Your search keyword '"Carr SB"' showing total 179 results

1. ECFS standards of care on CFTR-related disorders: Towards a comprehensive program for affected individuals

Author

De Wachter, E, De Boeck, K, Sermet-Gaudelus, I, Simmonds, NJ, Munck, A, Naehrlich, L, Barben, J, Boyd, C, Veen, SJ, Carr, SB, Fajac, I, Farrell, PM, Girodon, E, Gonska, T, Grody, WW, Jain, M, Jung, A, Kerem, E, Raraigh, KS, van Koningsbruggen-Rietschel, S, Waller, MD, Southern, KW, and Castellani, C

Published

2024

2. Impact of elexacaftor/tezacaftor/ivacaftor on fat-soluble vitamin levels in children with cystic fibrosis

Author

Schembri, L, primary, Warraich, S, additional, Bentley, S, additional, Carr, SB, additional, and Balfour-Lynn, IM, additional

Published

2023

3. Pregnancy rates and outcomes in women with cystic fibrosis in the UK: comparisons with the general population before and after the introduction of disease‐modifying treatment, 2003–17

Author

Esan, OB, primary, Schlüter, DK, additional, Phillips, R, additional, Cosgriff, R, additional, Paranjothy, S, additional, Williams, D, additional, Norman, R, additional, Carr, SB, additional, Duckers, J, additional, and Taylor‐Robinson, D, additional

Published

2021

4. Pregnancy rates and outcomes in women with cystic fibrosis in the UK: comparisons with the general population before and after the introduction of disease‐modifying treatment, 2003–17.

Author

Esan, OB, Schlüter, DK, Phillips, R, Cosgriff, R, Paranjothy, S, Williams, D, Norman, R, Carr, SB, Duckers, J, and Taylor‐Robinson, D

Subjects

PREGNANCY outcomes, CYSTIC fibrosis, ABORTION, CYSTIC fibrosis transmembrane conductance regulator

Abstract

Objective: To compare pregnancy rates and outcomes for women with cystic fibrosis in the UK with those of the general population and assess the effect of the introduction of disease‐modifying treatment. Design: A population‐based longitudinal study, 2003–17. Setting: United Kingdom. Population: Women aged 15–44 years in the UK cystic fibrosis (CF) Registry compared with women in England and Wales. Methods: We calculated pregnancy and live‐birth rates for the CF population and the general population of England and Wales. For women with CF we compared pregnancy rates before and after ivacaftor was introduced in 2013. We further used CF registry data to assess pregnancy outcomes for mothers with CF, and to assess the relationship between maternal pre‐pregnancy lung function and nutritional status and child gestational age. Main outcome measures: Pregnancy and live‐birth rates and child gestational age. Results: Of 3831 women with CF, 661 reported 818 pregnancies. Compared with the general population, the pregnancy rate was 3.3 times lower in the CF population (23.5 versus 77.7 per 1000 woman‐years); the live‐birth rate was 3.5 times lower (17.4 versus 61.4 per 1000 woman‐years) with 70% of pregnancies in CF women resulting in live births; termination of pregnancy rates were also lower (9% versus 22%). Pregnancy rates increased post‐ivacaftor for eligible women with CF, from 29.7 to 45.7 per 1000 woman‐years. There was no association between pre‐pregnancy lung function/nutrition status and gestational age. Conclusions: Pregnancy rates in women with CF are about one‐third of the rates in the general population with favourable outcomes, and increased for eligible women post‐ivacaftor. Pregnancy rates in women with CF are about a third of the rate in England and Wales with 70% live births. Ivacaftor increases the rate. [ABSTRACT FROM AUTHOR]

Published

2022

5. LUNG FUNCTION DECLINE IN CHILDHOOD: LONGITUDINAL ANALYSIS OF REGISTRY DATA IN THE US AND UK

Author

Schlueter, DK, Ostrenga, J, Carr, SB, Fink, A, Szczesniak, RD, Keogh, RH, Charman, S, Marshall, B, Goss, CH, and Taylor-Robinson, D

Published

2019

6. Fair selection of participants in clinical trials: The challenge to push the envelope further

Author

Davies, JC, Scott, S, Dobra, R, Brendell, R, Brownlee, K, Carr, SB, Cosgriff, R, Simmonds, NJ, London Network of Clinical Trials Accelerator Platform sites, Jahan, R, Jones, A, Matthews, J, Brown, S, Galono, K, Miles, K, Pao, C, Shafi, N, Watson, D, Orchard, C, Davies, G, Pike, K, Shah, S, Bossley, CJ, Fong, T, Macedo, P, Ruiz, G, Waller, M, and Baker, L

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, Registry, Cystic Fibrosis, Allocation, Respiratory System, Eligibility Determination, Ethics, Research, Resource Allocation, Clinical trials, medicine, Humans, Intensive care medicine, Selection (genetic algorithm), Clinical Trials as Topic, Health Equity, business.industry, Patient Selection, Equity (finance), 1103 Clinical Sciences, Equity, Clinical trial, London Network of Clinical Trials Accelerator Platform sites, Pediatrics, Perinatology and Child Health, business, Envelope (motion), Information Systems

Published

2019

7. Pulmonary exacerbations in patients with primary ciliary dyskinesia: an expert consensus definition for use in clinical trials

Author

Lucas, JS, Gahleitner, F, Amorim, A, Boon, M, Brown, P, Constant, C, Cook, S, Crowley, S, Destouches, DMS, Eber, E, Mussaffi, H, Haarman, E, Harris, A, Koerner-Rettberg, C, Kuehni, CE, Latzin, P, Loebinger, MR, Lorent, N, Maitre, B, Moreno-Galdo, A, Nielsen, KG, Ozcelik, U, Philipsen, LKD, Pohunek, P, Polverino, E, Rademacher, J, Robinson, P, Snijders, D, Yiallouros, P, Carr, SB, Lucas, JS, Gahleitner, F, Amorim, A, Boon, M, Brown, P, Constant, C, Cook, S, Crowley, S, Destouches, DMS, Eber, E, Mussaffi, H, Haarman, E, Harris, A, Koerner-Rettberg, C, Kuehni, CE, Latzin, P, Loebinger, MR, Lorent, N, Maitre, B, Moreno-Galdo, A, Nielsen, KG, Ozcelik, U, Philipsen, LKD, Pohunek, P, Polverino, E, Rademacher, J, Robinson, P, Snijders, D, Yiallouros, P, and Carr, SB

Abstract

Pulmonary exacerbations are a cause of significant morbidity in patients with primary ciliary dyskinesia (PCD) and are frequently used as an outcome measure in clinical research into chronic lung diseases. So far, there has been no consensus on the definition of pulmonary exacerbations in PCD. 30 multidisciplinary experts and patients developed a consensus definition for children and adults with PCD. Following a systematic review, the panel used a modified Delphi process with a combination of face-to-face meetings and e-surveys to develop a definition that can be used in research settings for children and adults with PCD. A pulmonary exacerbation was defined by the presence of three or more of the following seven items: 1) increased cough, 2) change in sputum volume and/or colour, 3) increased shortness of breath perceived by the patient or parent, 4) decision to start or change antibiotic treatment because of perceived pulmonary symptoms, 5) malaise, tiredness, fatigue or lethargy, 6) new or increased haemoptysis, and 7) temperature >38°C. The consensus panel proposed that the definition should be used for future clinical trials. The definition should be validated and the usability assessed during these studies.

Published

2019

8. S60 Upper vs. lower airway microbiological culture in children with respiratory symptoms

Author

Gardner, LE, primary, Hogg, C, additional, Carr, SB, additional, Shoemark, A, additional, Marsh, G, additional, and Davies, JC, additional

Published

2019

9. P240 Lung function and low bone mineral density in cystic fibrosis

Author

Edwards, DK, primary, Carr, SB, additional, and Cullinan, P, additional

Published

2019

10. P012 Preliminary experience of the use of oral posaconazole and terbinafine to treat lomentospora prolificans and scedosporium apiospermum in children with cystic fibrosis

Author

Bentley, Sian, primary, Balfour-Lynn, IM, additional, and Carr, SB, additional

Published

2019

11. A national study of non-Invasive ventilation and clinical outcomes in Cystic Fibrosis

Author

Archangelidi, O, Simmonds, NJ, Carr, SB, and Cullinan, P

Subjects

Respiratory System, 1103 Clinical Sciences

Published

2017

12. Data Resource Profile: The UK Cystic Fibrosis Registry

Author

Taylor-Robinson, D, Archangelidi, O, Carr, SB, Cosgriff, R, Gunn, E, Keogh, RH, MacDougall, A, Newsome, S, Schlüter, DK, Stanojevic, S, Bilton, D, and CF-EpinNet collaboration

Subjects

1117 Public Health And Health Services, Epidemiology, 0104 Statistics, CF-EpinNet collaboration

Published

2017

13. P8 Bone mineral density in children and adolescents with cystic fibrosis, should we be doing less monitoring?

Author

O’Toole, CF, primary, Bush, A, additional, and Carr, SB, additional

Published

2018

14. Recovery of baseline lung function after pulmonary exacerbation in children with primary ciliary dyskinesia

Author

Sunther, M, Bush, A, Hogg, C, McCann, L, and Carr, SB

Subjects

pulmonary exacerbation, Respiratory System, 1114 Paediatrics And Reproductive Medicine, lung function, bronchiectasis and primary ciliary dyskinesia

Abstract

RATIONALE: Spirometry in children with cystic fibrosis (CF) frequently fails to return to baseline after treatment for a pulmonary exacerbation. It is unclear whether the same is true for children with primary ciliary dyskinesia (PCD). OBJECTIVES: To determine in children with PCD treated with intravenous antibiotics for a pulmonary exacerbation: (1) the proportion who recover to baseline forced expiratory volume at 1 sec (FEV1 ) within 3 months after treatment and (2) to try to identify factors which are associated with failure to regain pre-exacerbation FEV1 . METHODS: Cohort study using the PCD database for children at the Royal Brompton Hospital, 2003-2013. We selected the first pulmonary exacerbation treated with intravenous antibiotics. The best FEV1 within 3 months after treatment was compared to the best FEV1 in the 12 months before treatment (baseline). Recovery to baseline was defined as any FEV1 after treatment that was greater than or equal to 90% of the baseline FEV1 . RESULTS: 32/150 children (21%) had at least one pulmonary exacerbation. 23/30 (77%) regained baseline spirometry within 3 months of treatment. There was no difference between responders and non-responders in any baseline characteristics. CONCLUSIONS: Around 25% of children with PCD fail to recover to baseline lung function within 3 months following treatment for a pulmonary exacerbation, similar to CF. Better treatment strategies are needed, and the results also suggest that prevention of exacerbations would be a useful end-point in clinical trials. Pediatr Pulmonol. 2016;9999:XX-XX. © 2016 Wiley Periodicals, Inc.

