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1. Considerations for the use of inhaled antibiotics for Pseudomonas aeruginosa in people with cystic fibrosis receiving CFTR modulator therapy

Author

Barry J Plant, Daniel Peckham, Pierre-Régis Burgel, Alan Smyth, Andreas Jung, Manfred Ballmann, Giovanni Taccetti, Harry Heijerman, Pavel Drevinek, Jochen G Mainz, and Carsten Schwarz

Subjects
Medicine, Diseases of the respiratory system, RC705-779
Abstract

The major cause of mortality in people with cystic fibrosis (pwCF) is progressive lung disease characterised by acute and chronic infections, the accumulation of mucus, airway inflammation, structural damage and pulmonary exacerbations. The prevalence of Pseudomonas aeruginosa rises rapidly in the teenage years, and this organism is the most common cause of chronic lung infection in adults with cystic fibrosis (CF). It is associated with an accelerated decline in lung function and premature death. New P. aeruginosa infections are treated with antibiotics to eradicate the organism, while chronic infections require long-term inhaled antibiotic therapy. The prevalence of P. aeruginosa infections has decreased in CF registries since the introduction of CF transmembrane conductance regulator modulators (CFTRm), but clinical observations suggest that chronic P. aeruginosa infections usually persist in patients receiving CFTRm. This indicates that pwCF may still need inhaled antibiotics in the CFTRm era to maintain long-term control of P. aeruginosa infections. Here, we provide an overview of the changing perceptions of P. aeruginosa infection management, including considerations on detection and treatment, the therapy burden associated with inhaled antibiotics and the potential effects of CFTRm on the lung microbiome. We conclude that updated guidance is required on the diagnosis and management of P. aeruginosa infection. In particular, we highlight a need for prospective studies to evaluate the consequences of stopping inhaled antibiotic therapy in pwCF who have chronic P. aeruginosa infection and are receiving CFTRm. This will help inform new guidelines on the use of antibiotics alongside CFTRm.

Published
2024
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2. Whole genomes from bacteria collected at diagnostic units around the world 2020

Author

Nag, Sidsel, Larsen, Gunhild, Szarvas, Judit, Birkedahl, Laura Elmlund Kohl, Gulyás, Gábor Máté, Ciok, Wojchiech Jakub, Lagermann, Timmie Mikkel, Tafaj, Silva, Bradbury, Susan, Collignon, Peter, Daley, Denise, Dougnon, Victorien, Fabiyi, Kafayath, Coulibaly, Boubacar, Dembélé, René, Nikiema, Georgette, Magloire, Natama, Ouindgueta, Isidore Juste, Hossain, Zenat Zebin, Begum, Anowara, Donchev, Deyan, Diggle, Mathew, Turnbull, LeeAnn, Lévesque, Simon, Berlinger, Livia, Sogaard, Kirstine Kobberoe, Guevara, Paula Diaz, Valderrama, Carolina Duarte, Maikanti, Panagiota, Amlerova, Jana, Drevinek, Pavel, Tkadlec, Jan, Dilas, Milica, Kaasch, Achim, Westh, Henrik Torkil, Bachtarzi, Mohamed Azzedine, Amhis, Wahiba, Salazar, Carolina Elisabeth Satán, Villacis, JoséEduardo, Lúzon, Mária Angeles Dominguez, Palau, Dámaris Berbel, Duployez, Claire, Paluche, Maxime, Asante-Sefa, Solomon, Moller, Mie, Ip, Margaret, Mareković, Ivana, Pál-Sonnevend, Agnes, Cocuzza, Clementiza Elvezia, Dambrauskiene, Asta, Macanze, Alexandre, Cossa, Anelsio, Mandomando, Inácio, Nwajiobi-Princewill, Philip, Okeke, Iruka N., Kehinde, Aderemi O., Adebiyi, Ini, Akintayo, Ifeoluwa, Popoola, Oluwafemi, Onipede, Anthony, Blomfeldt, Anita, Nyquist, Nora Elisabeth, Bocker, Kiri, Ussher, James, Ali, Amjad, Ullah, Nimat, Khan, Habibullah, Gustafson, Natalie Weiler, Jarrar, Ikhlas, Al-Hamad, Arif, Luvira, Viravarn, Paveenkittiporn, Wantana, Baran, Irmak, Mwansa, James C. L., Sikakwa, Linda, Yamba, Kaunda, Hendriksen, Rene Sjogren, and Aarestrup, Frank Moller

Published
2023
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3. Whole genomes from bacteria collected at diagnostic units around the world 2020

Author

Sidsel Nag, Gunhild Larsen, Judit Szarvas, Laura Elmlund Kohl Birkedahl, Gábor Máté Gulyás, Wojchiech Jakub Ciok, Timmie Mikkel Lagermann, Silva Tafaj, Susan Bradbury, Peter Collignon, Denise Daley, Victorien Dougnon, Kafayath Fabiyi, Boubacar Coulibaly, René Dembélé, Georgette Nikiema, Natama Magloire, Isidore Juste Ouindgueta, Zenat Zebin Hossain, Anowara Begum, Deyan Donchev, Mathew Diggle, LeeAnn Turnbull, Simon Lévesque, Livia Berlinger, Kirstine Kobberoe Sogaard, Paula Diaz Guevara, Carolina Duarte Valderrama, Panagiota Maikanti, Jana Amlerova, Pavel Drevinek, Jan Tkadlec, Milica Dilas, Achim Kaasch, Henrik Torkil Westh, Mohamed Azzedine Bachtarzi, Wahiba Amhis, Carolina Elisabeth Satán Salazar, JoséEduardo Villacis, Mária Angeles Dominguez Lúzon, Dámaris Berbel Palau, Claire Duployez, Maxime Paluche, Solomon Asante-Sefa, Mie Moller, Margaret Ip, Ivana Mareković, Agnes Pál-Sonnevend, Clementiza Elvezia Cocuzza, Asta Dambrauskiene, Alexandre Macanze, Anelsio Cossa, Inácio Mandomando, Philip Nwajiobi-Princewill, Iruka N. Okeke, Aderemi O. Kehinde, Ini Adebiyi, Ifeoluwa Akintayo, Oluwafemi Popoola, Anthony Onipede, Anita Blomfeldt, Nora Elisabeth Nyquist, Kiri Bocker, James Ussher, Amjad Ali, Nimat Ullah, Habibullah Khan, Natalie Weiler Gustafson, Ikhlas Jarrar, Arif Al-Hamad, Viravarn Luvira, Wantana Paveenkittiporn, Irmak Baran, James C. L. Mwansa, Linda Sikakwa, Kaunda Yamba, Rene Sjogren Hendriksen, and Frank Moller Aarestrup

Subjects
Science
Abstract

Abstract The Two Weeks in the World research project has resulted in a dataset of 3087 clinically relevant bacterial genomes with pertaining metadata, collected from 59 diagnostic units in 35 countries around the world during 2020. A relational database is available with metadata and summary data from selected bioinformatic analysis, such as species prediction and identification of acquired resistance genes.

