Deciphering the Structural Requirements of Nucleoside Bisubstrate Analogues for Inhibition of MbtA in Mycobacterium tuberculosis: A FB‐QSAR Study and Combinatorial Library Generation for Identifying Potential Hits

Maganti, Lakshmi; Das, Sanjit; Mascarenhas, Nahren Manuel; Ghoshal, Nanda

doi:10.1002/minf.201100056

Molecular Informatics

2011

DOI: 10.1002/minf.201100056

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Deciphering the Structural Requirements of Nucleoside Bisubstrate Analogues for Inhibition of MbtA in Mycobacterium tuberculosis: A FB‐QSAR Study and Combinatorial Library Generation for Identifying Potential Hits

Lakshmi Maganti

Sanjit Das

Nahren Manuel Mascarenhas

et al.

Abstract: The re-emergence of tuberculosis infections, which are resistant to conventional drug therapy, has steadily risen in the last decade. Inhibitors of aryl acid adenylating enzyme known as MbtA, involved in siderophore biosynthesis in Mycobacterium tuberculosis, are being explored as potential antitubercular agents. The ability to identify fragments that interact with a biological target is a key step in fragment based drug design (FBDD). To expand the boundaries of quantitative structure activity relationship (Q… Show more

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Cited by 3 publications

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“…There are also some other 2D-fragment-based QSAR methods, including Hologram QSAR (HQSAR), fragment-similarity based QSAR (FS-QSAR) and so on. Therefore, 2D fragment-based QSAR has been widely used as an important measure in fragment-based drug design 32 .…”

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confidence: 99%

Trend of Multi-Scale QSAR in Drug Design

Qiao¹,

Cai²,

He³

et al. 2014

Asian J. Chem.

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Quantitative structure-activity relationship (QSAR) indicates the relationship between structural property and biological activity of compounds, which are widely used in the field of pharmacy, materials science, agronomy, environment, etc. 1,2. The basic construction procedures of QSAR model include four important steps.Firstly, as the structural description of the training set compounds is recorded, this structural information and relative biological activity are used to construct correlation function model by suitable algorithm. Afterwards, statistical methods are applied for internal validation of the model. Finally, the test set is used for external test of the model. Reliable QSAR model should be satisfied with the requirement of internal validation and external validation 3,4. The main purpose of QSAR model is to predict the activity of compounds, guide compound design and optimize leads. Classification of QSAR methodologies: Different classification methods of QSAR were presented to make the study more reliable and credible. The two main methods, introduced as following, have been widely accepted by QSAR researchers.

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mentioning

confidence: 99%

Trend of Multi-Scale QSAR in Drug Design

Qiao¹,

Cai²,

He³

et al. 2014

Asian J. Chem.

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Quantitative Structure–Activity/Property Relationships: The Ubiquitous Links between Cause and Effect

et al. 2012

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Current literature demonstrates that almost every area of chemical and life sciences, as well as technology utilizes quantitative structure‐activity/property relationships (QSAR/QSPR) to accelerate development and increase efficiency. The designs of pharmaceuticals, agrichemicals, and consumer products as well as the assessment of their toxicity and environmental impact have become major areas of application QSAR/QSPR; the methods of which also penetrate into relatively new applications such as materials science and nanotechnology. In terms of methodology development the new trend is the integration of QSAR/QSPR with adjacent computational methods such as virtual screening and molecular dynamics. Such synergy offers unique opportunities and heralds a new era of computer‐aided molecular design.

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3D-QSAR studies and shape based virtual screening for identification of novel hits to inhibit MbtA inMycobacterium tuberculosis

Maganti

Ghoshal

2014

Journal of Biomolecular Structure and Dynamics

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Mycobacterium tuberculosis, the pathogen responsible for tuberculosis, uses various strategies to survive in a variety of host lesions. The re-emergence of multi-drug-resistant strains of M. tuberculosis underlines the necessity to discover new molecules. Inhibitors of aryl acid adenylating enzyme, MbtA, involved in siderophore biosynthesis in M. tuberculosis, are being explored as potential anti tubercular agents. In this study, we have used 3D-QSAR models and shape based virtual screening to identify novel MbtA inhibitors. 3D-QSAR studies were carried out on nucleoside bisubstrate derivatives. Both Comparative Molecular Field Analysis (r(2) = .944 and r(2)(pred) = .938) and Comparative Molecular Similarity Indices Analysis (r(2) = .892 and r(2)(pred) = .842) models, developed using Gasteiger charges with all fields, predicted efficiently. A total of 13 hits were identified as novel prospective inhibitors for MbtA by utilizing an insilico workflow. Out of 13 hits, five top ranked hits were used for further molecular dynamics studies to gain more insights about the stability of the complexes.

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Deciphering the Structural Requirements of Nucleoside Bisubstrate Analogues for Inhibition of MbtA in Mycobacterium tuberculosis: A FB‐QSAR Study and Combinatorial Library Generation for Identifying Potential Hits

Cited by 3 publications

References 45 publications

Trend of Multi-Scale QSAR in Drug Design

Trend of Multi-Scale QSAR in Drug Design

Quantitative Structure–Activity/Property Relationships: The Ubiquitous Links between Cause and Effect

3D-QSAR studies and shape based virtual screening for identification of novel hits to inhibit MbtA inMycobacterium tuberculosis

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