Published

2016

15. P246 The impact the introduction of a universal payment by results annual tariff cf centres upon the north south divide in england

Author

Nyangoma, SO, primary, Cullinan, P, additional, and Carr, SB, additional

Published

2017

16. P250 A national study of non-invasive ventilation and clinical outcomes in cystic fibrosis

Author

Archangelidi, O, primary, Simmonds, NJ, additional, Carr, SB, additional, and Cullinan, P, additional

Published

2017

17. S42 Eradication success of non-tuberculous mycobacterial infections in a paediatric cystic fibrosis population

Author

Hughes, DA, primary, Malfitano, A, additional, Davenport, A, additional, and Carr, SB, additional

Published

2016

18. P220 Using funnel plots to make meaningful centre comparisons

Author

Pierotti, L, primary, Mohammed, MA, additional, Wildman, M, additional, Bilton, D, additional, Boote, J, additional, Carr, SB, additional, Collins, K, additional, Cullinan, P, additional, Elston, C, additional, Harrison, S, additional, Norman, P, additional, and MacNeill, SJ, additional

Published

2015

19. Airway function in infants newly diagnosed with cystic fibrosis

Author

Ranganathan, SC, Dezateux, C., Bush, A., Carr, SB, Castle, RA, Madge, S., Price, J., Stroobant, J., Wade, A., Wallis, C., and Stocks, J.

Published

2001

20. An evaluation of two aerosol delivery systems for rhDNase

Author

Shah, PL, primary, Scott, SF, additional, Geddes, DM, additional, Conway, S, additional, Watson, A, additional, Nazir, T, additional, Carr, SB, additional, Wallis, C, additional, Marriott, C, additional, and Hodson, ME, additional

Published

1997

21. Lung function is abnormal in 3-month-old infants with cystic fibrosis diagnosed by newborn screening.

Author

Hoo AF, Thia LP, Nguyen TT, Bush A, Chudleigh J, Lum S, Ahmed D, Lynn IB, Carr SB, Chavasse RJ, Costeloe KL, Price J, Shankar A, Wallis C, Wyatt HA, Wade A, Stocks J, London Cystic Fibrosis Collaboration, Hoo, Ah-Fong, and Thia, Lena P

Abstract

Background: Long-term benefits of newborn screening (NBS) for cystic fibrosis (CF) have been established with respect to nutritional status, but effects on pulmonary health remain unclear.Hypothesis: With early diagnosis and commencement of standardised treatment, lung function at ∼3 months of age is normal in NBS infants with CF.Methods: Lung clearance index (LCI) and functional residual capacity (FRC) using multiple breath washout (MBW), plethysmographic (pleth) FRC and forced expirations from raised lung volumes were measured in 71 infants with CF (participants in the London CF Collaboration) and 54 contemporaneous healthy controls age ∼3 months.Results: Compared with controls, and after adjustment for body size and age, LCI, FRC(MBW) and FRC(pleth) were significantly higher in infants with CF (mean difference (95% CI): 0.5 (0.1 to 0.9), p=0.02; 0.4 (0.1 to 0.7), p=0.02 and 0.9 (0.4 to 1.3), p<0.001, z-scores, respectively), while forced expiratory volume (FEV(0.5)) and flows (FEF(25-75)) were significantly lower (-0.9 (-1.3 to -0.6), p<0.001 and -0.7 (-1.1 to -0.2), p=0.004, z-scores, respectively). 21% (15/70) of infants with CF had an elevated LCI (>1.96 z-scores) and 25% (17/68) an abnormally low FEV(0.5) (below -1.96 z-scores). While only eight infants with CF had abnormalities of LCI and FEV(0.5), using both techniques identified abnormalities in 35% (24/68). Hyperinflation (FRC(pleth) >1.96 z-scores) was identified in 18% (10/56) of infants with CF and was significantly correlated with diminished FEF(25-75) (r=-0.43, p<0.001) but not with LCI or FEV(0.5).Conclusion: Despite early diagnosis of CF by NBS and protocol-driven treatment in specialist centres, abnormal lung function, with increased ventilation inhomogeneity and hyperinflation and diminished airway function, is evident in many infants with CF diagnosed through NBS by 3 months of age. [ABSTRACT FROM AUTHOR]

Published

2012

22. Lung clearance index at 4 years predicts subsequent lung function in children with cystic fibrosis.

Author

Aurora P, Stanojevic S, Wade A, Oliver C, Kozlowska W, Lum S, Bush A, Price J, Carr SB, Shankar A, Stocks J, London Cystic Fibrosis Collaboration, Aurora, Paul, Stanojevic, Sanja, Wade, Angie, Oliver, Cara, Kozlowska, Wanda, Lum, Sooky, Bush, Andrew, and Price, John

Subjects

CYSTIC fibrosis diagnosis, CYSTIC fibrosis, LONGITUDINAL method, LUNGS, RESEARCH evaluation, PULMONARY function tests, CASE-control method

Abstract

Rationale: The markedly improved life expectancy of children with cystic fibrosis (CF) has created a new challenge, as traditional markers of lung disease are frequently normal in young children. This prevents identification of individuals who may benefit from more aggressive therapy and also obliges large study numbers and prolonged duration for intervention studies. There is an urgent need for alternative surrogates that detect early lung disease and track through early childhood.Objectives: This study aimed to determine whether multiple-breath washout (MBW) results at preschool age can predict subsequent abnormal lung function.Methods: Preschool children (3-5 yr) with CF and healthy control subjects underwent spirometry and MBW with testing repeated during early school age (6-10 yr). Primary outcomes were FEV1 from spirometry and lung clearance index (LCI) from MBW.Measurements and Main Results: Forty-eight children with CF and 45 healthy children completed testing. Thirty-five (73%) children with CF had abnormal LCI at preschool age, whereas only five had abnormal FEV1. The positive predictive value of preschool LCI for predicting any abnormal school-age result was 94%, with a negative predictive value of 62%. Only one child with abnormal FEV1 at school age had had a normal preschool LCI. In contrast, for preschool FEV1 the positive predictive value was 100%, but negative predictive value was only 25%.Conclusions: This study demonstrates that an abnormal preschool LCI predicts subsequent lung function abnormalities, whereas a normal preschool LCI usually remains normal. MBW has potential as a clinical and research outcome in young children with CF. [ABSTRACT FROM AUTHOR]

Published

2011

23. Craniofacial abnormalities, agenesis of the corpus callosum, polysyndactyly and abnormal skin and gut development - the Curry Jones syndrome

Author

Michael Baraitser, Marilyn C. Jones, Robin M. Winter, Carr Sb, Eccles Dm, Shortland D, Temple Ik, and Curry C

Subjects

Craniofacial abnormality, business.industry, Preaxial polysyndactyly, General Medicine, Curry Jones syndrome, Anatomy, medicine.disease, Pathology and Forensic Medicine, Craniosynostosis, stomatognathic diseases, Atrophy, Polysyndactyly, Pediatrics, Perinatology and Child Health, medicine, Abnormal skin, Agenesis of the corpus callosum, business, Genetics (clinical)

Abstract

Five children are described with a striking, asymmetric facial appearance, craniosynostosis, preaxial polysyndactyly, agenesis of the corpus callosum and unusual skin with streaky areas of atrophy. The gut and mucous membranes are involved in two patients. This paper includes two patients described by Gorlin (1990) under the designation of the Curry Jones syndrome.

Published

1995

24. P246 The impact the introduction of a universal payment by results annual tariff cf centres upon the north south divide in england

Author

Nyangoma, SO, Cullinan, P, and Carr, SB

Abstract

BackgroundOur preliminary work demonstrated inequalities in key demographic characteristics, clinical outcomes and medication use in Cystic Fibrosis (CF) patients between the relatively economically disadvantaged North of England compared to the South. The analyses presented here aimed to assess if this North-South divide has been closed following the introduction of a new and equal CF payment policy (“banding”) in 2012.MethodsWe compared the cross-sectional data from Annual Review Encounter in 2010 and 2015 for patients registered on the UK CF Registry. The data for each year were analysed separately and the North/South Results compared. We used Wilcoxon and t-tests to compare continuous outcomes, and the chi-squared test to compare proportions.ResultsThe 2010 and 2015 cohorts included 6417 and 8007 patients, respectively (Table 1). There were no significant gender differences. Mean age of the populations increased, the significantly higher age in the South in 2010 levelled out by 2015. A new gap in overall lung function emerged in 2015: 72.24% vs 73.5% (p=0.041), the significantly higher FEV1in children in the South remained, although the gap narrowed from 3.27% to 1.7%. The better FEV1in adults in the North disappeared post banding. More patients in the North were diagnosed before turning 3 months. Prescription of key medications (DNase and Hypertonic saline) increased overall between 2010 and 2015 but higher use in the South remained (p<0.001). Rates of chronic Pseudomonas aeuginosafell but remain significantly higher in the North. Rates of MSSA and NTM remain higher in the South.Abstract P246 Table 1Patient characteristicsPre Banding (2010 Annual Review Encounter)Post Banding (2015 Annual Review Encounter)OutcomeSouth of England/North of England (n=3017/3400)South of England/North of England (n=3887/4120)Summary statisticsp-valueSummary statisticsp-valueAge: Mean±SD19.71±13.24/18.81±12.520.005220.82±14.23/20.3±13.780.0967Median18/1819/19Gender, n(%)Female1423 (47.17)/1578 (46.41)1870 (48.11)/1894 (45.97)Age at diagnosis, n(%)<3 months; n (%)1280 (42.43)/1590 (46.76)0.00521852 (47.65)/2121 (51.48)<0.001≥18 years; n (%)188 (6.23)/191 (5.62)0.2296295 (7.59)/258 (6.26)0.0216FEV1 percent predicted(Overall) Mean±SD70.98±24.66/71.23±24.230.717273.5±24.53/72.24±24.840.041Age<16 Mean±SD84.51±17.99/81.57±19.800.002287.78±17.37/86.08±17.660.0361Age≥16 Mean±SD64.69±24.81/66.73±24.610.015367.6±24.63/66.6±25.130.1754Hypertonic Saline (n(%))433 (14.35)/311 (9.15)<0.0011319 (33.93)/860 (20.87)<0.001Dornase Alfa (n(%))1394 (46.2)/1393 (40.97)<0.0012572 (66.17)/2274 (55.19)<0.001 Chronic macrolides (n(%))1284 (42.56)/1445 (42.5)0.98221498 (38.54)/1607 (39.00)0.6856Asthma (n(%))534 (17.7)/393 (11.56)<0.001685 (17.62)/538 (13.06)<0.001CFRD (n(%))528 (30.14)/623 (32.5)0.1325838 (53.51)/957 (57.34)0.0389NTM (n(%))116 (3.84)/55 (1.62)<0.001297 (7.64)/193 (4.68)0.001Pseudomonas (n(%))1058 (35.07)/1359 (39.97)<0.0011100 (28.3)/1332 (32.33)0.0269ConclusionsThere appears to be a closing of the North-South gap in some key areas such as FEV1and age, this may suggest improved outcomes although survival analysis is not possible on small cohorts such as these. The higher use in the South of the high cost drug DNase must now be down to clinician preference rather than funding problems. These markers of overall improvements (higher mean age, higher FEV1, lower Pseudomonas) may be associated with the introduction of equality of funding in England but could equally represent improved care in general with similar improvements seen in other international registries.

