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Recent advances towards identification of new drug targets for Mycobacterium tuberculosis.

机译:鉴定结核分枝杆菌新药靶标的最新进展。

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摘要

Mycobacterium tuberculosis is a very successful pathogen that remains a leading infectious killer worldwide. The global situation has become precarious due to various factors such as the variable efficacy of the Bacille Calmette-Guerin (BCG) vaccine, drug resistance, delay in diagnosis, association with HIV, and other factors, creating a long-lasting reservoir of impending disease and infection. Surprisingly, no new drugs have been developed in the past 30 years. The release of the complete genome sequence of M. tuberculosis and the availability of advanced genetic tools have provided the powerful repertoire of potential drug targets that are now in hand and can be explored in a more rational and directional manner. In this review, the authors highlight some possible therapeutic targets in M. tuberculosis. The gene products involved in various processes, such as mycobacterial cell wall synthesis, ability to acquire or obtain essential nutrients, persistence, transcription regulation, energy metabolism and others, such as the PE-PGRS family and culture filtrate proteins, would be potential targets for the development of new drugs. Apart from these categories, the importance of signal transduction events in the virulence of mycobacteria is discussed in relation to their potential as therapeutic targets. The potential of all of these therapeutic targets should be investigated together with the potential of being able to synthesise future chemotherapeutic agents.
机译:结核分枝杆菌是一种非常成功的病原体,仍然是全球领先的传染性杀手。由于各种因素(例如,Bacille Calmette-Guerin(BCG)疫苗的疗效不一,耐药性,诊断延误,与HIV的关联以及其他因素),全球局势变得不稳定。和感染。令人惊讶的是,在过去的30年中没有开发出新药。结核分枝杆菌的完整基因组序列的释放和先进遗传工具的提供,提供了潜在药物靶标的强大功能库,这些药物靶标现在已经可以使用,可以以更合理和更具指导性的方式进行探索。在这篇综述中,作者强调了结核分枝杆菌的一些可能的治疗靶标。涉及各种过程的基因产物,例如分枝杆菌细胞壁的合成,获得或获得必需营养素的能力,持久性,转录调节,能量代谢以及诸如PE-PGRS家族和培养滤液蛋白等其他方面,将成为潜在的靶标。开发新药。除这些类别外,还讨论了信号转导事件在分枝杆菌毒力中的重要性及其作为治疗靶标的潜力。应该研究所有这些治疗靶标的潜力以及能够合成未来化学治疗剂的潜力。

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