Rugose atypical Vibrio cholerae O1 El Tor responsible for 2009 cholera outbreak in India

Goutam Chowdhury; Rupak K. Bhadra; Satyabrata Bag; Gururaja P. Pazhani; Bhabatosh Das; Pallabi Basu; K. Nagamani; Ranjan K. Nandy; Asish K. Mukhopadhyay; Thandavarayan Ramamurthy

doi:10.1099/jmm.0.000344

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f Rugose atypical Vibrio cholerae O1 El Tor responsible for 2009 cholera outbreak in India

Authors: Goutam Chowdhury¹ , Rupak K. Bhadra² , Satyabrata Bag^2,3 , Gururaja P. Pazhani⁴ , Bhabatosh Das³ , Pallabi Basu² , K. Nagamani⁵ , Ranjan K. Nandy¹ , Asish K. Mukhopadhyay¹ , Thandavarayan Ramamurthy^1,3
- VIEW AFFILIATIONS
- ¹ 1Department of Bacteriology, National Institute of Cholera and Enteric Diseases, Kolkata, India ² 2Infectious Diseases and Immunology Division, CSIR - Indian Institute of Chemical Biology, Kolkata, India ³ 3Center for Human Microbial Ecology, Translational Health Science and Technology Institute, Faridabad, India ⁴ 4National Institute of Pharmaceutical Education and Research, Kolkata, India ⁵ 5Division of Microbiology, Gandhi Medical College, Secunderabad, India
Correspondence Thandavarayan Ramamurthy [email protected]
First Published Online: 18 October 2016, Journal of Medical Microbiology 65: 1130-1136, doi: 10.1099/jmm.0.000344
Subject: Clinical Microbiology

Received: 11/03/2016
Accepted: 24/08/2016
Cover date: 18/10/2016

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Vibrio cholerae causes cholera outbreaks in endemic regions where the water quality and sanitation facilities remain poor. Apart from biotype and serotype changes, V. cholerae undergoes phase variation, which results in the generation of two morphologically different variants termed smooth and rugose. In this study, 12 rugose (R-VC) and 6 smooth (S-VC) V. cholerae O1 Ogawa isolates were identified in a cholera outbreak that occurred in Hyderabad, India. Antimicrobial susceptibility results showed that all the isolates were resistant to ampicillin, furazolidone and nalidixic acid. In addition, R-VC isolates were resistant to ciprofloxacin (92 %), streptomycin (92 %), erythromycin (83 %), trimethoprim-sulfamethoxazole (75 %) and tetracycline (75 %). Based on the ctxB gene analysis, all the isolates were identified as El Tor variant with mutation in two positions of ctxB, similar to the classical biotype. The R-VC isolates specifically showed excessive biofilm formation and were comparatively less motile. In addition, the majority of these isolates (~83 %) displayed random mutations in the hapR gene, which encodes haemagglutinin protease regulatory protein. In the PFGE analysis, R-VC and S-VC were placed in distinct clusters but remained clonally related. In the ribotyping analysis, all the R-VC isolates exhibited R-III pattern, which is a prevailing type among the current El Tor isolates. A hapR deletion mutant generated using an S-VC isolate expressed rugose phenotype. To our knowledge, this is the first report on the association of rugose V. cholerae O1 in a large cholera outbreak with extended antimicrobial resistance and random mutations in the haemagglutinin protease regulatory protein encoding gene (hapR).

The GenBank/EMBL/DDBJ accession numbers for the hapR sequences described in this paper are KT633830–KT633840.
One supplementary figure is available with the online Supplementary Material.

Keyword(s): cholera, V. cholerae O1, HapR, PFGE, antimicrobial resistance, rugose isolates

Abbreviations:

CT cholera toxin

R-VC rugose V. cholerae

S-VC smooth V. cholerae

VPS Vibrio polysaccharide

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Abbreviations:

CT	cholera toxin
R-VC	rugose V. cholerae
S-VC	smooth V. cholerae
VPS	Vibrio polysaccharide