Published

2017

25. P8 Bone mineral density in children and adolescents with cystic fibrosis, should we be doing less monitoring?

Author

O’Toole, CF, Bush, A, and Carr, SB

Abstract

BackgroundCystic fibrosis (CF) is a multi-system disease resulting from mutations in the CFTRgene. CF patients are at risk of developing osteopenia. Regular monitoring of bone mineral density (BMD) is currently recommended in the standards of care for CF.AimsTo explore the extent of low BMD in children with CF and identify risk factors associated with decreased BMD.Establish the rate of decline in BMD to inform future practice.MethodsAll children undergo routine DEXA scan at bi-annual assessments from 8 years of age. A single centre retrospective review of CF Registry records and online hospital records was conducted for children born 2000–2006. Z-score values were obtained for BMD and BMI as well as FEV1%/FVC% predicted (GLI), and possible confounding factors were also recorded.Abstract P8 Table 1DEXA sequenceScan 1Scan 2Scan 3Scan 4ANOVA sig.Number 96 87 60 18 Age in years (Mean,SD) 9.98 (1.9) 11.79 (1.8) 13.24 (1.5) 14.34 (1.5) M/F 37/59 33/54 25/35 8/10 L1-L4 −0.12 −0.37 −0.42 −0.96 0.008 L2 −0.27 −0.48 −0.59 −1.13 0.013 FEV1% 86% 83% 80% 78% 0.174 BMI Z-Score −0.03 −0.05 0.04 0.18 0.844 Vit-D 72 69 71 78 0.577 Results96 children (59 female) had a first DEXA scan at a mean age of 10 (±1.94 years). 262 DEXA scans were performed with a median of 2 per individual. Thirteen (13.5%) had an abnormal DEXA scan over the course of the study; only 2 of these were age <10 years (n=48 performed in this age range). Risk factors for abnormal BMD (z-score ≤−2) were: a BMI z-score ≤2;>50 days of intravenous antibiotics in the year before the scan; and FEV1%<50. The table shows mean results for sequential scans; rate of decline was unpredictable. The mean change per year was −0.1 z-scores (SD=±0.5). Neither Vit D levels nor the CF-related diabetes was related to baseline or changes in BMD.ConclusionLow lung function and BMI z-scores were the greatest indicators of being at risk of osteopaenia for the cohort. With a rate of decline of only 0.1 z-score per annum the frequency of DEXA scans could be decreased in low risk children.

Published

2018

26. P250 A national study of non-invasive ventilation and clinical outcomes in cystic fibrosis

Author

Archangelidi, O, Simmonds, NJ, Carr, SB, and Cullinan, P

Abstract

Introduction/ObjectivesNon-invasive ventilation (NIV) is often used as a ‘bridge’ to transplantation, for symptom control or as an adjunct to physiotherapy. Whether or not NIV is being appropriately used in UK patients with CF, successfully targeting those who will benefit most, is unknown; nor is there information on the life expectancy of those who start on NIV.MethodsThe present study is part of the CF-Epidemiological Network (CF-EpiNet project) and uses data from the UK Cystic Fibrosis Registry to describe the patterns of NIV use by patients in the UK. We examined the records of 11 120 patients and assembled a longitudinal, retrospective cohort from those seen between 2007 and 2015. We used Cox proportional hazard models to assess the survival of patients on NIV.Results1077 patients (715 adults and 362 children<16 years) had reported use of NIV recorded at least once. Usage increased after 2012 (figure 1). At the first recorded use of NIV the median (IQR) age was 21 years (14, 28), BMI 18.4 kg/m2(16.8, 22.7), 49.2% were male, 90.3% on PERT, 75.1% growing Pseudomonas, 54.6% homozygous F508del; the mean FVCpp was 64.5% and FEV1pp 47.2%. At this time 68.8% of patients had a FEV1pp <60%; 52% were <40%, while in adults this percentage reached 61%. In children there was a higher proportion starting treatment with better lung function ie ≥60% (33.8%). The median survival of patients who start NIV is 3.47 years. The hazard ratio for NIV use was 3.90 (95% CI: 3.06–4.96).[Figure]ConclusionsNot surprisingly, patients start NIV when their lung function is significantly impaired. Yet, increased proportions of people with FEV1pp ≥40% on NIV were also identified. The higher lung function at the start of NIV for children may reflect that it is used for purposes other than a bridge to transplant in this group; the registry only collects a yes/no variable for NIV use and not the reason for use. Survival after initiation of NIV is poor; this is likely reflect that NIV is a marker of disease severity but further analysis will be needed to explore this.

Published

2017

27. Associations between respiratory pathogens and lung function in primary ciliary dyskinesia: cross-sectional analysis from the PROVALF-PCD cohort.

Author

Rubbo B, Kant A, Zhang K, Allegorico A, Basilicata S, Boon M, Borrelli M, Calogero C, Carr SB, Carroll M, Constant C, Castillo Corullón S, Corvol H, Cutrera R, Dillenhöfer S, Emiralioglu N, Eralp E, Eryilmaz Polat S, Gardner L, Gokdemir Y, Harris A, Hogg C, Karadag B, Kobbernagel H, Koerner-Rettberg C, Kouis P, Lorent N, Marcou M, Mathin JK, Martinu V, Moreno-Galdó A, Morgan L, Nielsen KG, Omran H, Ozcelik U, Pohunek P, Raidt J, Robinson P, Rovira-Amigo S, Santamaria F, Schlegtendal A, Tamalet A, Thouvenin G, Ullmann N, Walker W, Yiallouros P, Kuehni CE, Latzin P, Beydon N, and Lucas JS

Abstract

Introduction: Respiratory pathogens are frequently isolated from airway samples in primary ciliary dyskinesia (PCD) patients. Few studies have investigated associations between these pathogens and lung function, with current management based on evidence from cystic fibrosis. We investigated the association between commonly isolated respiratory pathogens and lung function in PCD patients., Methods: Using a cross-sectional design, we prospectively collected clinical and concurrent microbiology data from 408 participants with probable or confirmed PCD, aged ≥5 years, from 12 countries. We used Global Lung Function Initiative 2012 references to calculate forced expiratory volume in 1 s (FEV 1 ) z-scores. For 351 patients (86%) with complete data, we assessed the association of the four most frequently isolated pathogens with lung function by fitting multilevel linear models with country as random intercept, adjusted for age at diagnosis, age at lung function, use of antibiotic prophylaxis and body mass index z-scores., Results: Individuals with Pseudomonas aeruginosa growth in culture had significantly lower FEV 1 z-scores (β= -0.87, 95% CI -1.40- -0.34), adjusted for presence of Haemophilus influenzae , methicillin-sensitive Staphylococcus aureus and Streptococcus pneumoniae , and for covariates. When stratified by age, associations remained strong for adults but not for children. Results were similar when ciliary defects by transmission electron microscopy were included in the models and when restricting analysis to only confirmed PCD cases., Conclusions: We found that P. aeruginosa was associated with worse lung function in individuals with PCD, particularly adults. These findings suggest that it is prudent to aim for P. aeruginosa eradication in the first instance, and to treat exacerbations promptly in colonised patients., Competing Interests: Conflict of interest: M. Boon declares receiving grants or contracts from the Fund Alphonse and Jean Forton, managed by the King Baudouin Foundation, and by the Belgian Cystic Fibrosis Association (number 2020-J1810150-217926); and payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from Vertex. Conflict of interest: S.B. Carr declares receiving payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from Chiesi Pharmaceuticals, and participation on a Data Safety Monitoring Board or Advisory Board for Vertex Pharmaceuticals. Conflict of interest: S. Dillenhöfer declares receiving support for attending meetings and/or travel from Vertex (Advance Program 2022). Conflict of interest: B. Karadag declares receiving payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from VEM Ilac, Abdi Ibrahim and OMRON, and participating on a Data Safety Monitoring Board or Advisory Board for Abdi Ibrahim. Conflict of interest: C. Koerner-Rettberg declares receiving speaker honoraria from Berlin Chemie, and advisory board participation and being a member of the medical board of the German PCD patient organisation. Conflict of interest: V. Martinu declares having received grants or contracts from Ministry of Health of the Czech Republic (grant number NV19-07-00210) and participation on an advisory board for indication of tobramycin in noncystic fibrosis bronchiectasis for Chiesi, and receiving payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from Chiesi Pharmaceuticals. Conflict of interest: A. Moreno-Galdó declares receiving personal payment for lectures from AstraZeneca, Sanofi-Pasteur and Janssen, receiving support for attending meetings or travel from Sanofi-Pasteur and Vivisol, participation on a Data Safety Monitoring Board or Advisory Board for AstraZeneca and Sanofi-Pasteur, and is President of the Spanish Society of Pediatric Pulmonology. Conflict of interest: U. Ozcelik is Head of the Turkish Respiratory Disease and Cystic Fibrosis Society (unpaid). Conflict of interest: P. Pohunek declares receiving payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from GlaxoSmithKline, AstraZeneca and Chiesi, and consulting fees, support for attending meetings and/or travel, and participation on a Data Safety Monitoring Board or Advisory Board from AstraZeneca and GlaxoSmithKline. Conflict of interest: J. Raidt declares receiving the following funds: DFG CRU326 RA3522/1. Conflict of interest: P. Latzin declares receiving grants or contracts from Vertex and OM Pharma, payment or honoraria for lectures, presentations, speakers’ bureaus, manuscript writing or educational events from Vertex, Vifor and OM Pharma, and participating on a Data Safety Monitoring Board or Advisory Board for the following: Polyphor, Santhera (DMC), Vertex, OM Pharma, Vifor, Allecra and Sanofi Aventis. Conflict of interest: J.S. Lucas declares receiving support for the present manuscript (funds the clinical investigations (spirometry, microbiology)) from NHS England, to the institution; and grants or contracts from COST ACTION to fund the BEATPCD COST Action BM1407, which funded the network that undertook this work, and the institution managed the funding. Conflict of interest: The other authors have nothing to disclose., (Copyright ©The authors 2024.)

Published

2024

28. Demographic factors associated with within-individual variability of lung function for adults with cystic fibrosis: A UK registry study.

