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1. Role of the first WHO mutation catalogue in the diagnosis of antibiotic resistance in Mycobacterium tuberculosis in the Valencia Region, Spain: a retrospective genomic analysis

Author

García-Marín, Ana María, Cancino-Muñoz, Irving, Torres-Puente, Manuela, Villamayor, Luis M, Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J, Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, González-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, María Montserrat, Vanaclocha, Hermelinda, González-Candelas, Fernando, Furió, Victoria, and Comas, Iñaki

Published
2024
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2. Role of the first WHO mutation catalogue in the diagnosis of antibiotic resistance in Mycobacterium tuberculosis in the Valencia Region, Spain: a retrospective genomic analysis

Author

European Research Council, Ministerio de Ciencia e Innovación (España), Generalitat Valenciana, Ministerio de Universidades (España), Consejo Superior de Investigaciones Científicas (España), CSIC - Plataforma Temática Interdisciplinar del CSIC Salud Global (PTI Salud Global), García-Marín, Ana María, Cancino-Muñoz, Irving, Torres-Puente, Manuela, Villamayor, Luis M., Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J., Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, González-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, María Montserrat, Vanaclocha, Hermelinda, González-Candelas, Fernando, Furió, Victoria, Valencia Region Tuberculosis Working Group, Comas, Iñaki, European Research Council, Ministerio de Ciencia e Innovación (España), Generalitat Valenciana, Ministerio de Universidades (España), Consejo Superior de Investigaciones Científicas (España), CSIC - Plataforma Temática Interdisciplinar del CSIC Salud Global (PTI Salud Global), García-Marín, Ana María, Cancino-Muñoz, Irving, Torres-Puente, Manuela, Villamayor, Luis M., Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J., Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, González-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, María Montserrat, Vanaclocha, Hermelinda, González-Candelas, Fernando, Furió, Victoria, Valencia Region Tuberculosis Working Group, and Comas, Iñaki

Abstract

Background: In June, 2021, WHO published the most complete catalogue to date of resistance-conferring mutations in Mycobacterium tuberculosis. Here, we aimed to assess the performance of genome-based antimicrobial resistance prediction using the catalogue and its potential for improving diagnostics in a real low-burden setting. Methods: In this retrospective population-based genomic study M tuberculosis isolates were collected from 25 clinical laboratories in the low-burden setting of the Valencia Region, Spain. Culture-positive tuberculosis cases reported by regional public health authorities between Jan 1, 2014, and Dec 31, 2016, were included. The drug resistance profiles of these isolates were predicted by the genomic identification, via whole-genome sequencing (WGS), of the high-confidence resistance-causing variants included in the catalogue and compared with the phenotype. We determined the minimum inhibitory concentration (MIC) of the isolates with discordant resistance profiles using the resazurin microtitre assay. Findings: WGS was performed on 785 M tuberculosis complex culture-positive isolates, and the WGS resistance prediction sensitivities were: 85·4% (95% CI 70·8–94·4) for isoniazid, 73·3% (44·9–92·2) for rifampicin, 50·0% (21·1–78·9) for ethambutol, and 57·1% (34·0–78·2) for pyrazinamide; all specificities were more than 99·6%. Sensitivity values were lower than previously reported, but the overall pan-susceptibility accuracy was 96·4%. Genotypic analysis revealed that four phenotypically susceptible isolates carried mutations (rpoB Leu430Pro and rpoB Ile491Phe for rifampicin and fabG1 Leu203Leu for isoniazid) known to give borderline resistance in standard phenotypic tests. Additionally, we identified three putative resistance-associated mutations (inhA Ser94Ala, katG Leu48Pro, and katG Gly273Arg for isoniazid) in samples with substantially higher MICs than those of susceptible isolates. Combining both genomic and phenotypic data, in accordance wit

Published
2024

3. Role of the first WHO mutation catalogue in the diagnosis of antibiotic resistance in Mycobacterium tuberculosis in the Valencia Region, Spain: a retrospective genomic analysis