Published
2023
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5. Reference percentiles for FEV1 and BMI in European children and adults with cystic fibrosis

Author

Boëlle Pierre-Yves, Viviani Laura, Busson Pierre-Francois, Olesen Hanne V, Ravilly Sophie, Stern Martin, Assael Baroukh M, Barreto Celeste, Drevinek Pavel, Thomas Muriel, Krivec Uros, Mei-Zahav Meir, Vibert Jean-François, Clement Annick, Mehta Anil, and Corvol Harriet

Subjects
Cystic fibrosis, Forced expiratory volume in one second, Body mass index, Registry, Medicine
Abstract

Abstract Background The clinical course of Cystic Fibrosis (CF) is usually measured using the percent predicted FEV1 and BMI Z-score referenced against a healthy population, since achieving normality is the ultimate goal of CF care. Referencing against age and sex matched CF peers may provide valuable information for patients and for comparison between CF centers or populations. Here, we used a large database of European CF patients to compute CF specific reference equations for FEV1 and BMI, derived CF-specific percentile charts and compared these European data to their nearest international equivalents. Methods 34859 FEV1 and 40947 BMI observations were used to compute European CF specific percentiles. Quantile regression was applied to raw measurements as a function of sex, age and height. Results were compared with the North American equivalent for FEV1 and with the WHO 2007 normative values for BMI. Results FEV1 and BMI percentiles illustrated the large variability between CF patients receiving the best current care. The European CF specific percentiles for FEV1 were significantly different from those in the USA from an earlier era, with higher lung function in Europe. The CF specific percentiles for BMI declined relative to the WHO standard in older children. Lung function and BMI were similar in the two largest contributing European Countries (France and Germany). Conclusion The CF specific percentile approach applied to FEV1 and BMI allows referencing patients with respect to their peers. These data allow peer to peer and population comparisons in CF patients.

Published
2012
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6. Use of colony-based bacterial strain typing for tracking the fate of Lactobacillus strains during human consumption

Author

Drevinek Pavel, Marchbank Angela, Mahenthiralingam Eshwar, Garaiova Iveta, and Plummer Sue

Subjects
Microbiology, QR1-502
Abstract

Abstract Background The Lactic Acid Bacteria (LAB) are important components of the healthy gut flora and have been used extensively as probiotics. Understanding the cultivable diversity of LAB before and after probiotic administration, and being able to track the fate of administered probiotic isolates during feeding are important parameters to consider in the design of clinical trials to assess probiotic efficacy. Several methods may be used to identify bacteria at the strain level, however, PCR-based methods such as Random Amplified Polymorphic DNA (RAPD) are particularly suited to rapid analysis. We examined the cultivable diversity of LAB in the human gut before and after feeding with two Lactobacillus strains, and also tracked the fate of these two administered strains using a RAPD technique. Results A RAPD typing scheme was developed to genetically type LAB isolates from a wide range of species, and optimised for direct application to bacterial colony growth. A high-throughput strategy for fingerprinting the cultivable diversity of human faeces was developed and used to determine: (i) the initial cultivable LAB strain diversity in the human gut, and (ii) the fate of two Lactobacillus strains (Lactobacillus salivarius NCIMB 30211 and Lactobacillus acidophilus NCIMB 30156) contained within a capsule that was administered in a small-scale human feeding study. The L. salivarius strain was not cultivated from the faeces of any of the 12 volunteers prior to capsule administration, but appeared post-feeding in four. Strains matching the L. acidophilus NCIMB 30156 feeding strain were found in the faeces of three volunteers prior to consumption; after taking the Lactobacillus capsule, 10 of the 12 volunteers were culture positive for this strain. The appearance of both Lactobacillus strains during capsule consumption was statistically significant (p < 0.05). Conclusion We have shown that genetic strain typing of the cultivable human gut microbiota can be evaluated using a high throughput RAPD technique based on single bacterial colonies. Validation of this strategy paves the way for future systematic studies on the fate and efficacy of bacterial probiotics during human clinical trials.

Published
2009
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8. Gene expression changes linked to antimicrobial resistance, oxidative stress, iron depletion and retained motility are observed when Burkholderia cenocepacia grows in cystic fibrosis sputum

Author

Ketchell Ian, Jones Andrew M, Ge Zhaoping, Holden Matthew TG, Drevinek Pavel, Gill Ryan T, and Mahenthiralingam Eshwar

Subjects
Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background Bacteria from the Burkholderia cepacia complex (Bcc) are the only group of cystic fibrosis (CF) respiratory pathogens that may cause death by an invasive infection known as cepacia syndrome. Their large genome (> 7000 genes) and multiple pathways encoding the same putative functions make virulence factor identification difficult in these bacteria. Methods A novel microarray was designed to the genome of Burkholderia cenocepacia J2315 and transcriptomics used to identify genes that were differentially regulated when the pathogen was grown in a CF sputum-based infection model. Sputum samples from CF individuals infected with the same B. cenocepacia strain as genome isolate were used, hence, other than a dilution into a minimal growth medium (used as the control condition), no further treatment of the sputum was carried out. Results A total of 723 coding sequences were significantly altered, with 287 upregulated and 436 downregulated; the microarray-observed expression was validated by quantitative PCR on five selected genes. B. cenocepacia genes with putative functions in antimicrobial resistance, iron uptake, protection against reactive oxygen and nitrogen species, secretion and motility were among the most altered in sputum. Novel upregulated genes included: a transmembrane ferric reductase (BCAL0270) implicated in iron metabolism, a novel protease (BCAL0849) that may play a role in host tissue destruction, an organic hydroperoxide resistance gene (BCAM2753), an oxidoreductase (BCAL1107) and a nitrite/sulfite reductase (BCAM1676) that may play roles in resistance to the host defenses. The assumptions of growth under iron-depletion and oxidative stress formulated from the microarray data were tested and confirmed by independent growth of B. cenocepacia under each respective environmental condition. Conclusion Overall, our first full transcriptomic analysis of B. cenocepacia demonstrated the pathogen alters expression of over 10% of the 7176 genes within its genome when it grows in CF sputum. Novel genetic pathways involved in responses to antimicrobial resistance, oxidative stress, and iron metabolism were revealed by the microarray analysis. Virulence factors such as the cable pilus and Cenocepacia Pathogenicity Island were unaltered in expression. However, B. cenocepacia sustained or increased expression of motility-associated genes in sputum, maintaining a potentially invasive phenotype associated with cepacia syndrome.

