Your search keyword '"Deisy Abril"' showing total 19 results

1. Estudio de microbiota fecal revela disbiosis específica en espondiloartritis, según subtipo, actividad de la enfermedad y tratamiento

Author

Consuelo Romero-Sánchez, Carlos Ferrer-Santos, Deisy Abril, Eduin Acosta-Hernández, Juliette De Avila, Alejandro Ramos-Casallas, Javier Escobar, Wilson Bautista-Molano, Diego Jaimes, Adriana Beltrán-Ostos, Juan Manuel Bello-Gualtero, Cristian Flórez-Sarmiento, Viviana Parra-Izquierdo, and Omar-Javier Calixto

Subjects

Espondiloartritis, Microbioma, Actividad de la enfermedad, Terapia biológica, Immunologic diseases. Allergy, RC581-607

Abstract

Objetivo: Comparar la diversidad y composición del microbioma gastrointestinal de pacientes con EspA. Métodos: La secuenciación MiSeq de la región V3-V4 del gen ARN ribosomal 16, se realizó en ADN aislado de heces. Se excluyeron pacientes con EspA y EII simultánea. Se evaluaron diferencias para los índices de riqueza y diversidad por medio de QIIME 2™. Las diferencias entre medias> 0,2%, con un valor de p< 0,05, se asumieron significativas. Aval del Comité de Ética Institucional. Resultados: 69 individuos incluidos, 49 con EspA (espondilitis anquilosante-EA 72,9%, artritis psoriásica-APs 18,8%, artritis reactiva-ARe 8,3%), cinco controles positivos-disbiosis y 15 controles-eubiosis. El tratamiento convencional en 42,9%, anti-IL-17 16,3%, y anti-TNF 40,8%. Por subtipo-EasP, se encontraron diferencias estadísticamente significativas a favor de EA para los índices de diversidad. Entre EA vs APs, hubo diferencia a favor de EA para Clostridium clostridioforme (p=0,002), Gemmiger formicilis (p=0,009), Roseburia inulivorans (p=0,008) y Lachnospira pectinoschiza. Entre EA vs ARe hubo diferencia a favor de EA para L. pectinoschiza (p=0,009), Ruminococcus callidus (p = 0,006), Clostridium ruminantium (p=0,031); G. formicilis (p=0,034). La diversidad y riqueza mostraron diferencias en pacientes con alta actividad para los índices de Simpson y Pielou. En alta actividad, se encontró menor enriquecimiento de Bacteroides eggerthii (p=0,0003), C. ruminantium (p= 0,026) y Alistipes putredinis (p= 0,035). El número de ASV fue superior en el grupo de anti IL-17 vs convencional (p=0.025), y una tendencia entre anti IL-17 vs anti-TNF (p=0,09). En anti TNF hubo menor proporción para C. clostridioforme (p=0,023), G. formicilis (p=0,030) y R. callidus (p= 0,003). Y en anti IL-17, Alistipes indistinctus (p= 0,012), estuvo disminuida. Conclusiones: Existen diferencias en la diversidad microbiana para los subtipos de EspA. El nivel de actividad de la enfermedad es plausible para influir en la composición de microbiota fecal. El tratamiento con anti-TNFα, puede influenciar el ambiente del microbioma favoreciendo la restauración de la microbiota intestinal, mientras los anti IL-17 podrían mantener un ambiente inflamatorio.

Published

2024

2. Colonoscopy aspiration lavages for mucosal metataxonomic profiling of spondylarthritis-associated gastrointestinal tract alterations

Author

Ricaurte A. Marquez-Ortiz, Moises Leon, Deisy Abril, Javier Escobar-Perez, Cristian Florez-Sarmiento, Viviana Parra-Izquierdo, Philippe Chalem, and Consuelo Romero-Sanchez

Subjects

Medicine, Science

Abstract

Abstract The study of the GI-tract microbiota of spondylarthritis (SpA) patients has focused on the analysis of feces samples, that picture mostly the luminal microbiota. The aim of this study was to determine the contribution of mucosal and luminal microbiome to the gut dysbiosis in SpA, using colonoscopy aspiration lavages (CAL), a recent alternative for regional studies of the GI-tract. We analyzed 59 CAL (from sigmoid colon and distal ileum), and 41 feces samples, from 32 SpA patients and 7 healthy individuals, using 16S rRNA gene-targeted metataxonomic profiling. It was found high prevalence of GI-tract manifestations among SpA patients (65.3%). Metataxonomic profiling, confirmed CAL samples from the lower GI tract (colon or ileum) presented a distinctive and undifferentiated bacteriome and separate from that found in feces’ samples or in the beginning of the GI tract (oral cavity (OC)). Lower GI-tract samples and feces of SpA patients exhibited similar behavior to the microbiota of IBD group with reduced microbial richness and diversity, comparing to the healthy controls. Interestingly, it was found increase in proinflammatory taxa in SpA patients, such as Enterobacteriaceae family (mostly in the ileum), Succinivibrio spp. and Prevotella stercorea. Conversely, SpA patients presented significant decrease in the SCFA producers Coprococcus catus and Eubacterium biforme. Our data support the value of CAL samples for the regional study of GI-tract and contribute with information of potential “disruptor taxa” involved in the GI-tract associated disorders observed in SpA patients.