Author

Palma M, Keogh RH, Carr SB, Szczesniak R, Taylor-Robinson D, Wood AM, Muniz-Terrera G, and Barrett JK

Subjects

Humans, Male, Female, Adult, United Kingdom epidemiology, Middle Aged, Adolescent, Forced Expiratory Volume, Longitudinal Studies, Disease Progression, Young Adult, Lung physiopathology, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Sex Factors, Age Factors, Cystic Fibrosis physiopathology, Cystic Fibrosis genetics, Cystic Fibrosis epidemiology, Registries, Respiratory Function Tests methods

Abstract

Background: Lung function is a key outcome used in the evaluation of disease progression in cystic fibrosis. The variability of individual lung function measurements over time (within-individual variability) has been shown to predict subsequent lung function changes. Nevertheless, the association between within-individual lung function variability and demographic and genetic covariates has not been quantified., Methods: We performed a longitudinal analysis of data from a cohort of 7099 adults with cystic fibrosis (between 18 and 49 years old) from the UK cystic fibrosis registry, containing annual review data between 1996 and 2020. A mixed-effects location-scale model is used to quantify mean FEV 1 (forced expiratory volume in 1 s) trajectories and FEV 1 within-individual variability as a function of sex, age at annual review, diagnosis after first year of life, homozygous F508 genotype and birth cohort., Results: Mean FEV 1 decreased with age and lung function variability showed a near-quadratic trend by age. Males showed higher FEV 1 mean and variability than females across the whole age range. Earlier diagnosis and homozygous F508 genotype were also associated with higher FEV 1 mean and variability. Individuals who died during follow-up showed on average higher lung function variability than those who survived., Conclusions: Key variables known to be linked with mean lung function in cystic fibrosis are also associated with an individual's lung function variability. This work opens new avenues to understand the role played by lung function variability in disease progression and its utility in predicting key outcomes such as mortality., Competing Interests: Declaration of competing interest JKB has received research funding for unrelated work from F. Hoffmann-La Roche Ltd., (Copyright © 2024 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2024

29. Impact of COVID-19 infection on lung function and nutritional status amongst individuals with cystic fibrosis: A global cohort study.

Author

Semenchuk J, Naito Y, Charman SC, Carr SB, Cheng SY, Marshall BC, Faro A, Elbert A, Gutierrez HH, Goss CH, Karadag B, Burgel PR, Colombo C, Salvatore M, Padoan R, Daneau G, Harutyunyan S, Kashirskaya N, Kirwan L, Middleton PG, Ruseckaite R, de Monestrol I, Naehrlich L, Mondejar-Lopez P, Jung A, van Rens J, Bakkeheim E, Orenti A, Zomer-van Ommen D, da Silva-Filho LVR, Fernandes FF, Zampoli M, and Stephenson AL

Subjects

Humans, Female, Male, Retrospective Studies, Adult, Forced Expiratory Volume, Body Mass Index, SARS-CoV-2, Respiratory Function Tests methods, Cystic Fibrosis physiopathology, Cystic Fibrosis complications, COVID-19 physiopathology, COVID-19 complications, COVID-19 epidemiology, Nutritional Status

Abstract

Background: Factors associated with severe COVID-19 infection have been identified; however, the impact of infection on longer-term outcomes is unclear. The objective of this study was to examine the impact of COVID-19 infection on the trajectory of lung function and nutritional status in people with cystic fibrosis (pwCF)., Methods: This is a retrospective global cohort study of pwCF who had confirmed COVID-19 infection diagnosed between January 1, 2020 and December 31, 2021. Forced expiratory volume in one second percent predicted (ppFEV 1 ) and body mass index (BMI) twelve months prior to and following a diagnosis of COVID-19 were recorded. Change in mean ppFEV 1 and BMI were compared using a t-test. A linear mixed-effects model was used to estimate change over time and to compare the rate of change before and after infection., Results: A total of 6,500 cases of COVID-19 in pwCF from 33 countries were included for analysis. The mean difference in ppFEV 1 pre- and post-infection was 1.4 %, (95 % CI 1.1, 1.7). In those not on modulators, the difference in rate of change pre- and post-infection was 1.34 %, (95 % CI -0.88, 3.56) per year (p = 0.24) and -0.74 % (-1.89, 0.41) per year (p = 0.21) for those on elexacaftor/tezacaftor/ivacaftor. No clinically significant change was noted in BMI or BMI percentile before and after COVID-19 infection., Conclusions: No clinically meaningful impact on lung function and BMI trajectory in the year following infection with COVID-19 was identified. This work highlights the ability of the global CF community to unify and address critical issues facing pwCF., Competing Interests: Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: The authors of this manuscript receive funding in the form of consulting fees or honoraria from Vertex Pharmaceuticals, Chiesi Pharmaceuticals, Enterprise Therapeutics, Gilead Sciences, GSK, Astra-Zeneca, Insmed, MSD, Sanofi, Viartis, Zambon, Limbic, Effrx Pharmaceuticals and Omron. Additionally, there is an author who serves on the Novartis Data and Safety Monitoring Board. There are several authors who are employed by the Cystic Fibrosis Foundation (CFF). The CFF, to advance drug development and search for a cure, have contracts with several companies to help fund the development of potential treatments and/or cures for cystic fibrosis. Pursuant to these contracts, CFF may receive milestone-based payments, equity interests, royalties on the net sales of therapies, and/or other forms of consideration. Resulting revenue received by CFF is used in support of our mission. See “How Drugs Get on the Pipeline” on the CFF website for more information. Additionally, CFF may license CFF Patient Registry data to some companies to monitor drug safety as part of the U.S. Food and Drug Administration's required Phase 4 clinical trials process and to encourage research aimed at improving the care of people with CF, while maintaining our obligation and commitment to protect the privacy of Registry participants. In connection with these licenses, and upon request, CFF may also assist company researchers in interpreting CFF Patient Registry data to aid in designing, analyzing, and interpreting real world studies in CF., (Copyright © 2024. Published by Elsevier B.V.)

Published

2024

30. Combined approaches, including long-read sequencing, address the diagnostic challenge of HYDIN in primary ciliary dyskinesia.

Author

Fleming A, Galey M, Briggs L, Edwards M, Hogg C, John S, Wilkinson S, Quinn E, Rai R, Burgoyne T, Rogers A, Patel MP, Griffin P, Muller S, Carr SB, Loebinger MR, Lucas JS, Shah A, Jose R, Mitchison HM, Shoemark A, Miller DE, and Morris-Rosendahl DJ

Subjects

Humans, Male, Female, High-Throughput Nucleotide Sequencing methods, High-Throughput Nucleotide Sequencing standards, Kartagener Syndrome genetics, Kartagener Syndrome diagnosis, Cilia pathology, Cilia genetics, Genetic Testing methods, Genetic Testing standards

Abstract

Primary ciliary dyskinesia (PCD), a disorder of the motile cilia, is now recognised as an underdiagnosed cause of bronchiectasis. Accurate PCD diagnosis comprises clinical assessment, analysis of cilia and the identification of biallelic variants in one of 50 known PCD-related genes, including HYDIN. HYDIN-related PCD is underdiagnosed due to the presence of a pseudogene, HYDIN2, with 98% sequence homology to HYDIN. This presents a significant challenge for Short-Read Next Generation Sequencing (SR-NGS) and analysis, and many diagnostic PCD gene panels do not include HYDIN. We have used a combined approach of SR-NGS with bioinformatic masking of HYDIN2, and state-of-the-art long-read Nanopore sequencing (LR&#95;NGS), together with analysis of respiratory cilia including transmission electron microscopy and immunofluorescence to address the underdiagnosis of HYDIN as a cause of PCD. Bioinformatic masking of HYDIN2 after SR-NGS facilitated the detection of biallelic HYDIN variants in 15 of 437 families, but compromised the detection of copy number variants. Supplementing testing with LR-NGS detected HYDIN deletions in 2 families, where SR-NGS had detected a single heterozygous HYDIN variant. LR-NGS was also able to confirm true homozygosity in 2 families when parental testing was not possible. Utilising a combined genomic diagnostic approach, biallelic HYDIN variants were detected in 17 families from 242 genetically confirmed PCD cases, comprising 7% of our PCD cohort. This represents the largest reported HYDIN cohort to date and highlights previous underdiagnosis of HYDIN-associated PCD. Moreover this provides further evidence for the utility of LR-NGS in diagnostic testing, particularly for regions of high genomic complexity., (© 2024. Crown.)

Published

2024

31. Evaluating the correspondence between the EQ-5D-5L and disease severity and quality of life in adults and adolescents with cystic fibrosis.

Author

Altabee R, Carr SB, Abbott J, Cameron R, Office D, Simmonds NJ, Whitty JA, Turner D, and Barton G

Abstract

Background: The EQ-5D is the recommended measure to capture health-related quality of life (HRQoL), recognised for use in health technology appraisal bodies. In order to assess whether it is appropriate to use the EQ-5D for making decisions about the cost-utility of treatments in cystic fibrosis (CF), this study assesses the performance of the EQ-5D-5L in adults and adolescents with CF., Method: This was a cross-sectional observational survey study of patients with CF attending a single large CF centre. Participants were asked to complete a survey that included two HRQoL measures; the EQ-5D-5L and CF Quality of Life (CFQoL) questionnaires., Results: Among 213 participants, the median EQ-5D-5L index score was 0.76 (IQR 0.66 - 0.84) and the visual analogue (EQ-VAS) was 70 (60 - 80). Both the EQ-5D index and EQ-VAS discriminated between disease severity based on lung function (p = 0.01 and p < 0.01, respectively) and pulmonary exacerbation (p = 0.02 and p < 0.01, respectively); however, EQ-VAS differentiated between more lung function severity groups compared to EQ-5D index. The EQ-5D-5L demonstrated convergent validity as its dimensions, index score, and EQ-VAS had significant correlations with most CFQoL domains. Though, EQ-VAS significantly predicted more domains of CFQoL (4 domains) compared to EQ-5D index (only 1 domain)., Conclusion: The generic EQ-5D-5L performed adequately in discriminating between CF disease severity, and its index score and EQ-VAS had moderate correlations with CFQoL. However, using a complementary condition-specific measure alongside the EQ-5D-5L can provide better insight of HRQoL in CF and benefit the process of cost-utility analysis., Competing Interests: Declaration of competing interest RA, JA, DO, RC, SC, NS, JW, DT, and GB have no direct conflicts of interest to declare in relation to this study. Outside of the submitted work, SC has served on advisory boards and/or given educational lectures for which she or her institution have received fees for (Vertex, Chiesi, and Profile Pharma). NS has served on advisory boards and/or given educational lectures for which he has received consultancy fees (Vertex, Gilead, Chiesi, Zambon, Roche, and Menarini)., (Copyright © 2024 The Author(s). Published by Elsevier Masson SAS.. All rights reserved.)

Published

2024

32. Analyses of 1236 genotyped primary ciliary dyskinesia individuals identify regional clusters of distinct DNA variants and significant genotype-phenotype correlations.

