Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae

Streptococcus pneumoniae (S. pneumoniae), the major etiological agent of community-acquired pneumonia (CAP) contributes significantly to the global burden of infectious diseases which is getting resistant day by day. Nearly 30% of the S. pneumoniae genomes encode hypothetical proteins (HPs), and bet...

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Autores principales: Chowdhury, Zeshan Mahmud, Bhattacharjee, Arittra, Ahammad, Ishtiaque, Hossain, Mohammad Uzzal, Jaber, Abdullah All, Rahman, Anisur, Dev, Preonath Chondrow, Salimullah, Md., Keya, Chaman Ara
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9387852/
https://www.ncbi.nlm.nih.gov/pubmed/35980906
http://dx.doi.org/10.1371/journal.pone.0272945
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author Chowdhury, Zeshan Mahmud
Bhattacharjee, Arittra
Ahammad, Ishtiaque
Hossain, Mohammad Uzzal
Jaber, Abdullah All
Rahman, Anisur
Dev, Preonath Chondrow
Salimullah, Md.
Keya, Chaman Ara
author_facet Chowdhury, Zeshan Mahmud
Bhattacharjee, Arittra
Ahammad, Ishtiaque
Hossain, Mohammad Uzzal
Jaber, Abdullah All
Rahman, Anisur
Dev, Preonath Chondrow
Salimullah, Md.
Keya, Chaman Ara
author_sort Chowdhury, Zeshan Mahmud
collection PubMed
description Streptococcus pneumoniae (S. pneumoniae), the major etiological agent of community-acquired pneumonia (CAP) contributes significantly to the global burden of infectious diseases which is getting resistant day by day. Nearly 30% of the S. pneumoniae genomes encode hypothetical proteins (HPs), and better understandings of these HPs in virulence and pathogenicity plausibly decipher new treatments. Some of the HPs are present across many Streptococcus species, systematic assessment of these unexplored HPs will disclose prospective drug targets. In this study, through a stringent bioinformatics analysis of the core genome and proteome of S. pneumoniae PCS8235, we identified and analyzed 28 HPs that are common in many Streptococcus species and might have a potential role in the virulence or pathogenesis of the bacteria. Functional annotations of the proteins were conducted based on the physicochemical properties, subcellular localization, virulence prediction, protein-protein interactions, and identification of essential genes, to find potentially druggable proteins among 28 HPs. The majority of the HPs are involved in bacterial transcription and translation. Besides, some of them were homologs of enzymes, binding proteins, transporters, and regulators. Protein-protein interactions revealed HP PCS8235_RS05845 made the highest interactions with other HPs and also has TRP structural motif along with virulent and pathogenic properties indicating it has critical cellular functions and might go under unconventional protein secretions. The second highest interacting protein HP PCS8235_RS02595 interacts with the Regulator of chromosomal segregation (RocS) which participates in chromosome segregation and nucleoid protection in S. pneumoniae. In this interacting network, 54% of protein members have virulent properties and 40% contain pathogenic properties. Among them, most of these proteins circulate in the cytoplasmic area and have hydrophilic properties. Finally, molecular docking and dynamics simulation demonstrated that the antimalarial drug Artenimol can act as a drug repurposing candidate against HP PCS8235_RS 04650 of S. pneumoniae. Hence, the present study could aid in drugs against S. pneumoniae.
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spelling pubmed-93878522022-08-19 Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae Chowdhury, Zeshan Mahmud Bhattacharjee, Arittra Ahammad, Ishtiaque Hossain, Mohammad Uzzal Jaber, Abdullah All Rahman, Anisur Dev, Preonath Chondrow Salimullah, Md. Keya, Chaman Ara PLoS One Research Article Streptococcus pneumoniae (S. pneumoniae), the major etiological agent of community-acquired pneumonia (CAP) contributes significantly to the global burden of infectious diseases which is getting resistant day by day. Nearly 30% of the S. pneumoniae genomes encode hypothetical proteins (HPs), and better understandings of these HPs in virulence and pathogenicity plausibly decipher new treatments. Some of the HPs are present across many Streptococcus species, systematic assessment of these unexplored HPs will disclose prospective drug targets. In this study, through a stringent bioinformatics analysis of the core genome and proteome of S. pneumoniae PCS8235, we identified and analyzed 28 HPs that are common in many Streptococcus species and might have a potential role in the virulence or pathogenesis of the bacteria. Functional annotations of the proteins were conducted based on the physicochemical properties, subcellular localization, virulence prediction, protein-protein interactions, and identification of essential genes, to find potentially druggable proteins among 28 HPs. The majority of the HPs are involved in bacterial transcription and translation. Besides, some of them were homologs of enzymes, binding proteins, transporters, and regulators. Protein-protein interactions revealed HP PCS8235_RS05845 made the highest interactions with other HPs and also has TRP structural motif along with virulent and pathogenic properties indicating it has critical cellular functions and might go under unconventional protein secretions. The second highest interacting protein HP PCS8235_RS02595 interacts with the Regulator of chromosomal segregation (RocS) which participates in chromosome segregation and nucleoid protection in S. pneumoniae. In this interacting network, 54% of protein members have virulent properties and 40% contain pathogenic properties. Among them, most of these proteins circulate in the cytoplasmic area and have hydrophilic properties. Finally, molecular docking and dynamics simulation demonstrated that the antimalarial drug Artenimol can act as a drug repurposing candidate against HP PCS8235_RS 04650 of S. pneumoniae. Hence, the present study could aid in drugs against S. pneumoniae. Public Library of Science 2022-08-18 /pmc/articles/PMC9387852/ /pubmed/35980906 http://dx.doi.org/10.1371/journal.pone.0272945 Text en © 2022 Chowdhury et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Chowdhury, Zeshan Mahmud
Bhattacharjee, Arittra
Ahammad, Ishtiaque
Hossain, Mohammad Uzzal
Jaber, Abdullah All
Rahman, Anisur
Dev, Preonath Chondrow
Salimullah, Md.
Keya, Chaman Ara
Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae
title Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae
title_full Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae
title_fullStr Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae
title_full_unstemmed Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae
title_short Exploration of Streptococcus core genome to reveal druggable targets and novel therapeutics against S. pneumoniae
title_sort exploration of streptococcus core genome to reveal druggable targets and novel therapeutics against s. pneumoniae
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9387852/
https://www.ncbi.nlm.nih.gov/pubmed/35980906
http://dx.doi.org/10.1371/journal.pone.0272945
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