Your search keyword '"Kerecuk L"' showing total 69 results

1. Epstein–Barr virus-associated lymphoproliferative disease in oral cavity in a renal transplant recipient: A case report

Author

Johnson, J., Kerecuk, L., Harrison, M., Taylor, J. O., and Odell, E.

Published

2007

2. What delay should there be between primary infectious mononucleosis and renal transplantation?

Author

Kerecuk, L., Amlot, P., Riad, H., and Webb, N. J. A.

Published

2006

3. Current management of transition of young people affected by rare renal conditions in the ERKNet

Author

Kreuzer, M., Drube, J., Prufe, J., Schaefer, F., Pape, L., Ariceta, G., Kerecuk, L., Bassanese, G., Wlodkowski, T., Capasso, G., Trepiccione, F., Biebuyck, N., Ferraro, Pietro Manuel, Galetti, F., Bouts, A., Ferraro P. M. (ORCID:0000-0002-1379-022X), Kreuzer, M., Drube, J., Prufe, J., Schaefer, F., Pape, L., Ariceta, G., Kerecuk, L., Bassanese, G., Wlodkowski, T., Capasso, G., Trepiccione, F., Biebuyck, N., Ferraro, Pietro Manuel, Galetti, F., Bouts, A., and Ferraro P. M. (ORCID:0000-0002-1379-022X)

Abstract

Transition in medical care is a high-risk period in adolescence and young adulthood. To date, data on transition policy, its application in practice, and transition procedures in patients with rare, hereditary kidney diseases in Europe is scarce. An online survey was developed and was distributed within the paediatric centres of the European Reference Network for Rare Kidney Diseases (ERKNet) aiming to assess the transition-relevant structures from the providers’ perspectives. Its items were based on the consensus statement on transition published by the International Society of Nephrology (ISN) and the International Paediatric Nephrology Association (IPNA) in 2011. Forty-six paediatric experts based at 28/32 ERKNet university hospitals participated. Annually, a median number of 14 patients (1–80) are transferred to adult based care. One centre continued to care for paediatric kidney transplant recipients throughout their entire lifespan. Choosing this option terminated the survey and no further data was obtained from this centre. 29/45 experts confirmed the application of an—at least unwritten—transition procedure (64%). Transition clinics are offered by 23 experts. Most physicians (40%) transfer patients at age 18–19, 10 experts at age <18. Most physicians transfer the patients to a university hospital and/or a community hospital. The transition guidelines have been implemented in ERKNet centres only partly and with huge heterogeneity. Implementation of transition tools and structures within ERKNet could improve health of children with hereditary kidney diseases. Adherence of experts to the transition-guidelines was significantly correlated with gross national income of their countries.

Published

2019

4. G608(P) Understanding the spiritual and emotional needs of siblings of children with a rare disease from the young person’s and parental perspectives

Author

Nash, P, primary, Bryson, L, additional, Roberts, E, additional, Kerecuk, L, additional, Gray, S, additional, and Nash, S, additional

Published

2019

5. G256(P) What are the preferences for receiving additional and carrier status findings in genomics testing amongst families affected by rare conditions? Findings from the rare disease arm of the 100,000 genomes project at a specialised paediatric centre in the UK

Author

Kokocinska, M, primary, Kerecuk, L, additional, and Parkes, S, additional

Published

2019

6. G609(P) Understanding the impact of ‘wish-granting’ interventions on children with life threatening health conditions and their families

Author

Heath, G, primary, Screti, C, additional, Pattison, H, additional, Knibb, R, additional, Kerecuk, L, additional, Cook, J, additional, and Dowling, L, additional

Published

2019

7. Mutations in multiple components of the nuclear pore complex cause nephrotic syndrome

Author

Braun, D.A., Lovric, S., Schapiro, D., Schneider, R., Marquez, J., Asif, M., Hussain, M.S., Daga, A., Widmeier, E., Rao, J., Ashraf, S., Tan, W., Lusk, C.P., Kolb, A., Jobst-Schwan, T., Schmidt, J.M., Hoogstraten, C.A., Eddy, K., Kitzler, T.M., Shril, S., Moawia, A., Schrage, K., Khayyat, A.I.A., Lawson, J.A., Gee, H.Y., Warejko, J.K., Hermle, T., Majmundar, A.J., Hugo, H., Budde, B., Motameny, S., Altmuller, J., Noegel, A.A., Fathy, H.M., Gale, D.P., Waseem, S.S., Khan, A., Kerecuk, L., Hashmi, S., Mohebbi, N., Ettenger, R., Serdaroglu, E., Alhasan, K.A., Hashem, M., Goncalves, S., Ariceta, G., Ubetagoyena, M., Antonin, W., Baig, S.M., Alkuraya, F.S., Shen, Q., Xu, H., Antignac, C., Lifton, R.P., Mane, S., Nurnberg, P., Khokha, M.K., Hildebrandt, F., Braun, D.A., Lovric, S., Schapiro, D., Schneider, R., Marquez, J., Asif, M., Hussain, M.S., Daga, A., Widmeier, E., Rao, J., Ashraf, S., Tan, W., Lusk, C.P., Kolb, A., Jobst-Schwan, T., Schmidt, J.M., Hoogstraten, C.A., Eddy, K., Kitzler, T.M., Shril, S., Moawia, A., Schrage, K., Khayyat, A.I.A., Lawson, J.A., Gee, H.Y., Warejko, J.K., Hermle, T., Majmundar, A.J., Hugo, H., Budde, B., Motameny, S., Altmuller, J., Noegel, A.A., Fathy, H.M., Gale, D.P., Waseem, S.S., Khan, A., Kerecuk, L., Hashmi, S., Mohebbi, N., Ettenger, R., Serdaroglu, E., Alhasan, K.A., Hashem, M., Goncalves, S., Ariceta, G., Ubetagoyena, M., Antonin, W., Baig, S.M., Alkuraya, F.S., Shen, Q., Xu, H., Antignac, C., Lifton, R.P., Mane, S., Nurnberg, P., Khokha, M.K., and Hildebrandt, F.

Abstract

Item does not contain fulltext, Steroid-resistant nephrotic syndrome (SRNS) almost invariably progresses to end-stage renal disease. Although more than 50 monogenic causes of SRNS have been described, a large proportion of SRNS remains unexplained. Recently, it was discovered that mutations of NUP93 and NUP205, encoding 2 proteins of the inner ring subunit of the nuclear pore complex (NPC), cause SRNS. Here, we describe mutations in genes encoding 4 components of the outer rings of the NPC, namely NUP107, NUP85, NUP133, and NUP160, in 13 families with SRNS. Using coimmunoprecipitation experiments, we showed that certain pathogenic alleles weakened the interaction between neighboring NPC subunits. We demonstrated that morpholino knockdown of nup107, nup85, or nup133 in Xenopus disrupted glomerulogenesis. Re-expression of WT mRNA, but not of mRNA reflecting mutations from SRNS patients, mitigated this phenotype. We furthermore found that CRISPR/Cas9 knockout of NUP107, NUP85, or NUP133 in podocytes activated Cdc42, an important effector of SRNS pathogenesis. CRISPR/Cas9 knockout of nup107 or nup85 in zebrafish caused developmental anomalies and early lethality. In contrast, an in-frame mutation of nup107 did not affect survival, thus mimicking the allelic effects seen in humans. In conclusion, we discovered here that mutations in 4 genes encoding components of the outer ring subunits of the NPC cause SRNS and thereby provide further evidence that specific hypomorphic mutations in these essential genes cause a distinct, organ-specific phenotype.

Published

2018

8. G33(P) Overview of rare renal diseases at a paediatric renal centre through the national registry of rare kidney diseases (radar) in the united kingdom

Author

Kerecuk, L, primary, Kokocinska, M, additional, Parkes, S, additional, Kainth, J, additional, and Dillon, M, additional

Published

2018

9. G400(P) An integrated ‘one-stop’ multi-disciplinary (mdt) clinic for children and young people with tuberous sclerosis complex (tsc)

Author

Raja, M, primary, Philip, S, additional, Agrawal, S, additional, McKerracher, G, additional, Rhodehouse, K, additional, Tuberville-Greenley, J, additional, Hussain, J, additional, and Kerecuk, L, additional

Published

2018

10. G465(P) Factors influencing renal transplant graft outcomes following transition: time to personalise services

Author

Gupta, A, primary, Kerecuk, L, additional, Lipkin, G, additional, Milford, D, additional, Hodson, J, additional, Pankhurst, T, additional, Edward, C, additional, Manley, M, additional, McLoughlin-Yip, L, additional, and Thompson, M, additional

Published

2017

11. G213 Abstract: Undiagnosed Diseases in a Specialist Children’s Hospital

Author

Vincent, H, primary, Roza, S Da, additional, and Kerecuk, L, additional

Published

2017

12. Kidney Versus Combined Kidney and Liver Transplantation in Young People With Autosomal Recessive Polycystic Kidney Disease: Data From the European Society for Pediatric Nephrology/European Renal Association-European Dialysis and Transplant (ESPN/ERA-EDTA) Registry

Author

Mekahli, D., Stralen, K.J. van, Bonthuis, M., Jager, K.J., Balat, A., Benetti, E., Godefroid, N., Edvardsson, V.O., Heaf, J.G., Jankauskiene, A., Kerecuk, L., Marinova, S., Puteo, F., Seeman, T., Zurowska, A., Pirenne, J., Schaefer, F., Groothoff, J.W., Hoitsma, A.J., et al., Mekahli, D., Stralen, K.J. van, Bonthuis, M., Jager, K.J., Balat, A., Benetti, E., Godefroid, N., Edvardsson, V.O., Heaf, J.G., Jankauskiene, A., Kerecuk, L., Marinova, S., Puteo, F., Seeman, T., Zurowska, A., Pirenne, J., Schaefer, F., Groothoff, J.W., Hoitsma, A.J., and et al.

Abstract

Item does not contain fulltext, BACKGROUND: The choice for either kidney or combined liver-kidney transplantation in young people with kidney failure and liver fibrosis due to autosomal recessive polycystic kidney disease (ARPKD) can be challenging. We aimed to analyze the characteristics and outcomes of transplantation type in these children, adolescents, and young adults. STUDY DESIGN: Cohort study. SETTING & PARTICIPANTS: We derived data for children, adolescents, and young adults with ARPKD with either kidney or combined liver-kidney transplants for 1995 to 2012 from the ESPN/ERA-EDTA Registry, a European pediatric renal registry collecting data from 36 European countries. FACTOR: Liver transplantation. OUTCOMES & MEASUREMENTS: Transplantation and patient survival. RESULTS: 202 patients with ARPKD aged 19 years or younger underwent transplantation after a median of 0.4 (IQR, 0.0-1.4) years on dialysis therapy at a median age of 9.0 (IQR, 4.1-13.7) years. 32 (15.8%) underwent combined liver-kidney transplantation, 163 (80.7%) underwent kidney transplantation, and 7 (3.5%) were excluded because transplantation type was unknown. Age- and sex-adjusted 5-year patient survival posttransplantation was 95.5% (95% CI, 92.4%-98.8%) overall: 97.4% (95% CI, 94.9%-100.0%) for patients with kidney transplantation in contrast to 87.0% (95% CI, 75.8%-99.8%) with combined liver-kidney transplantation. The age- and sex-adjusted risk for death after combined liver-kidney transplantation was 6.7-fold (95% CI, 1.8- to 25.4-fold) greater than after kidney transplantation (P=0.005). Five-year death-censored kidney transplant survival following combined liver-kidney and kidney transplantation was similar (92.1% vs 85.9%; P=0.4). LIMITATIONS: No data for liver disease of kidney therapy recipients. CONCLUSIONS: Combined liver-kidney transplantation in ARPKD is associated with increased mortality compared to kidney transplantation in our large observational study and was not associated with improved 5-year kidney transp

Published

2016

13. G115(P) Use of mTOR inhibitors in children with tuberous sclerosis complex for renal angiomyolipomatosis – does it have secondary benefits on seizures and adenoma sebaceum?

