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10. G234(P) Case report: premature adrenarche and pseudohypoparathyroidism – mechanistically linked or coincidence?

Author

Odone, JC, Kumar, Y, and Burren, CP

Abstract

AimsTo describe a case of premature adrenarche with pseudohypoparathyroidism, an as yet unreported combination.MethodsAn otherwise well 8 year old girl presented to a Paediatric Endocrine Clinic with early pubic hair development suggestive of premature adrenarche. Blood tests revealed hypocalcaemia, elevated phosphate and highly elevated parathyroid hormone (PTH) level, giving a biochemical diagnosis of pseudohypoparathyroidism. She had normal stature (height 50th – 75th centile) and no phenotypic features of Albright Hereditary Osteodystrophy (AHO) were identified: obesity, learning difficulties, brachydactyly, short stature, shortened 4th/5th metacarpals, dental hypoplasia or a rounded face.ResultsBlood tests revealed low corrected calcium 1.49 mmol/L (reference range 2.2–5.7), elevated phosphate 2.78 mmol/L (reference range 0.9–1.8) and serum PTH level almost 10 times the upper limit of normal at 66.4 pmol/L (reference range 1.6–6.9), with normal Vitamin D 94 nmol/L, normal thyroid function: Free T4 5.4 pmol/L (reference range 12–22); TSH 4.8 miu/L (reference range 0.27–4.2).Hand and wrist Xray for bone age assessment revealed mildly shortened 4th/5th metacarpals, a phenotypic feature of AHO. Genetic testing results and MRI head to screen for white matter calcification are awaited. These will help clarify which subtype of pseudohypoparathyroidism is responsible for this presentation.ManagementShe commenced oral calcium carbonate and alfacalcidol to correct the severe calcium deficiency and to normalise PTH levels. Progressively increasing doses have been required.ConclusionPseudohypoparathyroidism is a rare endocrine disorder characterised by resistance to the action of PTH. It has been classified within the AHO group. Recognition of a broader range of phenotypic features and underlying mutations has led to a novel classification system of iPPSD (inactivating PTH/PTHrP signalling disorders) developed by the EuroPHP network. GNAS1 mutations have been identified underlying various pseudohypoparathyroidism subtypes, resulting in reduced function of the G-protein coupled to the PTH receptor. G-proteins are also coupled to other hormone receptors; patients with AHO or iPPSD often present with a range of endocrine disorders, for example hypothyroidism. There are cases of individuals with GNAS1 mutations presenting concurrently with precocious puberty and pseudohypoparathyroidism but no reported case of premature adrenarche and pseudohypoparathyroidism. Awaited genetic studies in our case may be informative.

Published
2018
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11. Type 2 diabetes in adolescence – unearthed at the time of registration with the general practitioner (GP)

Author

Ng, GYT and Burren, CP

Abstract

Type 2 diabetes, or non-insulin-dependent diabetes mellitus (NIDDM), is often considered to be a diagnosis of adulthood. We present a 13 year old boy who was noted to have glycosuria on routine general practitioner (GP) urine testing. Clinical examination upon referral showed massive obesity, hypertension and prominent acanthosis nigricans, and investigations confirmed hyperinsulinaemia and hyperglycaemia. Metformin and a programme of weight reduction comprise the management of this young adolescent with type 2 diabetes. Such early diagnosis should permit the institution of appropriate management to avoid the early emergence of the complications of type 2 diabetes. Copyright © 2000 John Wiley & Sons, Ltd.

Published
2000

12. Congenital hallux valgus occurs in Fibrodysplasia Ossificans Progressiva and BMPR1B-associated dysplasia: an important distinction.

Author

Shirodkar D, Smithson SF, Keen R, Lester T, Banos-Pinero B, and Burren CP

Subjects
Humans, Female, Infant, Myositis Ossificans genetics, Hallux Valgus genetics, Hallux Valgus diagnostic imaging, Bone Morphogenetic Protein Receptors, Type I genetics
Abstract