Author

García-Marín, Ana María, primary, Cancino-Muñoz, Irving, additional, Torres-Puente, Manuela, additional, Villamayor, Luis M, additional, Borrás, Rafael, additional, Borrás-Máñez, María, additional, Bosque, Montserrat, additional, Camarena, Juan J, additional, Colomer-Roig, Ester, additional, Colomina, Javier, additional, Escribano, Isabel, additional, Esparcia-Rodríguez, Oscar, additional, Gil-Brusola, Ana, additional, Gimeno, Concepción, additional, Gimeno-Gascón, Adelina, additional, Gomila-Sard, Bárbara, additional, González-Granda, Damiana, additional, Gonzalo-Jiménez, Nieves, additional, Guna-Serrano, María Remedio, additional, López-Hontangas, José Luis, additional, Martín-González, Coral, additional, Moreno-Muñoz, Rosario, additional, Navarro, David, additional, Navarro, María, additional, Orta, Nieves, additional, Pérez, Elvira, additional, Prat, Josep, additional, Rodríguez, Juan Carlos, additional, Ruiz-García, María Montserrat, additional, Vanaclocha, Hermelinda, additional, González-Candelas, Fernando, additional, Furió, Victoria, additional, and Comas, Iñaki, additional

Published
2023
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5. High-resolution mapping of tuberculosis transmission: Whole genome sequencing and phylogenetic modelling of a cohort from Valencia Region, Spain

Author

Xu, Yuanwei, Cancino-Muñoz, Irving, Torres-Puente, Manuela, Villamayor, Luis M., Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J., Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, González-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, María Montserrat, Vanaclocha, Herme, Colijn, Caroline, and Comas, Iñaki

Subjects
Disease transmission -- Genetic aspects -- Health aspects, Telecommunications equipment -- Health aspects, DNA sequencing -- Health aspects, Type 2 diabetes -- Genetic aspects -- Health aspects, Phylogeny -- Health aspects, Genomes -- Health aspects, Epidemiology -- Health aspects, Tuberculosis -- Genetic aspects -- Health aspects, Genomics -- Health aspects, HIV, Diabetes mellitus, Public health, HIV patients, Public health movements, Cellular transmission equipment, Telecommunications equipment, Biological sciences
Abstract

Background Whole genome sequencing provides better delineation of transmission clusters in Mycobacterium tuberculosis than traditional methods. However, its ability to reveal individual transmission links within clusters is limited. Here, we used a 2-step approach based on Bayesian transmission reconstruction to (1) identify likely index and missing cases, (2) determine risk factors associated with transmitters, and (3) estimate when transmission happened. Methods and findings We developed our transmission reconstruction method using genomic and epidemiological data from a population-based study from Valencia Region, Spain. Tuberculosis (TB) incidence during the study period was 8.4 cases per 100,000 people. While the study is ongoing, the sampling frame for this work includes notified TB cases between 1 January 2014 and 31 December 2016. We identified a total of 21 transmission clusters that fulfilled the criteria for analysis. These contained a total of 117 individuals diagnosed with active TB (109 with epidemiological data). Demographic characteristics of the study population were as follows: 80/109 (73%) individuals were Spanish-born, 76/109 (70%) individuals were men, and the mean age was 42.51 years (SD 18.46). We found that 66/109 (61%) TB patients were sputum positive at diagnosis, and 10/109 (9%) were HIV positive. We used the data to reveal individual transmission links, and to identify index cases, missing cases, likely transmitters, and associated transmission risk factors. Our Bayesian inference approach suggests that at least 60% of index cases are likely misidentified by local public health. Our data also suggest that factors associated with likely transmitters are different to those of simply being in a transmission cluster, highlighting the importance of differentiating between these 2 phenomena. Our data suggest that type 2 diabetes mellitus is a risk factor associated with being a transmitter (odds ratio 0.19 [95% CI 0.02-1.10], p < 0.003). Finally, we used the most likely timing for transmission events to study when TB transmission occurred; we identified that 5/14 (35.7%) cases likely transmitted TB well before symptom onset, and these were largely sputum negative at diagnosis. Limited within-cluster diversity does not allow us to extrapolate our findings to the whole TB population in Valencia Region. Conclusions In this study, we found that index cases are often misidentified, with downstream consequences for epidemiological investigations because likely transmitters can be missed. Our findings regarding inferred transmission timing suggest that TB transmission can occur before patient symptom onset, suggesting also that TB transmits during sub-clinical disease. This result has direct implications for diagnosing TB and reducing transmission. Overall, we show that a transition to individual-based genomic epidemiology will likely close some of the knowledge gaps in TB transmission and may redirect efforts towards cost-effective contact investigations for improved TB control., Author(s): Yuanwei Xu 1, Irving Cancino-Muñoz 2, Manuela Torres-Puente 2, Luis M. Villamayor 3, Rafael Borrás 4, María Borrás-Máñez 5, Montserrat Bosque 6, Juan J. Camarena 7, Ester Colomer-Roig 3,7, [...]