Author

Raidt J, Riepenhausen S, Pennekamp P, Olbrich H, Amirav I, Athanazio RA, Aviram M, Balinotti JE, Bar-On O, Bode SFN, Boon M, Borrelli M, Carr SB, Crowley S, Dehlink E, Diepenhorst S, Durdik P, Dworniczak B, Emiralioğlu N, Erdem E, Fonnesu R, Gracci S, Große-Onnebrink J, Gwozdziewicz K, Haarman EG, Hansen CR, Hogg C, Holgersen MG, Kerem E, Körner RW, Kötz K, Kouis P, Loebinger MR, Lorent N, Lucas JS, Maj D, Mall MA, Marthin JK, Martinu V, Mazurek H, Mitchison HM, Nöthe-Menchen T, Özçelik U, Pifferi M, Pogorzelski A, Ringshausen FC, Roehmel JF, Rovira-Amigo S, Rumman N, Schlegtendal A, Shoemark A, Sperstad Kennelly S, Staar BO, Sutharsan S, Thomas S, Ullmann N, Varghese J, von Hardenberg S, Walker WT, Wetzke M, Witt M, Yiallouros P, Zschocke A, Ziętkiewicz E, Nielsen KG, and Omran H

Subjects

Humans, Male, Female, Adult, Child, Adolescent, Young Adult, Middle Aged, Europe, Registries, Axonemal Dyneins genetics, Forced Expiratory Volume, Child, Preschool, Kartagener Syndrome genetics, Kartagener Syndrome physiopathology, Genetic Variation, Mutation, Aged, Infant, Cytoskeletal Proteins, Proteins, Genotype, Genetic Association Studies, Phenotype

Abstract

Background: Primary ciliary dyskinesia (PCD) represents a group of rare hereditary disorders characterised by deficient ciliary airway clearance that can be associated with laterality defects. We aimed to describe the underlying gene defects, geographical differences in genotypes and their relationship to diagnostic findings and clinical phenotypes., Methods: Genetic variants and clinical findings (age, sex, body mass index, laterality defects, forced expiratory volume in 1 s (FEV 1 )) were collected from 19 countries using the European Reference Network's ERN-LUNG international PCD Registry. Genetic data were evaluated according to American College of Medical Genetics and Genomics guidelines. We assessed regional distribution of implicated genes and genetic variants as well as genotype correlations with laterality defects and FEV 1 ., Results: The study included 1236 individuals carrying 908 distinct pathogenic DNA variants in 46 PCD genes. We found considerable variation in the distribution of PCD genotypes across countries due to the presence of distinct founder variants. The prevalence of PCD genotypes associated with pathognomonic ultrastructural defects (mean 72%, range 47-100%) and laterality defects (mean 42%, range 28-69%) varied widely among countries. The prevalence of laterality defects was significantly lower in PCD individuals without pathognomonic ciliary ultrastructure defects (18%). The PCD cohort had a reduced median FEV 1 z-score (-1.66). Median FEV 1 z-scores were significantly lower in CCNO (-3.26), CCDC39 (-2.49) and CCDC40 (-2.96) variant groups, while the FEV 1 z-score reductions were significantly milder in DNAH11 (-0.83) and ODAD1 (-0.85) variant groups compared to the whole PCD cohort., Conclusion: This unprecedented multinational dataset of DNA variants and information on their distribution across countries facilitates interpretation of the genetic epidemiology of PCD and indicates that the genetic variant can predict diagnostic and phenotypic features such as the course of lung function., Competing Interests: Conflict of interest: The authors have no potential conflicts of interest to disclose., (Copyright ©The authors 2024.)

Published

2024

33. Chronicity Counts: The Impact of Pseudomonas aeruginosa , Staphylococcus aureus , and Coinfection in Cystic Fibrosis.

Author

Mossop M, Ish-Horowicz J, Hughes D, Dobra R, Cunanan AG, Rosenthal M, Carr SB, Ramadan N, Nolan LM, and Davies JC

Subjects

Humans, Male, Female, Adult, Chronic Disease, Child, Cystic Fibrosis complications, Cystic Fibrosis microbiology, Pseudomonas aeruginosa, Pseudomonas Infections complications, Coinfection microbiology, Staphylococcal Infections complications, Staphylococcus aureus

Published

2024

34. Pancreatic enzyme prescription following ivacaftor licensing: A retrospective analysis of the US and UK cystic fibrosis registries.

Author

Calthorpe R, Rosenfeld M, Goss CH, Green N, Derleth M, Carr SB, Smyth A, and Stewart I

Subjects

Humans, United Kingdom epidemiology, United States epidemiology, Male, Female, Retrospective Studies, Adult, Longitudinal Studies, Adolescent, Exocrine Pancreatic Insufficiency epidemiology, Exocrine Pancreatic Insufficiency drug therapy, Exocrine Pancreatic Insufficiency etiology, Child, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Cystic Fibrosis drug therapy, Cystic Fibrosis epidemiology, Aminophenols therapeutic use, Registries, Enzyme Replacement Therapy methods, Enzyme Replacement Therapy statistics & numerical data, Quinolones therapeutic use, Chloride Channel Agonists therapeutic use

Abstract

Background: Relieving gastrointestinal symptoms is a research priority in cystic fibrosis. Emerging evidence highlights effects of cystic fibrosis transmembrane conductance regulator (CFTR) modulators on gastrointestinal function, including pancreatic sufficiency. This study explores ivacaftor licensing and treatment on recorded pancreatic enzyme replacement therapy (PERT) prescription in the US and UK CF registries., Methods: Retrospective longitudinal registry study of recorded pancreatic PERT use between 2008 and 2017. Interrupted time series analysis in propensity-matched cohorts estimated annual change and step change according to ivacaftor eligibility before and after licensing year, 2012. Generalised estimating equations assessed adjusted risk of PERT use in individuals treated with ivacaftor after 2012 compared to untreated individuals., Results: In the US CF registry, the difference in annual change in prevalence of PERT use post-2012 between eligible cases and ineligible controls was -5.0 per 1000 people/year (95 %CI -7.6; -2.3, p = 0.001). The step change and annual change in prevalence of PERT use in eligible cases was not significantly different to controls in the UK CF registry. Relative to the relationship in 2013, ivacaftor treatment in the US CF registry was associated with a lower adjusted risk ratio of PERT use compared to untreated individuals by 2016 (0.97, 95 %CI 0.96; 0.99), which was not observed in the UK CF registry., Conclusions: Licensing of ivacaftor was followed by a lower prevalence of PERT use in the eligible US population compared to pre-licensing period, as well as lower risk of PERT use in those who received treatment. Inconsistencies in US and UK CF registries were observed., Competing Interests: Declaration of competing interest A.R. Smyth has research grants (paid to the University of Nottingham) from Vertex Pharmaceuticals and payment for an advisory board (paid to the University of Nottingham) from Viatris Pharmaceuticals, all outside the current work. A.R. Smyth has patents issued (Camara M, Williams P, Barrett D, Halliday N, Knox A, Smyth A, Fogarty A, Barr H, Forrester D. Alkyl quinolones as biomarkers of Pseudomonas aeruginosa infection and uses thereof. US2016131648-A1; https://pubchem.ncbi.nlm.nih.gov/patent/US-2016131648-A1 Outside the current work, A.R. Smyth reports participation on a Data Safety Monitoring Board for the North American Cystic Fibrosis Foundation Therapeutic Development Network., (Copyright © 2024. Published by Elsevier B.V.)

Published

2024

35. Defining the mechanism of galectin-3-mediated TGF-β1 activation and its role in lung fibrosis.

Author

Calver JF, Parmar NR, Harris G, Lithgo RM, Stylianou P, Zetterberg FR, Gooptu B, Mackinnon AC, Carr SB, Borthwick LA, Scott DJ, Stewart ID, Slack RJ, Jenkins RG, and John AE

Subjects

Humans, Lung metabolism, Lung pathology, Signal Transduction, Receptor, Transforming Growth Factor-beta Type II metabolism, Receptor, Transforming Growth Factor-beta Type II genetics, Receptors, Transforming Growth Factor beta metabolism, Protein Binding, Protein Serine-Threonine Kinases metabolism, Galectins metabolism, Collagen Type I metabolism, Cells, Cultured, Blood Proteins, Transforming Growth Factor beta1 metabolism, Galectin 3 metabolism, Galectin 3 genetics, Fibroblasts metabolism, Fibroblasts pathology, Idiopathic Pulmonary Fibrosis metabolism, Idiopathic Pulmonary Fibrosis pathology

Abstract

Integrin-mediated activation of the profibrotic mediator transforming growth factor-β1 (TGF-β1), plays a critical role in idiopathic pulmonary fibrosis (IPF) pathogenesis. Galectin-3 is believed to contribute to the pathological wound healing seen in IPF, although its mechanism of action is not precisely defined. We hypothesized that galectin-3 potentiates TGF-β1 activation and/or signaling in the lung to promote fibrogenesis. We show that galectin-3 induces TGF-β1 activation in human lung fibroblasts (HLFs) and specifically that extracellular galectin-3 promotes oleoyl-L-α-lysophosphatidic acid sodium salt-induced integrin-mediated TGF-β1 activation. Surface plasmon resonance analysis confirmed that galectin-3 binds to αv integrins, αvβ1, αvβ5, and αvβ6, and to the TGFβRII subunit in a glycosylation-dependent manner. This binding is heterogeneous and not a 1:1 binding stoichiometry. Binding interactions were blocked by small molecule inhibitors of galectin-3, which target the carbohydrate recognition domain. Galectin-3 binding to β1 integrin was validated in vitro by coimmunoprecipitation in HLFs. Proximity ligation assays indicated that galectin-3 and β1 integrin colocalize closely (≤40 nm) on the cell surface and that colocalization is increased by TGF-β1 treatment and blocked by galectin-3 inhibitors. In the absence of TGF-β1 stimulation, colocalization was detectable only in HLFs from IPF patients, suggesting the proteins are inherently more closely associated in the disease state. Galectin-3 inhibitor treatment of precision cut lung slices from IPF patients' reduced Col1a1, TIMP1, and hyaluronan secretion to a similar degree as TGF-β type I receptor inhibitor. These data suggest that galectin-3 promotes TGF-β1 signaling and may induce fibrogenesis by interacting directly with components of the TGF-β1 signaling cascade., Competing Interests: Conflict of interests R. G. J. is a trustee for Action for Pulmonary Fibrosis. A. E. J. is a founder and shareholder of Alevin Therapeutics. J. F. C., F. R. Z., A. C. M., and R. J. S. are Galecto employees with shares/options in the company. N. R. P. is a Roche employee. L. A. B. is a director and shareholder of FibroFind. G. H., R. M. L., P. S., S. B. C., D. J. S., and I. D. S. declare that they have no conflict of interests with the contents of this article., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

36. Advances in Cranial Surgery.

Author

Tariq F, Jumah F, Ravipati K, Ortiz-Torres M, Carr SB, and Chicoine MR

Subjects

Humans, Radiosurgery methods, Radiosurgery trends, Cerebral Hemorrhage surgery, Brain Neoplasms surgery, Neuroendoscopy methods, Neuroendoscopy trends, Neurosurgical Procedures methods, Neurosurgical Procedures trends

Abstract

The landscape of the cranial neurosurgery has changed tremendously in past couple of decades. The main frontiers including introduction of neuro-endoscopy, minimally invasive skull base approaches, SRS, laser interstitial thermal therapy and use of tubular retractors have revolutionized the management of intracerebral hemorrhages, deep seated tumors other intracranial pathologies. Introduction of these novel techniques is based on smaller incisions with maximal operative corridors, decreased blood loss, shorter hospital stays, decreased post-operative pain and cosmetically appealing scars that improves patient satisfaction and clinical outcomes. The sophisticated tools like neuroendoscopy have improved light source, and better visualization around the corners. Advanced navigated tools and channel-based retractors help us to target deeply seated lesions with increased precision and minimal disruption of the surrounding neurovascular tissues. Advent of stereotactic radiosurgery has provided us alternative feasible, safe and effective options for treatment of patients who are otherwise not medically stable to undergo complex cranial surgical interventions. This paper review advances in treatment of intracranial pathologies, and how the neurosurgeons and other medical providers at the University of Missouri-Columbia (UMC) are optimizing these treatments for their patients., Competing Interests: Disclosure: No financial disclosures reported. Artificial intelligence was not used in the study, research, preparation, or writing of this manuscript., (Copyright 2024 by the Missouri State Medical Association.)