Published

2023

3. Reference gene validation for the relative quantification of cannabinoid receptor expression in human odontoblasts via quantitative polymerase chain reaction

Author

Laura M. Navarro-Saiz, Lilia J. Bernal-Cepeda, Felipe García-Jiménez, Deisy Abril, and Jaime E. Castellanos

Subjects

Reference gene, Odontoblast, RT-qPCR, Cannabinoid receptor 1, Cannabinoid receptor 2, Dentistry, RK1-715

Abstract

Objective: The aim of this study was to identify and validate the reference genes in cultured human odontoblasts to quantify their cannabinoid receptor transcripts. Methods: The most stably transcribed genes in cultured human odontoblast cells were identified using the RefGenes tool and were selected for real-time polymerase chain reaction (PCR) amplification. Human odontoblast cells were differentiated from mesenchymal stem cells using a transforming growth factor-β-supplemented differentiation medium, and total RNA was purified. Reverse transcription-quantitative PCR and relative quantification analyses were performed using the Schefe's method. The relative expression dataset was analyzed to select the most stable genes. Results: The analysis showed that the transcripts of cholinergic receptor nicotinic beta 2 subunit, LIM homeobox transcription factor 1 beta, and family with sequence similarity 223 member B presented the lowest standard deviation (SD) in expression (SD: 0.2, 0.17, and 0.16, respectively). These genes showed similar expression levels as the target genes (cannabinoid receptors). Significant differences were found in the relative expression levels of cannabinoid receptors using the selected genes compared to those calculated using beta actin transcripts as references (p

Published

2022

4. Within patient genetic diversity of bla KPC harboring Klebsiella pneumoniae in a Colombian hospital and identification of a new NTEKPC platform

Author

Deisy Abril, Erika Vergara, Diana Palacios, Aura Lucía Leal, Ricaurte Alejandro Marquez-Ortiz, Johana Madroñero, Zayda Lorena Corredor Rozo, Zandra De La Rosa, Carlos A. Nieto, Natasha Vanegas, Jorge A. Cortés, and Javier Escobar-Perez

Subjects

Medicine, Science

Abstract

Abstract Resistance to carbapenems in Klebsiella pneumoniae has been mostly related with the worldwide dissemination of KPC, largely due to the pandemic clones belonging to the complex clonal (CC) 258. To unravel bla KPC post-endemic clinical impact, here we describe clinical characteristics of 68 patients from a high complexity hospital, and the molecular and genetic characteristics of their 139 bla KPC—K. pneumoniae (KPC-Kp) isolates. Of the 26 patients that presented relapses or reinfections, 16 had changes in the resistance profiles of the isolates recovered from the recurrent episodes. In respect to the genetic diversity of KPC-Kp isolates, PFGE revealed 45 different clonal complexes (CC). MLST for 12 representative clones showed ST258 was present in the most frequent CC (23.0%), however, remaining 11 representative clones belonged to non-CC258 STs (77.0%). Interestingly, 16 patients presented within-patient genetic diversity of KPC-Kp clones. In one of these, three unrelated KPC-Kp clones (ST258, ST504, and ST846) and a bla KPC—K. variicola isolate (ST182) were identified. For this patient, complete genome sequence of one representative isolate of each clone was determined. In K. pneumoniae isolates bla KPC was mobilized by two Tn3-like unrelated platforms: Tn4401b (ST258) and Tn6454 (ST504 and ST846), a new NTEKPC-IIe transposon for first time characterized also determined in the K. variicola isolate of this study. Genome analysis showed these transposons were harbored in different unrelated but previously reported plasmids and in the chromosome of a K. pneumoniae (for Tn4401b). In conclusion, in the bla KPC post-endemic dissemination in Colombia, different KPC-Kp clones (mostly non-CC258) have emerged due to integration of the single bla KPC gene in new genetic platforms. This work also shows the intra-patient resistant and genetic diversity of KPC-Kp isolates. This circulation dynamic could impact the effectiveness of long-term treatments.

