating innate immunity; human STING (hSTING) agonists are needed to test this therapeutic hypothesis in humans. The endogenous STING agonist is 2′3′-cGAMP, a second messenger that signals the presence of cytosolic double-stranded DNA. We report activity-guided partial purification and identification of ecto-nucleotide pyrophosphatase/phosphodiesterase (ENPP1) to be the dominant 2′3′-cGAMP hydrolyzing activity in cultured cells. The hydrolysis activity of ENPP1 was confirmed using recombinant protein and was depleted in tissue extracts and plasma from Enpp1~(?/?) mice. We synthesized a hydrolysis-resistant bisphosphothioate analog of 2′3′-cGAMP (2′3′-cG~sA~sMP) that has similar affinity for hSTING in vitro and is ten times more potent at inducing IFN-β secretion from human THP1 monocytes. Studies in mouse Enpp1~(?/?) lung fibroblasts indicate that resistance to hydrolysis contributes substantially to its higher potency. 2′3′-cGsAsMP is therefore improved over natural 2′3′-cGAMP as a model agonist and has potential as a vaccine adjuvant and cancer therapeutic.
机译:小鼠STING(TMEM173)激动剂可通过激活先天免疫来缩小甚至治愈实体瘤。需要人类STING(hSTING)激动剂来测试人类的这种治疗假设。内源性STING激动剂是2'3'-cGAMP,这是一个第二种信使,它指示细胞质双链DNA的存在。我们报告了活动指导的局部纯化和外切核苷酸焦磷酸酶/磷酸二酯酶(ENPP1)的鉴定是在培养细胞中占主导地位的2'3'-cGAMP水解活性。用重组蛋白证实了ENPP1的水解活性,并在Enpp1〜(β/β)小鼠的组织提取物和血浆中被消耗掉了。我们合成了2'3'-cGAMP(2'3'-cG〜sA〜sMP)的抗水解双硫代磷酸酯类似物,该类似物在体外对hSTING具有相似的亲和力,并且在诱导人THP1分泌IFN-β方面的功效是其的十倍。单核细胞。对小鼠Enpp1〜(α/β)肺成纤维细胞的研究表明,对水解的抗性实质上有助于其更高的效力。因此,作为模型激动剂,与天然2'3'-cGAMP相比,2'3'-cGsAsMP得到了改善,并具有作为疫苗佐剂和癌症治疗剂的潜力。

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