Your search keyword '"Tullis, D. Elizabeth"' showing total 13 results

1. Triaging Access to Critical Care Resources in Patients With Chronic Respiratory Diseases in the Event of a Major COVID-19 Surge: Key Highlights From the Canadian Thoracic Society (CTS) Position Statement.

Author

Gupta, Samir, Batt, Jane, Bourbeau, Jean, Chapman, Kenneth R., Gershon, Andrea, Granton, John, Hambly, Nathan, Hernandez, Paul, Kolb, Martin, Mehta, Sanjay, Mielniczuk, Lisa, Provencher, Steeve, Stephenson, Anne L., Swiston, John, Tullis, D. Elizabeth, Vozoris, Nicholas T., Wald, Joshua, Weatherald, Jason, and Bhutani, Mohit

Subjects

COVID-19, CHRONICALLY ill, PATIENT care, PRESBYCUSIS, CRITICAL care medicine

Abstract

Cystic Fibrosis Which cystic fibrosis patients have >80% predicted mortality during or in the 6 to 12 months after critical illness (level 1)? Level 3 criteria were validated in the GAP model, predicting a relatively low probability of 1-year mortality.[7] COPD Which COPD patients have >80% predicted mortality during or in the 6 to 12 months after critical illness (level 1)? Which COPD patients have >30% predicted mortality during or in the 6 to 12 months after critical illness (level 3)? Posted on March 28, 2020 https://www.corhealthontario.ca/Clinical-Triage-Protocol-for-Major-Surge-in-COVID-Pandemic-March-28-2020.pdf 5 S. Gupta, J. Batt, J. Bourbeau, Position statement from the Canadian Thoracic Society (CTS) on clinical triage thresholds in respiratory disease patients in the event of a major surge during the Covid-19 pandemic. [Extracted from the article]

Published

2020

2. A genome-wide association analysis reveals a potential role for recombination in the evolution of antimicrobial resistance in Burkholderia multivorans.

Author

Diaz Caballero, Julio, Guttman, David S., Clark, Shawn T., Hwang, David M., Yau, Yvonne C. W., Wang, Pauline W., Donaldson, Sylva L., Coburn, Bryan, Tullis, D. Elizabeth, and Waters, Valerie J.

Subjects

ANTI-infective agents, DRUG resistance in bacteria, BURKHOLDERIA infections, CYSTIC fibrosis, GENOMICS, MORTALITY

Abstract

Cystic fibrosis (CF) lung infections caused by members of the Burkholderia cepacia complex, such as Burkholderia multivorans, are associated with high rates of mortality and morbidity. We performed a population genomics study of 111 B. multivorans sputum isolates from one CF patient through three stages of infection including an early incident isolate, deep sampling of a one-year period of chronic infection occurring weeks before a lung transplant, and deep sampling of a post-transplant infection. We reconstructed the evolutionary history of the population and used a lineage-controlled genome-wide association study (GWAS) approach to identify genetic variants associated with antibiotic resistance. We found the incident isolate was basally related to the rest of the strains and more susceptible to antibiotics from three classes (β-lactams, aminoglycosides, quinolones). The chronic infection isolates diversified into multiple, distinct genetic lineages and showed reduced antimicrobial susceptibility to the same antibiotics. The post-transplant reinfection isolates derived from the same source as the incident isolate and were genetically distinct from the chronic isolates. They also had a level of susceptibility in between that of the incident and chronic isolates. We identified numerous examples of potential parallel pathoadaptation, in which multiple mutations were found in the same locus or even codon. The set of parallel pathoadaptive loci was enriched for functions associated with virulence and resistance. Our GWAS analysis identified statistical associations between a polymorphism in the ampD locus with resistance to β-lactams, and polymorphisms in an araC transcriptional regulator and an outer membrane porin with resistance to both aminoglycosides and quinolones. Additionally, these three loci were independently mutated four, three and two times, respectively, providing further support for parallel pathoadaptation. Finally, we identified a minimum of 14 recombination events, and observed that loci carrying putative parallel pathoadaptations and polymorphisms statistically associated with β-lactam resistance were over-represented in these recombinogenic regions. [ABSTRACT FROM AUTHOR]