Published

2024

37. A grumbling concern: A survey of gastrointestinal symptoms in cystic fibrosis in the modulator era.

Author

Calthorpe RJ, Goodchild N, Gleetus V, Premakumar V, Hayee B, Elliott Z, Evans B, Rowbotham NJ, Carr SB, Barr H, Horsley A, Peckham D, and Smyth AR

Abstract

Background: Gastrointestinal symptoms in cystic fibrosis (CF) are common and intrusive to daily life. Relieving gastrointestinal symptoms was identified as an important research priority and previously explored in an international survey in 2018. However, following the widespread introduction of cystic fibrosis transmembrane conductance regulator (CFTR) modulators in 2019, the landscape of CF treatment has changed. We repeated an online survey to further describe gastrointestinal symptoms and their effect on quality of life (QoL) in the CFTR modulator era., Methods: An electronic survey consisting of closed questions and free text responses was distributed via social media and professional networks for a period of one month between March - April 2022. People with CF (pwCF), their family and friends, and healthcare professionals (HCPs) were invited to take part., Results: There were 164 respondents: 88 pwCF (54%), 22 (13%) family, and 54 (33%) healthcare professionals (HCPs). A total of 89/110 (81%) pwCF or family members reported CFTR modulator treatment. The most commonly reported symptoms were wind / gas and rumbling stomach noises (borborygmi) in both the modulator and non-modulator groups in addition to loose motions (modulator group) and bloating (no modulator group). Abdominal pain and bloating had the greatest impact on QoL.For those on a CFTR modulator, the proportion of pwCF reporting "no change" or "worse" for all of the symptoms surveyed was greater than the proportion reporting an improvement. For some symptoms such as stomach pains and reduced appetite, improvements were perceived more commonly in HCPs than what was reported by pwCF. Following modulator introduction, dietary changes to manage GI symptoms were recommended by 28/35 (80%) of HCPs and reported by 38/76 (50%) lay respondents. Changes in medication were recommended by 19/35 (54%) HCPs and reported by 44/76 (58%) of patients and family members., Conclusion: This survey has shown that gastrointestinal symptoms remain prevalent in pwCF in the CFTR modulator era, though the nature of these symptoms may have changed. A better understanding of the underlying pathophysiology of these symptoms is essential. Future clinical studies should focus on improving symptoms and QoL., Competing Interests: Competing interests: A.R. Smyth has research grants (paid to the University of Nottingham) from Vertex Pharmaceuticals and payment for an advisory board (paid to the University of Nottingham) from Viatris Pharmaceuticals, all outside the current work. A.R. Smyth has patents issued (Camara M, Williams P, Barrett D, Halliday N, Knox A, Smyth A, Fogarty A, Barr H, Forrester D. Alkyl quinolones as biomarkers of Pseudomonas aeruginosa infection and uses thereof. US2016131648-A1; https://pubchem.ncbi.nlm.nih.gov/patent/US-2016131648-A1 Outside the current work, A.R. Smyth reports participation on a Data Safety Monitoring Board for the North American Cystic Fibrosis Foundation Therapeutic Development Network., (Copyright: © 2024 Calthorpe RJ et al.)

Published

2024

38. The adaptability of the ion-binding site by the Ag(I)/Cu(I) periplasmic chaperone SilF.

Author

Lithgo RM, Hanževački M, Harris G, Kamps JJAG, Holden E, Gianga TM, Benesch JLP, Jäger CM, Croft AK, Hussain R, Hobman JL, Orville AM, Quigley A, Carr SB, and Scott DJ

Subjects

Binding Sites, Ions metabolism, Molecular Chaperones genetics, Molecular Chaperones metabolism, Silver metabolism, Escherichia coli Proteins genetics, Escherichia coli Proteins metabolism, Copper metabolism, Escherichia coli metabolism

Abstract

The periplasmic chaperone SilF has been identified as part of an Ag(I) detoxification system in Gram-negative bacteria. Sil proteins also bind Cu(I) but with reported weaker affinity, therefore leading to the designation of a specific detoxification system for Ag(I). Using isothermal titration calorimetry, we show that binding of both ions is not only tighter than previously thought but of very similar affinities. We investigated the structural origins of ion binding using molecular dynamics and QM/MM simulations underpinned by structural and biophysical experiments. The results of this analysis showed that the binding site adapts to accommodate either ion, with key interactions with the solvent in the case of Cu(I). The implications of this are that Gram-negative bacteria do not appear to have evolved a specific Ag(I) efflux system but take advantage of the existing Cu(I) detoxification system. Therefore, there are consequences for how we define a particular metal resistance mechanism and understand its evolution in the environment., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

39. Comprehensive structural, infrared spectroscopic and kinetic investigations of the roles of the active-site arginine in bidirectional hydrogen activation by the [NiFe]-hydrogenase 'Hyd-2' from Escherichia coli .

Author

Evans RM, Beaton SE, Rodriguez Macia P, Pang Y, Wong KL, Kertess L, Myers WK, Bjornsson R, Ash PA, Vincent KA, Carr SB, and Armstrong FA

Abstract

The active site of [NiFe]-hydrogenases contains a strictly-conserved pendant arginine, the guanidine head group of which is suspended immediately above the Ni and Fe atoms. Replacement of this arginine (R479) in hydrogenase-2 from E. coli results in an enzyme that is isolated with a very tightly-bound diatomic ligand attached end-on to the Ni and stabilised by hydrogen bonding to the Nζ atom of the pendant lysine and one of the three additional water molecules located in the active site of the variant. The diatomic ligand is bound under oxidising conditions and is removed only after a prolonged period of reduction with H 2 and reduced methyl viologen. Once freed of the diatomic ligand, the R479K variant catalyses both H 2 oxidation and evolution but with greatly decreased rates compared to the native enzyme. Key kinetic characteristics are revealed by protein film electrochemistry: most importantly, a very low activation energy for H 2 oxidation that is not linked to an increased H/D isotope effect. Native electrocatalytic reversibility is retained. The results show that the sluggish kinetics observed for the lysine variant arise most obviously because the advantage of a more favourable low-energy pathway is massively offset by an extremely unfavourable activation entropy. Extensive efforts to establish the identity of the diatomic ligand, the tight binding of which is an unexpected further consequence of replacing the pendant arginine, prove inconclusive., Competing Interests: The authors report no conflict of interests., (This journal is © The Royal Society of Chemistry.)

Published

2023

40. Trajectories of early growth and subsequent lung function in cystic fibrosis: An observational study using UK and Canadian registry data.

Author

Macdougall A, Jarvis D, Keogh RH, Bowerman C, Bilton D, Davies G, Carr SB, and Stanojevic S

Subjects

Child, Humans, Child, Preschool, Infant, Forced Expiratory Volume, Routinely Collected Health Data, Canada epidemiology, Lung, United Kingdom epidemiology, Cystic Fibrosis

Abstract

Background: Understanding the pulmonary impact of changes in early life nutritional status over time in a paediatric CF population may help inform how to use nutritional assessment to guide clinical care. National registry data provides an opportunity to study patterns of weight gain over time at the level of the individual, and thus to gain detailed understanding of the relationship between early weight trajectories and later lung function in children with Cystic Fibrosis (CF)., Methods: Using data from the United Kingdom (UK) and Canadian CF Registries, a mixed effects linear regression model was used to describe children's weight and BMI z-score trajectories from age 1 to 5 years. The intercept (weight-for-age at age 1) and slope (weight-for-age trajectory) from this model were then used as covariates in a linear regression of first lung function measurement at age 6 years., Results: In both the UK and Canadian data, greater weight-for-age z-score at age 1 year and greater change in weight-for-age over time were associated with higher FEV 1 % predicted. A greater weight-for-age z-score at age 1 year was associated with a higher FEV 1 % predicted (UK: 3.78% (95% CI: 1.76; 4.70); Canada: 3.20% (95%CI: 1.76, 4.70)). These associations were reproduced for BMI z-scores and FVC% predicted., Conclusions: Early weight-for-age, specifically at age 1 year, and weight-for-age trajectories across early childhood are associated with later lung function. This relationship persists after adjustment for potential confounders. Current guidelines may need to be updated to place less emphasis on a specific cut-off (such as the 10th percentile) and encourage tracking of weight-for-age over time., Competing Interests: Declaration of Competing Interest CB, DJ and AM report no conflicts of interest. GD reports personal fees (speaker honoraria) from Vertex pharmaceuticals and Chiesi Limited, unrelated to the current work. SBC reports personal fees and other from Chiesi Pharmaceuticals, non-financial support and other from Vertex outside the submitted work. SS reports personal fees from Chiesi Pharmaceuticals unrelated to the current work., (Copyright © 2022 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2023

41. Response.

Author

Cameron RA, Rowley M, Simmonds NJ, Whitty JA, and Carr SB

Published

2023

42. Future therapies for cystic fibrosis.

Author

Allen L, Allen L, Carr SB, Davies G, Downey D, Egan M, Forton JT, Gray R, Haworth C, Horsley A, Smyth AR, Southern KW, and Davies JC

Subjects

Humans, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Mutation, Genetic Therapy, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics

Abstract

We are currently witnessing transformative change for people with cystic fibrosis with the introduction of small molecule, mutation-specific drugs capable of restoring function of the defective protein, cystic fibrosis transmembrane conductance regulator (CFTR). However, despite being a single gene disorder, there are multiple cystic fibrosis-causing genetic variants; mutation-specific drugs are not suitable for all genetic variants and also do not correct all the multisystem clinical manifestations of the disease. For many, there will remain a need for improved treatments. Those patients with gene variants responsive to CFTR modulators may have found these therapies to be transformational; research is now focusing on safely reducing the burden of symptom-directed treatment. However, modulators are not available in all parts of the globe, an issue which is further widening existing health inequalities. For patients who are not suitable for- or do not have access to- modulator drugs, alternative approaches are progressing through the trials pipeline. There will be challenges encountered in design and implementation of these trials, for which the established global CF infrastructure is a major advantage. Here, the Cystic Fibrosis National Research Strategy Group of the UK NIHR Respiratory Translational Research Collaboration looks to the future of cystic fibrosis therapies and consider priorities for future research and development., (© 2023. The Author(s).)