Author

Kumar, R, primary, Milford, D, additional, Kerecuk, L, additional, and Philip, SG, additional

Published

2016

14. G391(P) A case report highlighting unusual benign radiological lesions in a hydronephrotic kidney

Author

Tabb, E, primary, Clark, M, additional, and Kerecuk, L, additional

Published

2016

15. Autosomal dominant inheritance of non-syndromic renal hypoplasia and dysplasia: dramatic variation in clinical severity in a single kindred

Author

Kerecuk L, Sajoo A, McGregor L, Berg J, Haq MR, Sebire NJ, Bingham C, Edghill EL, Ellard S, Taylor J, Rigden S, Flinter FA, Woolf AS

Published

2007

16. Renal tract malformations: perspectives for nephrologists.

Author

Kerecuk, L., Schreuder, M.F., Woolf, A.S., Kerecuk, L., Schreuder, M.F., and Woolf, A.S.

Abstract

Contains fulltext : 71176.pdf (publisher's version ) (Closed access), Renal tract malformations are congenital anomalies of the kidneys and/or lower urinary tract. One challenging feature of these conditions is that they can present not only prenatally but also in childhood or adulthood. The most severe types of malformations, such as bilateral renal agenesis or dysplasia, although rare, lead to renal failure. With advances in dialysis and transplantation for young children, it is now possible to prevent the early death of at least some individuals with severe malformations. Other renal tract malformations, such as congenital pelviureteric junction obstruction and primary vesicoureteric reflux, are relatively common. Renal tract malformations are, collectively, the major cause of childhood end-stage renal disease. Their contribution to the number of adults on renal replacement therapy is less clear and has possibly been underestimated. Renal tract malformations can be familial, and specific mutations of genes involved in renal tract development can sometimes be found in affected individuals. These features provide information about the causes of malformations but also raise questions about whether to screen relatives. Whether prenatal decompression of obstructed renal tracts, or postnatal initiation of therapies such as prophylactic antibiotics or angiotensin blockade, improve long-term renal outcomes remains unclear.

Published

2008

17. Autosomal dominant inheritance of non-syndromic renal hypoplasia and dysplasia: dramatic variation in clinical severity in a single kindred

Author

Kerecuk, L., primary, Sajoo, A., additional, McGregor, L., additional, Berg, J., additional, Haq, M. R., additional, Sebire, N. J., additional, Bingham, C., additional, Edghill, E. L., additional, Ellard, S., additional, Taylor, J., additional, Rigden, S., additional, Flinter, F. A., additional, and Woolf, A. S., additional

Published

2006

18. Genetic Heterogeneity of Familial Congenital Anomalies of the Kidney and Urinary Tract

Author

Burgess, K., Sanna-Cherchi, S., Weng, P. L., Gianluca Caridi, Bodria, M., Testa, S., Kerecuk, L., Ardissino, G., Woolf, A. S., Scolari, F., Ghiggeri, G. M., and Gharavi, A.

19. G33(P) Overview of rare renal diseases at a paediatric renal centre through the national registry of rare kidney diseases (radar) in the united kingdom

Author

Kerecuk, L, Kokocinska, M, Parkes, S, Kainth, J, and Dillon, M

Abstract

AimsRare kidney diseases need better understanding and the starting point is collection of clinical data. Therefore our centre is participating in RaDaR which is a UK Renal Association initiative designed to gather information. RaDaR recruitment began in 2010 and now covers more than 40 conditions. There are around 10 000 recruits from 78 renal adult and paediatric units in the UK. Our Paediatric Renal Centre is the leading recruiting hospital in the UK.To describe the range of range of conditions and patient numbers recruited to RADAR at BCH which is a national tertiary renal referral hospital in the UK.MethodsThe RaDaR dataset is defined by the UK Renal Registry in association with the Rare Disease Groups, made up of experts in each eligible condition. Data fields include demographics, blood and urine results, medications, transplant and dialysis history, genetics and co-morbidities. Data is entered retrospectively from the patient’s medical records following consent.Results319 patients have been consented at BCH. The age range is from birth to 16 years with mean of 4.9 years with male to female ratio of 55%:45%. The most common condition is Idiopathic Nephrotic Syndrome (n=128; 39%), followed by Alport Syndrome (n=33; 10%), ARPKD (n=25; 8%), Hyperoxaluria (n=24; 7%) and STEC HUS (n=22; 7%). The other conditions with numbers of patients recruited so far include: ADPKD (n=14), aHUS (n=13); Cystinosis (n=9); Cystinuria (n=3); Dent and Lowe (n=7); HNF1b (n=6); Hypokalaemic Alkalosis (n=8); MPGN (n=14) and Vasculitis (n=7).ConclusionRaDaR provides important epidemiology data based on the whole country population which is shared amongst the renal team to develop further research into rare kidney diseases and improve the quality of care for these patients. It also gives an opportunity to define the best treatment practices across the country in the future.

Published

2018

20. G213 Abstract: Undiagnosed Diseases in a Specialist Children’s Hospital

Author

Vincent, H, Roza, S Da, and Kerecuk, L

Abstract

AimsThere is limited information on how many patients are undiagnosed. The aim was to evaluate the proportion of paediatric inpatients without a diagnosis on Undiagnosed Day in a specialist hospital serving both the general local population, and tertiary referrals in 34 specialties.MethodsOn ‘Undiagnosed Day 2016’ (29/04/16), all inpatient notes were reviewed to establish whether an overarching diagnosis existed. Demographics, specialty and reason for admission were collected, as well as how diagnosis was made (if at all). The data was analysed to show the proportion of patients with no definitive diagnosis per specialty.ResultsThere were 270 inpatients and data was collected for 269. The male to female ratio was 56%: 44%, ages ranged from 0–17 years. 49 out of the 269 patients (18.2%) had no overarching diagnosis, with the highest proportion by age being 8 years. This varied in each specialty including 15.2% in general paediatrics, 31% in neurology and 36% in respiratory and hepatology.Figure 167% of admissions were acute, 28% elective and 5% tertiary transfers. The proportion of undiagnosed patients was 31% in tertiary transfers, 22% in acute admissions and 15% in elective cases. Of all undiagnosed cases, 50% had multiple problems, affecting two or more systems. These patients may have a rare syndrome, multiple diagnoses, an uncommon presentation of a common condition or there may not be a diagnosis.ConclusionIn this snapshot review of inpatients in a major specialist UK hospital, 18.2% do not have an overarching diagnosis. Effective treatment is more challenging. For families, not having a prognosis and knowing whether other family members are affected is distressing. SWAN UK, the UK charity supporting undiagnosed families, reports the struggle of having their child’s needs taken seriously and in accessing services. In the UK, the 100K Genome Project is enrolling patients without an underlying genetic diagnosis.

Published

2017

21. G400(P) An integrated ‘one-stop’ multi-disciplinary (mdt) clinic for children and young people with tuberous sclerosis complex (tsc)

Author

Raja, M, Philip, S, Agrawal, S, McKerracher, G, Rhodehouse, K, Tuberville-Greenley, J, Hussain, J, and Kerecuk, L

Abstract

TSC is a complex, genetic disorder characterised by growth of benign tumours in various organs leading to epilepsy, renal, cardiac, skin, lung, liver and eye manifestations. Thus, patients affected attend multiple clinic appointments with different specialists. Developmental delay and TSC-associated neuropsychiatric disorders (TANDS) are common but often not addressed.AimsTo improve the care of children and young people affected by TSC by an integrated multidisciplinary team (MDT) ‘one–stop’ clinic.To provide psychological assessment of TANDS.MethodThe MDT TSC clinic was launched in April 2016 by coordinating neurology, nephrology, oncology, psychology consultants with the Rhoald Dhal Rare Disease (RD) Specialist nurses and Tuberous Sclerosis Advisor (TSA) on same visit. Psychology input was funded by a Pharma Joint Working Agreement. The RD nurse provides Information Packs and calls families to discuss what their main concerns are, thereby enabling clinicians to address what is relevant to patients.ResultsThe TSC MDT clinic has:Improved coordination of specialists and investigations.Feedback from PatientQuestionnaires: ‘this should have been started a long time ago’, ‘this is a fabulous idea, saves us time’, ‘having all the specialists together makes so much sense -they can explain in a way that we can understand’.55% of families were not aware of the TSA98 patients identified with TSC by joining lists kept by each specialty. Average patient age 10.3 years. (range: 1.6–21.1 years.). 38% had previous renal input; 42% had not had a renal ultrasound. 66% had neurology input but 33% had no brain imaging.The Appointment Burden before TSC clinic was reviewed: showed average appointment number/patient was 5.3/year (range 0.6–11.7/yr.).40% of Patients in TSC clinic required further psychology input20% referred for formal CAMHS review.Patients above age of 16 years. reviewed by the adult TSC transition nurses from adult sister hospital.ConclusionThe MDT TSC clinic has improved coordinated patient care including ensuring imaging is regularly carried out. It has identified high burden of psychological need. Overall, this ‘one-stop’ clinic system has improved the care the patients and families with TSC.

Published

2018

22. G465(P) Factors influencing renal transplant graft outcomes following transition: time to personalise services

Author

Gupta, A, Kerecuk, L, Lipkin, G, Milford, D, Hodson, J, Pankhurst, T, Edward, C, Manley, M, McLoughlin-Yip, L, and Thompson, M

Abstract

AimsThere has been much focus on building effective transition programmes for patients with chronic illness including chronic kidney disease. The structure of current transition programmes can be variable with financial as well as human resource restraints. We aimed to review factors, which influence graft function following the introduction of a transition programme for within our region to identify those at risk of poor outcome.MethodsData was collected for two groups of patients: nontransition group (pre 2006) and transitioned group (post 2006). This included transplant details, donor type, age at transplant and diagnosis of intellectual disability (ID). In addition, further data was retrospectively collected at 6 monthly intervals for age, height, creatinine, blood pressure, tacrolimus levels, non-attendances and rejection episodes. GFR was estimated using the modified Schwartz formula and analysed using segmented linear regression analysis. These models contained two covariates which estimated overall GFR gradient and the magnitude of change in gradient post-transfer. Follow-up was truncated at 2 years pre- and 4 years post transfer to prevent patients with longer follow-up becoming influential outliers.ResultsFollowing implementation of a transition programme rate of GRF decline was significantly lower for transitioned (n=30) compared with non-transitioned patients (p=0.028).GFR declined significantly faster pre-transition in patients who received deceased donor organs (p=0.004), were transplanted at <13 years old (p=0.016), had a lower GFR at transfer (p<0.001), no ID (p=0002) had more than 0.5 non-attendances at adult unit/year or the tour (p<0.001).After transition, patients that attended the tour (p=0.001) or attended with >0.5 attendances at the adult (p=0.022) unit did significantly better.Subgroup analysis for transitioned patients was then performed (see table). Comparing those with GFR of <30 (n=8) and 30 (n=22) at transfer, we found that patients in the lower GFR group had a significantly faster decline pre-transition ( 11.9 vs 4.9 ml/min/1.73 m2/year, p<0.001). Post-transfer improvement in the GFR <30 group was significantly greater than in 30 group (p=0.003), resulting in gradients in two groups being similar after transfer ( 2.4 vs 3.4 ml/min/1.73 m2/year).ConclusionsIdentifying those at risk of poor prognosis following transfer to adult care is crucial to help modify and personalise transition services.