Published

2021

5. Worldwide Dissemination of blaKPC Gene by Novel Mobilization Platforms in Pseudomonas aeruginosa: A Systematic Review

Author

Daniela Forero-Hurtado, Zayda Lorena Corredor-Rozo, Julián Santiago Ruiz-Castellanos, Ricaurte Alejandro Márquez-Ortiz, Deisy Abril, Natasha Vanegas, Gloria Inés Lafaurie, Leandro Chambrone, and Javier Escobar-Pérez

Subjects

Pseudomonas aeruginosa, carbapenem resistance, KPC, Tn4401, NTEKPC, interactive map, Therapeutics. Pharmacology, RM1-950

Abstract

The dissemination of blaKPC-harboring Pseudomonas aeruginosa (KPC-Pa) is considered a serious public health problem. This study provides an overview of the epidemiology of these isolates to try to elucidate novel mobilization platforms that could contribute to their worldwide spread. A systematic review in PubMed and EMBASE was performed to find articles published up to June 2022. In addition, a search algorithm using NCBI databases was developed to identify sequences that contain possible mobilization platforms. After that, the sequences were filtered and pair-aligned to describe the blaKPC genetic environment. We found 691 KPC-Pa isolates belonging to 41 different sequence types and recovered from 14 countries. Although the blaKPC gene is still mobilized by the transposon Tn4401, the non-Tn4401 elements (NTEKPC) were the most frequent. Our analysis allowed us to identify 25 different NTEKPC, mainly belonging to the NTEKPC-I, and a new type (proposed as IVa) was also observed. This is the first systematic review that consolidates information about the behavior of the blaKPC acquisition in P. aeruginosa and the genetic platforms implied in its successful worldwide spread. Our results show high NTEKPC prevalence in P. aeruginosa and an accelerated dynamic of unrelated clones. All information collected in this review was used to build an interactive online map.

Published

2023

6. Genome plasticity favours double chromosomal Tn4401b-bla KPC-2 transposon insertion in the Pseudomonas aeruginosa ST235 clone

Author

Deisy Abril, Ricaurte Alejandro Marquez-Ortiz, Betsy Castro-Cardozo, José Ignacio Moncayo-Ortiz, Narda María Olarte Escobar, Zayda Lorena Corredor Rozo, Niradiz Reyes, Catalina Tovar, Héctor Fabio Sánchez, Jaime Castellanos, Yina Marcela Guaca-González, Carmen Elisa Llanos-Uribe, Natasha Vanegas Gómez, and Javier Escobar-Pérez

Subjects

bla KPC-2, Pseudomonas aeruginosa, Carbapenems, Resistance, Colombia, ST235, Microbiology, QR1-502

Abstract

Abstract Background Pseudomonas aeruginosa Sequence Type 235 is a clone that possesses an extraordinary ability to acquire mobile genetic elements and has been associated with the spread of resistance genes, including genes that encode for carbapenemases. Here, we aim to characterize the genetic platforms involved in resistance dissemination in bla KPC-2 -positive P. aeruginosa ST235 in Colombia. Results In a prospective surveillance study of infections in adult patients attended in five ICUs in five distant cities in Colombia, 58 isolates of P. aeruginosa were recovered, of which, 27 (46.6%) were resistant to carbapenems. The molecular analysis showed that 6 (22.2%) and 4 (14.8%) isolates harboured the bla VIM and bla KPC-2 genes, respectively. The four bla KPC-2-positive isolates showed a similar PFGE pulsotype and belonged to ST235. Complete genome sequencing of a representative ST235 isolate shows a unique chromosomal contig of 7097.241 bp with eight different resistance genes identified and five transposons: a Tn6162-like with ant(2″)-Ia, two Tn402-like with ant(3″)-Ia and bla OXA-2 and two Tn4401b with bla KPC-2. All transposons were inserted into the genomic islands. Interestingly, the two Tn4401b copies harbouring bla KPC-2 were adjacently inserted into a new genomic island (PAGI-17) with traces of a replicative transposition process. This double insertion was probably driven by several structural changes within the chromosomal region containing PAGI-17 in the ST235 background. Conclusion This is the first report of a double Tn4401b chromosomal insertion in P. aeruginosa, just within a new genomic island (PAGI-17). This finding indicates once again the great genomic plasticity of this microorganism.

Published

2019

7. Estimation of the Difference in Colistin Plasma Levels in Critically Ill Patients with Favorable or Unfavorable Clinical Outcomes

Author

Jose Sanabria, Vivian Garzón, Tatiana Pacheco, Maria-Paula Avila, Julio-Cesar Garcia, Diego Jaimes, Angela Torres, Rosa-Helena Bustos, Javier Escobar-Perez, and Deisy Abril

Subjects

therapeutic drug monitoring (TDM), colistin, multi-drug resistance bacteria, Gram-negative bacteria, Pharmacy and materia medica, RS1-441

Abstract

In recent decades, antimicrobial resistance (AMR) has led to an increased use of therapeutic alternatives. Among these options, colistin continues to be an option for the treatment of multi-resistant (MDR) Gram-negative bacterial infections. However, due to its high toxicity (nephrotoxicity and neurotoxicity) and narrow therapeutic window, colistin treatment must be utilized carefully. Colistin-treated patients have been observed to have higher mortality due to inadequate therapeutic levels. The objective of this study was to estimate the difference in colistin plasma levels in critically ill patients, and its relationship to favorable or unfavorable clinical outcomes. This prospective observational study was conducted between September 2017 and June 2020 at the Universidad de La Sabana Clinic, in patients who had been treated with colistimethate sodium (CMS) for at least 72 h until day 7 of drug treatment in the critical care unit of a university hospital. There were no statistically significant differences in colistin levels between groups with favorable or unfavorable clinical outcomes (0.16 SD vs. 0.54 SD p-value = 0.167). There was higher mortality in patients with subtherapeutic levels (18% vs. 0%), and additionally, there was a greater rate of renal failure in the group with higher therapeutic levels (50% vs. 20.7%). Due to the loss of power of the study, we were unable to demonstrate a possible difference between colistin levels related to favorable or unfavorable clinical outcomes at day 7. However, we recommend further studies to evaluate the impact of measuring levels in terms of mortality and security.

