An integrative, multi-omics approach towards the prioritization of Klebsiella pneumoniae drug targets

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作者
Pablo Ivan Pereira Ramos
Darío Fernández Do Porto
Esteban Lanzarotti
Ezequiel J. Sosa
Germán Burguener
Agustín M. Pardo
Cecilia C. Klein
Marie-France Sagot
Ana Tereza R. de Vasconcelos
Ana Cristina Gales
Marcelo Marti
Adrián G. Turjanski
Marisa F. Nicolás
机构
[1] Fundação Oswaldo Cruz (FIOCRUZ),Instituto Gonçalo Moniz
[2] Laboratório Nacional de Computação Científica,Plataforma de Bioinformática Argentina (BIA), Instituto de Cálculo, Facultad de Ciencias Exactas y Naturales
[3] Petrópolis,Departamento de Química Biológica, Facultad de Ciencias Exactas y Naturales
[4] Universidad de Buenos Aires,Instituto de Química Biológica de la Facultad de Ciencias Exactas y Naturales (IQUIBICEN) CONICET
[5] Universidad de Buenos Aires,Laboratório Alerta. Division of Infectious Diseases, Department of Internal Medicine. Escola Paulista de Medicina
[6] Ciudad Universitaria,undefined
[7] Pabellón 2,undefined
[8] Ciudad Universitaria,undefined
[9] Pabellón 2,undefined
[10] Inria Grenoble Rhône-Alpes,undefined
[11] Université Claude Bernard Lyon 1,undefined
[12] Universidade Federal de São Paulo,undefined
[13] Centre for Genomic Regulation (CRG),undefined
[14] Departament de Genètica,undefined
[15] Microbiologia i Estadística,undefined
[16] Facultat de Biologia and Institut de Biomedicina (IBUB),undefined
[17] Universitat de Barcelona,undefined
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Klebsiella pneumoniae (Kp) is a globally disseminated opportunistic pathogen that can cause life-threatening infections. It has been found as the culprit of many infection outbreaks in hospital environments, being particularly aggressive towards newborns and adults under intensive care. Many Kp strains produce extended-spectrum β-lactamases, enzymes that promote resistance against antibiotics used to fight these infections. The presence of other resistance determinants leading to multidrug-resistance also limit therapeutic options, and the use of ‘last-resort’ drugs, such as polymyxins, is not uncommon. The global emergence and spread of resistant strains underline the need for novel antimicrobials against Kp and related bacterial pathogens. To tackle this great challenge, we generated multiple layers of ‘omics’ data related to Kp and prioritized proteins that could serve as attractive targets for antimicrobial development. Genomics, transcriptomics, structuromic and metabolic information were integrated in order to prioritize candidate targets, and this data compendium is freely available as a web server. Twenty-nine proteins with desirable characteristics from a drug development perspective were shortlisted, which participate in important processes such as lipid synthesis, cofactor production, and core metabolism. Collectively, our results point towards novel targets for the control of Kp and related bacterial pathogens.
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