Published

2017

23. Current management of transition of young people affected by rare renal conditions in the ERKNet

Author

Kreuzer, Martin, Drube, Jens, Prüfe, Jenny, Schaefer, Franz, Pape, Lars, Ariceta, Gema, Kerecuk, Larissa, Bassanese, Giulia, Wlodkowski, Tanja, Capasso, Giovanni, Trepiccione, Francesco, Biebuyck, Natalie, Ferraro, Pietro Manuel, Galetti, Flavia, Bouts, Antonia, Amsterdam Reproduction & Development (AR&D), Kreuzer, M., Drube, J., Prufe, J., Schaefer, F., Pape, L., Ariceta, G., Kerecuk, L., Bassanese, G., Wlodkowski, T., Capasso, G., Trepiccione, F., Biebuyck, N., Ferraro, P. M., Galetti, F., Bouts, A., Paediatric Nephrology, and ARD - Amsterdam Reproduction and Development

Subjects

Adult, Male, Nephrology, medicine.medical_specialty, Kidney Disease, Adolescent, MEDLINE, Kidney, Article, Young Adult, 03 medical and health sciences, Rare Diseases, Rare Disease, Internal medicine, Genetics, medicine, Humans, Settore MED/14 - NEFROLOGIA, In patient, Young adult, Child, Genetics (clinical), 0303 health sciences, business.industry, digestive, oral, and skin physiology, 030305 genetics & heredity, University hospital, Community hospital, Europe, Gross national income, Current management, Family medicine, Kidney Diseases, NA, Female, business, Human

Abstract

Transition in medical care is a high-risk period in adolescence and young adulthood. To date, data on transition policy, its application in practice, and transition procedures in patients with rare, hereditary kidney diseases in Europe is scarce. An online survey was developed and was distributed within the paediatric centres of the European Reference Network for Rare Kidney Diseases (ERKNet) aiming to assess the transition-relevant structures from the providers' perspectives. Its items were based on the consensus statement on transition published by the International Society of Nephrology (ISN) and the International Paediatric Nephrology Association (IPNA) in 2011. Forty-six paediatric experts based at 28/32 ERKNet university hospitals participated. Annually, a median number of 14 patients (1-80) are transferred to adult based care. One centre continued to care for paediatric kidney transplant recipients throughout their entire lifespan. Choosing this option terminated the survey and no further data was obtained from this centre. 29/45 experts confirmed the application of an-at least unwritten-transition procedure (64%). Transition clinics are offered by 23 experts. Most physicians (40%) transfer patients at age 18-19, 10 experts at age

Published

2019

24. Preferences for coordinated care for rare diseases: discrete choice experiment.

Author

Morris S, Walton H, Simpson A, Leeson-Beevers K, Bloom L, Hunter A, Ramsay AIG, Fulop NJ, Chitty LS, Kai J, Sutcliffe AG, Kokocinska M, Kerecuk L, Taylor CA, and Ng PL

Subjects

Humans, Male, Female, Surveys and Questionnaires, Adult, Middle Aged, Patient Preference, Health Personnel psychology, Young Adult, Rare Diseases

Abstract

Background: Evidence suggests that coordination of care for people affected by rare diseases is poor. In order to improve the way that care is coordinated it is necessary to understand the preferences of people affected by these conditions, and providers. The aim of this study was to examine patient, parent and carer, and health care professional preferences for different attributes of care coordination for people affected by rare diseases. We conducted a discrete choice experiment using online surveys. There were no restrictions on participants in terms of rare conditions, demographic factors other than age, or geographical location within the UK. Choice scenarios were based on the following attributes: annual cost of attending appointments; access to health records; access to clinical expertise; support of a care coordinator; access to a specialist centre; and, the existence of a documented plan for emergency care. Data were analysed using alternative-specific conditional logit regression models., Results: Valid responses were obtained from 996 individuals (528 patients, 280 carers, 188 health care professionals) between August and December 2019. All attributes significantly influenced the type of service respondents preferred. Patients, carers and health professionals' preferences for care coordination were influenced by: the cost of attending appointments; access to health records; clinical expertise; role of care coordinators; access to specialist centres; and the existence of plan for emergency care. There were no statistically significant differences in the preferences between patients and carers. Preferences of health professionals differed to those of patients and carers. Both patients and carers selected responses which granted them a greater degree of autonomy in relation to the role of care coordinators, whereas health professionals preferred services where care coordinators had more autonomy. Health care professionals also expressed a stronger preference for a documented formal emergency plan to be in place., Conclusions: The findings highlight that people value better coordinated care, in line with policy documents emphasising commitments to coordinated care for people affected by rare diseases. This study highlights the factors that could be included in service provision as ways of improving the coordination of care for people affected by rare diseases., (© 2024. The Author(s).)

Published

2024

25. Description and Cross-Sectional Analyses of 25,880 Adults and Children in the UK National Registry of Rare Kidney Diseases Cohort.

Author

Wong K, Pitcher D, Braddon F, Downward L, Steenkamp R, Masoud S, Annear N, Barratt J, Bingham C, Coward RJ, Chrysochou T, Game D, Griffin S, Hall M, Johnson S, Kanigicherla D, Karet Frankl F, Kavanagh D, Kerecuk L, Maher ER, Moochhala S, Pinney J, Sayer JA, Simms R, Sinha S, Srivastava S, Tam FWK, Thomas K, Turner AN, Walsh SB, Waters A, Wilson P, Wong E, Sy KTL, Huang K, Ye J, Nitsch D, Saleem M, Bockenhauer D, Bramham K, and Gale DP

Abstract

Introduction: The National Registry of Rare Kidney Diseases (RaDaR) collects data from people living with rare kidney diseases across the UK, and is the world's largest, rare kidney disease registry. We present the clinical demographics and renal function of 25,880 prevalent patients and sought evidence of bias in recruitment to RaDaR., Methods: RaDaR is linked with the UK Renal Registry (UKRR, with which all UK patients receiving kidney replacement therapy [KRT] are registered). We assessed ethnicity and socioeconomic status in the following: (i) prevalent RaDaR patients receiving KRT compared with patients with eligible rare disease diagnoses receiving KRT in the UKRR, (ii) patients recruited to RaDaR compared with all eligible unrecruited patients at 2 renal centers, and (iii) the age-stratified ethnicity distribution of RaDaR patients with autosomal dominant polycystic kidney disease (ADPKD) was compared to that of the English census., Results: We found evidence of disparities in ethnicity and social deprivation in recruitment to RaDaR; however, these were not consistent across comparisons. Compared with either adults recruited to RaDaR or the English population, children recruited to RaDaR were more likely to be of Asian ethnicity (17.3% vs. 7.5%, P -value < 0.0001) and live in more socially deprived areas (30.3% vs. 17.3% in the most deprived Index of Multiple Deprivation (IMD) quintile, P -value < 0.0001)., Conclusion: We observed no evidence of systematic biases in recruitment of patients into RaDaR; however, the data provide empirical evidence of negative economic and social consequences (across all ethnicities) experienced by families with children affected by rare kidney diseases., (© 2024 International Society of Nephrology. Published by Elsevier Inc.)

Published

2024

26. Effects of rare kidney diseases on kidney failure: a longitudinal analysis of the UK National Registry of Rare Kidney Diseases (RaDaR) cohort.

Author

Wong K, Pitcher D, Braddon F, Downward L, Steenkamp R, Annear N, Barratt J, Bingham C, Chrysochou C, Coward RJ, Game D, Griffin S, Hall M, Johnson S, Kanigicherla D, Karet Frankl F, Kavanagh D, Kerecuk L, Maher ER, Moochhala S, Pinney J, Sayer JA, Simms R, Sinha S, Srivastava S, Tam FWK, Turner AN, Walsh SB, Waters A, Wilson P, Wong E, Taylor CM, Nitsch D, Saleem M, Bockenhauer D, Bramham K, and Gale DP

Subjects

Humans, Glomerular Filtration Rate, Kidney, Radar, Rare Diseases, Registries, United Kingdom epidemiology, Infant, Newborn, Infant, Child, Preschool, Child, Adolescent, Young Adult, Adult, Middle Aged, Aged, Aged, 80 and over, Kidney Failure, Chronic epidemiology, Kidney Failure, Chronic therapy, Kidney Failure, Chronic etiology, Renal Insufficiency epidemiology, Renal Insufficiency, Chronic epidemiology, Renal Insufficiency, Chronic therapy, Renal Insufficiency, Chronic complications

Abstract

Background: Individuals with rare kidney diseases account for 5-10% of people with chronic kidney disease, but constitute more than 25% of patients receiving kidney replacement therapy. The National Registry of Rare Kidney Diseases (RaDaR) gathers longitudinal data from patients with these conditions, which we used to study disease progression and outcomes of death and kidney failure., Methods: People aged 0-96 years living with 28 types of rare kidney diseases were recruited from 108 UK renal care facilities. The primary outcomes were cumulative incidence of mortality and kidney failure in individuals with rare kidney diseases, which were calculated and compared with that of unselected patients with chronic kidney disease. Cumulative incidence and Kaplan-Meier survival estimates were calculated for the following outcomes: median age at kidney failure; median age at death; time from start of dialysis to death; and time from diagnosis to estimated glomerular filtration rate (eGFR) thresholds, allowing calculation of time from last eGFR of 75 mL/min per 1·73 m 2 or more to first eGFR of less than 30 mL/min per 1·73 m 2 (the therapeutic trial window)., Findings: Between Jan 18, 2010, and July 25, 2022, 27 285 participants were recruited to RaDaR. Median follow-up time from diagnosis was 9·6 years (IQR 5·9-16·7). RaDaR participants had significantly higher 5-year cumulative incidence of kidney failure than 2·81 million UK patients with all-cause chronic kidney disease (28% vs 1%; p<0·0001), but better survival rates (standardised mortality ratio 0·42 [95% CI 0·32-0·52]; p<0·0001). Median age at kidney failure, median age at death, time from start of dialysis to death, time from diagnosis to eGFR thresholds, and therapeutic trial window all varied substantially between rare diseases., Interpretation: Patients with rare kidney diseases differ from the general population of individuals with chronic kidney disease: they have higher 5-year rates of kidney failure but higher survival than other patients with chronic kidney disease stages 3-5, and so are over-represented in the cohort of patients requiring kidney replacement therapy. Addressing unmet therapeutic need for patients with rare kidney diseases could have a large beneficial effect on long-term kidney replacement therapy demand., Funding: RaDaR is funded by the Medical Research Council, Kidney Research UK, Kidney Care UK, and the Polycystic Kidney Disease Charity., Competing Interests: Declaration of interests ERM reports support for the current manuscript from VHL UK/Ireland and consulting fees from MSD. SM is chair of OxalEurope. MS reports support for the current manuscript from a Medical Research Council UK Precision Medicine programme grant (MR/R013942/1) and consulting fees from Travere Therapeutics. RJC reports support for the current manuscript from Kidney Research UK. JAS reports support for the current manuscript from Kidney Research UK, Northern Counties Kidney Research Fund, and the Medical Research Council UK (all payments to institution). JAS is Academic Vice President of the UK Kidney Association. FWKT reports support from the National Institute for Health and Care Research Imperial Biomedical Centre. DN is the UK Kidney Association Director of Informatics Research. DPG reports support for the current manuscript from St Peter's Trust for Kidney Bladder and Prostate Research, Medical Research Council, Kidney Research UK, Kidney Care UK, and Polycystic Kidney Disease Charity (all payments to institution). DPG chairs the Rare Diseases Committee of the UK Kidney Association and reports fees for consulting and presenting from Novartis, Alexion, Calliditas, Sanofi, Britannia, and Travere. All other authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

27. Decline in Left Ventricular Early Systolic Function with Worsening Kidney Function in Children with Chronic Kidney Disease: Insights from the 4C and HOT-KID Studies.