Published

2018

3. Clinical Outcomes Associated with Achromobacter Species Infection in Patients with Cystic Fibrosis.

Author

Somayaji, Ranjani, Stanojevic, Sanja, Tullis, D. Elizabeth, Stephenson, Anne L., Ratjen, Felix, and Waters, Valerie

Subjects

CYSTIC fibrosis treatment, COMPARATIVE studies, CYSTIC fibrosis, GRAM-negative bacterial diseases, LUNGS, LUNG transplantation, RESEARCH methodology, MEDICAL cooperation, RESEARCH, EVALUATION research, PROPORTIONAL hazards models, RETROSPECTIVE studies, DISEASE progression, GRAM-negative aerobic bacteria, DISEASE complications

Abstract

Rationale: Achromobacter species are increasingly identified in individuals with cystic fibrosis (CF), but the clinical outcomes in these patients remain poorly understood.Objectives: We aimed to determine the association of Achromobacter infection on clinical outcomes in pediatric and adult patients with CF.Methods: A cohort study of pediatric and adult patients with CF was conducted from 1997 to 2014 in Toronto, Ontario, Canada. Achromobacter spp. infection was categorized as no history of infection, intermittent infection, and chronic infection (two or more positive cultures in the preceding 12 months). Cox models were used to estimate risk of death or transplantation. Mixed-effects models were used to assess odds of pulmonary exacerbations and effect on lung function (FEV1%) by Achromobacter spp.Results: A total of 1,103 patients were followed-up over the course of 18 years; 88 patients (7.3%) had one or more culture for Achromobacter species. Chronic Achromobacter infection was associated with a greater risk of death or transplantation compared with in patients with no history of infection (adjusted hazard ratio, 2.03; 95% confidence interval, 1.05-3.95; P = 0.036). Pulmonary exacerbations were more common in patients with chronic infection, but after adjusting for confounding factors, the effect was no longer significant. The chronic group had lower FEV1%, but it did not worsen after developing chronic infection.Conclusions: Patients with CF and chronic Achromobacter infection are at increased risk of death or transplantation. [ABSTRACT FROM AUTHOR]

Published

2017

4. Navigating social and ethical challenges of biobanking for human microbiome research.

Author

Chuong, Kim H., Hwang, David M., Tullis, D. Elizabeth, Waters, Valerie J., Yau, Yvonne C. W., Guttman, David S., and O'Doherty, Kieran C.

Subjects

BIOBANKS, HUMAN microbiota, SCIENCE & ethics, CYSTIC fibrosis, DISEASE progression, LUNG microbiology, COMMUNICATION, DIAGNOSIS, MEDICAL ethics, MEDICAL research, PRIVACY, PUBLIC health, PUBLIC opinion, RESEARCH funding, RESEARCH ethics, TISSUE banks, DISCLOSURE

Abstract

Background: Biobanks are considered to be key infrastructures for research development and have generated a lot of debate about their ethical, legal and social implications (ELSI). While the focus has been on human genomic research, rapid advances in human microbiome research further complicate the debate.Discussion: We draw on two cystic fibrosis biobanks in Toronto, Canada, to illustrate our points. The biobanks have been established to facilitate sample and data sharing for research into the link between disease progression and microbial dynamics in the lungs of pediatric and adult patients. We begin by providing an overview of some of the ELSI associated with human microbiome research, particularly on the implications for the broader society. We then discuss ethical considerations regarding the identifiability of samples biobanked for human microbiome research, and examine the issue of return of results and incidental findings. We argue that, for the purposes of research ethics oversight, human microbiome research samples should be treated with the same privacy considerations as human tissues samples. We also suggest that returning individual microbiome-related findings could provide a powerful clinical tool for care management, but highlight the need for a more grounded understanding of contextual factors that may be unique to human microbiome research.Conclusions: We revisit the ELSI of biobanking and consider the impact that human microbiome research might have. Our discussion focuses on identifiability of human microbiome research samples, and return of research results and incidental findings for clinical management. [ABSTRACT FROM AUTHOR]

Published

2017

5. Global Analysis of the Fungal Microbiome in Cystic Fibrosis Patients Reveals Loss of Function of the Transcriptional Repressor Nrg1 as a Mechanism of Pathogen Adaptation.