Published
2019
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7. Population-based sequencing of Mycobacterium tuberculosis reveals how current population dynamics are shaped by past epidemics

Author

European Research Council, Ministerio de Ciencia e Innovación (España), Comas, Iñaki [0000-0001-5504-9408], Torres-Puente, Manuela [0000-0002-8352-180X], López, Mariana G. [0000-0002-2216-9232], Cancino-Muñoz, Irving, López, Mariana G., Torres-Puente, Manuela, Villamayor, Luis M., Borras, Rafael, Borras-Manez, Maria, Bosque, Montserrat, Camarena, Juan J., Colijn, Caroline, Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodriguez, Oscar, Garcia-Garcia, Francisco, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Barbara, Gonzales-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, Ma Montserrat, Vanaclocha, Hermelinda, Comas, Iñaki, European Research Council, Ministerio de Ciencia e Innovación (España), Comas, Iñaki [0000-0001-5504-9408], Torres-Puente, Manuela [0000-0002-8352-180X], López, Mariana G. [0000-0002-2216-9232], Cancino-Muñoz, Irving, López, Mariana G., Torres-Puente, Manuela, Villamayor, Luis M., Borras, Rafael, Borras-Manez, Maria, Bosque, Montserrat, Camarena, Juan J., Colijn, Caroline, Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodriguez, Oscar, Garcia-Garcia, Francisco, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Barbara, Gonzales-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, Ma Montserrat, Vanaclocha, Hermelinda, and Comas, Iñaki

Abstract

Transmission is a driver of tuberculosis (TB) epidemics in high-burden regions, with assumed negligible impact in low-burden areas. However, we still lack a full characterization of transmission dynamics in settings with similar and different burdens. Genomic epidemiology can greatly help to quantify transmission, but the lack of whole genome sequencing population-based studies has hampered its application. Here, we generate a population-based dataset from Valencia region and compare it with available datasets from different TB-burden settings to reveal transmission dynamics heterogeneity and its public health implications. We sequenced the whole genome of 785 Mycobacterium tuberculosis strains and linked genomes to patient epidemiological data. We use a pairwise distance clustering approach and phylodynamic methods to characterize transmission events over the last 150 years, in different TB-burden regions. Our results underscore significant differences in transmission between low-burden TB settings, i.e., clustering in Valencia region is higher (47.4%) than in Oxfordshire (27%), and similar to a high-burden area as Malawi (49.8%). By modeling times of the transmission links, we observed that settings with high transmission rate are associated with decades of uninterrupted transmission, irrespective of burden. Together, our results reveal that burden and transmission are not necessarily linked due to the role of past epidemics in the ongoing TB incidence, and highlight the need for in-depth characterization of transmission dynamics and specifically tailored TB control strategies.

Published
2022

8. Population-based sequencing of Mycobacterium tuberculosis reveals how current population dynamics are shaped by past epidemics

Author

Cancino-Muñoz, Irving, López, Mariana G, Torres-Puente, Manuela, Villamayor, Luis M, Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J, Colijn, Caroline, Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, García-García, Francisco, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, Gónzales-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedios, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, Ma Montserrat, Vanaclocha, Hermelinda, Comas, Iñaki, European Research Council, Ministerio de Ciencia e Innovación (España), Comas, Iñaki [0000-0001-5504-9408], Torres-Puente, Manuela [0000-0002-8352-180X], López, Mariana G. [0000-0002-2216-9232], Comas, Iñaki, Torres-Puente, Manuela, and López, Mariana G.

Subjects
Mycobacterium tuberculosis, epidemiology, genomic epidemiology, global health, transmission, tuberculosis, whole-genome sequencing, Whole-genome sequencing, General Immunology and Microbiology, Epidemiology, General Neuroscience, Global health, Transmission, Tuberculosis, Mycobacterium tuberculosis, General Medicine, Genomic epidemiology, General Biochemistry, Genetics and Molecular Biology
Abstract

23 páginas, 4 figuras, 1 tabla., Transmission is a driver of tuberculosis (TB) epidemics in high-burden regions, with assumed negligible impact in low-burden areas. However, we still lack a full characterization of transmission dynamics in settings with similar and different burdens. Genomic epidemiology can greatly help to quantify transmission, but the lack of whole genome sequencing population-based studies has hampered its application. Here, we generate a population-based dataset from Valencia region and compare it with available datasets from different TB-burden settings to reveal transmission dynamics heterogeneity and its public health implications. We sequenced the whole genome of 785 Mycobacterium tuberculosis strains and linked genomes to patient epidemiological data. We use a pairwise distance clustering approach and phylodynamic methods to characterize transmission events over the last 150 years, in different TB-burden regions. Our results underscore significant differences in transmission between low-burden TB settings, i.e., clustering in Valencia region is higher (47.4%) than in Oxfordshire (27%), and similar to a high-burden area as Malawi (49.8%). By modeling times of the transmission links, we observed that settings with high transmission rate are associated with decades of uninterrupted transmission, irrespective of burden. Together, our results reveal that burden and transmission are not necessarily linked due to the role of past epidemics in the ongoing TB incidence, and highlight the need for in-depth characterization of transmission dynamics and specifically tailored TB control strategies., European Research Council 638553-TB-ACCELERATE; European Research Council 101001038-TBRECONNECT; Ministerio de Ciencia e Innovación SAF2016-77346-R