Author

Gu H, Azukaitis K, Doyon A, Erdem S, Ranchin B, Harambat J, Lugani F, Boguslavskyi A, Cansick J, Finlay E, Gilbert R, Kerecuk L, Lunn A, Maxwell H, Morgan H, Shenoy M, Shroff R, Subramaniam P, Tizard J, Tse Y, Simpson J, Chowienczyk P, Schaefer F, and Sinha MD

Subjects

Adult, Child, Humans, Ventricular Function, Left physiology, Heart Ventricles diagnostic imaging, Kidney, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic diagnosis, Ventricular Dysfunction, Left diagnostic imaging, Ventricular Dysfunction, Left complications

Abstract

Introduction: Adults with childhood-onset chronic kidney disease (CKD) have an increased risk of cardiovascular disease. First-phase ejection fraction (EF1), a novel measure of early systolic function, may be a more sensitive marker of left ventricular dysfunction than other markers in children with CKD., Objective: To examine whether EF1 is reduced in children with CKD., Methods: Children from the 4C and HOT-KID studies were stratified according to estimated glomerular filtration rate (eGFR). The EF1 was calculated from the fraction of left ventricular (LV) volume ejected up to the time of peak aortic flow velocity., Results: The EF1 was measured in children ages 10.9 ± 3.7 (mean ± SD) years, 312 with CKD and 63 healthy controls. The EF1 was lower, while overall ejection fraction was similar, in those with CKD compared with controls and decreased across stages of CKD (29.3% ± 3.7%, 23.5% ± 4.5%, 19.8% ± 4.0%, 18.5% ± 5.1%, and 16.7% ± 6.6% in controls, CKD 1, 2, 3, and ≥ 4, respectively, P < .001). The relationship of EF1 to eGFR persisted after adjustment for relevant confounders (P < .001). The effect size for association of measures of LV structure or function with eGFR (SD change per unit change in eGFR) was greater for EF1 (β = 0.365, P < .001) than for other measures: LV mass index (β = -0.311), relative wall thickness (β = -0.223), E/e' (β = -0.147), and e' (β = 0.141) after adjustment for confounders in children with CKD., Conclusions: Children with CKD exhibit a marked and progressive decline in EF1 with falling eGFR. This suggests that EF1 is a more sensitive marker of LV dysfunction when compared to other structural or functional measures and that early LV systolic function is a key feature in the pathophysiology of cardiac dysfunction in CKD., Competing Interests: Conflicts of Interest None., (Copyright © 2023 American Society of Echocardiography. All rights reserved.)

Published

2024

28. Experiences of coordinated care for people in the UK affected by rare diseases: cross-sectional survey of patients, carers, and healthcare professionals.

Author

Walton H, Ng PL, Simpson A, Bloom L, Chitty LS, Fulop NJ, Hunter A, Jones J, Kai J, Kerecuk L, Kokocinska M, Leeson-Beevers K, Parkes S, Ramsay AIG, Sutcliffe A, Taylor C, and Morris S

Subjects

Adult, Humans, Cross-Sectional Studies, United Kingdom, Delivery of Health Care, Caregivers psychology, Rare Diseases therapy

Abstract

Background: Poorly coordinated care can have major impacts on patients and families affected by rare conditions, with negative physical health, psychosocial and financial consequences. This study aimed to understand how care is coordinated for rare diseases in the United Kingdom., Methods: We undertook a national survey in the UK involving 760 adults affected by rare diseases, 446 parents/carers of people affected by rare diseases, and 251 healthcare professionals who care for people affected by rare diseases., Results: Findings suggested that a wide range of patients, parents and carers do not have coordinated care. For example, few participants reported having a care coordinator (12% patients, 14% parents/carers), attending a specialist centre (32% patients, 33% parents/carers) or having a care plan (10% patients, 44% parents/carers). A very small number of patients (2%) and parents/carers (5%) had access to all three-a care coordinator, specialist centre and care plan. Fifty four percent of patients and 33% of parents/carers reported access to none of these. On the other hand, a higher proportion of healthcare professionals reported that families with rare conditions had access to care coordinators (35%), specialist centres (60%) and care plans (40%)., Conclusions: Care for families with rare conditions is generally not well coordinated in the UK, with findings indicating limited access to care coordinators, specialist centres and care plans. Better understanding of these issues can inform how care coordination might be improved and embrace the needs and preferences of patients and families affected by rare conditions., (© 2023. The Author(s).)

Published

2023

29. Certain heterozygous variants in the kinase domain of the serine/threonine kinase NEK8 can cause an autosomal dominant form of polycystic kidney disease.

Author

Claus LR, Chen C, Stallworth J, Turner JL, Slaats GG, Hawks AL, Mabillard H, Senum SR, Srikanth S, Flanagan-Steet H, Louie RJ, Silver J, Lerner-Ellis J, Morel C, Mighton C, Sleutels F, van Slegtenhorst M, van Ham T, Brooks AS, Dorresteijn EM, Barakat TS, Dahan K, Demoulin N, Goffin EJ, Olinger E, Larsen M, Hertz JM, Lilien MR, Obeidová L, Seeman T, Stone HK, Kerecuk L, Gurgu M, Yousef Yengej FA, Ammerlaan CME, Rookmaaker MB, Hanna C, Rogers RC, Duran K, Peters E, Sayer JA, van Haaften G, Harris PC, Ling K, Mason JM, van Eerde AM, and Steet R

Subjects

Animals, Humans, Infant, Newborn, Mice, Carrier Proteins metabolism, Cilia pathology, Kidney metabolism, Mutation, NIMA-Related Kinases genetics, NIMA-Related Kinases metabolism, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Serine genetics, Serine metabolism, TRPP Cation Channels genetics, TRPP Cation Channels metabolism, Polycystic Kidney Diseases genetics, Polycystic Kidney, Autosomal Dominant pathology

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) resulting from pathogenic variants in PKD1 and PKD2 is the most common form of PKD, but other genetic causes tied to primary cilia function have been identified. Biallelic pathogenic variants in the serine/threonine kinase NEK8 cause a syndromic ciliopathy with extra-kidney manifestations. Here we identify NEK8 as a disease gene for ADPKD in 12 families. Clinical evaluation was combined with functional studies using fibroblasts and tubuloids from affected individuals. Nek8 knockout mouse kidney epithelial (IMCD3) cells transfected with wild type or variant NEK8 were further used to study ciliogenesis, ciliary trafficking, kinase function, and DNA damage responses. Twenty-one affected monoallelic individuals uniformly exhibited cystic kidney disease (mostly neonatal) without consistent extra-kidney manifestations. Recurrent de novo mutations of the NEK8 missense variant p.Arg45Trp, including mosaicism, were seen in ten families. Missense variants elsewhere within the kinase domain (p.Ile150Met and p.Lys157Gln) were also identified. Functional studies demonstrated normal localization of the NEK8 protein to the proximal cilium and no consistent cilia formation defects in patient-derived cells. NEK8-wild type protein and all variant forms of the protein expressed in Nek8 knockout IMCD3 cells were localized to cilia and supported ciliogenesis. However, Nek8 knockout IMCD3 cells expressing NEK8-p.Arg45Trp and NEK8-p.Lys157Gln showed significantly decreased polycystin-2 but normal ANKS6 localization in cilia. Moreover, p.Arg45Trp NEK8 exhibited reduced kinase activity in vitro. In patient derived tubuloids and IMCD3 cells expressing NEK8-p.Arg45Trp, DNA damage signaling was increased compared to healthy passage-matched controls. Thus, we propose a dominant-negative effect for specific heterozygous missense variants in the NEK8 kinase domain as a new cause of PKD., (Copyright © 2023 International Society of Nephrology. All rights reserved.)

Published

2023

30. Intensive compared with less intensive blood pressure control to prevent adverse cardiac remodelling in children with chronic kidney disease (HOT-KID): a parallel-group, open-label, multicentre, randomised, controlled trial.

Author

Sinha MD, Gu H, Douiri A, Cansick J, Finlay E, Gilbert R, Kerecuk L, Lunn A, Maxwell H, Morgan H, Shenoy M, Shroff R, Subramaniam P, Tizard J, Tse Y, Rezavi R, Simpson JM, and Chowienczyk PJ

Subjects

Male, Child, Humans, Female, Blood Pressure, Angiotensin Receptor Antagonists pharmacology, Ventricular Remodeling, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Angiotensin-Converting Enzyme Inhibitors pharmacology, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic drug therapy

Abstract

Background: Optimal target blood pressure to reduce adverse cardiac remodelling in children with chronic kidney disease is uncertain. We hypothesised that lower blood pressure would reduce adverse cardiac remodelling., Methods: HOT-KID, a parallel-group, open-label, multicentre, randomised, controlled trial, was done in 14 clinical centres across England and Scotland. We included children aged 2-15 years with stage 1-4 chronic kidney disease-ie, an estimated glomerular filtration rate (eGFR) higher than 15 mL/min per 1·73 m 2 -and who could be followed up for 2 years. Children on antihypertensive medication were eligible as long as it could be changed to angiotensin-converting enzyme (ACE) inhibitors or angiotensin receptor blockers (ARBs) if they were not already receiving these therapies. Participants were randomly assigned (1:1) to standard treatment (auscultatory office systolic blood pressure target between the 50th and 75th percentiles) or intensive treatment (systolic target <40th percentile) by the chief investigator using a rapid, secure, web-based randomisation system. ACE inhibitors or ARBs were used as first-line agents, with the dose titrated every 2-4 weeks to achieve the target blood pressure levels. The primary outcome was mean annual difference in left ventricular mass index (LVMI) by echocardiography measured by a masked observer and was assessed in the intention-to-treat population, defined as all the children who underwent randomisation irrespective of the blood pressure reached. Secondary and safety outcomes were the differences between groups in mean left ventricular relative wall thickness, renal function, and adverse effects and were also assessed in the intention-to-treat population. This trial is registered with ISRCTN, ISRCTN25006406., Findings: Between Oct 30, 2012, and Jan 5, 2017, 64 participants were randomly assigned to the intensive treatment group and 60 to the standard treatment group (median age of participants was 10·0 years [IQR 6·8-12·6], 69 [56%] were male and 107 [86%] were of white ethnicity). Median follow-up was 38·7 months (IQR 28·1-52·2). Blood pressure was lower in the intensive treatment group compared with standard treatment group (mean systolic pressure lower by 4 mm Hg, p=0·0012) but in both groups was close to the 50th percentile. The mean annual reduction in LVMI was similar for intensive and standard treatments (-1·9 g/m 2·7 [95% CI -2·4 to -1·3] vs -1·2 g/m 2·7 [-1·5 to 0·8], with a treatment effect of -0·7 g/m 2·7 [95% CI -1·9 to 2·6] per year; p=0·76) and mean value in both groups at the end of follow-up within the normal range. At baseline, elevated relative wall thickness was more marked than increased LVMI and a reduction in relative wall thickness was greater for the intensive treatment group than for the standard treatment group (-0·010 [95% CI 0·015 to -0·006] vs -0·004 [-0·008 to 0·001], treatment effect -0·020 [95% CI -0·039 to -0·009] per year, p=0·0019). Six (5%) participants reached end-stage kidney disease (ie, an eGFR of <15 mL/min per 1·73 m 2 ; three in each group) during the course of the study. The risk difference between treatment groups was 0·02 (95% CI -0·15 to 0·19, p=0·82) for overall adverse events and 0·07 (-0·05 to 0·19, p=0·25) for serious adverse events. Intensive treatment was not associated with worse renal outcomes or greater adverse effects than standard treatment., Interpretation: These results suggest that cardiac remodelling in children with chronic kidney disease is related to blood pressure control and that a target office systolic blood pressure at the 50th percentile is close to the optimal target for preventing increased left ventricular mass., Funding: British Heart Foundation., Competing Interests: Declaration of interests We declare no competing interests., (Copyright © 2023 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2023

