Identification of Clostridioides difficile mutants with increased daptomycin resistance

达托霉素 生物 脂肽 突变体 单元格信封 微生物学 磷脂酰甘油 脂质Ⅱ 肽聚糖 生物化学 基因 金黄色葡萄球菌 细菌 万古霉素 遗传学 磷脂 大肠杆菌 磷脂酰胆碱
作者
Brianne R. Zbylicki,Claire Murphy,Jennifer Petsche,Ute Müh,Horia A. Dobrila,Theresa D. Ho,Mikaela N. Daum,Anthony G. Pannullo,David S. Weiss,Craig D. Ellermeier
出处
期刊:Journal of Bacteriology [American Society for Microbiology]
卷期号:206 (3)
标识
DOI:10.1128/jb.00368-23
摘要

ABSTRACT Daptomycin is a cyclic lipopeptide antibiotic used to treat infections caused by some Gram-positive bacteria. Daptomycin disrupts synthesis of the peptidoglycan (PG) cell wall by inserting into the cytoplasmic membrane and binding multiple forms of the undecaprenyl carrier lipid required for PG synthesis. Membrane insertion requires phosphatidylglycerol, so studies of daptomycin can provide insight into assembly and maintenance of the cytoplasmic membrane. Here, we studied the effects of daptomycin on Clostridioides difficile , the leading cause of healthcare-associated diarrhea. We observed that growth of C. difficile strain R20291 in the presence of sub-MIC levels of daptomycin resulted in a chaining phenotype, minicell formation, and lysis—phenotypes broadly consistent with perturbation of membranes and PG synthesis. We also selected for and characterized eight mutants with elevated daptomycin resistance. The mutations in these mutants were mapped to four genes: cdsA ( cdr20291_2041 ), ftsH2 ( cdr20291_3396 ), esrR ( cdr20291_1187 ), and draS ( cdr20291_2456 ). Of these four genes, only draS has been characterized previously. Follow-up studies indicate these mutations confer daptomycin resistance by two general mechanisms: reducing the amount of phosphatidylglycerol in the cytoplasmic membrane ( cdsA ) or altering the regulation of membrane processes ( ftsH2 , esrR , and draS ). Thus, the mutants described here provide insights into phospholipid synthesis and identify signal transduction systems involved in cell envelope biogenesis and stress response in C. difficile . IMPORTANCE C. difficile is the leading cause of healthcare-associated diarrhea and is a threat to public health due to the risk of recurrent infections. Understanding biosynthesis of the atypical cell envelope of C. difficile may provide insight into novel drug targets to selectively inhibit C. difficile . Here, we identified mutations that increased daptomycin resistance and allowed us to better understand phospholipid synthesis, cell envelope biogenesis, and stress response in C. difficile .
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