Background: Fibrodysplasia Ossificans Progressiva (FOP; OMIM #135100) is an ultrarare genetic disorder characterised by congenital bilateral hallux valgus (CBHV), intermittent soft tissue swellings and progressive heterotopic ossification. We report a three-month-old girl with great toe abnormalities similar to FOP, in whom comprehensive clinical workup and genetic investigations illustrates an alternative diagnosis., Case Presentation: A three-month-old girl presented with CBHV. The antenatal period was unremarkable, she was born by spontaneous vaginal delivery with an uneventful subsequent course, except for maternal concern of her bent toes which received reassurance from several health professionals. Her mother's persisting concerns were explored via the internet and social media leading her to request referral to an expert bone centre for consideration of FOP. On examination, she was thriving, there was no dysmorphism, subcutaneous lumps, skeletal or extra-skeletal deformity except for shortened great toes with lateral deviation of the proximal and distal phalanges. FOP was a feasible diagnosis, for which CBHV is highlighted as an early sign. A cautionary potential diagnosis of FOP was counselled, including advice to defer intramuscular immunisations until genetic results available. Genetic investigation was undertaken through rapid whole genomic sequencing (WGS), with analysis of data from a skeletal dysplasia gene panel, which demonstrated no ACVR1variants. The only finding was a heterozygous variant of unknown significance in BMPR1B (c1460T>A, p.(Val487Asp)), which encodes a bone morphogenic receptor involved in brachydactyly syndromes A1, A2 and D and acromesomelic dysplasia 3 (only the latter being an autosomal recessive condition)., Conclusion: This report highlights that CBHV serves as a vital diagnostic indicator of FOP and affected infants should be considered and investigated for FOP, including precautionary management whilst awaiting genetic studies. The second educational aspect is that CBHV may not represent a generalised skeletal disorder, or one much less significant than FOP. Receptor-ligand BMP and Activins mediated interactions are instrumental in the intricate embryology of the great toe. Recognition of non-FOP conditions caused by alterations in different genes are likely to increase with new genomic technology and large gene panels, enhancing understanding of bone signaling pathways., (© 2024. The Author(s).)

Published
2024
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13. Growth reference charts for children with hypochondroplasia.

Author

Cheung MS, Cole TJ, Arundel P, Bridges N, Burren CP, Cole T, Davies JH, Hagenäs L, Högler W, Hulse A, Mason A, McDonnell C, Merker A, Mohnike K, Sabir A, Skae M, Rothenbuhler A, Warner J, and Irving M

Subjects
Child, Humans, Female, Growth Charts, Prospective Studies, Body Height genetics, Reference Values, Dwarfism diagnosis, Dwarfism genetics, Osteochondrodysplasias, Bone and Bones abnormalities, Lordosis, Limb Deformities, Congenital
Abstract

Hypochondroplasia (HCH) is a rare skeletal dysplasia causing mild short stature. There is a paucity of growth reference charts for this population. Anthropometric data were collected to generate height, weight, and head circumference (HC) growth reference charts for children with a diagnosis of HCH. Mixed longitudinal anthropometric data and genetic analysis results were collected from 14 European specialized skeletal dysplasia centers. Growth charts were generated using Generalized Additive Models for Location, Scale, and Shape. Measurements for height (983), weight (896), and HC (389) were collected from 188 (79 female) children with a diagnosis of HCH aged 0-18 years. Of the 84 children who underwent genetic testing, a pathogenic variant in FGFR3 was identified in 92% (77). The data were used to generate growth references for height, weight, and HC, plotted as charts with seven centiles from 2nd to 98th, for ages 0-4 and 0-16 years. HCH-specific growth charts are important in the clinical care of these children. They help to identify if other comorbidities are present that affect growth and development and serve as an important benchmark for any prospective interventional research studies and trials., (© 2023 The Authors. American Journal of Medical Genetics Part A published by Wiley Periodicals LLC.)

Published
2024
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14. Effective Long-term Pediatric Pegvisomant Monotherapy to Final Height in X-linked Acrogigantism.

Author

Burren CP, Williams G, Coxson E, and Korbonits M

Abstract

X-linked acrogigantism (X-LAG) is characterized by extreme tall stature from early childhood resulting from duplication of the GPR101 gene, in turn resulting in GH excess. Most cases present with pituitary tumors secreting GH and prolactin. Diffuse pituitary hyperplasia is uncommon and normal prolactin is rare. We present a girl with tall stature from 3 years of age; her height was +4.25 SD score at 5 years, with no signs of syndromic disease. She had significant GH excess, serum IGF-1 4 times the upper limit of normal and normal circulating GHRH, with normal pituitary magnetic resonance imaging over 13 years. No abnormalities were found in either the AIP or MEN1 genes. Treatment with somatostatin analogues and dopamine agonists showed minimal therapeutic benefit, but significant side effects. She tested positive for duplication of GPR101 6 years after the initial diagnosis. She was then initiated on pegvisomant aged 12 years, achieving prompt IGF-1 normalization and growth cessation. Aged 16.5 years, she showed escape from IGF-1 control, and height velocity increased, but this responded well to a dose increase in pegvisomant, with reassuring long-term pediatric safety over 7 years. Her final height is +2.9 SD score. Currently, life-long pegvisomant treatment is planned with genetic counselling regarding future offspring., (© The Author(s) 2023. Published by Oxford University Press on behalf of the Endocrine Society.)