31. Developing a taxonomy of care coordination for people living with rare conditions: a qualitative study.

Author

Walton H, Simpson A, Ramsay AIG, Hudson E, Hunter A, Jones J, Ng PL, Leeson-Beevers K, Bloom L, Kai J, Kerecuk L, Kokocinska M, Sutcliffe AG, Morris S, and Fulop NJ

Subjects

Focus Groups, Humans, Qualitative Research, Rare Diseases, United Kingdom, Caregivers, Telephone

Abstract

Background: Improving care coordination is particularly important for individuals with rare conditions (who may experience multiple inputs into their care, across different providers and settings). To develop and evaluate strategies to potentially improve care coordination, it is necessary to develop a method for organising different ways of coordinating care for rare conditions. Developing a taxonomy would help to describe different ways of coordinating care and in turn facilitate development and evaluation of pre-existing and new models of care coordination for rare conditions. To the authors' knowledge, no studies have previously developed taxonomies of care coordination for rare conditions. This research aimed to develop and refine a care coordination taxonomy for people with rare conditions., Methods: This study had a qualitative design and was conducted in the United Kingdom. To develop a taxonomy, six stages of taxonomy development were followed. We conducted interviews (n = 30 health care professionals/charity representatives/commissioners) and focus groups (n = 4 focus groups, 22 patients/carers with rare/ultra-rare/undiagnosed conditions). Interviews and focus groups were audio-recorded with consent, and professionally transcribed. Findings were analysed using thematic analysis. Themes were used to develop a taxonomy, and to identify which types of coordination may work best in which situations. To refine the taxonomy, we conducted two workshops (n = 12 patients and carers group; n = 15 professional stakeholder group)., Results: Our taxonomy has six domains, each with different options. The six domains are: (1) Ways of organising care (local, hybrid, national), (2) Ways of organising those involved in care (collaboration between many or all individuals, collaboration between some individuals, a lack of collaborative approach), (3) Responsibility for coordination (administrative support, formal roles and responsibilities, supportive roles and no responsibility), (4) How often appointments and coordination take place (regular, on demand, hybrid), (5) Access to records (full or filtered access), and (6) Mode of care coordination (face-to-face, digital, telephone)., Conclusions: Findings indicate that there are different ways of coordinating care across the six domains outlined in our taxonomy. This may help to facilitate the development and evaluation of existing and new models of care coordination for people living with rare conditions., (© 2022. The Author(s).)

Published

2022

32. Genotype-phenotype correlation at codon 1740 of SETD2.

Author

Rabin R, Radmanesh A, Glass IA, Dobyns WB, Aldinger KA, Shieh JT, Romoser S, Bombei H, Dowsett L, Trapane P, Bernat JA, Baker J, Mendelsohn NJ, Popp B, Siekmeyer M, Sorge I, Sansbury FH, Watts P, Foulds NC, Burton J, Hoganson G, Hurst JA, Menzies L, Osio D, Kerecuk L, Cobben JM, Jizi K, Jacquemont S, Bélanger SA, Löhner K, Veenstra-Knol HE, Lemmink HH, Keller-Ramey J, Wentzensen IM, Punj S, McWalter K, Lenberg J, Ellsworth KA, Radtke K, Akbarian S, and Pappas J

Subjects

Child, Child, Preschool, Codon genetics, Epigenesis, Genetic genetics, Female, Genetic Association Studies, Humans, Infant, Intellectual Disability pathology, Loss of Function Mutation genetics, Male, Mutation, Missense, Nervous System Malformations genetics, Nervous System Malformations pathology, Neurodevelopmental Disorders physiopathology, Genetic Predisposition to Disease, Histone-Lysine N-Methyltransferase genetics, Intellectual Disability genetics, Neurodevelopmental Disorders genetics, Tubulin genetics

Abstract

The SET domain containing 2, histone lysine methyltransferase encoded by SETD2 is a dual-function methyltransferase for histones and microtubules and plays an important role for transcriptional regulation, genomic stability, and cytoskeletal functions. Specifically, SETD2 is associated with trimethylation of histone H3 at lysine 36 (H3K36me3) and methylation of α-tubulin at lysine 40. Heterozygous loss of function and missense variants have previously been described with Luscan-Lumish syndrome (LLS), which is characterized by overgrowth, neurodevelopmental features, and absence of overt congenital anomalies. We have identified 15 individuals with de novo variants in codon 1740 of SETD2 whose features differ from those with LLS. Group 1 consists of 12 individuals with heterozygous variant c.5218C>T p.(Arg1740Trp) and Group 2 consists of 3 individuals with heterozygous variant c.5219G>A p.(Arg1740Gln). The phenotype of Group 1 includes microcephaly, profound intellectual disability, congenital anomalies affecting several organ systems, and similar facial features. Individuals in Group 2 had moderate to severe intellectual disability, low normal head circumference, and absence of additional major congenital anomalies. While LLS is likely due to loss of function of SETD2, the clinical features seen in individuals with variants affecting codon 1740 are more severe suggesting an alternative mechanism, such as gain of function, effects on epigenetic regulation, or posttranslational modification of the cytoskeleton. Our report is a prime example of different mutations in the same gene causing diverging phenotypes and the features observed in Group 1 suggest a new clinically recognizable syndrome uniquely associated with the heterozygous variant c.5218C>T p.(Arg1740Trp) in SETD2., (© 2020 Wiley Periodicals LLC.)

Published

2020

33. Patient and clinician opinions of patient reported outcome measures (PROMs) in the management of patients with rare diseases: a qualitative study.

Author

Aiyegbusi OL, Isa F, Kyte D, Pankhurst T, Kerecuk L, Ferguson J, Lipkin G, and Calvert M

Subjects

Female, Focus Groups, Humans, Male, Qualitative Research, Rare Diseases therapy, Patient Reported Outcome Measures, Quality of Life, Rare Diseases psychology

Abstract

Background: Rare diseases may be life-threatening or chronically debilitating conditions. Patient care needs are often complex and challenging to coordinate and deliver effectively. Rare diseases and their clinical management may therefore substantially impact on patients' health-related quality of life (HRQOL). The use of patient-reported outcome measures (PROMs) may complement clinical assessments by elucidating patients' perspectives on their health status and care priorities. This study explored the opinions of patients and clinicians on the use of PROMs in the management of patients with rare diseases in routine clinical practice., Methods: A total of 15 semi-structured one-to-one interviews were conducted with four patients with primary sclerosing cholangitis (PSC); five renal transplant recipients; and six PSC doctors from University Hospitals Birmingham (UHB) NHS Foundation Trust. A focus group session was also conducted with 10 clinical staff members (doctors, nurses and other allied health professionals from UHB). The suitability and acceptability of the Chronic Liver Disease Questionnaire (CLDQ) and the Short Form 12 (SF12) were assessed by patients with PSC and their doctors while the Paediatric quality of life inventory Transplant Module (PedsQL-TM) and the EuroQoL-5 dimensions (EQ. 5D) were evaluated by the renal transplant recipients and their doctors. The discussions were audio recorded and transcribed verbatim. Coding of the transcripts was done using the Nvivo 11 Plus software. Thematic analysis was conducted to identify the main themes and subthemes., Results: Four themes were identified, namely: (i) potential benefits of PROMs in the management of rare diseases; (ii) views on selected questionnaires; (iii) practical considerations for implementation; and (iv) potential facilitators and barriers of implementation. Patients and clinicians suggested that the use of ePROMs may facilitate patient-centred care by promoting patient-clinician communication, highlighting aspects of HRQOL that are important to patients and encouraging patient involvement in their care. They also felt that the disease-specific CLDQ and PedsQL-TM were more relevant than the generic SF12 and EQ-5D., Conclusions: Patients with rare diseases often experience impaired HRQOL. The use of an ePROM system may enhance the routine management of patients with rare diseases.

Published

2020

34. Young adults have worse kidney transplant outcomes than other age groups.

Author

Pankhurst T, Evison F, Mytton J, Williamson S, Kerecuk L, and Lipkin G

Subjects

Adolescent, Adult, Age Factors, Aged, Child, Child, Preschool, Female, Graft Rejection etiology, Graft Survival, Humans, Kidney Failure, Chronic surgery, Kidney Transplantation adverse effects, Male, Middle Aged, Prognosis, Retrospective Studies, Survival Rate, Young Adult, Graft Rejection mortality, Kidney Failure, Chronic mortality, Kidney Transplantation mortality, Registries statistics & numerical data, Transplant Recipients statistics & numerical data

Abstract

Background: The objective of this study was to establish if renal transplant outcomes (graft and patient survival) for young adults in England were worse than for other age groups., Methods: Outcomes for all renal transplant recipients in England (n = 26 874) were collected from Hospital Episode Statistics and the Office for National Statistics databases over 12 years. Graft and patient outcomes, follow-up and admissions were studied for all patients, stratified by age bands., Results: Young adults (14-23 years) had substantially greater likelihood [hazard ratio (HR) = 1.26, 95% confidence interval (CI) 1.10-1.19; P < 0.001] of kidney transplant failure than any other age band. They had a higher non-attendance rate for clinic appointments (1.6 versus 1.2/year; P < 0.001) and more emergency admissions post-transplantation (25% of young adults on average are admitted each year, compared with 15-20% of 34- to 43-year olds). Taking into account deprivation, ethnicity, transplant type and transplant centre, in the 14- to 23-year group, return to dialysis remained significantly worse than all other age bands (HR = 1.41, 95% CI 1.26-1.57). For the whole cohort, increasing deprivation related to poorer outcomes and black ethnicity was associated with poorer outcomes. However, neither ethnicity nor deprivation was over-represented in the young adult cohort., Conclusions: Young adults who receive a kidney transplant have a significant increased likelihood of a return to dialysis in the first 10 years post-transplant when compared with those aged 34-43 years in multivariable analysis., (© The Author(s) 2020. Published by Oxford University Press on behalf of ERA-EDTA. All rights reserved.)