Published
2008
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9. Diversity of the parB and repA genes of the Burkholderia cepacia complex and their utility for rapid identification of Burkholderia cenocepacia

Author

Dowson Christopher G, Baldwin Adam, Drevinek Pavel, and Mahenthiralingam Eshwar

Subjects
Microbiology, QR1-502
Abstract

Abstract Background Burkholderia cenocepacia is the most prominent species of the B. cepacia complex (Bcc), a group of nine closely related and difficult to identify bacteria that cause serious infections in patients with cystic fibrosis. Despite its clinical relevance, identification of B. cenocepacia as a single species is unavailable, as it splits by a widely used recA gene-based PCR identification method into discrete phylogenetic subgroups IIIA, IIIB, IIIC and IIID. With the aim of identifying gene targets suitable for unified detection of B. cenocepacia strains, we examined sequence polymorphisms in the repA and parB genes. These essential genes are involved in the replication and partitioning of bacterial replicons, hence we also had the opportunity for the first time to investigate the evolution of the multireplicon (three chromosome) structure of Bcc genomes. Results Alignment of the repA and parB genes from publicly available Bcc genome sequences enabled the design of primers for their amplification and sequence analysis. Multilocus sequencing typing, a highly discriminatory method for Bcc species and strain discrimination, was used to select strains of unique sequence types (STs) that spanned the known Bcc genetic diversity. Sequence datasets of repA (83 isolates, 67 STs) and parB (120 isolates, 95 STs) genes from the second chromosome were aligned and examined phylogenetically to identify polymorphisms suitable for identification of B. cenocepacia. In contrast to parB, the Bcc repA sequences demonstrated distinct clustering of B. cenocepacia from other species, which enabled the design a species-specific multiplex PCR. The novel single-reaction B. cenocepacia detection method was tested on a panel of 142 different Bcc strains (142 STs) and distinguished recA groups IIIA, IIIB and IIID, from all other Bcc members with 100% sensitivity and 93% specificity. Conclusion The repA-based multiplex PCR is a useful aid to the rapid identification of the most clinically relevant B. cenocepacia recA subgroups IIIA, IIIB and IIID. Phylogenetic analysis of repA and parB genes demonstrated that acquisition of the second and third replicons of Bcc genomes occurred prior to their differentiation into discrete species and that the sharing of replicons across species had not occurred.

Published
2008
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10. The Role and Value of Professional Rapid Testing of Acute Respiratory Infections (ARIs) in Europe: A Special Focus on the Czech Republic, Poland, and Romania

Author

Pavel Drevinek, Robert Flisiak, Roxana Nemes, Katya A. Nogales Crespo, and Krzysztof Tomasiewicz

Subjects
acute respiratory infections, COVID-19, influenza, point-of-care testing, rapid testing, diagnostic testing, Medicine (General), R5-920
Abstract

This review aims to explore the role of professional diagnostic rapid testing of acute respiratory infections (ARIs), especially COVID-19 and influenza, ensuring proper disease management and treatment in Europe, and particularly in Czech Republic, Poland, and Romania. The paper was constructed based on a review of scientific evidence and national and international policies and recommendations, as well as a process of validation by four experts. The development of new testing technologies, treatment options, and increased awareness of the negative multidimensional impact of ARI profiles transformed differential diagnosis into a tangible and desirable reality. This review covers the following topics: (1) the multidimensional impact of ARIs, (2) ARI rapid diagnostic testing platforms and their value, (3) the policy landscape, (4) challenges and barriers to implementation, and (5) a set of recommendations illustrating a path forward. The findings indicate that rapid diagnostic testing, including at the point of care (POC), can have a positive impact on case management, antimicrobial and antibiotic stewardship, epidemiological surveillance, and decision making. Integrating this strategy will require the commitment of governments and the international and academic communities, especially as we identified room for improvement in the access and expansion of POC rapid testing in the focus countries and the inclusion of rapid testing in relevant policies.

Published
2024
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11. Epidemiology of Methicillin-Resistant Staphylococcus aureus in Slovakia, 2020 – Emergence of an Epidemic USA300 Clone in Community and Hospitals

Author

Jan Tkadlec, Anh Vu Le, Marie Brajerova, Anna Soltesova, Jozef Marcisin, Pavel Drevinek, and Marcela Krutova

Subjects
MRSA, PVL, USA300, Slovakia, CA-MRSA, spa typing, Microbiology, QR1-502
Abstract

ABSTRACT Methicillin-resistant Staphylococcus aureus (MRSA) is a leading cause of health care-associated infections. Additionally, over the decades, the spread of community-associated (CA-MRSA) clones has become a serious problem. The aim of this study was to gain data on the current epidemiology of MRSA in Slovakia. Between January 2020 and March 2020, single-patient MRSA isolates (invasive and/or colonizing) were collected in Slovakia from hospitalized inpatients (16 hospitals) or outpatients (77 cities). Isolates were characterized via antimicrobial susceptibility testing, spa typing, SCCmec typing, the detection of mecA/mecC, genes coding for Panton-Valentine leukocidin (PVL), and the arcA gene (part of the arginine catabolic mobile element [ACME]). Out of 412 isolates, 167 and 245 originated from hospitalized patients and outpatients, respectively. Inpatients were most likely older (P

Published
2023
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12. Elexacaftor-tezacaftor-ivacaftor in patients with cystic fibrosis ineligible for clinical trials: a 24-week observational study

Author

Libor Fila, Alzbeta Grandcourtova, Alena Bilkova, and Pavel Drevinek

Subjects
cystic fibrosis, variant specific therapy, elexacaftor-tezacaftor-ivacaftor, lung function, nutritional status, sweat chloride concentration, Therapeutics. Pharmacology, RM1-950
Abstract

Introduction: Seminal clinical trials with the triple combination of elexacaftor-tezacaftor-ivacaftor (ETI) demonstrated clinical efficacy in people with cystic fibrosis (pwCF) who carry at least one F508del mutation. However, due to exclusion criteria of these clinical trials, the effect of ETI was not studied in a substantial number of pwCF. Thus, we ran a single center trial to evaluate a clinical efficacy of ETI treatment in adult pwCF who were ineligible for enrollment in registration studies.Methods: PwCF on ETI with prior lumacaftor-ivacaftor therapy, severe airway obstruction, well-preserved lung function, or with airway infection with pathogens at risk of more rapid decline in lung function formed the study group, while all the others on ETI formed the control group. Lung function, nutritional status and sweat chloride concentration were assessed before and after initialization of ETI therapy over a 6-month period.Results: Approximately a half of the ETI-treated pwCF at the adult Prague CF center (49 of 96) were assigned to the study group. Their mean changes in body mass index ( + 1.04 kg/m2) and in sweat chloride concentration (−48.4 mmol/L) were similar to the control group ( + 1.02 kg/m2; −49.7 mmol/L), while the mean change in percent predicted forced expiratory volume in 1 s (ppFEV1; + 10.3 points) was significantly lower than in the control group ( + 15.8 points) (p = 0.0015). In the subgroup analysis, pwCF with severe airway obstruction (ppFEV1 90) showed a less potential for improvement in lung function during the ETI treatment than controls (median change in ppFEV1 + 4.9 points and + 9.5 points, respectively).Conclusion: PwCF not eligible for inclusion in clinical trials demonstrated improvement in lung function and nutritional status following the initiation of treatment with the ETI combination. Moderate increase in ppFEV1 was observed in those with severe airway obstruction or well-preserved lung function.

