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Targeting Polyamines and Inflammation for Cancer Prevention

机译:针对多胺和炎症进行癌症预防

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Increased polyamine synthesis and inflammation have long been associated with intraepithelial neoplasia, which are risk factors for cancer development in humans. Targeting polyamine metabolism (by use of polyamine synthesis inhibitors or polyamine catabolism activators) and inflammation (by use of nonsteroidal anti-inflammatory drugs) has been studied for many cancers, including colon, prostate, and skin. Genetic epidemiology results indicate that a genetic variant associated with the expression of a polyamine biosynthetic gene is associated with risk of colon and prostate cancers. A clinical trial of difluoromethylomithine (DFMO), a selective inhibitor of polyamine synthesis, showed that the 1 year treatment duration reduced prostate volume and serum prostate-specific antigen doubling time in men with a family history of prostate cancer. A second, clinical trial of DFMO in combination with sulindac, a NSAID in patients with prior colon polyps found that the 3-year treatment was associated with a 70% reduction of all, and over a 90% reduction of advanced and/or multiple metachronous colon adenomas. In this chapter, we discuss that similar combination prevention strategies of targeting polyatnines and inflammation can be effective in reducing risk factors associated with the development of human cancers.
机译:增加的多胺合成和炎症长期与上皮内瘤形成有关,这是人类癌症发育的危险因素。针对多胺代谢(通过使用多胺合成抑制剂或多胺分解代谢活化剂)和炎症(通过使用非甾体类抗炎药)已经研究了许多癌症,包括结肠,前列腺和皮肤。遗传流行病学结果表明,与多胺生物合成基因的表达相关的遗传变异与结肠癌和前列腺癌的风险有关。二氟甲基二氯胺(DFMO)的临床试验,一种多胺合成的选择性抑制剂,表明,1年治疗持续时间降低了前列腺体积和血清前列腺特异性抗原倍增时间,具有前列腺癌的家族史。第二种临床试验与苏林加相结合的,患有先前结肠息肉的NSAID的NSAID发现,3年治疗与均外的70%递减为70%,高达90%的高度和/或多种同学减少结肠腺瘤。在本章中,我们讨论了靶向聚列和炎症的类似组合预防策略可有效降低与人类癌症的发展相关的危险因素。

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