Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum

India confines more than 17% of the world’s population and has a diverse genetic makeup with several clinically relevant rare mutations belonging to many sub-group which are undervalued in global sequencing datasets like the 1000 Genome data (1KG) containing limited samples for Indian ethnicity. Suc...

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Autores principales: Panda, Gayatri, Mishra, Neha, Sharma, Disha, Kutum, Rintu, Bhoyar, Rahul C., Jain, Abhinav, Imran, Mohamed, Senthilvel, Vigneshwar, Divakar, Mohit Kumar, Mishra, Anushree, Garg, Parth, Banerjee, Priyanka, Sivasubbu, Sridhar, Scaria, Vinod, Ray, Arjun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9294532/
https://www.ncbi.nlm.nih.gov/pubmed/35865963
http://dx.doi.org/10.3389/fphar.2022.858345
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author Panda, Gayatri
Mishra, Neha
Sharma, Disha
Kutum, Rintu
Bhoyar, Rahul C.
Jain, Abhinav
Imran, Mohamed
Senthilvel, Vigneshwar
Divakar, Mohit Kumar
Mishra, Anushree
Garg, Parth
Banerjee, Priyanka
Sivasubbu, Sridhar
Scaria, Vinod
Ray, Arjun
author_facet Panda, Gayatri
Mishra, Neha
Sharma, Disha
Kutum, Rintu
Bhoyar, Rahul C.
Jain, Abhinav
Imran, Mohamed
Senthilvel, Vigneshwar
Divakar, Mohit Kumar
Mishra, Anushree
Garg, Parth
Banerjee, Priyanka
Sivasubbu, Sridhar
Scaria, Vinod
Ray, Arjun
author_sort Panda, Gayatri
collection PubMed
description India confines more than 17% of the world’s population and has a diverse genetic makeup with several clinically relevant rare mutations belonging to many sub-group which are undervalued in global sequencing datasets like the 1000 Genome data (1KG) containing limited samples for Indian ethnicity. Such databases are critical for the pharmaceutical and drug development industry where diversity plays a crucial role in identifying genetic disposition towards adverse drug reactions. A qualitative and comparative sequence and structural study utilizing variant information present in the recently published, largest curated Indian genome database (IndiGen) and the 1000 Genome data was performed for variants belonging to the kinase coding genes, the second most targeted group of drug targets. The sequence-level analysis identified similarities and differences among different populations based on the nsSNVs and amino acid exchange frequencies whereas a comparative structural analysis of IndiGen variants was performed with pathogenic variants reported in UniProtKB Humsavar data. The influence of these variations on structural features of the protein, such as structural stability, solvent accessibility, hydrophobicity, and the hydrogen-bond network was investigated. In-silico screening of the known drugs to these Indian variation-containing proteins reveals critical differences imparted in the strength of binding due to the variations present in the Indian population. In conclusion, this study constitutes a comprehensive investigation into the understanding of common variations present in the second largest population in the world and investigating its implications in the sequence, structural and pharmacogenomic landscape. The preliminary investigation reported in this paper, supporting the screening and detection of ADRs specific to the Indian population could aid in the development of techniques for pre-clinical and post-market screening of drug-related adverse events in the Indian population.
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spelling pubmed-92945322022-07-20 Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum Panda, Gayatri Mishra, Neha Sharma, Disha Kutum, Rintu Bhoyar, Rahul C. Jain, Abhinav Imran, Mohamed Senthilvel, Vigneshwar Divakar, Mohit Kumar Mishra, Anushree Garg, Parth Banerjee, Priyanka Sivasubbu, Sridhar Scaria, Vinod Ray, Arjun Front Pharmacol Pharmacology India confines more than 17% of the world’s population and has a diverse genetic makeup with several clinically relevant rare mutations belonging to many sub-group which are undervalued in global sequencing datasets like the 1000 Genome data (1KG) containing limited samples for Indian ethnicity. Such databases are critical for the pharmaceutical and drug development industry where diversity plays a crucial role in identifying genetic disposition towards adverse drug reactions. A qualitative and comparative sequence and structural study utilizing variant information present in the recently published, largest curated Indian genome database (IndiGen) and the 1000 Genome data was performed for variants belonging to the kinase coding genes, the second most targeted group of drug targets. The sequence-level analysis identified similarities and differences among different populations based on the nsSNVs and amino acid exchange frequencies whereas a comparative structural analysis of IndiGen variants was performed with pathogenic variants reported in UniProtKB Humsavar data. The influence of these variations on structural features of the protein, such as structural stability, solvent accessibility, hydrophobicity, and the hydrogen-bond network was investigated. In-silico screening of the known drugs to these Indian variation-containing proteins reveals critical differences imparted in the strength of binding due to the variations present in the Indian population. In conclusion, this study constitutes a comprehensive investigation into the understanding of common variations present in the second largest population in the world and investigating its implications in the sequence, structural and pharmacogenomic landscape. The preliminary investigation reported in this paper, supporting the screening and detection of ADRs specific to the Indian population could aid in the development of techniques for pre-clinical and post-market screening of drug-related adverse events in the Indian population. Frontiers Media S.A. 2022-07-05 /pmc/articles/PMC9294532/ /pubmed/35865963 http://dx.doi.org/10.3389/fphar.2022.858345 Text en Copyright © 2022 Panda, Mishra, Sharma, Kutum, Bhoyar, Jain, Imran, Senthilvel, Divakar, Mishra, Garg, Banerjee, Sivasubbu, Scaria and Ray. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Panda, Gayatri
Mishra, Neha
Sharma, Disha
Kutum, Rintu
Bhoyar, Rahul C.
Jain, Abhinav
Imran, Mohamed
Senthilvel, Vigneshwar
Divakar, Mohit Kumar
Mishra, Anushree
Garg, Parth
Banerjee, Priyanka
Sivasubbu, Sridhar
Scaria, Vinod
Ray, Arjun
Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum
title Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum
title_full Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum
title_fullStr Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum
title_full_unstemmed Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum
title_short Comprehensive Assessment of Indian Variations in the Druggable Kinome Landscape Highlights Distinct Insights at the Sequence, Structure and Pharmacogenomic Stratum
title_sort comprehensive assessment of indian variations in the druggable kinome landscape highlights distinct insights at the sequence, structure and pharmacogenomic stratum
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9294532/
https://www.ncbi.nlm.nih.gov/pubmed/35865963
http://dx.doi.org/10.3389/fphar.2022.858345
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