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New Insights in blaKPC Gene Mobilization in Pseudomonas aeruginosa: Acquisition of blaKPC-3 and Identification of a New Tn2-like NTE Mobilizing blaKPC-2

  • Deisy Abril (First Author)
  • , Juan Bravo Ojeda (Second Author)
  • , Julio Cesar Garcia Casallas (Correspondent Author)
  • , Aura Lucia Leal Castro (Fourth Autor)
  • , Carlos Humberto Saavedra Trujillo (Fifth Author)
  • , Johana Madroñero (Another Number Author)
  • , Rosa Elena Bustos Cruz (Another Number Author)
  • , Ricaurte Alejandro Márquez Ortiz (Another Number Author)
  • , Zayda Lorena Corredor Rozo (Another Number Author)
  • , Natasha Vanegas Gómez (Another Number Author)
  • , Javier Escobar-Pérez (Correspondent Author)
  • Universidad El Bosque
  • Universidad Nacional de Colombia
  • University of Technology Sydney

Research output: Contribution to journalArticlepeer-review

Abstract

Carbapenem-resistant Pseudomonas aeruginosa is a major cause of healthcare associated infections in hospitalized patients and what is more warring with reduced therapeutic options. The KPC is a powerful enzyme capable of hydrolyzing the carbapenems, described first in Klebsiella pneumoniae and it already has found in P. aeruginosa. Objective: To perform a comparative genomic analysis of two new genetic platforms mobilizing the bla KPC-2 and bla KPC-3 in two ST111 and ST235 pandemic clones of P. aeruginosa in Colombia, South America. Methods: Sixty-six bla KPC-harboring P. aeruginosa isolates were identified and characterized during a prospective study conducted in six high complex hospitals in Colombia. Genetic platforms mobilizing the bla KPC were analyzed. Results: The bla KPC-2 and bla KPC-3 were identified in 24 and 42 isolates, respectively. The bla KPC-2-harboring isolates belonged to ST235 and bla KPC-3 to ST111. The whole genome sequencing indicated that the bla KPC-3 gene was mobilized by the Tn4401b within a 55-kb-size environmental origin plasmid, which, in other isolates, was inserted into the chromosome through a transposition event of ISPa38. Regarding the bla KPC-2 gene, this was mobilized by a new Non-Tn4401 Element (NTE) derived from transposon Tn2 (proposed as variant IIg), which has been transposed into a 43-Kb-size little-studied plasmid related to Klebsiella spp. Conclusions: Our results reveal a new acquisition event of bla KPC in P. aeruginosa, in this case bla KPC-3. Likewise, the pandemic high-risk clones ST111 and ST235 of P. aeruginosa continues to spread bla KPC gene through different mobile genetic elements, jumping of conventional Tn4401b and acquiring new Tn2-derived NTE, which were inserted in diverse plasmids.

Original languageEnglish
Article number947
Pages (from-to)1
Number of pages21
JournalAntibiotics
Volume14
Issue number9
DOIs
StatePublished - 19 Sep 2025

Strategic Focuses

  • Vida Humana Plena (Vita)​

Article Classification

  • Full research article

Indexación Internacional (Artículo)

  • ISI Y SCOPUS

Scopus-Q Quartil

  • Q1

ISI- Q Quartil

  • Q1

Categoría Publindex

  • A1

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