Literature DB >> 31343934

Hypervirulence and carbapenem resistance: two distinct evolutionary directions that led high-risk Klebsiella pneumoniae clones to epidemic success.

Yi-Chyi Lai1,2, Min-Chi Lu3,4, Po-Ren Hsueh5,6.   

Abstract

Introduction: Over the past few decades, Klebsiella pneumoniae has become a significant threat to public health and is now listed as an ESKAPE pathogen. Evolving with versatile capabilities, K. pneumoniae is a population composed of genetically and phenotypically diverse bacteria. However, epidemic K. pneumoniae are restricted to specific clonal lineages. The clonal group CG23 comprises hypervirulent K. pneumoniae displaying limited resistance to antimicrobials and is frequently associated with the community-acquired invasive syndrome. On the other hand, CG258 is another clonal group of K. pneumoniae that has evolved resistance to carbapenems, primarily by acquiring the carbapenemase-encoding genes through nosocomial carriage. Areas covered: With a focus on the high-risk K. pneumoniae clonal lineages CG23 and CG258, we review recent advances including the newly discovered lineage-specific genomic features, and the molecular basis of K. pneumoniae-associated epidemiology, antimicrobial resistance, and hypervirulence. Expert opinion: Both CG23 and CG258 can establish reservoirs in susceptible individuals. Empirical antimicrobial regimens that are prescribed for immediate treatments frequently create selective pressures that favor the high-risk lineages to develop into prominent colonizers. This dilemma reinforces the need for effective therapies that require rapid and accurate diagnosis of epidemic K. pneumoniae.

Entities:  

Keywords:  CG23; CG258; Klebsiella pneumoniae; carbapenemase-producing; hypervirulence

Mesh:

Substances:

Year:  2019        PMID: 31343934     DOI: 10.1080/14737159.2019.1649145

Source DB:  PubMed          Journal:  Expert Rev Mol Diagn        ISSN: 1473-7159            Impact factor:   5.225


  9 in total

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2.  Molecular characterisation of carbapenem-resistant Klebsiella pneumoniae clinical isolates: preliminary experience from a tertiary care teaching hospital in the Himalayas.

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Review 3.  Innate Host Defense against Klebsiella pneumoniae and the Outlook for Development of Immunotherapies.

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Journal:  J Innate Immun       Date:  2021-10-08       Impact factor: 7.111

4.  Clinical and Microbiological Prognostic Factors of in-Hospital Mortality Caused by Hypervirulent Klebsiella pneumoniae Infections: A Retrospective Study in a Tertiary Hospital in Southwestern China.

Authors:  Yu Tang; Hang Liu; Jinxin Zhao; Miao Yi; Yaling Yuan; Yun Xia
Journal:  Infect Drug Resist       Date:  2020-10-21       Impact factor: 4.003

5.  Fecal Klebsiella pneumoniae Carriage Is Intermittent and of High Clonal Diversity.

Authors:  Sarah Lepuschitz; Kathrin Hauser; Agnes Schriebl; Claudia Schlagenhaufen; Anna Stöger; Ali Chakeri; Kornelia Vötsch; Shiva Pekard-Amenitsch; Burkhard Springer; Franz Allerberger; Werner Ruppitsch
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6.  Hypervirulent Klebsiella pneumoniae of Lineage ST66-K2 Caused Tonsillopharyngitis in a German Patient.

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7.  Resistance evolution of hypervirulent carbapenem-resistant Klebsiella pneumoniae ST11 during treatment with tigecycline and polymyxin.

Authors:  Xi Jin; Qiong Chen; Fang Shen; Yan Jiang; Xueqing Wu; Xiaoting Hua; Ying Fu; Yunsong Yu
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8.  Characterization and Full Genome Sequence of Novel KPP-5 Lytic Phage against Klebsiella pneumoniae Responsible for Recalcitrant Infection.

Authors:  Ahmed R Sofy; Noha K El-Dougdoug; Ehab E Refaey; Rehab A Dawoud; Ahmed A Hmed
Journal:  Biomedicines       Date:  2021-03-28

9.  Safety and Efficacy of a Phage, kpssk3, in an in vivo Model of Carbapenem-Resistant Hypermucoviscous Klebsiella pneumoniae Bacteremia.

Authors:  Yunlong Shi; Yuan Peng; Yixin Zhang; Yu Chen; Cheng Zhang; Xiaoqiang Luo; Yajie Chen; Zhiqiang Yuan; Jing Chen; Yali Gong
Journal:  Front Microbiol       Date:  2021-05-20       Impact factor: 5.640

  9 in total

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