Elucidating the resistance mechanisms and binding pattern of novel Oxa-48-like carbapenemases covalent inhibitors: A hybrid experimental and in silico approach
•The isolates were resistant to SXT, AMP, FEP CTX, CIP, TET, MEM, and IPM, while effective antibiotics were TGC, FOS, FOX, SCF and TZP.•The sequencing and mutational analysis of the OXA-48 gene revealed 45-point mutations.•Five novel missense mutations (Thr104:Ala104, Asn110:Asp110, Glu168:Gln168, S...
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Published in | Journal of molecular structure Vol. 1321; p. 140073 |
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Main Authors | , , , , , , , , , , , |
Format | Journal Article |
Language | English |
Published |
Elsevier B.V
05.02.2025
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Subjects | |
Online Access | Get full text |
ISSN | 0022-2860 |
DOI | 10.1016/j.molstruc.2024.140073 |
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Abstract | •The isolates were resistant to SXT, AMP, FEP CTX, CIP, TET, MEM, and IPM, while effective antibiotics were TGC, FOS, FOX, SCF and TZP.•The sequencing and mutational analysis of the OXA-48 gene revealed 45-point mutations.•Five novel missense mutations (Thr104:Ala104, Asn110:Asp110, Glu168:Gln168, Ser171:Ala171 and Arg214:Ser214).•These mutations can contribute to the antibiotic affinity decrease and cause resistance.•10 compounds (ZINC103533306, ZINC103531564, ZINC3861001, ZINC103533375, ZINC12411532, ZINC103533290, ZINC12376465, ZINC85875819, ZINC59586513 and ZINC13370550) showed best fit and high interactions with the OXA-48 active pocket.
Klebsiella pneumoniae is a Gram negative bacteria that can cause harm to the public's health and vulnerability has increased due to the emergence of highly virulent strains resistant to carbapenem antibiotics. The K. pneumoniae resistance mechanism involves extended-spectrum beta-lactamases, which are enzymes that can break down a broad range of antibiotics. The particular concern is Class D β-lactamases like OXA-48, which further complicates treatment options for infections caused by K. pneumoniae. The current study screened 7800 samples from three hospitals in Pakistan and found 353 positive samples of K. pneumoniae. The isolates were resistant to SXT, AMP, FEP CTX, CIP, TET, MEM, and IPM, while effective antibiotics were TGC, FOS, FOX, SCF and TZP. The sequencing and mutational analysis of the OXA-48 gene revealed 45-point mutations, including five novel missense mutations (Thr104:Ala104, Asn110:Asp110, Glu168:Gln168, Ser171:Ala171 and Arg214:Ser214). These mutations can contribute to the antibiotic affinity decrease and cause resistance. Furthermore, the study aimed to develop covalent inhibitors of OXA-48 (wild type and mutant) carbapenemases using a combination of molecular docking and molecular dynamic (MD) simulation approaches from natural products from the ZNINC20 database. 10 compounds (ZINC103533306, ZINC103531564, ZINC3861001, ZINC103533375, ZINC12411532, ZINC103533290, ZINC12376465, ZINC85875819, ZINC59586513 and ZINC13370550) showed best fit and high interactions with the OXA-48 active pocket. The binding free energies calculated from the MD showed that these compounds have high affinity with both the wild type and mutated OXA-48 protein. The selected compounds showed good drug-like properties and can be the leading inhibitors to combat the resistant K. pneumoniae strains. |
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AbstractList | •The isolates were resistant to SXT, AMP, FEP CTX, CIP, TET, MEM, and IPM, while effective antibiotics were TGC, FOS, FOX, SCF and TZP.•The sequencing and mutational analysis of the OXA-48 gene revealed 45-point mutations.•Five novel missense mutations (Thr104:Ala104, Asn110:Asp110, Glu168:Gln168, Ser171:Ala171 and Arg214:Ser214).•These mutations can contribute to the antibiotic affinity decrease and cause resistance.•10 compounds (ZINC103533306, ZINC103531564, ZINC3861001, ZINC103533375, ZINC12411532, ZINC103533290, ZINC12376465, ZINC85875819, ZINC59586513 and ZINC13370550) showed best fit and high interactions with the OXA-48 active pocket.