Published
2023
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15. Building global development strategies for cf therapeutics during a transitional cftr modulator era

Author

Mayer-Hamblett, N., van Koningsbruggen-Rietschel, S., Nichols, D.P., VanDevanter, D.R., Davies, J.C., Lee, T., Durmowicz, A.G., Ratjen, F., Konstan, M.W., Pearson, K., Bell, S.C., Clancy, J.P., Taylor-Cousar, J.L., De Boeck, K., Donaldson, S.H., Downey, D.G., Flume, P.A., Drevinek, P., Goss, C.H., Fajac, I., Magaret, A.S., Quon, B.S., Singleton, S.M., VanDalfsen, J.M., and Retsch-Bogart, G.Z.

Published
2020
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17. The association of a reduced susceptibility to moxifloxacin in causative Clostridium (Clostridioides) difficile strain with the clinical outcome of patients

Author

Marcela Krutova, Vaclav Capek, Elka Nycova, Sabina Vojackova, Magda Balejova, Lenka Geigerova, Renata Tejkalova, Lenka Havlinova, Iva Vagnerova, Pavel Cermak, Lenka Ryskova, Petr Jezek, Dana Zamazalova, Denisa Vesela, Alice Kucharova, Dana Nemcova, Martina Curdova, Otakar Nyc, and Pavel Drevinek

Subjects
Clostridium difficile infection, Clostridioides difficile infection, Czech Republic, PCR ribotype 001, PCR ribotype 176, Moxifloxacin, Infectious and parasitic diseases, RC109-216
Abstract

Abstract Objectives To investigate the relationship between Clostridium (Clostridioides) difficile strain characteristics and C. difficile infection (CDI) outcome. Methods Between October and December 2017, 16 hospitals collected epidemiological data according to the European Centre for Disease Prevention and Control (ECDC) surveillance protocol for CDI. C. difficile isolates were characterized by ribotyping, toxin genes detection and antibiotic susceptibility testing to metronidazole, vancomycin and moxifloxacin. Results The overall mean CDI incidence density was 4.5 [95% CI 3.6–5.3] cases per 10,000 patient-days. From the 433 CDI cases, 330 (76.2%) were healthcare-associated, 52 (12.0%) cases were community-associated or of unknown origin and 51 (11.8%) CDI cases recurrent; a complicated course of CDI was reported in 65 cases (15.0%). Eighty-eight (20.3%) of patients died and 59 of them within 30 days after the CDI diagnosis. From the 379 C. difficile isolates, the most prevalent PCR ribotypes were 001 (n = 127, 33.5%) and 176 (n = 44, 11.6%). A total of 186 (49.1%) isolates showed a reduced susceptibility to moxifloxacin (> 4 mg/L) and 96.4% of them had Thr82Ile in the GyrA. Nineteen isolates revealed reduced susceptibility to metronidazole and two isolates to vancomycin (> 2 mg/L). A fatal outcome was associated with a reduced susceptibility to moxifloxacin, the advanced age of the patients and a complicated course of CDI (p

Published
2020
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18. Factors for severe outcomes following SARS-CoV-2 infection in people with cystic fibrosis in Europe

Author

Andreas Jung, Annalisa Orenti, Fiona Dunlevy, Elina Aleksejeva, Egil Bakkeheim, Vladimir Bobrovnichy, Siobhán B. Carr, Carla Colombo, Harriet Corvol, Rebecca Cosgriff, Géraldine Daneau, Deniz Dogru, Pavel Drevinek, Andrea Dugac Vukic, Isabelle Fajac, Alice Fox, Stojka Fustik, Vincent Gulmans, Satenik Harutyunyan, Elpis Hatziagorou, Irena Kasmi, Hana Kayserová, Elena Kondratyeva, Uroš Krivec, Halyna Makukh, Kestutis Malakauskas, Edward F. McKone, Meir Mei-Zahav, Isabelle de Monestrol, Hanne Vebert Olesen, Rita Padoan, Tsitsino Parulava, Maria Dolores Pastor-Vivero, Luísa Pereira, Guergana Petrova, Andreas Pfleger, Liviu Pop, Jacqui G. van Rens, Milan Rodic´, Marc Schlesser, Valérie Storms, Oxana Turcu, Lukasz Woz´niacki, Panayiotis Yiallouros, Anna Zolin, Damian G. Downey, and Lutz Naehrlich

Subjects
Medicine
Abstract

Background Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection in people with cystic fibrosis (pwCF) can lead to severe outcomes. Methods In this observational study, the European Cystic Fibrosis Society Patient Registry collected data on pwCF and SARS-CoV-2 infection to estimate incidence, describe clinical presentation and investigate factors associated with severe outcomes using multivariable analysis. Results Up to December 31, 2020, 26 countries reported information on 828 pwCF and SARS-CoV-2 infection. Incidence was 17.2 per 1000 pwCF (95% CI: 16.0–18.4). Median age was 24 years, 48.4% were male and 9.4% had lung transplants. SARS-CoV-2 incidence was higher in lung-transplanted (28.6; 95% CI: 22.7–35.5) versus non-lung-transplanted pwCF (16.6; 95% CI: 15.4–17.8) (p≤0.001). SARS-CoV-2 infection caused symptomatic illness in 75.7%. Factors associated with symptomatic SARS-CoV-2 infection were age >40 years, at least one F508del mutation and pancreatic insufficiency. Overall, 23.7% of pwCF were admitted to hospital, 2.5% of those to intensive care, and regretfully 11 (1.4%) died. Hospitalisation, oxygen therapy, intensive care, respiratory support and death were 2- to 6-fold more frequent in lung-transplanted versus non-lung-transplanted pwCF. Factors associated with hospitalisation and oxygen therapy were lung transplantation, cystic fibrosis-related diabetes (CFRD), moderate or severe lung disease and azithromycin use (often considered a surrogate marker for Pseudomonas aeruginosa infection and poorer lung function). Conclusion SARS-CoV-2 infection yielded high morbidity and hospitalisation in pwCF. PwCF with forced expiratory volume in 1 s

Published
2021
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19. Whole genomes from bacteria collected at diagnostic units around the world 2020