Published

2020

35. Tuberous Sclerosis Complex (TSC): Expert Recommendations for Provision of Coordinated Care.

Author

Annear NMP, Appleton RE, Bassi Z, Bhatt R, Bolton PF, Crawford P, Crowe A, Tossi M, Elmslie F, Finlay E, Gale DP, Henderson A, Jones EA, Johnson SR, Joss S, Kerecuk L, Lipkin G, Morrison PJ, O'Callaghan FJ, Cadwgan J, Ong ACM, Sampson JR, Shepherd C, and Kingswood JC

Published

2019

36. A step-wise approach for establishing a multidisciplinary team for the management of tuberous sclerosis complex: a Delphi consensus report.

Author

Auvin S, Bissler JJ, Cottin V, Fujimoto A, Hofbauer GFL, Jansen AC, Jóźwiak S, Kerecuk L, Kingswood JC, Moavero R, Torra R, and Villanueva V

Subjects

Consensus, Humans, Interdisciplinary Communication, Disease Management, Tuberous Sclerosis

Abstract

Background: Tuberous sclerosis complex (TSC) is a rare autosomal dominant genetic disorder associated with mutations in TSC1 and TSC2 genes, upregulation of mammalian target of rapamycin signaling, and subsequent tumor formation in various organs. Due to the many manifestations of TSC and their potential complications, management requires the expertise of multiple medical disciplines. A multidisciplinary care approach is recommended by consensus guidelines. Use of multidisciplinary teams (MDTs) has been shown to be beneficial in treating other complex diseases, such as cancer. In a lifelong disease such as TSC, an MDT may facilitate the transition from pediatric to adult care. However, little guidance exists in the literature regarding how to organize an MDT in TSC., Methods: To discuss the best approach to assembling an MDT, this project was initiated in October 2017 with a meeting of 12 physicians from various specialties and various countries. Following this first meeting, the experts generated statements on the most important aspects to implement in establishing an MDT for TSC by 3 rounds of selection using a Delphi process via electronic correspondence. Finally, TSC patient advocates reviewed the findings and provided additional insights from a patient perspective., Results: A 3-step roadmap was recommended, starting with identifying a single individual to begin organizing care (Step 1), then establishing a small core team (Step 2), and finally, establishing a larger multi-disciplinary team (Step 3). Because of the multisystemic nature of TSC, the MDT should include specialists such as a neurologist, a neurosurgeon, a nephrologist, a urologist, a pulmonologist, an ophthalmologist, a cardiologist, a dermatologist, a geneticist, and a psychiatrist/psychologist. The MDT should recommend a care plan for each patient based on the individual's needs and in consultation with him/her or his/her family. Some of the most important aspects of an MDT that were agreed upon included identifying a case manager to help coordinate care, providing access to health care professionals of varying specialties, and including a lead physician who takes medical responsibility for patients' overall care., Conclusions: The results of our consensus provide guidance to support the initiation of an MDT in TSC.

Published

2019

37. Mutations in multiple components of the nuclear pore complex cause nephrotic syndrome.

Author

Braun DA, Lovric S, Schapiro D, Schneider R, Marquez J, Asif M, Hussain MS, Daga A, Widmeier E, Rao J, Ashraf S, Tan W, Lusk CP, Kolb A, Jobst-Schwan T, Schmidt JM, Hoogstraten CA, Eddy K, Kitzler TM, Shril S, Moawia A, Schrage K, Khayyat AIA, Lawson JA, Gee HY, Warejko JK, Hermle T, Majmundar AJ, Hugo H, Budde B, Motameny S, Altmüller J, Noegel AA, Fathy HM, Gale DP, Waseem SS, Khan A, Kerecuk L, Hashmi S, Mohebbi N, Ettenger R, Serdaroğlu E, Alhasan KA, Hashem M, Goncalves S, Ariceta G, Ubetagoyena M, Antonin W, Baig SM, Alkuraya FS, Shen Q, Xu H, Antignac C, Lifton RP, Mane S, Nürnberg P, Khokha MK, and Hildebrandt F

Subjects

Animals, Cell Line, Disease Models, Animal, Gene Knockdown Techniques, Humans, Nephrotic Syndrome genetics, Nephrotic Syndrome pathology, Nuclear Pore Complex Proteins genetics, Xenopus Proteins genetics, Xenopus laevis, Zebrafish, Zebrafish Proteins genetics, Nephrotic Syndrome metabolism, Nuclear Pore Complex Proteins metabolism, Xenopus Proteins metabolism, Zebrafish Proteins metabolism

Abstract

Steroid-resistant nephrotic syndrome (SRNS) almost invariably progresses to end-stage renal disease. Although more than 50 monogenic causes of SRNS have been described, a large proportion of SRNS remains unexplained. Recently, it was discovered that mutations of NUP93 and NUP205, encoding 2 proteins of the inner ring subunit of the nuclear pore complex (NPC), cause SRNS. Here, we describe mutations in genes encoding 4 components of the outer rings of the NPC, namely NUP107, NUP85, NUP133, and NUP160, in 13 families with SRNS. Using coimmunoprecipitation experiments, we showed that certain pathogenic alleles weakened the interaction between neighboring NPC subunits. We demonstrated that morpholino knockdown of nup107, nup85, or nup133 in Xenopus disrupted glomerulogenesis. Re-expression of WT mRNA, but not of mRNA reflecting mutations from SRNS patients, mitigated this phenotype. We furthermore found that CRISPR/Cas9 knockout of NUP107, NUP85, or NUP133 in podocytes activated Cdc42, an important effector of SRNS pathogenesis. CRISPR/Cas9 knockout of nup107 or nup85 in zebrafish caused developmental anomalies and early lethality. In contrast, an in-frame mutation of nup107 did not affect survival, thus mimicking the allelic effects seen in humans. In conclusion, we discovered here that mutations in 4 genes encoding components of the outer ring subunits of the NPC cause SRNS and thereby provide further evidence that specific hypomorphic mutations in these essential genes cause a distinct, organ-specific phenotype.

Published

2018

38. Patient-reported outcome measures used in patients with primary sclerosing cholangitis: a systematic review.

Author

Isa F, Turner GM, Kaur G, Kyte D, Slade A, Pankhurst T, Kerecuk L, Keeley T, Ferguson J, and Calvert M

Subjects

Female, Humans, Male, Cholangitis, Sclerosing psychology, Patient Reported Outcome Measures, Quality of Life

Abstract

Background: Primary Sclerosing Cholangitis (PSC) is a rare chronic, cholestatic liver condition in which patients can experience a range of debilitating symptoms. Patient reported outcome measures (PROMs) could provide a valuable insight into the impact of PSC on patient quality of life and symptoms. A previous review has been conducted on the quality of life instruments used in liver transplant recipients. However, there has been no comprehensive review evaluating PROM use or measurement properties in PSC patients' to-date. The aim of the systematic review was to: (a) To identify and categorise which PROMs are currently being used in research involving the PSC population (b) To investigate the measurement properties of PROMs used in PSC., Methods: A systematic review of Medline, EMBASE and CINAHL, from inception to February 2018, was undertaken. The methodological quality of included studies was assessed using the Consensus-based Standards for selection of health Measurement Instruments (COSMIN) checklist., Results: Thirty-seven studies were identified, which included 36 different PROMs. Seven PROMs were generic, 10 disease-specific, 17 symptom-specific measures and 2 measures on dietary intake. The most common PROMs were the Short form-36 (SF-36) (n = 15) and Chronic liver disease questionnaire (CLDQ) (n = 6). Only three studies evaluated measurement properties, two studies evaluated the National Institute of Diabetes Digestive and Kidney Diseases Liver Transplant (NIDDK-QA) and one study evaluated the PSC PRO; however, according to the COSMIN guidelines, methodological quality was poor for the NIDDK-QA studies and fair for the PSC PRO study., Conclusion: A wide variety of PROMs have been used to assess health-related quality of life and symptom burden in patients with PSC; however only two measures (NIDDK-QA and PSC PRO) have been formally validated in this population. The newly developed PSC PRO requires further validation in PSC patients with diverse demographics, comorbidities and at different stages of disease; however this is a promising new measure with which to assess the impact of PSC on patient quality of life and symptoms.

Published

2018

39. Patient reported outcome measures in rare diseases: a narrative review.

Author

Slade A, Isa F, Kyte D, Pankhurst T, Kerecuk L, Ferguson J, Lipkin G, and Calvert M

Subjects

Humans, Quality of Life, Patient Reported Outcome Measures, Rare Diseases

Abstract

Background: Rare diseases can lead to a significant reduction in quality of life for patients and their families. Ensuring the patients voice is central to clinical decision making is key to delivering, evaluating and understanding the efficacy of therapeutic interventions. Patient reported outcome measures (PROMs) are used to capture the patient's views about their health status and facilitate our understanding of the impact of these diseases and their treatments on patient's quality of life and symptoms., Main Text: This review explores some of the current issues around the utilisation of PROMs in rare diseases, including small patient populations and dearth of valid PROMs. Difficulties in validating new or current PROMs for use in clinical trials and research are discussed. The review highlights potential solutions for some of the issues outlined in the review and the implementation of PROMs in research and clinical practice are discussed., Conclusion: Patient input throughout the development of PROMs including qualitative research is essential to ensure that outcomes that matter to people living with rare disease are appropriately captured. Given the large number of rare diseases, small numbers of patients living with each condition and the cost of instrument development, creative and pragmatic solutions to PROM development and use may be necessary. Solutions include qualitative interviews, modern psychometrics and resources such as item banking and computer adaptive testing. Use of PROMs in rare disease research and clinical practice offers the potential to improve patient care and clinical outcomes.

Published

2018

40. Factor H autoantibody is associated with atypical hemolytic uremic syndrome in children in the United Kingdom and Ireland.