Klebsiella pneumoniae is a Gram negative bacteria that can cause harm to the public's health and vulnerability has increased due to the emergence of highly virulent strains resistant to carbapenem antibiotics. The K. pneumoniae resistance mechanism involves extended-spectrum beta-lactamases, which are enzymes that can break down a broad range of antibiotics. The particular concern is Class D β-lactamases like OXA-48, which further complicates treatment options for infections caused by K. pneumoniae. The current study screened 7800 samples from three hospitals in Pakistan and found 353 positive samples of K. pneumoniae. The isolates were resistant to SXT, AMP, FEP CTX, CIP, TET, MEM, and IPM, while effective antibiotics were TGC, FOS, FOX, SCF and TZP. The sequencing and mutational analysis of the OXA-48 gene revealed 45-point mutations, including five novel missense mutations (Thr104:Ala104, Asn110:Asp110, Glu168:Gln168, Ser171:Ala171 and Arg214:Ser214). These mutations can contribute to the antibiotic affinity decrease and cause resistance. Furthermore, the study aimed to develop covalent inhibitors of OXA-48 (wild type and mutant) carbapenemases using a combination of molecular docking and molecular dynamic (MD) simulation approaches from natural products from the ZNINC20 database. 10 compounds (ZINC103533306, ZINC103531564, ZINC3861001, ZINC103533375, ZINC12411532, ZINC103533290, ZINC12376465, ZINC85875819, ZINC59586513 and ZINC13370550) showed best fit and high interactions with the OXA-48 active pocket. The binding free energies calculated from the MD showed that these compounds have high affinity with both the wild type and mutated OXA-48 protein. The selected compounds showed good drug-like properties and can be the leading inhibitors to combat the resistant K. pneumoniae strains. |
ArticleNumber | 140073 |
Author | Wei, Dong-Qing Albekairi, Norah A. Absar, Muhammad Alshammari, Abdulrahman Khan, Ibrar Rehman, Noor Sehra, Gul e Ahmad, Sajjad Ali, Amjad Azam, Sadiq Ullah, Asad Waqas, Muhammad |
Author_xml | – sequence: 1 givenname: Gul e surname: Sehra fullname: Sehra, Gul e email: Gulesehramujib@uop.edu.pk organization: Centre of Biotechnology & Microbiology, University of Peshawar, Khyber Pakhtunkhwa, Pakistan – sequence: 2 givenname: Sadiq surname: Azam fullname: Azam, Sadiq email: drazam@uop.edu.pk organization: Centre of Biotechnology & Microbiology, University of Peshawar, Khyber Pakhtunkhwa, Pakistan – sequence: 3 givenname: Sajjad surname: Ahmad fullname: Ahmad, Sajjad email: sajjad.ahmad@abasyn.edu.pk organization: Department of Health and Biological Sciences, Abasyn University, Peshawar, Pakistan – sequence: 4 givenname: Amjad surname: Ali fullname: Ali, Amjad organization: Department of Biotechnology and Genetic Engineering, Hazara University Mansehra, Mansehra 2100, Pakistan – sequence: 5 givenname: Ibrar surname: Khan fullname: Khan, Ibrar email: ibrarkhan1984@uop.edu.pk organization: Centre of Biotechnology & Microbiology, University of Peshawar, Khyber Pakhtunkhwa, Pakistan – sequence: 6 givenname: Asad surname: Ullah fullname: Ullah, Asad organization: Centre of Biotechnology & Microbiology, University of Peshawar, Khyber Pakhtunkhwa, Pakistan – sequence: 7 givenname: Muhammad orcidid: 0000-0001-6115-9689 surname: Waqas fullname: Waqas, Muhammad organization: Department of Biotechnology and Genetic Engineering, Hazara University Mansehra, Mansehra 2100, Pakistan – sequence: 8 givenname: Noor surname: Rehman fullname: Rehman, Noor organization: Department of Pathology, Khyber Teaching Hospital, Peshawar, Khyber Pakhtunkhwa, Pakistan – sequence: 9 givenname: Muhammad surname: Absar fullname: Absar, Muhammad organization: Department of Microbiology and Parasitology, school of Medical Sciences, University Sain Malaysia, Kubang Kerian 16150, Malaysia – sequence: 10 givenname: Abdulrahman surname: Alshammari fullname: Alshammari, Abdulrahman email: abdalshammari@ksu.edu.sa organization: Department of Pharmacology and Toxicology, College of Pharmacy, King Saud University, Post Box 2455, Riyadh, 11451, Saudi Arabia – sequence: 11 givenname: Norah A. surname: Albekairi fullname: Albekairi, Norah A. email: nalbekairi@ksu.edu.sa organization: Department of Pharmacology and Toxicology, College of Pharmacy, King Saud University, Post Box 2455, Riyadh, 11451, Saudi Arabia – sequence: 12 givenname: Dong-Qing orcidid: 0000-0003-4200-7502 surname: Wei fullname: Wei, Dong-Qing email: dqwei@sjtu.edu.cn organization: State Key Laboratory of Microbial Metabolism, Joint International Research Laboratory of Metabolic & Developmental Sciences and School of Life Sciences and Biotechnology, Shanghai Jiao Tong University, Shanghai 200030, PR China |
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Keywords | β-lactamases Molecular dynamic simulations OXA-48 Drug resistance Klebsiella pneumoniae |
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SubjectTerms | Drug resistance Klebsiella pneumoniae Molecular dynamic simulations OXA-48 β-lactamases |
Title | Elucidating the resistance mechanisms and binding pattern of novel Oxa-48-like carbapenemases covalent inhibitors: A hybrid experimental and in silico approach |
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