Published

2021

8. Pseudomonas aeruginosa Coharboring BlaKPC-2 and BlaVIM-2 Carbapenemase Genes

Author

Tatiana Pacheco, Rosa Helena Bustos-Cruz, Deisy Abril, Sara Arias, Lina Uribe, Jenny Rincón, Julio-Cesar García, and Javier Escobar-Perez

Subjects

Pseudomonas aeruginosa, carbapenems, carbapenemases, Verona Integron-encoded metallo-β-lactamase (VIM), Klebsiella pneumoniae carbepenemase (KPC), drug resistance, Therapeutics. Pharmacology, RM1-950

Abstract

Pseudomonas aeruginosa, a bacterium commonly isolated from hospital settings, exhibits intrinsic resistance to a number of antibiotics and can acquire resistance during antibiotic therapy. Resistance towards carbapenems is increasing due to its overuse in the treatment of infections caused by extended-spectrum β-lactamase (ESBL) producing organisms. Nonetheless, carbapenems are essential for the treatment of high-risk infections and are one of the remaining weapons in the fight against “extreme drug resistance” of Gram-negative/positive bacilli. Herein, we describe a case report of infections caused by P. aeruginosa strains that carry blaVIM-2 and blaKPC-2 carbapenemase genes simultaneously, identified in five patients who were admitted to a high complexity health institution in Colombia. Molecular characterization included PCR screening for blaKPC, blaGES, blaOXA-48, blaIMP, blaNDM, and blaVIM carbapenemase and other resistance genes as well as analysis of the genetic relationships by genome macro-restriction and Pulsed-Field Gel Electrophoresis (PFGE) separation. In conclusion, these infections represent a major challenge to public health due to the risk of the infection spreading compounded by the fact that limited treatment options are available, thereby increasing the risk of increased morbidity and mortality.

Published

2019

9. Genome sequencing of three bacteria associated to black band disease from a Colombian reef-building coral

Author

Juan Henao, Hermes Pérez, Deisy Abril, Katterine Ospina, Adriana Piza, Kelly Botero, Cristhian Rincón, Jhon Donato, Andrea Hurtado, Erika García, Vanessa Otero, Alexander Del Risco, Brenda Guerra, Yina Cifuentes, Alvaro Ordoñez, Daniel Rojas, Karen Suarez, Daniel Osorio, and Andrés Pinzón

Subjects

Black band disease, Genome announcement, Coral reefs, Stappia indica, Nitratireductor aquibiodomus, Genetics, QH426-470

Abstract

We announce the draft genome sequence of three Gram-negative bacteria isolated from coral tissues affected with the black band disease (BBD), identified with the NCBI's Assembly Database accession numbers: MBQF, MAYB and MBQE. These genome drafts constitute an useful tool for the characterisation of these bacteria and for the understanding of the relationship between the microbial consortia associated with the disease and the onset and progression of the pathology.

Published

2017

10. Within patient genetic diversity of bla KPC harboring Klebsiella pneumoniae in a Colombian hospital and identification of a new NTEKPC platform

Author

Johana Madroñero, Ricaurte Alejandro Marquez-Ortiz, Erika Vergara, Carlos A. Nieto, Javier Escobar-Perez, Zayda Lorena Corredor Rozo, Deisy Abril, Jorge E. Cortes, Aura Lucía Leal, Diana Palacios, Natasha Vanegas, and Zandra De La Rosa

Subjects

Whole genome sequencing, Genetics, Genetic diversity, Multidisciplinary, biology, Klebsiella pneumoniae, Science, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, bacterial infections and mycoses, Genome, Plasmid, Pulsed-field gel electrophoresis, polycyclic compounds, Multilocus sequence typing, Medicine, Gene