Author

Brocklebank V, Johnson S, Sheerin TP, Marks SD, Gilbert RD, Tyerman K, Kinoshita M, Awan A, Kaur A, Webb N, Hegde S, Finlay E, Fitzpatrick M, Walsh PR, Wong EKS, Booth C, Kerecuk L, Salama AD, Almond M, Inward C, Goodship TH, Sheerin NS, Marchbank KJ, and Kavanagh D

Subjects

Adolescent, Antibodies, Monoclonal, Humanized therapeutic use, Atypical Hemolytic Uremic Syndrome blood, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome therapy, Child, Child, Preschool, Complement Factor H immunology, Complement System Proteins analysis, Complement System Proteins genetics, Female, Humans, Immunosuppression Therapy adverse effects, Immunosuppression Therapy methods, Infant, Ireland, Kidney Failure, Chronic blood, Kidney Failure, Chronic genetics, Kidney Failure, Chronic therapy, Male, Plasma Exchange, Recurrence, Renal Dialysis, Retrospective Studies, United Kingdom, Atypical Hemolytic Uremic Syndrome immunology, Autoantibodies blood, Kidney Failure, Chronic immunology, Kidney Transplantation

Abstract

Factor H autoantibodies can impair complement regulation, resulting in atypical hemolytic uremic syndrome, predominantly in childhood. There are no trials investigating treatment, and clinical practice is only informed by retrospective cohort analysis. Here we examined 175 children presenting with atypical hemolytic uremic syndrome in the United Kingdom and Ireland for factor H autoantibodies that included 17 children with titers above the international standard. Of the 17, seven had a concomitant rare genetic variant in a gene encoding a complement pathway component or regulator. Two children received supportive treatment; both developed established renal failure. Plasma exchange was associated with a poor rate of renal recovery in seven of 11 treated. Six patients treated with eculizumab recovered renal function. Contrary to global practice, immunosuppressive therapy to prevent relapse in plasma exchange-treated patients was not adopted due to concerns over treatment-associated complications. Without immunosuppression, the relapse rate was high (five of seven). However, reintroduction of treatment resulted in recovery of renal function. All patients treated with eculizumab achieved sustained remission. Five patients received renal transplants without specific factor H autoantibody-targeted treatment with recurrence in one who also had a functionally significant CFI mutation. Thus, our current practice is to initiate eculizumab therapy for treatment of factor H autoantibody-mediated atypical hemolytic uremic syndrome rather than plasma exchange with or without immunosuppression. Based on this retrospective analysis we see no suggestion of inferior treatment, albeit the strength of our conclusions is limited by the small sample size., (Copyright © 2017 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2017

41. Genomic and clinical profiling of a national nephrotic syndrome cohort advocates a precision medicine approach to disease management.

Author

Bierzynska A, McCarthy HJ, Soderquest K, Sen ES, Colby E, Ding WY, Nabhan MM, Kerecuk L, Hegde S, Hughes D, Marks S, Feather S, Jones C, Webb NJ, Ognjanovic M, Christian M, Gilbert RD, Sinha MD, Lord GM, Simpson M, Koziell AB, Welsh GI, and Saleem MA

Subjects

Adolescent, Age of Onset, Child, Child, Preschool, Cohort Studies, Disease Progression, Exome, Female, Genetic Association Studies, Genetic Predisposition to Disease, Heredity, High-Throughput Nucleotide Sequencing, Humans, Infant, Intracellular Signaling Peptides and Proteins genetics, Kaplan-Meier Estimate, Kidney pathology, Kidney Failure, Chronic diagnosis, Kidney Failure, Chronic genetics, Kidney Failure, Chronic therapy, Male, Membrane Proteins genetics, Nephrotic Syndrome diagnosis, Nephrotic Syndrome genetics, Nephrotic Syndrome therapy, Pedigree, Phenotype, Predictive Value of Tests, Prognosis, Registries, Risk Factors, United Kingdom, WT1 Proteins genetics, Young Adult, Genomics methods, Mutation, Nephrotic Syndrome congenital, Precision Medicine

Abstract

Steroid Resistant Nephrotic Syndrome (SRNS) in children and young adults has differing etiologies with monogenic disease accounting for 2.9-30% in selected series. Using whole exome sequencing we sought to stratify a national population of children with SRNS into monogenic and non-monogenic forms, and further define those groups by detailed phenotypic analysis. Pediatric patients with SRNS were identified via a national United Kingdom Renal Registry. Whole exome sequencing was performed on 187 patients, of which 12% have a positive family history with a focus on the 53 genes currently known to be associated with nephrotic syndrome. Genetic findings were correlated with individual case disease characteristics. Disease causing variants were detected in 26.2% of patients. Most often this occurred in the three most common SRNS-associated genes: NPHS1, NPHS2, and WT1 but also in 14 other genes. The genotype did not always correlate with expected phenotype since mutations in OCRL, COL4A3, and DGKE associated with specific syndromes were detected in patients with isolated renal disease. Analysis by primary/presumed compared with secondary steroid resistance found 30.8% monogenic disease in primary compared with none in secondary SRNS permitting further mechanistic stratification. Genetic SRNS progressed faster to end stage renal failure, with no documented disease recurrence post-transplantation within this cohort. Primary steroid resistance in which no gene mutation was identified had a 47.8% risk of recurrence. In this unbiased pediatric population, whole exome sequencing allowed screening of all current candidate genes. Thus, deep phenotyping combined with whole exome sequencing is an effective tool for early identification of SRNS etiology, yielding an evidence-based algorithm for clinical management., (Copyright © 2016 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2017

42. Kidney Versus Combined Kidney and Liver Transplantation in Young People With Autosomal Recessive Polycystic Kidney Disease: Data From the European Society for Pediatric Nephrology/European Renal Association-European Dialysis and Transplant (ESPN/ERA-EDTA) Registry.

Author

Mekahli D, van Stralen KJ, Bonthuis M, Jager KJ, Balat A, Benetti E, Godefroid N, Edvardsson VO, Heaf JG, Jankauskiene A, Kerecuk L, Marinova S, Puteo F, Seeman T, Zurowska A, Pirenne J, Schaefer F, and Groothoff JW

Subjects

Adolescent, Child, Child, Preschool, Cohort Studies, Female, Humans, Infant, Liver Cirrhosis mortality, Male, Polycystic Kidney, Autosomal Recessive mortality, Registries, Renal Insufficiency mortality, Societies, Medical, Survival Analysis, Kidney Transplantation, Liver Cirrhosis etiology, Liver Cirrhosis surgery, Liver Transplantation, Polycystic Kidney, Autosomal Recessive complications, Renal Insufficiency etiology, Renal Insufficiency surgery

Abstract

Background: The choice for either kidney or combined liver-kidney transplantation in young people with kidney failure and liver fibrosis due to autosomal recessive polycystic kidney disease (ARPKD) can be challenging. We aimed to analyze the characteristics and outcomes of transplantation type in these children, adolescents, and young adults., Study Design: Cohort study., Setting & Participants: We derived data for children, adolescents, and young adults with ARPKD with either kidney or combined liver-kidney transplants for 1995 to 2012 from the ESPN/ERA-EDTA Registry, a European pediatric renal registry collecting data from 36 European countries., Factor: Liver transplantation., Outcomes & Measurements: Transplantation and patient survival., Results: 202 patients with ARPKD aged 19 years or younger underwent transplantation after a median of 0.4 (IQR, 0.0-1.4) years on dialysis therapy at a median age of 9.0 (IQR, 4.1-13.7) years. 32 (15.8%) underwent combined liver-kidney transplantation, 163 (80.7%) underwent kidney transplantation, and 7 (3.5%) were excluded because transplantation type was unknown. Age- and sex-adjusted 5-year patient survival posttransplantation was 95.5% (95% CI, 92.4%-98.8%) overall: 97.4% (95% CI, 94.9%-100.0%) for patients with kidney transplantation in contrast to 87.0% (95% CI, 75.8%-99.8%) with combined liver-kidney transplantation. The age- and sex-adjusted risk for death after combined liver-kidney transplantation was 6.7-fold (95% CI, 1.8- to 25.4-fold) greater than after kidney transplantation (P=0.005). Five-year death-censored kidney transplant survival following combined liver-kidney and kidney transplantation was similar (92.1% vs 85.9%; P=0.4)., Limitations: No data for liver disease of kidney therapy recipients., Conclusions: Combined liver-kidney transplantation in ARPKD is associated with increased mortality compared to kidney transplantation in our large observational study and was not associated with improved 5-year kidney transplant survival. Long-term follow-up of both kidney and liver involvement are needed to better delineate the optimal transplantation strategy., (Copyright © 2016 National Kidney Foundation, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2016

43. Chromosome 17q12 microdeletions but not intragenic HNF1B mutations link developmental kidney disease and psychiatric disorder.

Author

Clissold RL, Shaw-Smith C, Turnpenny P, Bunce B, Bockenhauer D, Kerecuk L, Waller S, Bowman P, Ford T, Ellard S, Hattersley AT, and Bingham C

Subjects

Adolescent, Adult, Base Sequence genetics, Child, Female, Haploinsufficiency, Heterozygote, Humans, Male, Middle Aged, Mutation, Phenotype, Referral and Consultation, Young Adult, Chromosomes, Human, Pair 17 genetics, Hepatocyte Nuclear Factor 1-beta genetics, Kidney Diseases genetics, Neurodevelopmental Disorders genetics, Sequence Deletion genetics

Abstract

Heterozygous mutations of the HNF1B gene are the commonest known monogenic cause of developmental kidney disease. Half of patients have a deletion (approximately 1.3 Mb) of chromosome 17q12, encompassing HNF1B plus 14 additional genes. This 17q12 deletion has been linked with an increased risk of neurodevelopmental disorders, such as autism. Here we compared the neurodevelopmental phenotype of 38 patients with HNF1B-associated renal disease due to an intragenic mutation in 18 patients or due to 17q12 deletion in 20 patients to determine whether haploinsufficiency of HNF1B is responsible for the neurodevelopmental phenotype. Significantly, brief behavioral screening in children with the deletion showed high levels of psychopathology and its impact. Eight individuals (40%) with a deletion had a clinical diagnosis of a neurodevelopmental disorder compared to none with an intragenic mutation. The 17q12 deletions were also associated with more autistic traits. Two independent clinical geneticists were able to predict the presence of a deletion with a sensitivity of 83% and specificity of 79% when assessing facial dysmorphic features as a whole. Thus, the 17q12 deletions but not HNF1B intragenic mutations are associated with neurodevelopmental disorders. Hence, the HNF1B gene is not involved in the neurodevelopmental phenotype of these patients. Nephrologists need to be aware of this association to ensure appropriate referral to psychiatric services., (Copyright © 2016 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2016

44. Autosomal dominant polycystic kidney disease in children.

Author

Polubothu S, Richardson A, Kerecuk L, and Sinha M

Subjects

Cardiovascular Diseases etiology, Child, Disease Management, Early Diagnosis, Humans, Cardiovascular Diseases prevention & control, Early Medical Intervention methods, Mass Screening methods, Mass Screening organization & administration, Polycystic Kidney, Autosomal Dominant complications, Polycystic Kidney, Autosomal Dominant diagnosis

Published

2016

45. Consensus expert recommendations for the diagnosis and management of autosomal recessive polycystic kidney disease: report of an international conference.