Published

2023

43. Treatment Preference Among People With Cystic Fibrosis: The Importance of Reducing Treatment Burden.

Author

Cameron RA, Office D, Matthews J, Rowley M, Abbott J, Simmonds NJ, Whitty JA, and Carr SB

Subjects

Adult, Female, Humans, Male, Quality of Life, Cystic Fibrosis Transmembrane Conductance Regulator, Respiratory Function Tests, Lung, Cystic Fibrosis complications

Abstract

Background: There is a growing consensus that the perspective of the patient should be considered in the evaluation of novel interventions., Research Question: What treatment outcomes matter to people with cystic fibrosis (CF), and what trade-offs would they make to realize these outcomes?, Study Design and Methods: Adults attending a specialist CF center were invited to complete an online discrete choice experiment (DCE). The DCE required participants to evaluate hypothetical CF treatment profiles, defined by impact on lung function, pulmonary exacerbations, abdominal symptoms, life expectancy, quality of life, inhaled medicine usage, and physiotherapy requirement. Choice data were analyzed, using multinomial logit and latent class models., Results: One hundred and three people with CF completed the survey (median age, 35 years; range, 18-76 years); 52% were female; mean FEV 1 % predicted, 69% [SD, 22%]). On average, an improvement in life expectancy by 10 years or more had the greatest impact on treatment preference, followed by a 15% increase in lung function. However, it was shown that people would trade substantial reductions in these key outcomes to reduce treatment time or burden. Preference profiles were not uniform across the sample: three distinct subgroups were identified, each placing markedly different importance on the relative importance of both life expectancy and lung function compared with other attributes., Interpretation: The relative importance of treatment burden to people with CF, compared with life expectancy and lung function, suggests it should be routinely captured in clinical trials as an important secondary outcome measure. When considering the patient perspective, it is important that decision-makers recognize that the values of people with CF are not homogeneous., (Copyright © 2022 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2022

44. Projecting the impact of triple CFTR modulator therapy on intravenous antibiotic requirements in cystic fibrosis using patient registry data combined with treatment effects from randomised trials.

Author

Keogh RH, Cosgriff R, Andrinopoulou ER, Brownlee KG, Carr SB, Diaz-Ordaz K, Granger E, Jewell NP, Lewin A, Leyrat C, Schlüter DK, van Smeden M, Szczesniak RD, and Connett GJ

Subjects

Aminophenols therapeutic use, Anti-Bacterial Agents therapeutic use, Benzodioxoles therapeutic use, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Humans, Mutation, Observational Studies as Topic, Randomized Controlled Trials as Topic, Registries, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics

Abstract

Background: Cystic fibrosis (CF) is a life-threatening genetic disease, affecting around 10 500 people in the UK. Precision medicines have been developed to treat specific CF-gene mutations. The newest, elexacaftor/tezacaftor/ivacaftor (ELEX/TEZ/IVA), has been found to be highly effective in randomised controlled trials (RCTs) and became available to a large proportion of UK CF patients in 2020. Understanding the potential health economic impacts of ELEX/TEZ/IVA is vital to planning service provision., Methods: We combined observational UK CF Registry data with RCT results to project the impact of ELEX/TEZ/IVA on total days of intravenous (IV) antibiotic treatment at a population level. Registry data from 2015 to 2017 were used to develop prediction models for IV days over a 1-year period using several predictors, and to estimate 1-year population total IV days based on standards of care pre-ELEX/TEZ/IVA. We considered two approaches to imposing the impact of ELEX/TEZ/IVA on projected outcomes using effect estimates from RCTs: approach 1 based on effect estimates on FEV 1 % and approach 2 based on effect estimates on exacerbation rate., Results: ELEX/TEZ/IVA is expected to result in significant reductions in population-level requirements for IV antibiotics of 16.1% (~17 800 days) using approach 1 and 43.6% (~39 500 days) using approach 2. The two approaches require different assumptions. Increased understanding of the mechanisms through which ELEX/TEZ/IVA acts on these outcomes would enable further refinements to our projections., Conclusions: This work contributes to increased understanding of the changing healthcare needs of people with CF and illustrates how Registry data can be used in combination with RCT evidence to estimate population-level treatment impacts., Competing Interests: Competing interests: SBC reports personal fees and other from Chiesi Pharmaceuticals, non-financial support and other from Vertex, other from Zambon, other from Insmed, outside the submitted work., (© Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY. Published by BMJ.)

Published

2022

45. The disease-specific clinical trial network for primary ciliary dyskinesia: PCD-CTN.

Author

Raidt J, Maitre B, Pennekamp P, Altenburg J, Anagnostopoulou P, Armengot M, Bloemsma LD, Boon M, Borrelli M, Brinkmann F, Carr SB, Carroll MP, Castillo-Corullón S, Coste A, Cutrera R, Dehlink E, Destouches DMS, Di Cicco ME, Dixon L, Emiralioglu N, Erdem Eralp E, Haarman EG, Hogg C, Karadag B, Kobbernagel HE, Lorent N, Mall MA, Marthin JK, Martinu V, Narayanan M, Ozcelik U, Peckham D, Pifferi M, Pohunek P, Polverino E, Range S, Ringshausen FC, Robson E, Roehmel J, Rovira-Amigo S, Santamaria F, Schlegtendal A, Szépfalusi Z, Tempels P, Thouvenin G, Ullmann N, Walker WT, Wetzke M, Yiallouros P, Omran H, and Nielsen KG

Abstract

Primary ciliary dyskinesia (PCD) is a rare genetic disorder characterised by impaired mucociliary clearance leading to irreversible lung damage. In contrast to other rare lung diseases like cystic fibrosis (CF), there are only few clinical trials and limited evidence-based treatments. Management is mainly based on expert opinions and treatment is challenging due to a wide range of clinical manifestations and disease severity. To improve clinical and translational research and facilitate development of new treatments, the clinical trial network for PCD (PCD-CTN) was founded in 2020 under the framework of the European Reference Network (ERN)-LUNG PCD Core. Applications from European PCD sites interested in participating in the PCD-CTN were requested. Inclusion criteria consisted of patient numbers, membership of ERN-LUNG PCD Core, use of associated standards of care, experience in PCD and/or CF clinical research, resources to run clinical trials, good clinical practice (GCP) certifications and institutional support. So far, applications from 22 trial sites in 18 European countries have been approved, including >1400 adult and >1600 paediatric individuals with PCD. The PCD-CTN is headed by a coordinating centre and consists of a steering and executive committee, a data safety monitoring board and committees for protocol review, training and standardisation. A strong association with patient organisations and industrial companies are further cornerstones. All participating trial sites agreed on a code of conduct. As CTNs from other diseases have demonstrated successfully, this newly formed PCD-CTN operates to establish evidence-based treatments for this orphan disease and to bring new personalised treatment approaches to patients., Competing Interests: Conflict of interest: J. Raidt declares grants for Clinical Research Unit “Male Germ Cells: from Genes to Function” (CRU 326) – Subproject RA3522/1-1 from the Deutsche Forschungsgemeinschaft, in connection with the present manuscript; that they are a holder of patent WO 2020/165352 A1 (Treatment of ciliopathies); and an unpaid role as a Deputy Director of PCD-CTN. Conflict of interest: B. Maitre declares unpaid roles as a Deputy Director of PCD-CTN and as a member of the scientific committee of RADICO PCD. Conflict of interest: P. Pennekamp declares research grants to their institution from NEOCYST (BMBF, 01GM1903A); and that they are a holder of patent WO 2020/165352 A1 (Treatment of ciliopathies). Conflict of interest: M. Armengot declares research grant FIS PI19/00949 from Instituto de Salud Carlos III, in connection with the present manuscript. Conflict of interest: M. Boon declares Forton grant 2020-J1810150-217926 from the King Baudouin Foundation, in the 36 months prior to manuscript submission. Conflict of interest: S.B. Carr declares grants to their institution from the National Institute of Health Research (Programme Development Grant 202952; Health Technology Assessment Grant NIHR121889; HTA grant 14/22/23; NIHR RfPb QOL-PCD; NIHR RfPb VALU- CF); consulting fees paid to their institution by Vertex Pharmaceuticals; personal and institutional honoraria from Chiesi Pharmaceuticals; payment to their institution for participation on a Data Safety Monitoring Board or Advisory Board from Profile Pharma, Pharmaxis and Vertex Pharmaceuticals, all in the 36 months prior to manuscript submission; and that they are Chair of the UK CF Registry Steering Committee (payment to their institution) and of the European CF Society Patient Registry Scientific Committee (unpaid). Conflict of interest: M.A. Mall declares research grant 82DZL009B1 from the German Federal Ministry of Education and Research, in connection with the present manuscript. Conflict of interest: M. Narayanan declares that they have been a co-applicant on the National Institute for Health Research – Research for patient benefit (NIHR –RfPB) grant for ‘Parent reported quality of life measures for young children with primary ciliary dyskinesia (QOL-PCD study)’ in the 36 months prior to manuscript submission; and that they are a member of the British Paediatric Respiratory Society executive committee and the British Thoracic Society standards of care committee. Conflict of interest: P. Pohunek declares research grants from the Ministry of Health of the Czech Republic (NV19-07-00210) and Charles University Grant Agency (670119P) in connection with the present manuscript. Conflict of interest: S. Range declares an unpaid role as medical advisor to PCD Support. Conflict of interest: F.C. Ringshausen declares grants to their institution from the German Center for Lung Research (DZL), the German Center for Infection Research (DZIF), IMI (EU/EFPIA), iABC Consortium (including Alaxia, Basilea, Novartis and Polyphor), Mukoviszidose Institute, Novartis, Insmed Germany, Grifols, Bayer and InfectoPharm; consulting fees from Parion, Grifols, Zambon, Insmed and the Helmholtz-Zentrum für Infektionsforschung; payments or honoraria from I!DE Werbeagentur GmbH; Interkongress GmbH; AstraZeneca; Insmed; Grifols and Universitätsklinikum Frankfurt am Main; payment to their institution for expert testimony at the Social Court Cologne; support for attending meetings from German Kartagener Syndrome and PCD PAG and Mukoviszidose e.V; participation on a Data Safety Monitoring Board or Advisory Board for Insmed, Grifols and Shionogi; fees for clinical trial participation paid to their institution by Abbvie, AstraZeneca, Boehringer Ingelheim, Celtaxsys, Corbus, Insmed, Novartis, Parion, University of Dundee, Vertex and Zambon; and honorary roles as Coordinator of the ERN-LUNG Bronchiectasis Core Network, Chair of the German Bronchiectasis Registry PROGNOSIS, Member of the SteerCo of the European Bronchiectasis Registry EMBARC, Member of the SteerCo of the European NTM Registry EMBARC-NTM, Co-Speaker of the Medical Advisory Board of the German Kartagener Syndrome and PCD PAG, Speaker of the Respiratory Infections and TB group of the German Respiratory Society (DGP), Speaker of the Cystic Fibrosis group of German Respiratory Society (DGP), PI of the DZL, member of the protocol review committee of the PCD-CTN and Member of Physician Association of the German Cystic Fibrosis PAG. Conflict of interest: J. Roehmel declares payments or honoraria from Vertex Pharmaceuticals, in the 36 months prior to manuscript submission. Conflict of interest: G. Thouvenin declares unpaid membership of the RADICO PCD scientific committee. Conflict of interest: H. Omran declares grants for Clinical Research Unit “Male Germ Cells: from Genes to Function” (CRU 326) – Subproject RA3522/1-1 from the Deutsche Forschungsgemeinschaft, from Interdisziplinaeres Zentrum für Klinische Forschung Muenster (Om2/009/12; Om2/015/16; Om2/010/20), from BESTCILIA (EU FP7 GA 305404) and from Registry Warehouse (Horizon2020 GA 777295), all in connection with the present manuscript; in addition to grants to their institution from LYSOCIL (Horizon2020 GA n°811087) NEOCYST (BMBF, 01GM1903A) and Transkripttherapie für primäre ziliäre Dyskinesien (Zentrales Innovationsprojekt Mittelstand (ZIM), BMWi; ZF-4610102SK8), in the 36 months prior to manuscript submission; that they are a holder of patent WO 2020/165352 A1 (Treatment of ciliopathies); and unpaid roles as Head of the ERN-LUNG PCD Core and as a member of the PCD Family Support Group medical advisory board. Conflict of interest: K.G. Nielsen declares funding for the present manuscript from the Danish Children's Lung Foundation (Børnelungefonden); and an unpaid role as a Director of the PCD-CTN. Conflict of interest: All other authors declare no competing interests., (Copyright ©The authors 2022.)