Abstract

Resistance to carbapenems in Klebsiellapneumoniae has been mostly related with the worldwide dissemination of KPC, largely due to the pandemic clones belonging to the complex clonal (CC) 258. To unravel blaKPC post-endemic clinical impact, here we describe clinical characteristics of 68 patients from a high complexity hospital, and the molecular and genetic characteristics of their 139 blaKPC—K.pneumoniae (KPC-Kp) isolates. Of the 26 patients that presented relapses or reinfections, 16 had changes in the resistance profiles of the isolates recovered from the recurrent episodes. In respect to the genetic diversity of KPC-Kp isolates, PFGE revealed 45 different clonal complexes (CC). MLST for 12 representative clones showed ST258 was present in the most frequent CC (23.0%), however, remaining 11 representative clones belonged to non-CC258 STs (77.0%). Interestingly, 16 patients presented within-patient genetic diversity of KPC-Kp clones. In one of these, three unrelated KPC-Kp clones (ST258, ST504, and ST846) and a blaKPC—K.variicola isolate (ST182) were identified. For this patient, complete genome sequence of one representative isolate of each clone was determined. In K.pneumoniae isolates blaKPC was mobilized by two Tn3-like unrelated platforms: Tn4401b (ST258) and Tn6454 (ST504 and ST846), a new NTEKPC-IIe transposon for first time characterized also determined in the K.variicola isolate of this study. Genome analysis showed these transposons were harbored in different unrelated but previously reported plasmids and in the chromosome of a K.pneumoniae (for Tn4401b). In conclusion, in the blaKPC post-endemic dissemination in Colombia, different KPC-Kp clones (mostly non-CC258) have emerged due to integration of the single blaKPC gene in new genetic platforms. This work also shows the intra-patient resistant and genetic diversity of KPC-Kp isolates. This circulation dynamic could impact the effectiveness of long-term treatments.

Published

2021

11. In Silico Analysis and PCR Characterization of non-Tn4401 Transposable Elements in Pseudomonas aeruginosa

Author

Julián Ruiz-Castellanos, Ricaurte Alejandro Márquez-Ortiz, Deisy Abril, Daniela Forero Hurtado, Ginna Tíjaro, Zayda Corredor-Rozo, Javier Escobar-Pérez, and Natasha Vanegas

Published

2022

12. Within-patient Genetic Diversity of blaKPC Harboring K. pneumoniae Isolates in a Colombian High Complexity Hospital. Identification of a New Tn3-based NTEKPC-IIe Mobilization Platform

Author

Natasha Vanegas, Jorge Alberto Cortés, Zandra De La Rosa, Erika Vergara, Ricaurte Alejandro Marquez-Ortiz, Aura Lucía Leal, Javier Escobar-Perez, Carlos A. Nieto, Zayda Lorena Corredor Rozo, Johana Madroñero, Diana Palacios, and Deisy Abril

Subjects

Genetic diversity, Mobilization, High complexity, K pneumoniae, Identification (biology), Computational biology, Biology

Abstract

Resistance to carbapenems in Klebsiella pneumoniae has been mostly related with the worldwide dissemination of KPC, largely due to the pandemic clones belonging to the complex clonal (CC) 258. To unravel blaKPC post-endemic clinical impact, here we describe clinical characteristics of 68 patients from a high complexity hospital, and the molecular and genetic characteristics of their 139 blaKPC - K. pneumoniae (KPC-Kp) isolates. Of the 26 patients that presented relapses or reinfections, 16 had changes in the resistance profiles of the isolates recovered from the recurrent episodes. In respect to the genetic diversity of KPC-Kp isolates, PFGE revealed 45 different clonal complexes (CC). MLST for 12 representative clones showed ST258 was present in the most frequent CC (23.0%), however, remaining 11 representative clones belonged to non-CC258 STs (77.0%). Interestingly, 16 patients presented within-patient genetic diversity of KPC-Kp clones. In one of these, three unrelated KPC-Kp clones (ST258, ST504, and ST846) and a blaKPC - K. variicola isolate (ST182) were identified. For this patient, complete genome sequence of one representative isolate of each clone was determined. In K. pneumoniae isolates blaKPC was mobilized by two Tn3-like unrelated platforms: Tn4401b (ST258) and Tn6454 (ST504 and ST846), a new NTEKPC-IIe transposon for first time characterized also determined in the K. variicola isolate of this study. Genome analysis showed these transposons were harbored in different unrelated but previously reported plasmids and in the chromosome of a K. pneumoniae (for Tn4401b). In conclusion, in the blaKPC post-endemic dissemination in Colombia, different KPC-Kp clones (mostly non-CC258) have emerged due to integration of the single blaKPC gene in new genetic platforms. This work also shows the intra-patient resistant and genetic diversity of KPC-Kp isolates. This circulation dynamic could impact the effectiveness of long-term treatments.

Published

2021

13. Genome plasticity favours double chromosomal Tn4401b-bla KPC-2 transposon insertion in the Pseudomonas aeruginosa ST235 clone

Author

Héctor Fabio Sánchez, Ricaurte Alejandro Marquez-Ortiz, Zayda Lorena Corredor Rozo, Catalina Tovar, Yina Marcela Guaca-González, Niradiz Reyes, José Ignacio Moncayo-Ortiz, Natasha Vanegas Gómez, Jaime E. Castellanos, Carmen Elisa Llanos-Uribe, Narda María Olarte Escobar, Betsy Castro-Cardozo, Deisy Abril, Javier Escobar-Perez, Castellanos, Jaime [0000-0003-1596-8383], Escobar-Pérez, Javier [0000-0002-0432-6978], and Abril Riaño, Deisy Julieth [0000-0002-6686-6283]