Author

Kim, Sang Hu, Clark, Shawn T., Surendra, Anuradha, Copeland, Julia K., Wang, Pauline W., Ammar, Ron, Collins, Cathy, Tullis, D. Elizabeth, Nislow, Corey, Hwang, David M., Guttman, David S., and Cowen, Leah E.

Subjects

COLLAGEN diseases, TRANSCRIPTIONAL repressor CTCF, FIBROSIS, HUMAN microbiota, FILAMENTATION instability, DISEASE risk factors

Abstract

The microbiome shapes diverse facets of human biology and disease, with the importance of fungi only beginning to be appreciated. Microbial communities infiltrate diverse anatomical sites as with the respiratory tract of healthy humans and those with diseases such as cystic fibrosis, where chronic colonization and infection lead to clinical decline. Although fungi are frequently recovered from cystic fibrosis patient sputum samples and have been associated with deterioration of lung function, understanding of species and population dynamics remains in its infancy. Here, we coupled high-throughput sequencing of the ribosomal RNA internal transcribed spacer 1 (ITS1) with phenotypic and genotypic analyses of fungi from 89 sputum samples from 28 cystic fibrosis patients. Fungal communities defined by sequencing were concordant with those defined by culture-based analyses of 1,603 isolates from the same samples. Different patients harbored distinct fungal communities. There were detectable trends, however, including colonization with Candida and Aspergillus species, which was not perturbed by clinical exacerbation or treatment. We identified considerable inter- and intra-species phenotypic variation in traits important for host adaptation, including antifungal drug resistance and morphogenesis. While variation in drug resistance was largely between species, striking variation in morphogenesis emerged within Candida species. Filamentation was uncoupled from inducing cues in 28 Candida isolates recovered from six patients. The filamentous isolates were resistant to the filamentation-repressive effects of Pseudomonas aeruginosa, implicating inter-kingdom interactions as the selective force. Genome sequencing revealed that all but one of the filamentous isolates harbored mutations in the transcriptional repressor NRG1; such mutations were necessary and sufficient for the filamentous phenotype. Six independent nrg1 mutations arose in Candida isolates from different patients, providing a poignant example of parallel evolution. Together, this combined clinical-genomic approach provides a high-resolution portrait of the fungal microbiome of cystic fibrosis patient lungs and identifies a genetic basis of pathogen adaptation. [ABSTRACT FROM AUTHOR]

Published

2015

6. Effects of Recipient Age and Diagnosis on Health-related Quality-of-Life Benefit of Lung Transplantation.

Author

Singer, Lianne G., Chowdhury, Noori A., Faughnan, Marie E., Granton, John, Keshavjee, Shaf, Marras, Theodore K., Tullis, D. Elizabeth, Waddell, Thomas K., and Tomlinson, George

Subjects

AGE distribution, CYSTIC fibrosis, HEALTH status indicators, HEALTH surveys, INTERSTITIAL lung diseases, LONGITUDINAL method, OBSTRUCTIVE lung diseases, LUNG transplantation, PULMONARY hypertension, QUALITY of life, RESEARCH funding, TRANSPLANTATION of organs, tissues, etc., TREATMENT effectiveness, QUALITY-adjusted life years