Author

Guay-Woodford LM, Bissler JJ, Braun MC, Bockenhauer D, Cadnapaphornchai MA, Dell KM, Kerecuk L, Liebau MC, Alonso-Peclet MH, Shneider B, Emre S, Heller T, Kamath BM, Murray KF, Moise K, Eichenwald EE, Evans J, Keller RL, Wilkins-Haug L, Bergmann C, Gunay-Aygun M, Hooper SR, Hardy KK, Hartung EA, Streisand R, Perrone R, and Moxey-Mims M

Subjects

Child, Child, Preschool, Humans, Infant, Infant, Newborn, Practice Guidelines as Topic, Prenatal Diagnosis, Polycystic Kidney, Autosomal Recessive diagnosis, Polycystic Kidney, Autosomal Recessive therapy

Published

2014

46. Simultaneous sequencing of 24 genes associated with steroid-resistant nephrotic syndrome.

Author

McCarthy HJ, Bierzynska A, Wherlock M, Ognjanovic M, Kerecuk L, Hegde S, Feather S, Gilbert RD, Krischock L, Jones C, Sinha MD, Webb NJ, Christian M, Williams MM, Marks S, Koziell A, Welsh GI, and Saleem MA

Subjects

Adolescent, Child, Child, Preschool, Drug Resistance genetics, Epistasis, Genetic, Female, Genetic Testing trends, Genetic Variation, Genotype, Humans, Infant, Infant, Newborn, Male, Nephrotic Syndrome drug therapy, Nephrotic Syndrome genetics, Phenotype, Polymorphism, Genetic, Predictive Value of Tests, Sequence Analysis, DNA trends, United Kingdom, Algorithms, Genetic Testing methods, Nephrotic Syndrome congenital, Sequence Analysis, DNA methods, Transcriptome

Abstract

Background and Objectives: Up to 95% of children presenting with steroid-resistant nephrotic syndrome in early life will have a pathogenic single-gene mutation in 1 of 24 genes currently associated with this disease. Others may be affected by polymorphic variants. There is currently no accepted diagnostic algorithm for clinical genetic testing. The hypothesis was that the increasing reliability of next generation sequencing allows comprehensive one-step genetic investigation of this group and similar patient groups., Design, Setting, Participants, & Measurements: This study used next generation sequencing to screen 446 genes, including the 24 genes known to be associated with hereditary steroid-resistant nephrotic syndrome. The first 36 pediatric patients collected through a national United Kingdom Renal Registry were chosen with comprehensive phenotypic detail. Significant variants detected by next generation sequencing were confirmed by conventional Sanger sequencing., Results: Analysis revealed known and novel disease-associated variations in expected genes such as NPHS1, NPHS2, and PLCe1 in 19% of patients. Phenotypically unexpected mutations were also detected in COQ2 and COL4A4 in two patients with isolated nephropathy and associated sensorineural deafness, respectively. The presence of an additional heterozygous polymorphism in WT1 in a patient with NPHS1 mutation was associated with earlier-onset disease, supporting modification of phenotype through genetic epistasis., Conclusions: This study shows that next generation sequencing analysis of pediatric steroid-resistant nephrotic syndrome patients is accurate and revealing. This analysis should be considered part of the routine genetic workup of diseases such as childhood steroid-resistant nephrotic syndrome, where the chance of genetic mutation is high but requires sequencing of multiple genes.

Published

2013

47. Systemic arterial hypertension in children following renal transplantation: prevalence and risk factors.

Author

Sinha MD, Kerecuk L, Gilg J, and Reid CJ

Subjects

Child, Child, Preschool, Diastole, Female, Humans, Hypertension epidemiology, Hypertension physiopathology, Kidney Transplantation physiology, Male, Prevalence, Retrospective Studies, Risk Factors, Systole, United Kingdom epidemiology, Hypertension etiology, Kidney Transplantation adverse effects

Abstract

Background: Control of blood pressure (BP) following renal transplantation may improve allograft and patient survival. Our aims were (i) to describe the distribution of BP and the prevalence of systolic and/or diastolic hypertension in children over the first 5 years following renal transplantation and (ii) to evaluate clinical risk factors and centre-specific factors associated with hypertension in this population., Methods: We conducted a retrospective case note review of all current paediatric kidney transplant patients in the UK, with data collected at 6 months, 1, 2 and 5 years following transplantation in subjects with hypertension (systolic and/or diastolic BP > 95th > ) and non-hypertensive subjects BP ≤ 95th > ., Results: In total, 27.3% (117/428), 27.6% (118/428), 26.0% (95/365) and 25.6% (50/195) of the patients were hypertensive (systolic and/or diastolic BP > 95th > ) at 6 months, 1, 2 and 5 years following transplantation, respectively. A total of 58.4% of the patients at 6 months, 52.8% at 1 year, 48.2% at 2 years and 48.2% at 5 years were receiving anti-hypertensive therapy, of whom 31.6-36.6% remained hypertensive. When subjects were identified as being hypertensive, on anti-hypertensive medication or had untreated hypertension (systolic and/or diastolic BP > 95th > ), 66.4, 61.0, 56.4 and 55.9% of patients were hypertensive at 6 months, 1, 2 and 5 years, respectively. In a multivariate model, odds ratios for systolic hypertension were 4.16 (deceased versus living donor), 2.65 (lowest versus highest quartile of height z-score) and 2.07 (if on anti-hypertensive; yes versus no). There was significant variation in prevalent rates of hypertension between centres (P < 0.0001) that remained significant (P = 0.003) after adjustment for all the factors in the multivariate model., Conclusions: Control of BP after kidney transplantation remains sub-optimal in paediatric centres in the UK. Just over 25% of patients remain hypertensive 5 years following transplantation. Significant differences between centres remain unexplained and may reflect differences in assessment and management of hypertension.

Published

2012

48. Progression to hypertension in non-hypertensive children following renal transplantation.

Author

Sinha MD, Gilg JA, Kerecuk L, and Reid CJ

Subjects

Adolescent, Antihypertensive Agents therapeutic use, Blood Pressure Monitoring, Ambulatory, Child, Child, Preschool, Disease Progression, Female, Follow-Up Studies, Glomerular Filtration Rate, Humans, Hypertension drug therapy, Male, Prognosis, Renal Insufficiency, Chronic mortality, Renal Insufficiency, Chronic surgery, Retrospective Studies, Risk Factors, Survival Rate, Hypertension etiology, Hypertension mortality, Kidney Transplantation adverse effects, Renal Insufficiency, Chronic complications

Abstract

Background: The aim of this study was to evaluate in non-hypertensive children following renal transplantation (TX) the rates and determinants of transition to hypertension., Methods: Retrospective case note review of all current paediatric kidney transplant patients in the UK. At baseline (6 months following TX), all included subjects were non-hypertensive with systolic and/or diastolic clinic blood pressure (BP) ≤95th percentile while on no anti-hypertensive therapy. We assessed progression from optimal (systolic and/or diastolic clinic BP<50th percentile), normal (systolic and/or diastolic clinic BP≥50th but <90th percentile) and pre-hypertension (systolic and/or diastolic clinic BP 90th-95th percentile) to hypertension (systolic and/or diastolic clinic BP>95th percentile). If systolic and diastolic BP levels belonged to different categories, the higher of the two levels were used for categorization., Results: At baseline, 146 of 524 (27.9%) children (106 male) median [inter-quartile range (IQR)] age 7.8 years (4.8, 11.8) were non-hypertensive and not on any anti-hypertensive therapy; there were 34 patients (23.2%) with optimal BP, 90 (61.6%) with normal BP and 22 (15.1%) with pre-hypertension. They were followed up for a median of 2.0 (1.0, 4.0) years post-TX. At the end of follow-up, BP was optimal in 37 patients (25.3%), normal in 35 (24.0%), high normal in 2 (1.4%) and 72 (49.3%) had progressed to hypertension. The Kaplan-Meier estimated time at which 50% of patients developed hypertension was 2.0 years for the pre-hypertension and 3.0 years in the normal BP group as opposed to 40% risk at 7-year post-TX in the optimal group (P=0.001 between the three groups). The differences between BP groups remained significant after adjustment for all risk factors on multivariate analysis., Conclusions: Just over 49% of our initially non-hypertensive patients progressed to hypertension following TX. BP needs careful monitoring post-TX and ideally should be maintained in the 'normal' and 'optimal' range.

Published

2012

49. Expression of Fraser syndrome genes in normal and polycystic murine kidneys.

Author

Kerecuk L, Long DA, Ali Z, Anders C, Kolatsi-Joannou M, Scambler PJ, and Woolf AS

Subjects

Animals, Dexamethasone pharmacology, Disease Models, Animal, Embryo Culture Techniques, Extracellular Matrix Proteins metabolism, Fraser Syndrome metabolism, Fraser Syndrome pathology, Gene Expression Regulation, Genes, Reporter, Immunohistochemistry, Lac Operon, Membrane Proteins metabolism, Mice, Mice, Inbred C57BL, Mice, Transgenic, Mutation, Nephrons drug effects, Nephrons embryology, Nephrons pathology, Polycystic Kidney, Autosomal Recessive metabolism, Polycystic Kidney, Autosomal Recessive pathology, Rats, Receptors, Cell Surface genetics, Extracellular Matrix Proteins genetics, Fraser Syndrome genetics, Membrane Proteins genetics, Nephrons metabolism, Polycystic Kidney, Autosomal Recessive genetics

Abstract

Background: Fraser syndrome (FS) features renal agenesis and cystic kidneys. Mutations of FRAS1 (Fraser syndrome 1)and FREM2 (FRAS1-related extracellular matrix protein 2)cause FS. They code for basement membrane proteins expressed in metanephric epithelia where they mediate epithelial/mesenchymal signalling. Little is known about whether and where these molecules are expressed in more mature kidneys., Methods: In healthy and congenital polycystic kidney (cpk)mouse kidneys we sought Frem2 expression using a LacZ reporter gene and quantified Fras family transcripts. Fras1 immunohistochemistry was undertaken in cystic kidneys from cpk mice and PCK (Pkhd1 mutant) rats (models of autosomal recessive polycystic kidney disease) and in wildtype metanephroi rendered cystic by dexamethasone., Results: Nascent nephrons transiently expressed Frem2 in both tubule and podocyte epithelia. Maturing and adult collecting ducts also expressed Frem2. Frem2 was expressed in cpk cystic epithelia although Frem2 haploinsufficiency did not significantly modify cystogenesis in vivo. Fras1 transcripts were significantly upregulated, and Frem3 downregulated, in polycystic kidneys versus the non-cystic kidneys of littermates. Fras1 was immunodetected in cpk, PCK and dexamethasone-induced cystepithelia., Conclusions: These descriptive results are consistent with the hypothesis that Fras family molecules play diverse roles in kidney epithelia. In future, this should be tested by conditional deletion of FS genes in nephron segments and collecting ducts.

Published

2012

50. Improved long-term graft function in pediatric transplant renal recipients with chronic allograft nephropathy.

Author

Kerecuk L, Horsfield C, and Taylor J

Subjects

Adolescent, Child, Child, Preschool, Graft Survival, Humans, Immunosuppressive Agents adverse effects, Infant, Kidney Diseases surgery, Postoperative Complications, Retrospective Studies, Transplantation, Homologous, Immunosuppressive Agents therapeutic use, Kidney Diseases etiology, Kidney Transplantation adverse effects

Abstract

CAN is the leading cause of graft loss in pediatric renal transplant recipients. A retrospective single centre analysis of pediatric transplant patients with CAN treated with MMF in conjunction with CNI minimisation/withdrawal is reported. 35 children were successfully started on MMF. The mean age at transplant was 7.9 +/- 0.1 years. MMF was introduced 3.5 +/- 0.1 years after transplantation and patients were followed up for a mean of 32.2 +/- 0.5 months. CAN was confirmed on biopsy in 31 patients. CNI was stopped in 23 patients at a mean time of 16.5 +/- 0.6 months after MMF introduction and minimised in the remaining patients. Prior to MMF introduction, GFR was deteriorating by 21.6 +/- 0.07 ml/min/1.73 m(2)/yr. After MMF, there was an overall improvement in GFR of 4.0 +/- 0.03 ml/min/1.73 m(2)/yr. This was most marked in the first six months when the GFR improved by 20.8 +/- 0.06 ml/min/1.73 m(2)/day. Mean acute rejection episode rate prior to MMF was significantly reduced after MMF introduction. MMF was discontinued in a total of 4 patients due to adverse effects. CNI minimisation/withdrawal with MMF introduction is safe and leads to significant initial improvement with subsequent stabilisation of GFR and improved long term graft survival in pediatric renal transplant recipients with CAN.

Published

2009