Macrolides such as erythromycin are the empirical treatment of
Bordetella pertussis
infections. China has experienced an increase in erythromycin-resistant
B. pertussis
isolates since they were first reported in 2013. Here, we undertook a genomic study on Chinese
B. pertussis
isolates from 2012 to 2015 to elucidate the origins and phylogenetic relationships of erythromycin-resistant
B. pertussis
isolates in China. A total of 167 Chinese
B. pertussis
isolates were used for antibiotic sensitivity testing and multiple locus variable-number tandem repeat (VNTR) analysis (MLVA). All except four isolates were erythromycin-resistant and of the four erythromycin-sensitive isolates, three were
non-ptxP1
. MLVA types (MT), MT55, MT104 and MT195 were the predominant types. Fifty of those isolates were used for whole genome sequencing and phylogenetic analysis. Genome sequencing and phylogenetic analysis revealed three independent erythromycin-resistant lineages and all resistant isolates carried a mutation in the 23S rRNA gene. A novel
fhaB3
allele was found uniquely in Chinese
ptxP1
isolates and these Chinese
ptxP1-ptxA1-fhaB3
had a 5-fold higher mutation rate than the global
ptxP1-ptxA1 B. pertussis
population. Our results suggest that the evolution of Chinese
B. pertussis
is likely to be driven by selection pressure from both vaccination and antibiotics. The emergence of the new non-vaccine
fhaB3
allele in Chinese
B. pertussis
population may be a result of selection from vaccination, whereas the expansion of
ptxP1-fhaB3
lineages was most likely to be the result of selection pressure from antibiotics. Further monitoring of
B. pertussis
in China is required to better understand the evolution of the pathogen.
This study described a pertussis outbreak caused by macrolide-resistant B. pertussis in a primary school and indicated that close contact of index case causes the bacterial transmission.
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