Abstract

Rationale: The average age of lung transplant recipients is increasing, and the mix of recipient indications for transplantation is changing. Objectives: To determine whether the health-related quality-of-life (HRQL) benefit of lung transplantation differs by recipient age and diagnosis. Methods: In this prospective cohort study, we obtained serial HRQL measurements in adults with advanced lung disease who subsequently underwent lung transplantation (2004-2012). HRQL assessments included the St. George's Respiratory Questionnaire, 36-Item Short-Form Health Survey (SF-36), EQ-5D, Standard Gamble, and Visual Analog Scale for current health. We used linear mixed effects models for associations between age or diagnosis and changes in HRQL with transplantation. To address potential survivorship bias, we fitted Markov models to the distribution of discrete post-transplant health states (HRQL better than pretransplant, not better, or dead) and estimated quality-adjusted life-years post-transplant. Measurements and Main Results: A total of 430 subjects were listed, 387 were transplanted, and 326 provided both pretransplant and post-transplant data. Transplantation conferred large improvements in all HRQL measures: St. George's change of -47 units (95% confidence interval, -48 to -44), 36-Item Short-Form Health Survey physical component summary score of 17.7 (16.5-18.9), EQ-5D of 0.27 (0.24-0.30), Standard Gamble of 0.48 (0.44-0.51), and Visual Analog of 44 (42-47). Age was not associated with meaningful differences in the HRQL benefits of transplantation. There was less HRQL benefit in interstitial lung disease than in cystic fibrosis. Conclusions: Lung transplantation confers large HRQL benefits, which vary by recipient diagnosis, but do not differ substantially in older recipients. [ABSTRACT FROM AUTHOR]

Published

2015

7. Analysis of the Cystic Fibrosis Lung Microbiota via Serial Illumina Sequencing of Bacterial 16S rRNA Hypervariable.

Author

Maughan, Heather, Wang, Pauline W., Caballero, Julio Diaz, Fung, Pauline, Yunchen Gong, Donaldson, Sylva L., Lijie Yuan, Keshavjee, Shaf, Yu Zhang, Yau, Yvonne C. W., Waters, Valerie J., Tullis, D. Elizabeth, Hwang, David M., and Guttman, David S.

Subjects

BACTERIA, NUCLEOTIDE sequence, MICROORGANISMS, RIBOSOMAL RNA, GENOMES, CYSTIC fibrosis, PATIENTS

Abstract

The characterization of bacterial communities using DNA sequencing has revolutionized our ability to study microbes in nature and discover the ways in which microbial communities affect ecosystem functioning and human health. Here we describe Serial Illumina Sequencing (SI-Seq): a method for deep sequencing of the bacterial 16S rRNA gene using next- generation sequencing technology. SI-Seq serially sequences portions of the V5, V6 and V7 hypervariable regions from barcoded 16S rRNA amplicons using an Illumina short-read genome analyzer. SI-Seq obtains taxonomic resolution similar to 454 pyrosequencing for a fraction of the cost, and can produce hundreds of thousands of reads per sample even with very high multiplexing. We validated SI-Seq using single species and mock community controls, and via a comparison to cystic fibrosis lung microbiota sequenced using 454 FLX Titanium. Our control runs show that SI-Seq has a dynamic range of at least five orders of magnitude, can classify >96% of sequences to the genus level, and performs just as well as 454 and paired-end Illumina methods in estimation of standard microbial ecology diversity measurements. We illustrate the utility of SI-Seq in a pilot sample of central airway secretion samples from cystic fibrosis patients. [ABSTRACT FROM AUTHOR]

Published

2012

8. Pulmonary Bacterial Communities in Surgically Resected Noncystic Fibrosis Bronchiectasis Lungs Are Similar to Those in Cystic Fibrosis.

Author

Maughan, Heather, Cunningham, Kristopher S., Wang, Pauline W., Yu Zhang, Cypel, Marcelo, Chaparro, Cecilia, Tullis, D. Elizabeth, Waddell, Thomas K., Keshavjee, Shaf, Liu, Mingyao, Guttman, David S., and Hwang, David M.

