Emergence of ciprofloxacin heteroresistance in clinical Pseudomonas aeruginosa

doi:10.3969/j.issn.1674-8115.2022.07.001

Abstract

Abstract: Objective

·To investigate ciprofloxacin heteroresistance in Pseudomonas aeruginosa (PA).

Methods

·Ciprofloxacin heteroresistance in 227 clinical PA strains was initially identified by disk diffusion. Meanwhile, susceptibilities of these strains was classified according to the diameter of the inhibition zone. The stability of the identified heteroresistant strains was tested by measuring the sensitivity after serial passage under antibiotic-free conditions. Mechanisms mediating heteroresistance were analyzed by whole-genome sequencing. Susceptibilities of resistant subpopulations to different antibiotics were also detected.

Results

·Based on disk diffusion, 142 (62.6%), 26 (11.5%), and 59 (26.0%) of 227 isolates were classified as susceptible, intermediate and resistant to ciprofloxacin respectively. Eighteen putative heteroresistant strains were detected through primary disk diffusion selection, and 11 among them were further verified as stable heteroresistant strains by population analysis profiling (PAP). By whole-genome sequencing, 8 and 2 among 11 resistant subpopulations carried mutations in mexS and mutations in gyrA individually. In addition, mutations in fleQ, PA2632 or PAKAF_02255 were detected respectively. Both mexS and gyrA mutants led to moxifloxacin resistance, and some mexS mutants also showed resistance to chloramphenicol and imipenem.

Conclusion

·Ciprofloxacin heteroresistance rate inPA is 4.8% (11/227). As a screening method for heteroresistance of PA, the disk diffusion has low sensitivity and has a certain false negative rate. The mutation mexS is the predominant mutation type in resistant subpopulations and it might enhance the overexpression of efflux pump MexEF-OprN, thus mediating resistance to different antibiotics including ciprofloxacin.

Key words: Pseudomonas aeruginosa, ciprofloxacin, heteroresistance, disk diffusion, population analysis profiling (PAP)

CLC Number:

R378

LI Congcong, YAO Yufeng, ZHANG Chuanzhen. Emergence of ciprofloxacin heteroresistance in clinical Pseudomonas aeruginosa[J]. Journal of Shanghai Jiao Tong University (Medical Science), 2022, 42(7): 839-845.

Figures/Tables 5

TrendMD

References 21

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Strain	MIC
Strain	CIP	MXF	IPM	MEM	CHL
30	0.5	8	0.5	0.25	16
30R	4	64	0.5	0.25	>128
1595	8	64	>1 024	>1 024	>128
1595R	64	64	>1 024	>1 024	>128
6655	0.125	1	0.5	0.25	32
6655R	4	64	4	0.5	>128
7314	0.06	0.5	1	4	16
7314R	1	2	1	4	16
7318	0.125	0.5	1	0.125	8
7318R	2	64	4	0.125	>128
7500	0.125	1	0.5	0.125	16
7500R	2	16	4	0.5	>128
7637	0.06	0.5	0.5	0.25	16
7637R	1	8	2	0.5	>128
7755	0.06	0.06	2	0.06	8
7755R	1	0.5	2	0.06	>128
7866	0.5	2	8	8	32
7866R	4	64	8	4	>128
7895	0.06	0.5	0.5	<0.06	4
7895R	2	16	0.5	<0.06	>128
A601	0.125	1	1	1	32
A601R	1	4	1	1	32

Strain	MIC
Strain	CIP	MXF	IPM	MEM	CHL
30	0.5	8	0.5	0.25	16
30R	4	64	0.5	0.25	>128
1595	8	64	>1 024	>1 024	>128
1595R	64	64	>1 024	>1 024	>128
6655	0.125	1	0.5	0.25	32
6655R	4	64	4	0.5	>128
7314	0.06	0.5	1	4	16
7314R	1	2	1	4	16
7318	0.125	0.5	1	0.125	8
7318R	2	64	4	0.125	>128
7500	0.125	1	0.5	0.125	16
7500R	2	16	4	0.5	>128
7637	0.06	0.5	0.5	0.25	16
7637R	1	8	2	0.5	>128
7755	0.06	0.06	2	0.06	8
7755R	1	0.5	2	0.06	>128
7866	0.5	2	8	8	32
7866R	4	64	8	4	>128
7895	0.06	0.5	0.5	<0.06	4
7895R	2	16	0.5	<0.06	>128
A601	0.125	1	1	1	32
A601R	1	4	1	1	32

Strain	ST	Mutation （based on genome and Sanger sequencing）
30	508
30R	508	988‒998 bp deletion （mexS， frameshift）， rg131His （PA2632）
6655	508
6655R	508	354 insert T （mexS， frameshift）， Glu18Lys （hypothetical protein）
7314	204
7314R	204	Thr83Ile （gyrA）
7318	498
7318R	498	Phe259Ser （mexS）
7500	3 610
7500R	3 610	740‒754 bp deletion （mexS， frameshift）， 554 bp deletion （fleQ）
7637	532
7637R	532	423 bp deletion （mexS， frameshift）
7755	‒
7755R	‒	Trp42Leu （mexS）
7866	498
7866R	498	Gln147Lys （mexS）
7895	1 238
7895R	1 238	Pro46Leu （mexS）
A601	1 212
A601R	1 212	Thr83Ile （gyrA）

Strain	ST	Mutation （based on genome and Sanger sequencing）
30	508
30R	508	988‒998 bp deletion （mexS， frameshift）， rg131His （PA2632）
6655	508
6655R	508	354 insert T （mexS， frameshift）， Glu18Lys （hypothetical protein）
7314	204
7314R	204	Thr83Ile （gyrA）
7318	498
7318R	498	Phe259Ser （mexS）
7500	3 610
7500R	3 610	740‒754 bp deletion （mexS， frameshift）， 554 bp deletion （fleQ）
7637	532
7637R	532	423 bp deletion （mexS， frameshift）
7755	‒
7755R	‒	Trp42Leu （mexS）
7866	498
7866R	498	Gln147Lys （mexS）
7895	1 238
7895R	1 238	Pro46Leu （mexS）
A601	1 212
A601R	1 212	Thr83Ile （gyrA）