Published
2022

11. Population-based sequencing of Mycobacterium tuberculosis reveals how current population dynamics are shaped by past epidemics.

Author

Canano-Muñoz, Irving, López, Mariana G., Torres-Puente, Manuela, Villamayor, Luis M., Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J., Colijn, Caroline, Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, García-García, Francisco, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, Gónzales-Granda, Damiana, and Gonzalo-Jiménez, Nieves

Published
2022
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13. Clinical factors associated with a Candida albicans Germ Tube Antibody positive test in Intensive Care Unit patients

Author

Martín-Mazuelos Estrella, Giménez María J, Ramírez Paula, Camarena Juan J, Cuétara María S, Alkorta Miriam, Quindós Guillermo, Zaragoza Rafael, Pemán Javier, Linares-Sicilia María J, and Pontón José

Subjects
Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background Poor outcomes of invasive candidiasis (IC) are associated with the difficulty in establishing the microbiological diagnosis at an early stage. New scores and laboratory tests have been developed in order to make an early therapeutic intervention in an attempt to reduce the high mortality associated with invasive fungal infections. Candida albicans IFA IgG has been recently commercialized for germ tube antibody detection (CAGTA). This test provides a rapid and simple diagnosis of IC (84.4% sensitivity and 94.7% specificity). The aim of this study is to identify the patients who could be benefited by the use of CAGTA test in critical care setting. Methods A prospective, cohort, observational multicentre study was carried out in six medical/surgical Intensive care units (ICU) of tertiary-care Spanish hospitals. Candida albicans Germ Tube Antibody test was performed twice a week if predetermined risk factors were present, and serologically demonstrated candidiasis was considered if the testing serum dilution was ≥ 1:160 in at least one sample and no other microbiological evidence of invasive candidiasis was found. Results Fifty-three critically ill non-neutropenic patients (37.7% post surgery) were included. Twenty-two patients (41.5%) had CAGTA-positive results, none of them with positive blood culture for Candida. Neither corrected colonization index nor antifungal treatment had influence on CAGTA results. This finding could corroborate that the CAGTA may be an important biomarker to distinguish between colonization and infection in these patients. The presence of acute renal failure at the beginning of the study was more frequent in CAGTA-negative patients. Previous surgery was statistically more frequent in CAGTA-positive patients. Conclusions This study identified previous surgery as the principal clinical factor associated with CAGTA-positive results and emphasises the utility of this promising technique, which was not influenced by high Candida colonization or antifungal treatment. Our results suggest that detection of CAGTA may be important for the diagnosis of invasive candidiasis in surgical patients admitted in ICU.

Published
2011
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15. High-resolution mapping of tuberculosis transmission: Whole genome sequencing and phylogenetic modelling of a cohort from Valencia Region, Spain

Author

European Research Council, Ministerio de Economía y Competitividad (España), Engineering and Physical Sciences Research Council (UK), Comas, Iñaki [0000-0001-5504-9408], Torres-Puente, Manuela [0000-0002-8352-180X], Xu, Yuanwei, Cancino-Muñoz, Irving, Torres-Puente, Manuela, Villamayor, Luis M., Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J., Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, González-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, María Montserrat, Vanaclocha, Hermelinda, Colijn, Caroline, Comas, Iñaki, European Research Council, Ministerio de Economía y Competitividad (España), Engineering and Physical Sciences Research Council (UK), Comas, Iñaki [0000-0001-5504-9408], Torres-Puente, Manuela [0000-0002-8352-180X], Xu, Yuanwei, Cancino-Muñoz, Irving, Torres-Puente, Manuela, Villamayor, Luis M., Borrás, Rafael, Borrás-Máñez, María, Bosque, Montserrat, Camarena, Juan J., Colomer-Roig, Ester, Colomina, Javier, Escribano, Isabel, Esparcia-Rodríguez, Oscar, Gil-Brusola, Ana, Gimeno, Concepción, Gimeno-Gascón, Adelina, Gomila-Sard, Bárbara, González-Granda, Damiana, Gonzalo-Jiménez, Nieves, Guna-Serrano, María Remedio, López-Hontangas, José Luis, Martín-González, Coral, Moreno-Muñoz, Rosario, Navarro, David, Navarro, María, Orta, Nieves, Pérez, Elvira, Prat, Josep, Rodríguez, Juan Carlos, Ruiz-García, María Montserrat, Vanaclocha, Hermelinda, Colijn, Caroline, and Comas, Iñaki