Abstract

Background. Recurrent bacterial infections play a key role in the pathogenesis of bronchiectasis, but conventional microbiologic methods may fail to identify pathogens in many cases. We characterized and compared the pulmonary bacterial communities of cystic fibrosis (CF) and non-CF bronchiectasis patients using a culture-independent molecular approach. Methods. Bacterial 16S rRNA gene libraries were constructed from lung tissue of 10 non-CF bronchiectasis and 21 CF patients, followed by DNA sequencing of isolates from each library. Community characteristics were analyzed and compared between the two groups. Results. A wide range of bacterial diversity was detected in both groups, with between 1 and 21 bacterial taxa found in each patient. Pseudomonas was the most common genus in both groups, comprising 49% of sequences detected and dominating numerically in 13 patients. Although Pseudomonas appeared to be dominant more often in CF patients than in non-CF patients, analysis of entire bacterial communities did not identify significant differences between these two groups. Conclusions. Our data indicate significant diversity in the pulmonary bacterial community of both CF and non-CF bronchiectasis patients and suggest that this community is similar in surgically resected lungs of CF and non-CF bronchiectasis patients. [ABSTRACT FROM AUTHOR]

Published

2012

9. Amiloride-insensitive nasal potential difference varies with the menstrual cycle in cystic fibrosis.

Author

Sweezey, Neil B., Smith, David, Corey, Mary, Ellis, Lynda, Carpenter, Susan, Tullis, D. Elizabeth, Durie, Peter, and O'Brodovich, Hugh M.

Published

2007

10. Clinical Manifestations of Cystic Fibrosis Among Patients With Diagnosis in Adulthood.

Author

Gilljam, Marita, Ellis, Lynda, Corey, Mary, Zielenski, Julian, Durie, Peter, and Tullis, D. Elizabeth

Subjects

CYSTIC fibrosis, GENETIC disorders, PANCREATIC diseases, LUNG diseases, DIAGNOSIS, DISEASES

Abstract

Objective: To define the clinical characteristics and diagnostic parameters of patients with cystic fibrosis (CF) diagnosed in adulthood. Design: Retrospective cohort study. Setting: Tertiary care center. Patients and methods: All patients with a diagnosis of CF made at the Toronto CF Clinics between 1960 and June 2001. Data were collected prospectively and analyzed retrospectively. Results: There were 73 of 1,051 patients (7%) with CF diagnosed in adulthood. Over time, an increasing number and proportion of patients received a diagnosis in adulthood: 27 patients (3%) before 1990, compared to 46 patients (18%) after 1990 (p <0.001). The mean sweat chloride level was lower for those with CF diagnosed as adults, compared to those with a diagnosis as children (75 ± 26 mmol/L and 100 ± 19 mmol/L, respectively; p <0.001) [mean ± SD], and adults were more likely to have pancreatic sufficiency (PS) than children (73% vs 13%, respectively; p < 0.0001). In 46 adults who received a diagnosis since 1990, the reason for the initial sweat test was pancreatitis (2 patients, 4%), pulmonary symptoms (18 patients, 39%), pulmonary and GI symptoms (10 patients, 22%), infertility (12 patients, 26%), and genetic screening (4 patients, 9%). Other manifestations were biliary cirrhosis (one patient) and diabetes mellitus (four patients, 9%). The diagnosis could be confirmed by sweat test alone in 30 of 46 patients (65%), by mutation analysis alone in 15 patients (33%), and by a combination in 31 patients (67%). Nasal potential difference (PD) measurements alone confirmed the diagnosis in the remaining 15 patients (33%). Conclusion: Patients with CF presenting in adulthood often have PS, inconclusive sweat test results, and a high prevalence of mutations that are not commonly seen in CF diagnosed in childhood. Although most patients have lung disease of variable degrees, single-organ manifestations such as congenital bilateral absence of the vas deferens and pancreatitis are seen. Repeated sweat tests and extensive mutation analysis are often required. Nasal PD may aid the diagnosis, but has not been standardized for clinical diagnosis. [ABSTRACT FROM AUTHOR]

Published

2004

11. The Repeatability of Forced Expiratory Volume Measurements in Adults With Cystic Fibrosis.

Author

Stanbrook, Matthew B., Corey, Mary, and Tullis, D. Elizabeth

Subjects

CYSTIC fibrosis, LUNG diseases, RESPIRATION, PULMONARY function tests, RESPIRATORY diseases, CLINICAL trials

