Metabolic remodeling by RNA polymerase gene mutations is associated with reduced β-lactam susceptibility in oxacillin-susceptible MRSA
Author:
Watanabe Shinya1ORCID, Nsofor Chijioke A.12, Thitiananpakorn Kanate1, Tan Xin-Ee1ORCID, Aiba Yoshifumi1, Takenouchi Remi3, Kiga Kotaro14ORCID, Sasahara Teppei1, Miyanaga Kazuhiko1, Veeranarayanan Srivani1, Shimamori Yuzuki1, Lian Adeline Yeo Syin1, Nguyen Thuy Minh1, Nguyen Huong Minh1, Alessa Ola1, Kumwenda Geoffrey Peterkins1, Jayathilake Sarangi1, Revilleza Jastin Edrian Cocuangco1, Baranwal Priyanka1, Nishikawa Yutaro1, Li Feng-Yu1, Kawaguchi Tomofumi1, Sankaranarayanan Sowmiya1, Arbaah Mahmoud1, Zhang Yuancheng1, Maniruzzaman1, Liu Yi1, Sarah Hossain1, Li Junjie1, Sugano Takashi1, Ho Thi My Duyen1, Batbold Anujin1, Nayanjin Tergel1, Cui Longzhu1
Affiliation:
1. Division of Bacteriology, Department of Infection and Immunity, Jichi Medical University, Tochigi, Japan 2. Department of Biotechnology, School of Biological Sciences, Federal University of Technology Owerri Nigeria, Owerri, Nigeria 3. School of Medicine, Jichi Medical University, Tochigi, Japan 4. Research Center for Drug and Vaccine Development, National Institute of Infectious Diseases, Tokyo, Japan
Abstract
ABSTRACT
The emergence of oxacillin-susceptible methicillin-resistant
Staphylococcus aureus
(OS-MRSA) has imposed further challenges to the clinical management of MRSA infections. When exposed to β-lactam antibiotics, these strains can easily acquire reduced β-lactam susceptibility through chromosomal mutations, including those in RNA polymerase (RNAP) genes such as
rpoBC
, which may then lead to treatment failure. Despite the increasing prevalence of such strains and the apparent challenges they pose for diagnosis and treatment, there is limited information available on the actual mechanisms underlying such chromosomal mutation-related transitions to reduced β-lactam susceptibility, as it does not directly associate with the expression of
mecA
. This study investigated the cellular physiology and metabolism of six missense mutants with reduced oxacillin susceptibility, each carrying respective mutations on RpoB
H929P
, RpoB
Q645H
, RpoC
G950R
, RpoC
G498D
, RpiA
A64E
, and FruB
A211E
, using capillary electrophoresis-mass spectrometry-based metabolomics analysis. Our results showed that
rpoBC
mutations caused RNAP transcription dysfunction, leading to an intracellular accumulation of ribonucleotides. These mutations also led to the accumulation of UDP-Glc/Gal and UDP-GlcNAc, which are precursors of UTP-associated peptidoglycan and wall teichoic acid. Excessive amounts of building blocks then contributed to the cell wall thickening of mutant strains, as observed in transmission electron microscopy, and ultimately resulted in decreased susceptibility to β-lactam in OS-MRSA.
IMPORTANCE
The emergence of oxacillin-susceptible methicillin-resistant
Staphylococcus aureus
(OS-MRSA) strains has created new challenges for treating MRSA infections. These strains can become resistant to β-lactam antibiotics through chromosomal mutations, including those in the RNA polymerase (RNAP) genes such as
rpoBC
, leading to treatment failure. This study investigated the mechanisms underlying reduced β-lactam susceptibility in four
rpoBC
mutants of OS-MRSA. The results showed that
rpoBC
mutations caused RNAP transcription dysfunction, leading to an intracellular accumulation of ribonucleotides and precursors of peptidoglycan as well as wall teichoic acid. This, in turn, caused thickening of the cell wall and ultimately resulted in decreased susceptibility to β-lactam in OS-MRSA. These findings provide insights into the mechanisms of antibiotic resistance in OS-MRSA and highlight the importance of continued research in developing effective treatments to combat antibiotic resistance.
Funder
MEXT | Japan Society for the Promotion of Science Takeda Science Foundation Japan Agency for Medical Research and Development
Publisher
American Society for Microbiology
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