Subjects

Microbiology (medical), Replicative transposition, Resistance, lcsh:QR1-502, Biology, Colombia, ST235, Microbiology, Genome, lcsh:Microbiology, Carbapenémicos, 03 medical and health sciences, Chromosomal Insertion, Genomic island, Bacterias aerobias gramnegativas, Genetics, Whole genome sequencing, 0303 health sciences, Contig, 030306 microbiology, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, Genética, Infecciones por pseudomonas, bla KPC-2, Carbapenems, Chromosomal region, Pseudomonas aeruginosa, Mobile genetic elements

Abstract

Background Pseudomonas aeruginosa Sequence Type 235 is a clone that possesses an extraordinary ability to acquire mobile genetic elements and has been associated with the spread of resistance genes, including genes that encode for carbapenemases. Here, we aim to characterize the genetic platforms involved in resistance dissemination in bla KPC-2 -positive P. aeruginosa ST235 in Colombia. Results In a prospective surveillance study of infections in adult patients attended in five ICUs in five distant cities in Colombia, 58 isolates of P. aeruginosa were recovered, of which, 27 (46.6%) were resistant to carbapenems. The molecular analysis showed that 6 (22.2%) and 4 (14.8%) isolates harboured the bla VIM and bla KPC-2 genes, respectively. The four bla KPC-2-positive isolates showed a similar PFGE pulsotype and belonged to ST235. Complete genome sequencing of a representative ST235 isolate shows a unique chromosomal contig of 7097.241 bp with eight different resistance genes identified and five transposons: a Tn6162-like with ant(2″)-Ia, two Tn402-like with ant(3″)-Ia and bla OXA-2 and two Tn4401b with bla KPC-2. All transposons were inserted into the genomic islands. Interestingly, the two Tn4401b copies harbouring bla KPC-2 were adjacently inserted into a new genomic island (PAGI-17) with traces of a replicative transposition process. This double insertion was probably driven by several structural changes within the chromosomal region containing PAGI-17 in the ST235 background. Conclusion This is the first report of a double Tn4401b chromosomal insertion in P. aeruginosa, just within a new genomic island (PAGI-17). This finding indicates once again the great genomic plasticity of this microorganism.

Published

2019

14. First Report and Comparative Genomics Analysis of a blaOXA-244–Harbouring Escherichia coli Isolate Recovered in American Continent

Author

Ricaurte Alejandro Marquez-Ortiz, Ingrid Gisell Bustos Moya, Javier Escobar-Perez, Diego Fernando Josa Montero, Deisy Abril, Isabel Torres Molina, Zayda Lorena Corredor Rozo, and Natasha Vanegas Gómez

Subjects

Genetics, Comparative genomics, medicine, Biology, medicine.disease_cause, Escherichia coli

Abstract

The carbapenemase OXA-244 is a derivate of OXA-48, and its detection is very difficult in laboratories. Here we report the identification and genomic analysis of an Escherichia coli isolate (28Eco12) harbouring the blaOXA-244 gene identified in Colombia, South America. The 28Eco12 isolate was identified during a retrospective study and it was recovered from a patient treated in Colombia. The complete nucleotide sequence was established using the PacBio platform. A comparative genomics analysis with other blaOXA-244–harbouring Escherichia coli strains was performed. The 28Eco12 isolate belonged to sequence type (ST) 38 and its genome was composed of two molecules, a chromosome of 5,343,367 bp and a plasmid of 92,027 bp, which belonged to the incompatibility group IncY and did not harbour resistance genes. The blaOXA-244 gene was chromosomally-encoded and mobilized by an ISR1-related Tn6237 composite transposon. Notably, this transposon was inserted and located within a new genomic island. For our knowledge this is the first report of a blaOXA-244–harbouring Escherichia coli isolate in American continent.Our results suggest that the introduction of the OXA-244-producing E. coli isolate was through clonal expansion of the ST38 pandemic clone. Other isolates producing OXA-244 could be circulating silently on the American continent.

Published

2019

15. First Report and Comparative Genomics Analysis of a

Author

Deisy, Abril, Ingrid Gisell, Bustos Moya, Ricaurte Alejandro, Marquez-Ortiz, Diego Fernando, Josa Montero, Zayda Lorena, Corredor Rozo, Isabel, Torres Molina, Natasha, Vanegas Gómez, and Javier, Escobar-Perez

Subjects

resistance, Brief Report, blaOXA-244, Escherichia coli, carbapenems, Colombia

Abstract

The carbapenemase OXA-244 is a derivate of OXA-48, and its detection is very difficult in laboratories. Here, we report the identification and genomic analysis of an Escherichia coli isolate (28Eco12) harboring the blaOXA-244 gene identified in Colombia, South America. The 28Eco12 isolate was identified during a retrospective study, and it was recovered from a patient treated in Colombia. The complete nucleotide sequence was established using the PacBio platform. A comparative genomics analysis with other blaOXA-244–harboring Escherichia coli strains was performed. The 28Eco12 isolate belonged to sequence type (ST) 38, and its genome was composed of two molecules, a chromosome of 5,343,367 bp and a plasmid of 92,027 bp, which belonged to the incompatibility group IncY and did not harbor resistance genes. The blaOXA-244 gene was chromosomally encoded and mobilized by an ISR1-related Tn6237 composite transposon. Notably, this transposon was inserted and located within a new genomic island. To our knowledge, this is the first report of a blaOXA-244–harboring Escherichia coli isolate in America. Our results suggest that the introduction of the OXA-244-producing E. coli isolate was through clonal expansion of the ST38 pandemic clone. Other isolates producing OXA-244 could be circulating silently in America.