Abstract

Study objective: To determine the repeatability of measurements of FEV[sub 1] in adults with lung disease due to cystic fibrosis (CF). Design: Single cohort study nested within a randomized controlled trial. Setting: Adult CF of a university teaching hospital. Subjects were participants in a randomized trial of an experimental mucolytic drug. Patients: Twenty-one adults (mean age, 27.5 ± 9.2 years [± SD]) with CF and mild-to-moderate airflow obstruction (FEV[sub 1] 70 ± 15% predicted). Patients were in clinically stable condition prior to and during the study. Interventions: Repeated FEV[sub 1] measurements were obtained at specific times of the day for 9 consecutive days, for a total of 31 measurements from each subject. Statistical measures of repeatability were calculated. Variation over the course of 1 day and variation from I day to the next were examined separately. Measurements and results: For day-to-day FEV[sub 1] measurements, the within-subject SD was 0.145 L (4.5% of predicted), indicating greater variation compared to values previously established in normal subjects. The coefficient of repeatability indicated that day-to-day measurements could differ by as much as 13% of predicted in the absence of clinical change. For measurements within a single day, variation was not observed to be greater than normal. Conclusions: In adults with CF, day-to-day variation in FEV[sub 1] measurements is greater than normal and similar to that seen in other obstructive lung diseases. Changes in FEV[sub 1] over time in adults with CF can likely be interpreted using the same criteria that apply to asthma or COPD. Key words: adult; cystic fibrosis; forced expiratory volume; reproducibility of results; respiratory function tests. [ABSTRACT FROM AUTHOR]

Published

2004

12. Pregnancy in Cystic Fibrosis.

Author

Gilljam, Marita, Antoniou, Maria, Shin, Janey, Dupuis, Annie, Corey, Mary, and Tullis, D. Elizabeth

Subjects

CYSTIC fibrosis, PREGNANCY complications, DIABETES, HUMAN fertility

Abstract

Objective: To assess the effect of pregnancy on pulmonary function and survival in women with cystic fibrosis (CF) and to assess the fetal outcome. Design: Cohort study. The data analyzed were collected from the Toronto CF database, chart review, and patient questionnaire. Setting: Tertiary-care center. Patients: All women with CF who, at the time of diagnosis or pregnancy, attended the Toronto Cystic Fibrosis Clinics between 1961 and 1998. Results: From 1963 to 1998, there were 92 pregnancies in 54 women. There were 11 miscarriages and 7 therapeutic abortions. Forty-nine women gave birth to 74 children. The mean follow-up time was 11 ± 8 years. One patient was lost to follow-up shortly after delivery, and one was lost after 12 years. The overall mortality rate was 19% (9 of 48 patients). Absence of Burkholderia cepacia (p < 0.001), pancreatic sufficiency (p = 0.01), and prepregnancy FEV[sub 1] > 50% predicted (p = 0.03) were associated with better survival rates. When adjusted for the same parameters, pregnancy did not affect survival compared to the entire adult female CF population. The decline in FEV[sub 1] was comparable to that in the total CF population. Three women had diabetes mellitus, and seven developed gestational diabetes. There were six preterm infants and one neonatal death. CF was diagnosed in two children. Conclusions: The maternal and fetal outcome is good for most women with CF. Risk factors for mortality are similar to those for the nonpregnant CF population. Pregnancies should be planned so that there is opportunity for counseling and optimization of the medical condition. Good communication between the CF team and the obstetrician is important. [ABSTRACT FROM AUTHOR]

Published

2000

13. Microbiome networks and change-point analysis reveal key community changes associated with cystic fibrosis pulmonary exacerbations.

Author

Layeghifard, Mehdi, Li, Hannah, Wang, Pauline W., Donaldson, Sylva L., Coburn, Bryan, Clark, Shawn T., Caballero, Julio Diaz, Zhang, Yu, Tullis, D. Elizabeth, Yau, Yvonne C. W., Waters, Valerie, Hwang, David M., and Guttman, David S.

Published

2019