Author

Nag, S, Larsen, G, Szarvas, J, Birkedahl, L, Gulyas, G, Ciok, W, Lagermann, T, Tafaj, S, Bradbury, S, Collignon, P, Daley, D, Dougnon, V, Fabiyi, K, Coulibaly, B, Dembele, R, Nikiema, G, Magloire, N, Ouindgueta, I, Hossain, Z, Begum, A, Donchev, D, Diggle, M, Turnbull, L, Levesque, S, Berlinger, L, Sogaard, K, Guevara, P, Valderrama, C, Maikanti, P, Amlerova, J, Drevinek, P, Tkadlec, J, Dilas, M, Kaasch, A, Westh, H, Bachtarzi, M, Amhis, W, Salazar, C, Villacis, J, Luzon, M, Palau, D, Duployez, C, Paluche, M, Asante-Sefa, S, Moller, M, Ip, M, Marekovic, I, Pal-Sonnevend, A, Cocuzza, C, Dambrauskiene, A, Macanze, A, Cossa, A, Mandomando, I, Nwajiobi-Princewill, P, Okeke, I, Kehinde, A, Adebiyi, I, Akintayo, I, Popoola, O, Onipede, A, Blomfeldt, A, Nyquist, N, Bocker, K, Ussher, J, Ali, A, Ullah, N, Khan, H, Gustafson, N, Jarrar, I, Al-Hamad, A, Luvira, V, Paveenkittiporn, W, Baran, I, Mwansa, J, Sikakwa, L, Yamba, K, Hendriksen, R, Aarestrup, F, Nag S., Larsen G., Szarvas J., Birkedahl L. E. K., Gulyas G. M., Ciok W. J., Lagermann T. M., Tafaj S., Bradbury S., Collignon P., Daley D., Dougnon V., Fabiyi K., Coulibaly B., Dembele R., Nikiema G., Magloire N., Ouindgueta I. J., Hossain Z. Z., Begum A., Donchev D., Diggle M., Turnbull L. A., Levesque S., Berlinger L., Sogaard K. K., Guevara P. D., Valderrama C. D., Maikanti P., Amlerova J., Drevinek P., Tkadlec J., Dilas M., Kaasch A., Westh H. T., Bachtarzi M. A., Amhis W., Salazar C. E. S., Villacis J. E., Luzon M. A. D., Palau D. B., Duployez C., Paluche M., Asante-Sefa S., Moller M., Ip M., Marekovic I., Pal-Sonnevend A., Cocuzza C. E., Dambrauskiene A., Macanze A., Cossa A., Mandomando I., Nwajiobi-Princewill P., Okeke I. N., Kehinde A. O., Adebiyi I., Akintayo I., Popoola O., Onipede A., Blomfeldt A., Nyquist N. E., Bocker K., Ussher J., Ali A., Ullah N., Khan H., Gustafson N. W., Jarrar I., Al-Hamad A., Luvira V., Paveenkittiporn W., Baran I., Mwansa J. C. L., Sikakwa L., Yamba K., Hendriksen R. S., Aarestrup F. M., Nag, S, Larsen, G, Szarvas, J, Birkedahl, L, Gulyas, G, Ciok, W, Lagermann, T, Tafaj, S, Bradbury, S, Collignon, P, Daley, D, Dougnon, V, Fabiyi, K, Coulibaly, B, Dembele, R, Nikiema, G, Magloire, N, Ouindgueta, I, Hossain, Z, Begum, A, Donchev, D, Diggle, M, Turnbull, L, Levesque, S, Berlinger, L, Sogaard, K, Guevara, P, Valderrama, C, Maikanti, P, Amlerova, J, Drevinek, P, Tkadlec, J, Dilas, M, Kaasch, A, Westh, H, Bachtarzi, M, Amhis, W, Salazar, C, Villacis, J, Luzon, M, Palau, D, Duployez, C, Paluche, M, Asante-Sefa, S, Moller, M, Ip, M, Marekovic, I, Pal-Sonnevend, A, Cocuzza, C, Dambrauskiene, A, Macanze, A, Cossa, A, Mandomando, I, Nwajiobi-Princewill, P, Okeke, I, Kehinde, A, Adebiyi, I, Akintayo, I, Popoola, O, Onipede, A, Blomfeldt, A, Nyquist, N, Bocker, K, Ussher, J, Ali, A, Ullah, N, Khan, H, Gustafson, N, Jarrar, I, Al-Hamad, A, Luvira, V, Paveenkittiporn, W, Baran, I, Mwansa, J, Sikakwa, L, Yamba, K, Hendriksen, R, Aarestrup, F, Nag S., Larsen G., Szarvas J., Birkedahl L. E. K., Gulyas G. M., Ciok W. J., Lagermann T. M., Tafaj S., Bradbury S., Collignon P., Daley D., Dougnon V., Fabiyi K., Coulibaly B., Dembele R., Nikiema G., Magloire N., Ouindgueta I. J., Hossain Z. Z., Begum A., Donchev D., Diggle M., Turnbull L. A., Levesque S., Berlinger L., Sogaard K. K., Guevara P. D., Valderrama C. D., Maikanti P., Amlerova J., Drevinek P., Tkadlec J., Dilas M., Kaasch A., Westh H. T., Bachtarzi M. A., Amhis W., Salazar C. E. S., Villacis J. E., Luzon M. A. D., Palau D. B., Duployez C., Paluche M., Asante-Sefa S., Moller M., Ip M., Marekovic I., Pal-Sonnevend A., Cocuzza C. E., Dambrauskiene A., Macanze A., Cossa A., Mandomando I., Nwajiobi-Princewill P., Okeke I. N., Kehinde A. O., Adebiyi I., Akintayo I., Popoola O., Onipede A., Blomfeldt A., Nyquist N. E., Bocker K., Ussher J., Ali A., Ullah N., Khan H., Gustafson N. W., Jarrar I., Al-Hamad A., Luvira V., Paveenkittiporn W., Baran I., Mwansa J. C. L., Sikakwa L., Yamba K., Hendriksen R. S., and Aarestrup F. M.

Abstract

The Two Weeks in the World research project has resulted in a dataset of 3087 clinically relevant bacterial genomes with pertaining metadata, collected from 59 diagnostic units in 35 countries around the world during 2020. A relational database is available with metadata and summary data from selected bioinformatic analysis, such as species prediction and identification of acquired resistance genes.

Published
2023

20. Microbiological diagnostics of bloodstream infections in Europe—an ESGBIES survey

Author

Idelevich, E.A., Seifert, H., Sundqvist, M., Scudeller, L., Amit, S., Balode, A., Bilozor, A., Drevinek, P., Kocak Tufan, Z., Koraqi, A., Lamy, B., Mareković, I., Miciuleviciene, J., Müller Premru, M., Pascual, A., Pournaras, S., Saegeman, V., Schønheyder, H.C., Schrenzel, J., Strateva, T., Tilley, R., Wiersinga, W.J., Zabicka, D., Carmeli, Y., and Becker, K.