Published
2023
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15. A systematic analysis of splicing variants identifies new diagnoses in the 100,000 Genomes Project.

Author

Blakes AJM, Wai HA, Davies I, Moledina HE, Ruiz A, Thomas T, Bunyan D, Thomas NS, Burren CP, Greenhalgh L, Lees M, Pichini A, Smithson SF, Taylor Tavares AL, O'Donovan P, Douglas AGL, Whiffin N, Baralle D, and Lord J

Subjects
Exons, Humans, Introns, RNA, RNA Splicing, Rare Diseases genetics
Abstract

Background: Genomic variants which disrupt splicing are a major cause of rare genetic diseases. However, variants which lie outside of the canonical splice sites are difficult to interpret clinically. Improving the clinical interpretation of non-canonical splicing variants offers a major opportunity to uplift diagnostic yields from whole genome sequencing data., Methods: Here, we examine the landscape of splicing variants in whole-genome sequencing data from 38,688 individuals in the 100,000 Genomes Project and assess the contribution of non-canonical splicing variants to rare genetic diseases. We use a variant-level constraint metric (the mutability-adjusted proportion of singletons) to identify constrained functional variant classes near exon-intron junctions and at putative splicing branchpoints. To identify new diagnoses for individuals with unsolved rare diseases in the 100,000 Genomes Project, we identified individuals with de novo single-nucleotide variants near exon-intron boundaries and at putative splicing branchpoints in known disease genes. We identified candidate diagnostic variants through manual phenotype matching and confirmed new molecular diagnoses through clinical variant interpretation and functional RNA studies., Results: We show that near-splice positions and splicing branchpoints are highly constrained by purifying selection and harbour potentially damaging non-coding variants which are amenable to systematic analysis in sequencing data. From 258 de novo splicing variants in known rare disease genes, we identify 35 new likely diagnoses in probands with an unsolved rare disease. To date, we have confirmed a new diagnosis for six individuals, including four in whom RNA studies were performed., Conclusions: Overall, we demonstrate the clinical value of examining non-canonical splicing variants in individuals with unsolved rare diseases., (© 2022. The Author(s).)

Published
2022
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16. Monitoring Skull Base Abnormalities in Children with Osteogenesis Imperfecta - Review of Current Practice and a Suggested Clinical Pathway.

Author

Wadanamby S, El Garwany S, Connolly D, Arundel P, Bishop NJ, DeVile CJ, Calder AD, Crowe B, Burren CP, Saraff V, and Offiah AC

Subjects
Child, Critical Pathways, Humans, Prospective Studies, Retrospective Studies, Skull Base diagnostic imaging, Osteogenesis Imperfecta diagnostic imaging
Abstract

Objectives: In the context of a lack of national consensus on the benefits of skull base imaging in children with osteogenesis imperfecta (OI), this study aims to analyse and correlate the clinical symptoms and radiological images of children with severe OI., Methods: A retrospective case notes and image analysis was carried out on children with complex OI between 2012 and 2018 at a specialist tertiary centre. Data were collected on patient demographic factors, clinical data, imaging findings (presence of Wormian bones, platybasia, basilar impression (McGregor's technique) and basilar invagination (McRae's technique)), and clinical features at the time of imaging., Results: Of the 127 patients in the OI database, 94 were included. A total of 321 radiographs, 21 CT scans and 39 MRI scans were analysed. Average frequency of radiographs was 8 per 10 years. Of the 94 patients, 58 (62%), 10 (11%), 1 (1%) demonstrated platybasia, basilar impression, and basilar invagination, respectively. Of the radiographs analysed, platybasia, basilar impression, basilar invagination, and the presence of Wormian bones, could not be evaluated in 71 (22.3%), 48 (15.2%), 61 (19.5%) and 28 (9.4%) radiographs respectively (due to poor positioning, anatomical abnormalities, and poor image quality). Of the 140 radiographs with platybasia, 17 (12%) also demonstrated basilar impression compared to only 3 (2.9%) out of the 99 without platybasia (p = 0.03). No significant associations were seen between the presence of Wormian bones and basilar impression. Of the 39 MRIs, additional information on CSF flow rate, spinal cord signal and cerebellar morphology was reported in 14 (36%). There was a lack of concordance between MRI and matched radiographs in 7.1% (1/14) and 36% (5/14) for platybasia and basilar impression respectively, with full concordance for basilar invagination. Fewer than 5% had positive clinical symptoms/signs at the time of imaging; 2% (7/321) had macrocephaly, 0.6% (2/321) headache, all other neurological features were absent). Clinical features were not documented in >85% of patients., Conclusion: The apparent low prevalence of clinical symptoms and signs and of radiologically identified cranio-cervical abnormalities, suggests that current levels of serial imaging may be excessive. Until larger prospective studies clarify these issues, we suggest a clinical pathway for base of skull imaging which proposes a risk stratification approach to radiographic frequency and suggests parameters for proceeding to MRI., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published
2022
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17. Mutations That Affect the Surface Expression of TRPV6 Are Associated with the Upregulation of Serine Proteases in the Placenta of an Infant.