Published

2019

16. First report and comparative genomics analysis of a blaoxa-244-haarboring escherichia coli isolate recovered in the American continent

Author

Ricaurte Alejandro Marquez-Ortiz, Diego Fernando Josa Montero, Deisy Abril, Natasha Vanegas Gómez, Isabel Torres Molina, Zayda Lorena Corredor Rozo, Ingrid Gisell Bustos Moya, Javier Escobar-Perez, Escobar-Pérez, Javier [0000-0002-0432-6978], and Abril Riaño, Deisy Julieth [0000-0002-6686-6283]

Subjects

0301 basic medicine, Microbiology (medical), Transposable element, 030106 microbiology, Resistance, Biology, medicine.disease_cause, Biochemistry, Microbiology, Genome, 03 medical and health sciences, Código genético, Plasmid, Enterobacteriaceae, Genomic island, medicine, Informes de casos, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Escherichia coli, Genetics, Comparative genomics, Nucleic acid sequence, 030104 developmental biology, Infectious Diseases, Composite transposon, Carbapenems, BlaOXA-244

Abstract

The carbapenemase OXA-244 is a derivate of OXA-48, and its detection is very difficult in laboratories. Here, we report the identification and genomic analysis of an Escherichia coli isolate (28Eco12) harboring the blaOXA-244 gene identified in Colombia, South America. The 28Eco12 isolate was identified during a retrospective study, and it was recovered from a patient treated in Colombia. The complete nucleotide sequence was established using the PacBio platform. A comparative genomics analysis with other blaOXA-244–harboring Escherichia coli strains was performed. The 28Eco12 isolate belonged to sequence type (ST) 38, and its genome was composed of two molecules, a chromosome of 5,343,367 bp and a plasmid of 92,027 bp, which belonged to the incompatibility group IncY and did not harbor resistance genes. The blaOXA-244 gene was chromosomally encoded and mobilized by an ISR1-related Tn6237 composite transposon. Notably, this transposon was inserted and located within a new genomic island. To our knowledge, this is the first report of a blaOXA-244–harboring Escherichia coli isolate in America. Our results suggest that the introduction of the OXA-244-producing E. coli isolate was through clonal expansion of the ST38 pandemic clone. Other isolates producing OXA-244 could be circulating silently in America.

Published

2019

17. Genome plasticity favours double chromosomal Tn4401b-bla

Author

Deisy, Abril, Ricaurte Alejandro, Marquez-Ortiz, Betsy, Castro-Cardozo, José Ignacio, Moncayo-Ortiz, Narda María, Olarte Escobar, Zayda Lorena, Corredor Rozo, Niradiz, Reyes, Catalina, Tovar, Héctor Fabio, Sánchez, Jaime, Castellanos, Yina Marcela, Guaca-González, Carmen Elisa, Llanos-Uribe, Natasha, Vanegas Gómez, and Javier, Escobar-Pérez

Subjects

DNA, Bacterial, Genomic Islands, Whole Genome Sequencing, Resistance, Microbial Sensitivity Tests, Chromosomes, Bacterial, Colombia, ST235, beta-Lactamases, Anti-Bacterial Agents, Bacterial Typing Techniques, Intensive Care Units, Bacterial Proteins, Carbapenems, bla KPC-2, Drug Resistance, Multiple, Bacterial, Pseudomonas aeruginosa, DNA Transposable Elements, Humans, Prospective Studies, Genome, Bacterial, Multilocus Sequence Typing, Research Article