Abstract

BACKGROUND: Whole genome sequencing provides better delineation of transmission clusters in Mycobacterium tuberculosis than traditional methods. However, its ability to reveal individual transmission links within clusters is limited. Here, we used a 2-step approach based on Bayesian transmission reconstruction to (1) identify likely index and missing cases, (2) determine risk factors associated with transmitters, and (3) estimate when transmission happened. METHODS AND FINDINGS: We developed our transmission reconstruction method using genomic and epidemiological data from a population-based study from Valencia Region, Spain. Tuberculosis (TB) incidence during the study period was 8.4 cases per 100,000 people. While the study is ongoing, the sampling frame for this work includes notified TB cases between 1 January 2014 and 31 December 2016. We identified a total of 21 transmission clusters that fulfilled the criteria for analysis. These contained a total of 117 individuals diagnosed with active TB (109 with epidemiological data). Demographic characteristics of the study population were as follows: 80/109 (73%) individuals were Spanish-born, 76/109 (70%) individuals were men, and the mean age was 42.51 years (SD 18.46). We found that 66/109 (61%) TB patients were sputum positive at diagnosis, and 10/109 (9%) were HIV positive. We used the data to reveal individual transmission links, and to identify index cases, missing cases, likely transmitters, and associated transmission risk factors. Our Bayesian inference approach suggests that at least 60% of index cases are likely misidentified by local public health. Our data also suggest that factors associated with likely transmitters are different to those of simply being in a transmission cluster, highlighting the importance of differentiating between these 2 phenomena. Our data suggest that type 2 diabetes mellitus is a risk factor associated with being a transmitter (odds ratio 0.19 [95% CI 0.02-1.10], p < 0.003). Fina

Published
2019

16. DNA amplification fingerprinting for subtyping Neisseria gonorrhoeae strains

Author

Camarena, Juan J., Nogueira, Jose M., Dasi, Miguel A., Moreno, Fermin, Garcia, Rosa, Ledesma, Eduardo, Llorca, Julia, and Hernandez, Javier

Subjects
DNA testing -- Analysis, Neisseria gonorrhoeae -- Identification and classification, Gene amplification -- Evaluation, Health
Abstract

Background and Objectives: DNA amplification fingerprinting is used in most epidemiologic studies as a substitute for conventional typing methods. DNA amplification fingerprinting and conventional typing methods were compared in this epidemiologic study of Neisseria gonorrhoeae. Goal of This Study: To differentiate 70 Neisseria gonorrhoeae isolates from untreated patients with urogenital gonococcal infection. Study Design: Gonococcal strains were characterized by auxotyping, serotyping, plasmid profile, antibiotic sensitivity, and DNA amplification fingerprinting. The method of unweighted pair-group average linkage was used for cluster analysis. Discriminatory power was calculated applying Simpson's index. Results: Amplification of Neisseria gonorrhoeae DNA with primers OPA-03 and OPA-13 produced well-resolved patterns of 15 and 22 DNA fragments, respectively, with a discriminatory power (0.978 with OPA-13 and 0.967 with OPA-03) comparable to that obtained with auxotyping/serotyping combination (D:0.968) or with auxotype/serotype/plasmid profile combination (D:0.983). Correlation between DNA amplification fingerprinting pattern and auxotype (serotype class was not always uniform. Some strains with the same auxotype/serotype-/plasmid profile were subdivided by DNA amplification fingerprinting, and vice versa. Conclusion: Although auxotype/serotype class and DNA amplification fingerprinting can be used in the epidemiologic characterization of strains, DNA amplification fingerprinting offers a better discriminatory index than the separate serotyping. It is especially useful for differentiating serologically identical strains and nontypable strains. A combination of serotyping and DNA amplification fingerprinting seems to be the best way to differentiate Neisseria gonorrhoeae strains in epidemiologic studies, bringing together the most simple techniques and the best discriminatory power among isolates., DNA amplification fingerprinting (DAF) appears to be a useful method of identifying different strains of Neisseria (N.) gonorrhoeae for epidemiological studies. N. gonorrhoeae is the organism responsible for gonorrhea. DAF of 70 N. gonorrhoeae isolates was compared with conventional typing methods including antibiotic sensitivity, plasmid profile, auxotyping and serotyping. DAF with two different primers identified 15 and 22 DNA fragments. When the strains were evaluated by a combination of auxotyping, serotyping and plasmid profile, 16 groups were identified. The discriminatory index of each method was similar to that found for DAF. The advantages of DAF are that the test is simple, reproducible and fast. Serotyping with monoclonal antibodies had the best discriminatory index.