Published
2019
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22. Direct detection of ESKAPEc pathogens from whole blood using the T2Bacteria Panel allows early antimicrobial stewardship intervention in patients with sepsis

Author

Pavel Drevinek, Jakub Hurych, Milena Antuskova, Jan Tkadlec, Jan Berousek, Zuzana Prikrylova, Jiri Bures, Jaromir Vajter, Martin Soucek, Jan Masopust, Vendula Martinkova, Jaroslava Adamkova, Veronika Hysperska, and Eliska Bebrova

Subjects
antimicrobial stewardship, bacteremia, blood culture, rapid diagnostics, sepsis, T2MR, Microbiology, QR1-502
Abstract

Abstract In the microbiological diagnosis of bloodstream infections (BSI), blood culture (BC) is considered the gold standard test despite its limitations such as low sensitivity and slow turnaround time. A new FDA‐cleared and CE‐marked platform utilizing magnetic resonance to detect amplified DNA of the six most common and/or problematic BSI pathogens (Enterococcus faecium, Staphylococcus aureus, Klebsiella pneumoniae, Acinetobacter baumannii, Pseudomonas aeruginosa, and Escherichia coli; referred to as ESKAPEc) is available and may shorten the time to diagnosis and potentially improve antimicrobial utilization. Whole blood samples from hospitalized patients with clinical signs of sepsis were analyzed using the T2Bacteria Panel (T2Biosystems) and compared to simultaneously collected BC. Discrepant results were evaluated based on clinical infection criteria, combining supporting culture results and the opinion of treating physicians. A total of 55 samples from 53 patients were evaluated. The sensitivity and specificity of the T2Bacteria panel was 94% (16 out of 17 detections of T2Bacteria‐targeted organisms) and 100%, respectively, with 36.4% (8 of 22) causes of BSI detected only by this method. The T2Bacteria Panel detected pathogens on average 55 hours faster than standard BC. In our study, 9 of 15 patients with positive T2Bacteria Panel results received early‐targeted antibiotic therapy and/or modification of antimicrobial treatment based on T2Bacteria Panel findings. Given the high reliability, faster time to detection, and easy workflow, the technique qualifies as a point‐of‐care testing approach.

Published
2021
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24. Limited diagnostic possibilities for bloodstream infections with broad‐range methods: A promising PCR/electrospray ionization‐mass spectrometry platform is no longer available

Author

Jan Tkadlec, Eliska Bebrova, Jan Berousek, Tomas Vymazal, Jaroslava Adamkova, Vendula Martinkova, Claus Moser, Dragos Florea, and Pavel Drevinek

Subjects
16S PCR, bloodstream infections, broad‐range PCR, molecular diagnostics, PCR/ESI‐MS, Microbiology, QR1-502
Abstract

Abstract Fast and accurate detection of causative agents of bloodstream infections remains a challenge of today's microbiology. We compared the performance of cutting‐edge technology based on polymerase chain reaction coupled with electrospray ionization‐mass spectrometry (PCR/ESI‐MS) with that of conventional broad‐range 16S rRNA PCR and blood culture to address the current diagnostic possibilities for bloodstream infections. Of 160 blood samples tested, PCR/ESI‐MS revealed clinically meaningful microbiological agents in 47 samples that were missed by conventional diagnostic approaches (29.4% of all analyzed samples). Notably, PCR/ESI‐MS shortened the time to positivity of the blood culture‐positive samples by an average of 34 hr. PCR/ESI‐MS technology substantially improved current diagnostic tools and represented an opportunity to make bloodstream infections diagnostics sensitive, accurate, and timely with a broad spectrum of microorganisms covered.

Published
2020
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26. The Intestinal Carriage of Plasmid-Mediated Colistin-Resistant Enterobacteriaceae in Tertiary Care Settings

Author

Jan Tkadlec, Alzbeta Kalova, Marie Brajerova, Tereza Gelbicova, Renata Karpiskova, Eva Smelikova, Otakar Nyc, Pavel Drevinek, and Marcela Krutova

Subjects
E. coli, colistin, mcr, Czech Republic, IncX4, silent carriage, Therapeutics. Pharmacology, RM1-950
Abstract

Background: In order to estimate the prevalence of plasmid borne colistin resistance and to characterize in detail the mcr-positive isolates, we carried out a sentinel testing survey on the intestinal carriage of plasmid-mediated colistin-resistant Enterobacteriaceae in hospitalized patients. Methods: Between June 2018 and September 2019, 1922 faecal samples from hospitalised patients were analysed by selective culture in presence of colistin (3.5 mg/L), and in parallel by direct detection of the mcr-1 to mcr-8 genes by qPCR. The mcr-positive isolates were characterised by whole-genome sequencing. Results: The prevalence of the mcr-1 gene was 0.21% (n = 4/1922); the mcr-2 to 8 genes were not detected. The mcr-1 gene was found to be localised in the IncX4 (n = 3) and IncHI2 (n = 1) plasmid type. One Escherichia coli isolate was susceptible to colistin due to the inactivation of the mcr-1 gene through the insertion of the IS2 element; however, the colistin resistance was inducible by culture in low concentrations of colistin. One human mcr-1 positive E. coli isolate was related genetically to the mcr-1 E. coli isolate derived from turkey meat of Czech origin. Conclusions:mcr-mediated colistin resistance currently poses little threat to patients hospitalised in Czech healthcare settings. The presence of the mcr-1 gene in the human population has a possible link to domestically produced, retail meat.

Published
2021
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27. Biofilm Formation among Stenotrophomonas maltophilia Isolates Has Clinical Relevance: The ANSELM Prospective Multicenter Study

Author

Arianna Pompilio, Marco Ranalli, Alessandra Piccirilli, Mariagrazia Perilli, Dragana Vukovic, Branislava Savic, Marcela Krutova, Pavel Drevinek, Daniel Jonas, Ersilia V. Fiscarelli, Vanessa Tuccio Guarna Assanti, María M. Tavío, Fernando Artiles, and Giovanni Di Bonaventura

Subjects
Stenotrophomonas maltophilia, biofilm formation, clinical relevance, antibiotic resistance, multicenter study, Biology (General), QH301-705.5
Abstract

The ability to form biofilms is a recognized trait of Stenotrophomonas maltophilia, but the extent of its clinical relevance is still unclear. The present multicenter prospective study (ANSELM) aims at investigating the association between biofilm formation and clinical outcomes of S. maltophilia infections. One hundred and nine isolates were collected from various geographical origins and stratified according to their clinical relevance. Biofilm formation was evaluated by the microtiter plate assay and correlated with microbiological and clinical data from the associated strains. Antibiotic susceptibility of the planktonic cells was tested by the disk diffusion technique, while antibiotic activity against mature biofilms was spectrophotometrically assessed. Most strains (91.7%) were able to form biofilm, although bloodborne strains produced biofilm amounts significantly higher than strains causing hospital- rather than community-acquired infections, and those recognized as “definite” pathogens. Biofilm formation efficiency was positively correlated with mechanical ventilation (p = 0.032), whereas a negative relationship was found with antibiotic resistance (r2 = 0.107; p < 0.001), specifically in the case of the pathogenic strains. Mature S. maltophilia biofilms were markedly more resistant (up to 128 times) to cotrimoxazole and levofloxacin compared with their planktonic counterparts, especially in the case of bloodborne strains. Our findings indicate that biofilm formation by S. maltophilia is obviously a contributing factor in the pathogenesis of infections, especially in deep ones, thus warranting additional studies with larger cohort of patients and isolates.

