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通过选择性抑制支原体编码的分解代谢酶改善基于嘌呤和嘧啶抗代谢物的抗癌治疗。

Improvement of purine and pyrimidine antimetabolite-based anticancer treatment by selective suppression of mycoplasma-encoded catabolic enzymes.

作者信息

Liekens Sandra, Bronckaers Annelies, Balzarini Jan

机构信息

Rega Institute for Medical Research, K U Leuven, Leuven, Belgium.

出版信息

Lancet Oncol. 2009 Jun;10(6):628-35. doi: 10.1016/S1470-2045(09)70037-3.

Abstract

Most mycoplasmas are present as commensals, colonising the mucosa of our respiratory and gastrointestinal tract. Experimental data suggest that the long-term association of certain mycoplasma species with mammalian cells might favour host-cell transformation and malignancy. Moreover, increased mycoplasma infection has been noted in several cancers. Despite efforts to develop target-specific anticancer drugs, current cancer treatment still relies on the use of nucleobase or nucleoside-based analogues. Here, we provide experimental evidence that nucleoside-metabolising catabolic enzymes expressed by mycoplasmas substantially compromise the efficacy of nucleoside antimetabolites used in the treatment of cancer. We also suggest potential methods for improving future chemotherapy by suppressing mycoplasma-mediated catabolism of the anticancer nucleoside analogues.

摘要

大多数支原体以共生菌的形式存在,定殖于我们呼吸道和胃肠道的黏膜。实验数据表明,某些支原体物种与哺乳动物细胞的长期关联可能有利于宿主细胞转化和恶性肿瘤的发生。此外,在几种癌症中已观察到支原体感染增加。尽管人们努力开发靶向特异性抗癌药物,但目前的癌症治疗仍然依赖于使用基于核碱基或核苷的类似物。在此,我们提供实验证据表明,支原体表达的核苷代谢分解酶会严重损害用于癌症治疗的核苷抗代谢物的疗效。我们还提出了通过抑制支原体介导的抗癌核苷类似物分解代谢来改善未来化疗的潜在方法。

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