Published
1995

17. Clinical factors associated with a Candida albicans Germ Tube Antibody positive test in Intensive Care Unit patients

Author

Pemán, Javier, Zaragoza, Rafael, Quindós Andrés, Guillermo, Alkorta, Miriam, Cuétara, María S., Camarena, Juan J., Ramírez, Paula, Giménez, María J., Martín Mazuelos, Estrella, Linares Sicilia, María J., Pontón, José, and Candida albicans Germ Tube Antibody Detection in Critically Ill Patients Study Group

Subjects
Male, law.invention, Cohort Studies, Medical microbiology, law, Amphotericin B, Candida albicans, Prospective Studies, Prospective cohort study, Aged, 80 and over, Immunoassay, biology, Candidiasis, INFECTIOUS DISEASES, Middle Aged, invasive candidiasis, Intensive care unit, Intensive Care Units, Infectious Diseases, fungal infections, Biomarker (medicine), Female, amphotericin-B, Research Article, medicine.drug, Cohort study, early diagnosis, medicine.medical_specialty, Critical Illness, Mycology, surgical patients, species infections, lcsh:Infectious and parasitic diseases, critically ill patiens, blood cultures, Internal medicine, medicine, Humans, lcsh:RC109-216, Intensive care medicine, Antibodies, Fungal, Aged, business.industry, medicine.disease, biology.organism_classification, antifungal therapy, Spain, Systemic candidiasis, business, systemic candidiasis
Abstract

Background Poor outcomes of invasive candidiasis (IC) are associated with the difficulty in establishing the microbiological diagnosis at an early stage. New scores and laboratory tests have been developed in order to make an early therapeutic intervention in an attempt to reduce the high mortality associated with invasive fungal infections. Candida albicans IFA IgG has been recently commercialized for germ tube antibody detection (CAGTA). This test provides a rapid and simple diagnosis of IC (84.4% sensitivity and 94.7% specificity). The aim of this study is to identify the patients who could be benefited by the use of CAGTA test in critical care setting. Methods A prospective, cohort, observational multicentre study was carried out in six medical/surgical Intensive care units (ICU) of tertiary-care Spanish hospitals. Candida albicans Germ Tube Antibody test was performed twice a week if predetermined risk factors were present, and serologically demonstrated candidiasis was considered if the testing serum dilution was ≥ 1:160 in at least one sample and no other microbiological evidence of invasive candidiasis was found. Results Fifty-three critically ill non-neutropenic patients (37.7% post surgery) were included. Twenty-two patients (41.5%) had CAGTA-positive results, none of them with positive blood culture for Candida. Neither corrected colonization index nor antifungal treatment had influence on CAGTA results. This finding could corroborate that the CAGTA may be an important biomarker to distinguish between colonization and infection in these patients. The presence of acute renal failure at the beginning of the study was more frequent in CAGTA-negative patients. Previous surgery was statistically more frequent in CAGTA-positive patients. Conclusions This study identified previous surgery as the principal clinical factor associated with CAGTA-positive results and emphasises the utility of this promising technique, which was not influenced by high Candida colonization or antifungal treatment. Our results suggest that detection of CAGTA may be important for the diagnosis of invasive candidiasis in surgical patients admitted in ICU.

Published
2011

18. Clinical factors associated with a Candida albicans Germ Tube Antibody positive test in Intensive Care Unit patients

Author

Inmunología, microbiología y parasitología, Immunologia, mikrobiologia eta parasitologia, Pemán, Javier, Zaragoza, Rafael, Quindós Andrés, Guillermo, Alkorta, Miriam, Cuétara, María S., Camarena, Juan J., Ramírez, Paula, Giménez, María J., Martín Mazuelos, Estrella, Linares Sicilia, María J., Pontón, José, Candida albicans Germ Tube Antibody Detection in Critically Ill Patients Study Group, Inmunología, microbiología y parasitología, Immunologia, mikrobiologia eta parasitologia, Pemán, Javier, Zaragoza, Rafael, Quindós Andrés, Guillermo, Alkorta, Miriam, Cuétara, María S., Camarena, Juan J., Ramírez, Paula, Giménez, María J., Martín Mazuelos, Estrella, Linares Sicilia, María J., Pontón, José, and Candida albicans Germ Tube Antibody Detection in Critically Ill Patients Study Group