Published
2020
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28. Ivacaftor in cystic fibrosis adults: Czech experience with six years of follow-up

Author

Libor Fila, Lucie Valentova Bartakova, Alzbeta Grandcourtova, Miloslav Marel, Radovan Drnek, Alena Bilkova, Milan Macek, and Pavel Drevinek

Subjects
cystic fibrosis, adults, lung disease, ivacaftor, Medicine
Abstract

Aims: Ivacaftor is a revolutionary treatment option for cystic fibrosis (CF) patients with G551D and other gating mutations. The aim of this study was to evaluate the clinical status of patients on ivacaftor who were followed for up to 6 years together with an evaluation of ivacaftor therapy in one patient with an initial FEV1 less than 40% of predicted value. Methods: Data on development of clinical status and sinopulmonary-related therapies were obtained from patient health records during ivacaftor treatment lasting for up to six years and were compared with an equivalent period before ivacaftor administration. Results: Five CF adults with a median age 28.6 years (range 21.4-35.6 years) with median FEV1 45% pred. (range 16-85% pred.) were included in the study. Four subjects were also participants in the STRIVE and PERSIST studies. Altogether, twenty-four patient-years of ivacaftor treatment were analyzed. The median FEV1 decline per year decreased from -4.5 to -0.9% pred. (P = 0.043). Reduction in number of days on antibiotic treatment and hospital stays was 21% (P < 0.001) and 75% (P = 0.003), respectively. Improvement and stabilization of lung function was observed for up to six years of treatment. In a patient with severe airway obstruction, an increase in the FEV1 value (30.4% from baseline) was documented during the first twelve months of treatment. Conclusion: Ivacaftor therapy resulted in improved and stabilized lung function in up to six years of treatment with a reduction in number of days on antibiotic treatment and hospital stays. Its efficiency was also displayed in a patient with severe airway obstruction.

Published
2016
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29. Increasing incidence of Clostridium difficile ribotype 001 associated with severe course of the infection and previous fluoroquinolone use in the Czech Republic, 2015

Author

Krutova, M., Matejkova, J., Drevinek, P., Kuijper, E. J., Nyc, O., Tejkalova, Renata, Petrlova, Katarina, Hanslianova, Marketa, Balejova, Magda, Paleckova, Vera, Melichar, Antonin, Ryskova, Lenka, Nemcova, Dana, Vesela, Denisa, Rumlerova, Miloslava, Havlinova, Lenka, Nyc, Otakar, Zamazalova, Dana, Laskafeldova, Katerina, Vagnerova, Iva, Uhorskai, Pavlina, Geigerova, Lenka, Jezek, Petr, Hajna, Marketa, Kucharova, Alice, Bartonikova, Natasa, Curdova, Martina, Vanis, Vaclav, Skacani, Helena, and on behalf of the study group

Published
2017
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30. What matters in chronic Burkholderia cenocepacia infection in cystic fibrosis: Insights from comparative genomics.

Author

Jaroslav Nunvar, Vaclav Capek, Karel Fiser, Libor Fila, and Pavel Drevinek

Subjects
Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5
Abstract

Burkholderia cenocepacia causes severe pulmonary infections in cystic fibrosis (CF) patients. Since the bacterium is virtually untreatable by antibiotics, chronic infections persist for years and might develop into fatal septic pneumonia (cepacia syndrome, CS). To devise new strategies to combat chronic B. cenocepacia infections, it is essential to obtain comprehensive knowledge about their pathogenesis. We conducted a comparative genomic analysis of 32 Czech isolates of epidemic clone B. cenocepacia ST32 isolated from various stages of chronic infection in 8 CF patients. High numbers of large-scale deletions were found to occur during chronic infection, affecting preferentially genomic islands and nonessential replicons. Recombination between insertion sequences (IS) was inferred as the mechanism behind deletion formation; the most numerous IS group was specific for the ST32 clone and has undergone transposition burst since its divergence. Genes functionally related to transition metal metabolism were identified as hotspots for deletions and IS insertions. This functional category was also represented among genes where nonsynonymous point mutations and indels occurred parallelly among patients. Another category exhibiting parallel mutations was oxidative stress protection; mutations in catalase KatG resulted in impaired detoxification of hydrogen peroxide. Deep sequencing revealed substantial polymorphism in genes of both categories within the sputum B. cenocepacia ST32 populations, indicating extensive adaptive evolution. Neither oxidative stress response nor transition metal metabolism genes were previously reported to undergo parallel evolution during chronic CF infection. Mutations in katG and copper metabolism genes were overrepresented in patients where chronic infection developed into CS. Among professional phagocytes, macrophages use both hydrogen peroxide and copper for their bactericidal activity; our results thus tentatively point to macrophages as suspects in pathogenesis towards the fatal CS.

Published
2017
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34. The Effect of 2-Thiocyanatopyridine Derivative 11026103 on Burkholderia Cenocepacia: Resistance Mechanisms and Systemic Impact

Author

Jaroslav Nunvar, Andrew M. Hogan, Silvia Buroni, Svetlana Savina, Vadim Makarov, Silvia T. Cardona, and Pavel Drevinek

Subjects
Burkholderia cenocepacia, chemical mutagenesis, RNA-Seq, whole-genome sequencing, Tn-Seq, chemical genetics, Therapeutics. Pharmacology, RM1-950
Abstract

Bacteria of the Burkholderia cepacia complex (Bcc) are associated with significant decline of lung functions in cystic fibrosis patients. Bcc infections are virtually impossible to eradicate due to their irresponsiveness to antibiotics. The 2-thiocyanatopyridine derivative 11026103 is a novel, synthetic compound active against Burkholderia cenocepacia. To characterize mechanisms of resistance to 11026103, B. cenocepacia was subjected to chemical mutagenesis, followed by whole genome sequencing. Parallel mutations in resistant isolates were localized in a regulatory protein of the efflux system Resistance-Nodulation-Division (RND)-9 (BCAM1948), RNA polymerase sigma factor (BCAL2462) and its cognate putative anti-sigma factor (BCAL2461). Transcriptomic analysis identified positive regulation of a major facilitator superfamily (MFS) efflux system BCAL1510-1512 by BCAL2462. Artificial overexpression of both efflux systems increased resistance to the compound. The effect of 11026103 on B. cenocepacia was analyzed by RNA-Seq and a competitive fitness assay utilizing an essential gene knockdown mutant library. 11026103 exerted a pleiotropic effect on transcription including profound downregulation of cluster of orthologous groups (COG) category “Translation, ribosomal structure, and biogenesis”. The competitive fitness assay identified many genes which modulated susceptibility to 11026103. In summary, 11026103 exerts a pleiotropic cellular response in B. cenocepacia which can be prevented by efflux system-mediated export.