Published

2022

46. Factors associated with clinical progression to severe COVID-19 in people with cystic fibrosis: A global observational study.

Author

Carr SB, McClenaghan E, Elbert A, Faro A, Cosgriff R, Abdrakhmanov O, Brownlee K, Burgel PR, Byrnes CA, Cheng SY, Colombo C, Corvol H, Daneau G, Goss CH, Gulmans V, Gutierrez H, Harutyunyan S, Helmick M, Jung A, Kashirskaya N, McKone E, Melo J, Middleton PG, Mondejar-Lopez P, de Monestrol I, Nährlich L, Padoan R, Parker M, Pastor-Vivero MD, Rizvi S, Ruseckaite R, Salvatore M, da Silva-Filho LVRF, Versmessen N, Zampoli M, Marshall BC, and Stephenson AL

Subjects

Cystic Fibrosis Transmembrane Conductance Regulator, Ethnicity, Humans, Minority Groups, Oxygen, SARS-CoV-2, COVID-19 epidemiology, COVID-19 therapy, Cystic Fibrosis complications, Cystic Fibrosis epidemiology, Cystic Fibrosis therapy

Abstract

Background: This international study aimed to characterise the impact of acute SARS-CoV-2 infection in people with cystic fibrosis and investigate factors associated with severe outcomes. Methods Data from 22 countries prior to 13 th December 2020 and the introduction of vaccines were included. It was de-identified and included patient demographics, clinical characteristics, treatments, outcomes and sequalae following SARS-CoV-2 infection. Multivariable logistic regression was used to investigate factors associated with clinical progression to severe COVID-19, using the primary outcome of hospitalisation with supplemental oxygen., Results: SARS-CoV-2 was reported in 1555 people with CF, 1452 were included in the analysis. One third were aged <18 years, and 9.4% were solid-organ transplant recipients. 74.5% were symptomatic and 22% were admitted to hospital. In the non-transplanted cohort, 39.5% of patients with ppFEV1<40% were hospitalised with oxygen verses 3.2% with ppFEV >70%: a 17-fold increase in odds. Worse outcomes were independently associated with older age, non-white race, underweight body mass index, and CF-related diabetes. Prescription of highly effective CFTR modulator therapies was associated with a significantly reduced odds of being hospitalised with oxygen (AOR 0.43 95%CI 0.31-0.60 p<0.001). Transplanted patients were hospitalised with supplemental oxygen therapy (21.9%) more often than non-transplanted (8.8%) and was independently associated with the primary outcome (Adjusted OR 2.45 95%CI 1.27-4.71 p=0.007)., Conclusions: This is the first study to show that there is a protective effect from the use of CFTR modulator therapy and that people with CF from an ethnic minority are at more risk of severe infection with SARS-CoV-2., Competing Interests: COI Statement All authors declare no conflicts of interest in relationship to this work. Outside of this work the following authors declare payments or honoraria to them or their institution for a combination of lectures, presentations, educational events, advisory boards, steering groups, grants or consultancy fees: SC-Vertex, Chiesi, Profile, Zambon. RC- Vertex, P-RB – Astra-Zeneca, Boehringer Ingelheim, GSK, Insmed, Chiesi, Pfizer, Vertex, Zambon. I deM – Vertex,LN – Vertex, Boehringer,LVS-F – Vertex, AS -Vertex., (Copyright © 2022. Published by Elsevier B.V.)

Published

2022

47. An Update on CFTR Modulators as New Therapies for Cystic Fibrosis.

Author

King JA, Nichols AL, Bentley S, Carr SB, and Davies JC

Subjects

Aminophenols pharmacology, Aminophenols therapeutic use, Benzodioxoles pharmacology, Benzodioxoles therapeutic use, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Drug Combinations, Genetic Therapy, Humans, Mutation, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics

Abstract

Over the past decade there have been significant developments in the field of Cystic Fibrosis Transmembrane Regulator modulator drugs. Following treatment in patients with cystic fibrosis with common gating mutations using the potentiator drug ivacaftor, successive development of corrector drugs used in combination has led to highly effective modulator therapy being available to more than 85% of the cystic fibrosis population over 12 years of age in the form of elexacaftor/tezacaftor/ivacaftor. In this article, we review the evidence from clinical trials and mounting real-world observational and registry data that demonstrates the impact highly effective modulators have on both pulmonary and extra-pulmonary manifestations of cystic fibrosis. As clinical trials progress to younger patient groups, we discuss the challenges to demonstrating drug efficacy in early life, and also consider practicalities of drug development in an ever-shrinking modulator-naïve population. Drug-drug interactions are an important consideration in people with cystic fibrosis, where polypharmacy is commonplace, but also as the modulated population look to remain healthier for longer, we identify trials that aim to address treatment burden too. Inequity of care, through drug cost or ineligibility for modulators by genotype, is widening without apparent strategies to address this; however, we present evidence of hopeful early-stage drug development for non-modulatable genes and summarise the current state of gene-therapy development., (© 2022. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published

2022

48. Initiating home spirometry for children during the COVID-19 pandemic - A practical guide.

Author

Richardson CH, Orr NJ, Ollosson SL, Irving SJ, Balfour-Lynn IM, and Carr SB

Subjects

Child, Humans, Pandemics, Asthma, COVID-19, Spirometry

Abstract

The COVID-19 pandemic has led to a rapid escalation in use of home monitoring and video consultations in children with a variety of chronic respiratory conditions. Our department set up a home spirometry service from scratch once it became evident that we needed to keep patients away from hospital clinics whenever possible. We faced a number of challenges but now have around 400 children using home spirometers. There are a number of portable spirometers available, some with online platforms. The technology, particularly the software/apps interface, has been improved by the companies in response to issues that have arisen. We believe the use of home monitoring is here to stay., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2022

49. Childhood bronchiectasis, so little is known.

Author

Carr SB and Unger SA

Subjects

Child, Humans, Infant, Bronchiectasis epidemiology, Bronchiectasis etiology

Abstract

Competing Interests: Competing interests: None declared.

Published

2022

50. Exploring the nature of perceived treatment burden: a study to compare treatment burden measures in adults with cystic fibrosis [version 1; peer review: 2 approved].

Author

Altabee R, Carr SB, Abbott J, Cameron R, Office D, Matthews J, Simmonds N, Cosgriff R, Turner D, and Whitty J

Abstract

Background: Despite the importance of reducing treatment burden for people with cystic fibrosis (CF), it has not been fully understood as a concept. This study aims to quantify the treatment burden perceived by CF adults and explore the association between different validated treatment burden measures., Methods: This is a cross-sectional observational study of CF adults attending a single large UK adult center. Participants completed an online survey that contained three different treatment burden scales; CF Questionnaire-Revised (CFQ-R) subscale, CF Quality of Life (CFQoL) subscale, and the generic multimorbidity treatment burden questionnaire (MTBQ)., Results: Among 101 participants, the median reported treatment burden by the CFQ-R subscale was 55.5 (IQR 33.3 - 66.6), the CFQoL subscale was 66.6 (IQR 46.6 - 86.6), and the MTBQ reversed global score was 84.6 (IQR 73.1 - 92.3). No correlation was found between respondents' demographic or clinical variables and treatment burden measured via any of the three measures. All treatment burden measures showed correlations against each other. More treatments were associated with high treatment burden as measured by the CFQ-R, CFQoL subscales, and the MTBQ. However, longer treatment time and more complex treatment plans were correlated with high treatment burden as measured by the CFQ-R and CFQoL subscales, but not with the MTBQ., Conclusions: Treatment burden is a substantial issue in CF. Currently, the only available way to evaluate it is with the CF-specific quality of life measure treatment burden subscales (CFQ-R and CFQoL); both indicated that treatment burden increases with more treatments, longer treatment time, and more complex treatments., Competing Interests: Competing interests: RA, JA, RCo, DO, JM, RCa, DT, SC, NS and JW have no direct conflicts of interest to declare in relation to this study. Outside of the submitted work, SC has served on advisory boards and/or given educational lectures for which she or her institution have received fees for (Vertex, Chiesi, and Profile Pharma). NS has served on advisory boards and/or given educational lectures for which he has received consultancy fees (Vertex, Gilead, Chiesi, Zambon, Roche, and Menarini).

Published

2022