Abstract

Background: Poor outcomes of invasive candidiasis (IC) are associated with the difficulty in establishing the microbiological diagnosis at an early stage. New scores and laboratory tests have been developed in order to make an early therapeutic intervention in an attempt to reduce the high mortality associated with invasive fungal infections. Candida albicans IFA IgG has been recently commercialized for germ tube antibody detection (CAGTA). This test provides a rapid and simple diagnosis of IC (84.4% sensitivity and 94.7% specificity). The aim of this study is to identify the patients who could be benefited by the use of CAGTA test in critical care setting. Methods: A prospective, cohort, observational multicentre study was carried out in six medical/surgical Intensive care units (ICU) of tertiary-care Spanish hospitals. Candida albicans Germ Tube Antibody test was performed twice a week if predetermined risk factors were present, and serologically demonstrated candidiasis was considered if the testing serum dilution was >= 1: 160 in at least one sample and no other microbiological evidence of invasive candidiasis was found. Results: Fifty-three critically ill non-neutropenic patients (37.7% post surgery) were included. Twenty-two patients (41.5%) had CAGTA-positive results, none of them with positive blood culture for Candida. Neither corrected colonization index nor antifungal treatment had influence on CAGTA results. This finding could corroborate that the CAGTA may be an important biomarker to distinguish between colonization and infection in these patients. The presence of acute renal failure at the beginning of the study was more frequent in CAGTA-negative patients. Previous surgery was statistically more frequent in CAGTA-positive patients. Conclusions: This study identified previous surgery as the principal clinical factor associated with CAGTA-positive results and emphasises the utility of this promising technique, which was not influenced by high Candida c

Published
2011

20. PNEUMOCOCCAL PYOMYOSITIS

Author

Bret??n, J. Rafael, primary, Pi, Graciela, additional, Lacruz, Luc??a, additional, Calvo, Inmaculada, additional, Rodr??guez, Inmaculada, additional, S??nchez, Alejandro, additional, Camarena, Juan J., additional, and Hern??ndez, Roberto, additional

Published
2001
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22. Epidemiological Cutoff Values for Fluconazole, Itraconazole, Posaconazole, and Voriconazole for Six CandidaSpecies as Determined by the Colorimetric Sensititre YeastOne Method

Author

Cantón, Emilia, Pemán, Javier, Iñiguez, Carmen, Hervás, David, Lopez-Hontangas, Jose L., Pina-Vaz, Cidalia, Camarena, Juan J., Campos-Herrero, Isolina, García-García, Inmaculada, García-Tapia, Ana M., Guna, Remedios, Merino, Paloma, Pérez del Molino, Luisa, Rubio, Carmen, and Suárez, Anabel

Abstract

ABSTRACTIn the absence of clinical breakpoints (CBP), epidemiological cutoff values (ECVs) are useful to separate wild-type (WT) isolates (without mechanisms of resistance) from non-WT isolates (those that can harbor some resistance mechanisms), which is the goal of susceptibility tests. Sensititre YeastOne (SYO) is a widely used method to determine susceptibility of Candidaspp. to antifungal agents. The CLSI CBP have been established, but not for the SYO method. The ECVs for four azoles, obtained using MIC distributions determined by the SYO method, were calculated via five methods (three statistical methods and based on the MIC50and modal MIC). Respectively, the median ECVs (in mg/liter) of the five methods for fluconazole, itraconazole, posaconazole, and voriconazole (in parentheses: the percentage of isolates inhibited by MICs equal to or less than the ECVs; the number of isolates tested) were as follows: 2 (94.4%; 944), 0.5 (96.7%; 942), 0.25 (97.6%; 673), and 0.06 (96.7%; 849) for Candida albicans; 4 (86.1%; 642), 0.5 (99.4%; 642), 0.12 (93.9%; 392), and 0.06 (86.9%; 559) for C. parapsilosis; 8 (94.9%; 175), 1 (93.7%; 175), 2 (93.6%; 125), and 0.25 (90.4%; 167) for C. tropicalis; 128 (98.6%; 212), 4 (95.8%; 212), 4 (96.0%; 173), and 2 (98.5; 205) for C. glabrata; 256 (100%; 53), 1 (98.1%; 53), 1 (100%; 33), and 1 (97.9%; 48) for C. krusei; 4 (89.2%; 93), 0.5 (100%; 93), 0.25 (100%; 33), and 0.06 (87.7%; 73) for C. orthopsilosis. All methods included =94% of isolates and yielded similar ECVs (within 1 dilution). These ECVs would be suitable for monitoring emergence of isolates with reduced susceptibility by using the SYO method.

