Vashisht Rohit, Bhat Ashwini G, Kushwaha Shreeram, Bhardwaj Anshu, Brahmachari Samir K
CSIR-Open Source Drug Discovery Unit, New Delhi, India.
J Transl Med. 2014 Oct 11;12:263. doi: 10.1186/s12967-014-0263-5.
The effectiveness of current therapeutic regimens for Mycobacterium tuberculosis (Mtb) is diminished by the need for prolonged therapy and the rise of drug resistant/tolerant strains. This global health threat, despite decades of basic research and a wealth of legacy knowledge, is due to a lack of systems level understanding that can innovate the process of fast acting and high efficacy drug discovery.
The enhanced functional annotations of the Mtb genome, which were previously obtained through a crowd sourcing approach was used to reconstruct the metabolic network of Mtb in a bottom up manner. We represent this information by developing a novel Systems Biology Spindle Map of Metabolism (SBSM) and comprehend its static and dynamic structure using various computational approaches based on simulation and design.
The reconstructed metabolism of Mtb encompasses 961 metabolites, involved in 1152 reactions catalyzed by 890 protein coding genes, organized into 50 pathways. By accounting for static and dynamic analysis of SBSM in Mtb we identified various critical proteins required for the growth and survival of bacteria. Further, we assessed the potential of these proteins as putative drug targets that are fast acting and less toxic. Further, we formulate a novel concept of metabolic persister genes (MPGs) and compared our predictions with published in vitro and in vivo experimental evidence. Through such analyses, we report for the first time that de novo biosynthesis of NAD may give rise to bacterial persistence in Mtb under conditions of metabolic stress induced by conventional anti-tuberculosis therapy. We propose such MPG's as potential combination of drug targets for existing antibiotics that can improve their efficacy and efficiency for drug tolerant bacteria.
The systems level framework formulated by us to identify potential non-toxic drug targets and strategies to circumvent the issue of bacterial persistence can substantially aid in the process of TB drug discovery and translational research.
当前用于治疗结核分枝杆菌(Mtb)的治疗方案的有效性因需要长期治疗以及耐药/耐受菌株的出现而降低。尽管经过了数十年的基础研究并积累了大量传统知识,但这种全球健康威胁仍然存在,原因是缺乏能够推动快速起效且高效药物发现过程的系统层面的理解。
先前通过众包方法获得的结核分枝杆菌基因组增强功能注释被用于自下而上地重建结核分枝杆菌的代谢网络。我们通过开发一种新颖的代谢系统生物学纺锤体图(SBSM)来呈现这些信息,并使用基于模拟和设计的各种计算方法来理解其静态和动态结构。
重建的结核分枝杆菌代谢涵盖961种代谢物,涉及由890个蛋白质编码基因催化的1152个反应,组织成50条途径。通过对结核分枝杆菌中SBSM的静态和动态分析,我们确定了细菌生长和存活所需的各种关键蛋白质。此外,我们评估了这些蛋白质作为快速起效且低毒的潜在药物靶点的潜力。此外,我们提出了代谢持留基因(MPG)的新概念,并将我们的预测与已发表的体外和体内实验证据进行了比较。通过此类分析,我们首次报告,在传统抗结核治疗诱导的代谢应激条件下,NAD的从头生物合成可能导致结核分枝杆菌中的细菌持留。我们提出将此类MPG作为现有抗生素潜在的联合药物靶点,以提高其对耐受药物细菌的疗效和效率。
我们制定的用于识别潜在无毒药物靶点以及规避细菌持留问题的策略的系统层面框架,可极大地有助于结核病药物发现和转化研究过程。
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