Genomic analysis unveils genome degradation events and gene flux in the emergence and persistence of S. Paratyphi A lineages

Jobin John Jacob; Agila K Pragasam; Karthick Vasudevan; Aravind Velmurugan; Monisha Priya Teekaraman; Tharani Priya Thirumoorthy; Pallab Ray; Madhu Gupta; Arti Kapil; Sulochana Putil Bai; Savitha Nagaraj; Karnika Saigal; Temsunaro Rongsen Chandola; Maria Thomas; Ashish Bavdekar; Sheena Evelyn Ebenezer; Jayanthi Shastri; Anuradha De; Shantha Dutta; Anna P Alexander; Roshine Mary Koshy; Dasaratha R Jinka; Ashita Singh; Sunil Kumar Srivastava; Shalini Anandan; Gordon Dougan; Jacob John; Gagandeep Kang; Balaji Veeraraghavan; Ankur Mutreja

doi:10.1371/journal.ppat.1010650

Genomic analysis unveils genome degradation events and gene flux in the emergence and persistence of S. Paratyphi A lineages

PLoS Pathog. 2023 Apr 28;19(4):e1010650. doi: 10.1371/journal.ppat.1010650. eCollection 2023 Apr.

Authors

Jobin John Jacob¹, Agila K Pragasam¹, Karthick Vasudevan^{1

2}, Aravind Velmurugan¹, Monisha Priya Teekaraman¹, Tharani Priya Thirumoorthy¹, Pallab Ray³, Madhu Gupta³, Arti Kapil⁴, Sulochana Putil Bai⁵, Savitha Nagaraj⁶, Karnika Saigal⁷, Temsunaro Rongsen Chandola⁸, Maria Thomas⁹, Ashish Bavdekar¹⁰, Sheena Evelyn Ebenezer¹¹, Jayanthi Shastri¹², Anuradha De¹², Shantha Dutta¹³, Anna P Alexander¹⁴, Roshine Mary Koshy¹⁵, Dasaratha R Jinka¹⁶, Ashita Singh¹⁷, Sunil Kumar Srivastava¹⁸, Shalini Anandan¹, Gordon Dougan¹⁹, Jacob John¹, Gagandeep Kang¹, Balaji Veeraraghavan¹, Ankur Mutreja¹⁹

Affiliations

¹ Christian Medical College, Vellore, India.
² REVA University, Bangalore, India.
³ Post Graduate Institute of Medical & Educational Research, Chandigarh, India.
⁴ All India Institute of Medical Sciences, New Delhi, India.
⁵ Kanchi Kamakoti Childs Trust Hospital, Chennai, India.
⁶ St. John's Medical College, Bengaluru, India.
⁷ Chacha Nehru Bal Chikitsalaya, Delhi, India.
⁸ Centre for Health Research & Development-Society for Applied Studies, New Delhi, India.
⁹ Christian Medical College, Ludhiana, India.
¹⁰ KEM Hospital & Research Centre, Pune, India.
¹¹ The Duncan Hospital, Raxaul, India.
¹² Topiwala National Medical College & BYL Nair Charitable Hospital, Mumbai, India.
¹³ ICMR-National Institute of Cholera and Enteric Diseases, Kolkata, India.
¹⁴ Lady Willingdon Hospital, Manali, India.
¹⁵ Makunda Christian Leprosy & General Hospital, Karimjang, India.
¹⁶ Rural Development Trust Hospital, Bathalapalli, Andhra Pradesh, India.
¹⁷ Chinchpada Christian Hospital, Nandurbar, India.
¹⁸ Department of Microbiology, SSN College, University of Delhi, Delhi, India.
¹⁹ Cambridge Institute of Therapeutic Immunology & Infectious Disease (CITIID), Department of Medicine, University of Cambridge, Cambridge, United Kingdom.

Abstract

Paratyphoid fever caused by S. Paratyphi A is endemic in parts of South Asia and Southeast Asia. The proportion of enteric fever cases caused by S. Paratyphi A has substantially increased, yet only limited data is available on the population structure and genetic diversity of this serovar. We examined the phylogenetic distribution and evolutionary trajectory of S. Paratyphi A isolates collected as part of the Indian enteric fever surveillance study "Surveillance of Enteric Fever in India (SEFI)." In the study period (2017-2020), S. Paratyphi A comprised 17.6% (441/2503) of total enteric fever cases in India, with the isolates highly susceptible to all the major antibiotics used for treatment except fluoroquinolones. Phylogenetic analysis clustered the global S. Paratyphi A collection into seven lineages (A-G), and the present study isolates were distributed in lineages A, C and F. Our analysis highlights that the genome degradation events and gene acquisitions or losses are key molecular events in the evolution of new S. Paratyphi A lineages/sub-lineages. A total of 10 hypothetically disrupted coding sequences (HDCS) or pseudogenes-forming mutations possibly associated with the emergence of lineages were identified. The pan-genome analysis identified the insertion of P2/PSP3 phage and acquisition of IncX1 plasmid during the selection in 2.3.2/2.3.3 and 1.2.2 genotypes, respectively. We have identified six characteristic missense mutations associated with lipopolysaccharide (LPS) biosynthesis genes of S. Paratyphi A, however, these mutations confer only a low structural impact and possibly have minimal impact on vaccine effectiveness. Since S. Paratyphi A is human-restricted, high levels of genetic drift are not expected unless these bacteria transmit to naive hosts. However, public-health investigation and monitoring by means of genomic surveillance would be constantly needed to avoid S. Paratyphi A serovar becoming a public health threat similar to the S. Typhi of today.

Copyright: © 2023 Jacob et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Anti-Bacterial Agents
Genomics
Humans
Phylogeny
Salmonella paratyphi A / genetics
Salmonella typhi / genetics
Typhoid Fever* / microbiology

Substances

Anti-Bacterial Agents

Grants and funding

This work was funded by grants from Bill & Melinda Gates Foundation, USA (Investment ID INV-009497 OPP1159351 to GK, BV and AM) for the Project “National Surveillance System for Enteric Fever in India. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.