Published
2013
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23. Application of an Optimized and Highly Discriminatory Method Based on Arbitrarily Primed PCR for Epidemiologic Analysis of Methicillin-Resistant Staphylococcus aureusNosocomial Infections

Author

Olmos, Antonio, Camarena, Juan J., Nogueira, Jose´ M., Navarro, Juan C., Risen, Julia, and Sa´nchez, Roberto

Abstract

ABSTRACTThe optimization of an arbitrarily primed PCR method for typing 96 methicillin-resistant Staphylococcus aureus(MRSA) isolates was compared with pulsed-field gel electrophoresis. Identical results in the differentiation of MRSA clones and identification of the main cluster that included 82 strains (88% of patients) were obtained by both techniques.

Published
1998
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24. PNEUMOCOCCAL PYOMYOSITIS.

Author

Bretón, J. Rafael, Pi, Graciela, Lacruz, Lucía, Calvo, Inmaculada, Rodríguez, Inmaculada, Sánchez, Alejandro, Camarena, Juan J., and Hernández, Roberto

Published
2001
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25. Kinetic Patterns of Candida albicansGerm Tube Antibody in Critically Ill Patients: Influence on Mortality

Author

Zaragoza, Rafael, Pema´n, Javier, Quindo´s, Guillermo, Iruretagoyena, Jose R., Cue´tara, Mari´a S., Rami´rez, Paula, Go´mez, Maria D., Camarena, Juan J., Viudes, Angel, and Ponto´n, Jose´

Abstract

ABSTRACTThe influence of kinetic patterns of Candida albicansgerm tube antibodies (CAGTA) on mortality was analyzed in six intensive care units. Statistically significant lower mortality rates were found in patients with patterns of increasing CAGTA titers who had been treated with antifungal agents. Thus, antifungal treatment should be considered when CAGTA titers are increasing in critically ill patients.

Published
2009
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26. Epidemiological cutoff values for fluconazole, itraconazole, posaconazole, and voriconazole for six Candida species as determined by the colorimetric Sensititre YeastOne method.

Author

Cantón E, Pemán J, Iñiguez C, Hervás D, Lopez-Hontangas JL, Pina-Vaz C, Camarena JJ, Campos-Herrero I, García-García I, García-Tapia AM, Guna R, Merino P, Pérez del Molino L, Rubio C, and Suárez A

Subjects
Candida isolation & purification, Humans, Microbial Sensitivity Tests, Antifungal Agents pharmacology, Azoles pharmacology, Candida drug effects, Candidiasis microbiology
Abstract

In the absence of clinical breakpoints (CBP), epidemiological cutoff values (ECVs) are useful to separate wild-type (WT) isolates (without mechanisms of resistance) from non-WT isolates (those that can harbor some resistance mechanisms), which is the goal of susceptibility tests. Sensititre YeastOne (SYO) is a widely used method to determine susceptibility of Candida spp. to antifungal agents. The CLSI CBP have been established, but not for the SYO method. The ECVs for four azoles, obtained using MIC distributions determined by the SYO method, were calculated via five methods (three statistical methods and based on the MIC50 and modal MIC). Respectively, the median ECVs (in mg/liter) of the five methods for fluconazole, itraconazole, posaconazole, and voriconazole (in parentheses: the percentage of isolates inhibited by MICs equal to or less than the ECVs; the number of isolates tested) were as follows: 2 (94.4%; 944), 0.5 (96.7%; 942), 0.25 (97.6%; 673), and 0.06 (96.7%; 849) for Candida albicans; 4 (86.1%; 642), 0.5 (99.4%; 642), 0.12 (93.9%; 392), and 0.06 (86.9%; 559) for C. parapsilosis; 8 (94.9%; 175), 1 (93.7%; 175), 2 (93.6%; 125), and 0.25 (90.4%; 167) for C. tropicalis; 128 (98.6%; 212), 4 (95.8%; 212), 4 (96.0%; 173), and 2 (98.5; 205) for C. glabrata; 256 (100%; 53), 1 (98.1%; 53), 1 (100%; 33), and 1 (97.9%; 48) for C. krusei; 4 (89.2%; 93), 0.5 (100%; 93), 0.25 (100%; 33), and 0.06 (87.7%; 73) for C. orthopsilosis. All methods included ≥94% of isolates and yielded similar ECVs (within 1 dilution). These ECVs would be suitable for monitoring emergence of isolates with reduced susceptibility by using the SYO method.

Published
2013
Full Text
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