Published
2019
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37. Understanding the Pathogenicity of Burkholderia contaminans, an Emerging Pathogen in Cystic Fibrosis.

Author

Jaroslav Nunvar, Lucie Kalferstova, Ruhi A M Bloodworth, Michal Kolar, Jose Degrossi, Silvina Lubovich, Silvia T Cardona, and Pavel Drevinek

Subjects
Medicine, Science
Abstract

Several bacterial species from the Burkholderia cepacia complex (Bcc) are feared opportunistic pathogens that lead to debilitating lung infections with a high risk of developing fatal septicemia in cystic fibrosis (CF) patients. However, the pathogenic potential of other Bcc species is yet unknown. To elucidate clinical relevance of Burkholderia contaminans, a species frequently isolated from CF respiratory samples in Ibero-American countries, we aimed to identify its key virulence factors possibly linked with an unfavorable clinical outcome. We performed a genome-wide comparative analysis of two isolates of B. contaminans ST872 from sputum and blood culture of a female CF patient in Argentina. RNA-seq data showed significant changes in expression for quorum sensing-regulated virulence factors and motility and chemotaxis. Furthermore, we detected expression changes in a recently described low-oxygen-activated (lxa) locus which encodes stress-related proteins, and for two clusters responsible for the biosynthesis of antifungal and hemolytic compounds pyrrolnitrin and occidiofungin. Based on phenotypic assays that confirmed changes in motility and in proteolytic, hemolytic and antifungal activities, we were able to distinguish two phenotypes of B. contaminans that coexisted in the host and entered her bloodstream. Whole genome sequencing revealed that the sputum and bloodstream isolates (each representing a distinct phenotype) differed by over 1,400 mutations as a result of a mismatch repair-deficient hypermutable state of the sputum isolate. The inferred lack of purifying selection against nonsynonymous mutations and the high rate of pseudogenization in the derived isolate indicated limited evolutionary pressure during evolution in the nutrient-rich, stable CF sputum environment. The present study is the first to examine the genomic and transcriptomic differences between longitudinal isolates of B. contaminans. Detected activity of a number of putative virulence factors implies a genuine pathogenic nature of this novel Bcc species.

Published
2016
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38. Recommendations for the classification of diseases as CFTR-related disorders

Author

Bombieri, C., Claustres, M., De Boeck, K., Derichs, N., Dodge, J., Girodon, E., Sermet, I., Schwarz, M., Tzetis, M., Wilschanski, M., Bareil, C., Bilton, D., Castellani, C., Cuppens, H., Cutting, G.R., Drevínek, P., Farrell, P., Elborn, J.S., Jarvi, K., Kerem, B., Kerem, E., Knowles, M., Macek, M., Jr, Munck, A., Radojkovic, D., Seia, M., Sheppard, D.N., Southern, K.W., Stuhrmann, M., Tullis, E., Zielenski, J., Pignatti, P.F., and Ferec, C.

Published
2011
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42. Speeding up access to new drugs for CF: Considerations for clinical trial design and delivery

Author

Davies, JC, Drevinek, P, Elborn, JS, Kerem, E, Lee, T, European CF Society (ECFS) Strategic Planning Task Force on ‘Speeding up access to new 4 drugs for CF’, Amaral, MD, and De Boeck, K

Subjects
0301 basic medicine, Pulmonary and Respiratory Medicine, Cystic Fibrosis, Process (engineering), Respiratory System, Cystic Fibrosis Transmembrane Conductance Regulator, 03 medical and health sciences, 0302 clinical medicine, Drug Development, Membrane Transport Modulators, Drug Discovery, Humans, Medicine, Drug pipeline, Pharmaceutical industry, Clinical Trials as Topic, business.industry, Task force, Clinical study design, 1103 Clinical Sciences, Public relations, CFTR modulators, Quality Improvement, Clinical trial design, 030104 developmental biology, 030228 respiratory system, Drug development, Research Design, Mutation, Pediatrics, Perinatology and Child Health, business, European CF Society (ECFS) Strategic Planning Task Force on ‘Speeding up access to new 4 drugs for CF’, Patient organisations
Abstract

The last decade has witnessed developments in the CF drug pipeline which are both exciting and unprecedented, bringing with them previously unconsidered challenges. The Task Force group was brought together to consider these challenges and possible strategies to address them. Over the last 18 months, we have discussed internally and gathered views from a broad range of individuals representing patient organisations, clinical and research teams, the pharmaceutical industry and regulatory agencies. In this and the accompanying article, we discuss two main areas of focus: i) optimising trial design and delivery for speed and efficiency; ii) drug development for patients with rare CFTR mutations. We propose some strategies to tackle the challenges ahead and highlight areas where further thought is needed. We see this as the start of a process rather than the end and hope herewith to engage the wider community in seeking solutions to improved treatments for all patients with CF.

Published
2019

49. Multilocus sequence typing breathes life into a microbial metagenome.

Author

Eshwar Mahenthiralingam, Adam Baldwin, Pavel Drevinek, Elke Vanlaere, Peter Vandamme, John J LiPuma, and Chris G Dowson

Subjects
Medicine, Science
Abstract

Shot-gun sequencing of DNA isolated from the environment and the assembly of metagenomes from the resulting data has considerably advanced the study of microbial diversity. However, the subsequent matching of these hypothetical metagenomes to cultivable microorganisms is a limitation of such cultivation-independent methods of population analysis. Using a nucleotide sequence-based genetic typing method, multilocus sequence typing, we were able for the first time to match clonal cultivable isolates to a published and controversial bacterial metagenome, Burkholderia SAR-1, which derived from analysis of the Sargasso Sea. The matching cultivable isolates were all associated with infection and geographically widely distributed; taxonomic analysis demonstrated they were members of Burkholderia cepacia complex Group K. Comparison of the Burkholderia SAR-1 metagenome to closely related B. cepacia complex genomes indicated that it was greater than 98% intact in terms of conserved genes, and it also shared complete sequence identity with the cultivable isolates at random loci beyond the genes sampled by the multilocus sequence typing. Two features of the extant cultivable clones support the argument that the Burkholderia SAR-1 sequence may have been a contaminant in the original metagenomic survey: (i) their growth in conditions reflective of sea water was poor, suggesting the ocean was not their preferred habitat, and (ii) several of the matching isolates were epidemiologically linked to outbreaks of infection that resulted from contaminated medical devices or products, indicating an adaptive fitness of this bacterial strain towards contamination-associated environments. The ability to match identical cultivable strains of bacteria to a hypothetical metagenome is a unique feature of nucleotide sequence-based microbial typing methods; such matching would not have been possible with more traditional methods of genetic typing, such as those based on pattern matching of genomic restriction fragments or amplified DNA fragments. Overall, we have taken the first steps in moving the status of the Burkholderia SAR-1 metagenome from a hypothetical entity towards the basis for life of cultivable strains that may now be analysed in conjunction with the assembled metagenomic sequence data by the wider scientific community.

Published
2006
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