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Focusing on DNA Repair and Damage Tolerance Mechanisms in Mycobacterium tuberculosis: An Emerging Therapeutic Theme

机译:专注于结核分枝杆菌的DNA修复和损伤耐受机制:新兴的治疗题材

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Tuberculosis (TB) is one such disease that has become a nuisance in the world scenario and one of the most deadly diseases of the current times. The etiological agent of tuberculosis, Mycobacterium tuberculosis (M. tb) kills millions of people each year. Not only 1.7 million people worldwide are estimated to harbor M. tb in the latent form but also 5 to 15 percent of which are expected to acquire an infection during a lifetime. Though curable, a long duration of drug regimen and expense leads to low patient adherence. The emergence of multi-, extensive- and total- drug-resistant strains of M. tb further complicates the situation. Owing to high TB burden, scientists worldwide are trying to design novel therapeutics to combat this disease. Therefore, to identify new drug targets, there is a growing interest in targeting DNA repair pathways to fight this infection. Thus, this review aims to explore DNA repair and damage tolerance as an efficient target for drug development by understanding M. tb DNA repair and tolerance machinery and its regulation, its role in pathogenesis and survival, mutagenesis, and consequently, in the development of drug resistance.
机译:结核病(TB)是一种这种疾病,它在世界情景中成为滋扰,当前最致命的疾病之一。结核病的病因,结核分枝杆菌(TB)每年杀死数百万人。估计全球170万人估计为潜在的潜在形式,其中5%至15%,预计将在一生中获得感染。虽然可固化,但长期的药物方案和费用导致低患者的粘附。 M. TB的多,广泛和全毒性抗药菌株的出现进一步复杂化了情况。由于TB负担高,全世界科学家正试图设计新的治疗方法来打击这种疾病。因此,为了鉴定新的药物靶标,对靶向DNA修复途径产生越来越感兴趣以对抗这种感染。因此,本综述旨在通过了解M.TB DNA修复和耐受机械及其调节,探讨DNA修复和损害耐受性作为药物开发的有效目标及其调节,其在发病机制和生存,诱变,诱变中,在药物的发育中反抗。

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