Structural and free energy landscape of novel mutations in ribosomal protein S1 (rpsA) associated with pyrazinamide resistance

Structural and free energy landscape of novel mutations in ribosomal protein S1 (rpsA) associated with pyrazinamide resistance

Resistance to key first-line drugs is a major hurdle to achieve the global end tuberculosis (TB) targets. A prodrug, pyrazinamide (PZA) is the only drug, effective in latent TB, recommended in drug resistance and susceptible Mycobacterium tuberculosis (MTB) isolates. The prodrug conversion into acti...

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Veröffentlicht in:Scientific reports 2019-05, Vol.9 (1), p.7482-7482, Article 7482
Hauptverfasser: Khan, Muhammad Tahir, Khan, Abbas, Rehman, Ashfaq Ur, Wang, Yanjie, Akhtar, Khalid, Malik, Shaukat Iqbal, Wei, Dong-Qing
Format: Artikel
Sprache:eng
Schlagworte:
119/118
45/23
45/70
631/114/2397
692/699/255/1318
Amidohydrolases - chemistry
Amidohydrolases - genetics
Amidohydrolases - metabolism
Antitubercular Agents - chemistry
Antitubercular Agents - pharmacology
Binding Sites
Drug resistance
Drug Resistance, Bacterial
Free energy
Genes
Humanities and Social Sciences
Molecular Docking Simulation
multidisciplinary
Mutation
PncA gene
Protein Binding
Protein folding
Proteins
Pyrazinamide
Pyrazinamide - chemistry
Pyrazinamide - pharmacology
Ribosomal protein S1
Ribosomal Proteins - chemistry
Ribosomal Proteins - genetics
Ribosomal Proteins - metabolism
Science
Science (multidisciplinary)
Tuberculosis
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Zusammenfassung:Resistance to key first-line drugs is a major hurdle to achieve the global end tuberculosis (TB) targets. A prodrug, pyrazinamide (PZA) is the only drug, effective in latent TB, recommended in drug resistance and susceptible Mycobacterium tuberculosis (MTB) isolates. The prodrug conversion into active form, pyrazinoic acid (POA), required the activity of pncA gene encoded pyrazinamidase (PZase). Although pncA mutations have been commonly associated with PZA resistance but a small number of resistance cases have been associated with mutationss in RpsA protein. Here in this study a total of 69 PZA resistance isolates have been sequenced for pncA mutations. However, samples that were found PZA resistant but pncA wild type ( pncA WT ), have been sequenced for rpsA and panD genes mutation. We repeated a drug susceptibility testing according to the WHO guidelines on 18 pncA WT MTB isolates. The rpsA and panD genes were sequenced. Out of total 69 PZA resistant isolates, 51 harbored 36 mutations in pncA gene (GeneBank Accession No. MH46111) while, fifteen different mutations including seven novel, were detected in the fourth S1 domain of RpsA known as C-terminal (MtRpsA CTD ) end. We did not detect any mutations in panD gene. Among the rpsA mutations, we investigated the molecular mechanism of resistance behind mutations, D342N, D343N, A344P, and I351F, present in the MtRpsA CTD through molecular dynamic simulations (MD). WT showed a good drug binding affinity as compared to mutants (MTs), D342N, D343N, A344P, and I351F. Binding pocket volume, stability, and fluctuations have been altered whereas the total energy, protein folding, and geometric shape analysis further explored a significant variation between WT and MTs. In conclusion, mutations in MtRpsA CTD might be involved to alter the RpsA activity, resulting in drug resistance. Such molecular mechanism behind resistance may provide a better insight into the resistance mechanism to achieve the global TB control targets.
ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-019-44013-9