Abstract

Background Pseudomonas aeruginosa Sequence Type 235 is a clone that possesses an extraordinary ability to acquire mobile genetic elements and has been associated with the spread of resistance genes, including genes that encode for carbapenemases. Here, we aim to characterize the genetic platforms involved in resistance dissemination in blaKPC-2-positive P. aeruginosa ST235 in Colombia. Results In a prospective surveillance study of infections in adult patients attended in five ICUs in five distant cities in Colombia, 58 isolates of P. aeruginosa were recovered, of which, 27 (46.6%) were resistant to carbapenems. The molecular analysis showed that 6 (22.2%) and 4 (14.8%) isolates harboured the blaVIM and blaKPC-2 genes, respectively. The four blaKPC-2-positive isolates showed a similar PFGE pulsotype and belonged to ST235. Complete genome sequencing of a representative ST235 isolate shows a unique chromosomal contig of 7097.241 bp with eight different resistance genes identified and five transposons: a Tn6162-like with ant(2″)-Ia, two Tn402-like with ant(3″)-Ia and blaOXA-2 and two Tn4401b with blaKPC-2. All transposons were inserted into the genomic islands. Interestingly, the two Tn4401b copies harbouring blaKPC-2 were adjacently inserted into a new genomic island (PAGI-17) with traces of a replicative transposition process. This double insertion was probably driven by several structural changes within the chromosomal region containing PAGI-17 in the ST235 background. Conclusion This is the first report of a double Tn4401b chromosomal insertion in P. aeruginosa, just within a new genomic island (PAGI-17). This finding indicates once again the great genomic plasticity of this microorganism. Electronic supplementary material The online version of this article (10.1186/s12866-019-1418-6) contains supplementary material, which is available to authorized users.

Published

2017

18. Pseudomonas aeruginosa Coharboring BlaKPC-2 and BlaVIM-2 Carbapenemase Genes

Author

Deisy Abril, Sara Arias, J. García, Tatiana Pacheco, Lina Uribe, Javier Escobar-Perez, Jenny Rincón, Rosa Helena Bustos-Cruz, Escobar-Pérez, Javier [0000-0002-0432-6978], and Abril Riaño, Deisy Julieth [0000-0002-6686-6283]

Subjects

0301 basic medicine, Microbiology (medical), Bacilli, carbapenemases, medicine.drug_class, 030106 microbiology, Antibiotics, Case Report, Drug resistance, Resistencia a medicamentos, medicine.disease_cause, Biochemistry, Microbiology, Genome, 03 medical and health sciences, Infección hospitalaria, Enterobacteriaceae, polycyclic compounds, medicine, Pulsed-field gel electrophoresis, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Gene, drug resistance, biology, Pseudomonas aeruginosa, lcsh:RM1-950, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, biology.organism_classification, Verona Integron-encoded metallo-β-lactamase, lcsh:Therapeutics. Pharmacology, Klebsiella pneumoniae carbepenemase (KPC), 030104 developmental biology, Infectious Diseases, Carbapenems, carbapenems, Verona Integron-encoded metallo-β-lactamase (VIM), Bacteria

Abstract

Pseudomonas aeruginosa, a bacterium commonly isolated from hospital settings, exhibits intrinsic resistance to a number of antibiotics and can acquire resistance during antibiotic therapy. Resistance towards carbapenems is increasing due to its overuse in the treatment of infections caused by extended-spectrum β-lactamase (ESBL) producing organisms. Nonetheless, carbapenems are essential for the treatment of high-risk infections and are one of the remaining weapons in the fight against “extreme drug resistance” of Gram-negative/positive bacilli. Herein, we describe a case report of infections caused by P. aeruginosa strains that carry blaVIM-2 and blaKPC-2 carbapenemase genes simultaneously, identified in five patients who were admitted to a high complexity health institution in Colombia. Molecular characterization included PCR screening for blaKPC, blaGES, blaOXA-48, blaIMP, blaNDM, and blaVIM carbapenemase and other resistance genes as well as analysis of the genetic relationships by genome macro-restriction and Pulsed-Field Gel Electrophoresis (PFGE) separation. In conclusion, these infections represent a major challenge to public health due to the risk of the infection spreading compounded by the fact that limited treatment options are available, thereby increasing the risk of increased morbidity and mortality.

Published

2019

19. Genome sequencing of three bacteria associated to black band disease from a Colombian reef-building coral

Author

Alexander Del Risco, Yina Cifuentes, Jhon Donato, Katterine Ospina, Hermes Pérez, Andrea Hurtado, Brenda Guerra, Daniel Rojas, Erika García, Cristhian Rincón, Karen Suarez, Andrés Pinzón, Deisy Abril, Kelly Botero, Adriana Piza, Vanessa Otero, Alvaro Ordoñez, Daniel Osorio, and Juan David Velásquez Henao

Subjects

0301 basic medicine, Coral reefs, lcsh:QH426-470, Coral, Biology, Biochemistry, Genome, DNA sequencing, 03 medical and health sciences, Data in Brief, Genome announcement, Genetics, medicine, Black band disease, Nitratireductor aquibiodomus, natural sciences, Whole genome sequencing, geography, geography.geographical_feature_category, Ecology, Coral reef, medicine.disease, biology.organism_classification, lcsh:Genetics, 030104 developmental biology, Stappia indica, Molecular Medicine, Bacteria, Biotechnology

Abstract

We announce the draft genome sequence of three Gram-negative bacteria isolated from coral tissues affected with the black band disease (BBD), identified with the NCBI's Assembly Database accession numbers: MBQF, MAYB and MBQE. These genome drafts constitute an useful tool for the characterisation of these bacteria and for the understanding of the relationship between the microbial consortia associated with the disease and the onset and progression of the pathology.

Published

2016