Author

Fecher-Trost C, Wolske K, Wesely C, Löhr H, Klawitter DS, Weissgerber P, Gradhand E, Burren CP, Mason AE, Winter M, and Wissenbach U

Subjects
Amino Acid Sequence, Animals, Calcium Channels metabolism, Calcium Channels physiology, Case-Control Studies, Cathepsin G genetics, Female, Gene Expression Regulation, Enzymologic, High-Temperature Requirement A Serine Peptidase 1 genetics, Humans, Infant, Mice, Knockout, Osteochondrodysplasias etiology, Osteochondrodysplasias metabolism, Placenta metabolism, Pregnancy, Proteome analysis, TRPV Cation Channels metabolism, TRPV Cation Channels physiology, Mice, Calcium Channels genetics, Cathepsin G metabolism, High-Temperature Requirement A Serine Peptidase 1 metabolism, Mutation, Osteochondrodysplasias pathology, Placenta pathology, Proteome metabolism, TRPV Cation Channels genetics
Abstract

Recently, we reported a case of an infant with neonatal severe under-mineralizing skeletal dysplasia caused by mutations within both alleles of the TRPV6 gene. One mutation results in an in frame stop codon (R 510 stop) that leads to a truncated, nonfunctional TRPV6 channel, and the second in a point mutation (G 660 R) that, surprisingly, does not affect the Ca 2+ permeability of TRPV6. We mimicked the subunit composition of the unaffected heterozygous parent and child by coexpressing the TRPV6 G 660 R and R 510 stop mutants and combinations with wild type TRPV6. We show that both the G 660 R and R 510 stop mutant subunits are expressed and result in decreased calcium uptake, which is the result of the reduced abundancy of functional TRPV6 channels within the plasma membrane. We compared the proteomic profiles of a healthy placenta with that of the diseased infant and detected, exclusively in the latter two proteases, HTRA1 and cathepsin G. Our results implicate that the combination of the two mutant TRPV6 subunits, which are expressed in the placenta of the diseased child, is responsible for the decreased calcium uptake, which could explain the skeletal dysplasia. In addition, placental calcium deficiency also appears to be associated with an increase in the expression of proteases.

Published
2021
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18. AIFM1-associated X-linked spondylometaphyseal dysplasia with cerebral hypomyelination.

Author

Edgerley K, Barnicoat A, Offiah AC, Calder AD, Mankad K, Thomas NS, Bunyan DJ, Williams M, Buxton C, Majumdar A, Vijayakumar K, Hilliard T, Turner J, Burren CP, Monsell F, and Smithson SF

Subjects
Bone Development genetics, Exons, Genetic Diseases, X-Linked diagnosis, Genetic Diseases, X-Linked diagnostic imaging, Genetic Diseases, X-Linked pathology, Humans, Male, Mutation genetics, Nervous System Malformations diagnosis, Nervous System Malformations diagnostic imaging, Nervous System Malformations pathology, Osteochondrodysplasias diagnosis, Osteochondrodysplasias diagnostic imaging, Osteochondrodysplasias pathology, Pedigree, Apoptosis Inducing Factor genetics, Genetic Diseases, X-Linked genetics, Genetic Predisposition to Disease, Nervous System Malformations genetics, Osteochondrodysplasias genetics
Abstract

Spondylometaphyseal dysplasia with cerebral hypomyelination (SMD-H) is a very rare but distinctive phenotype, unusually combining spondylometaphyseal dysplasia with hypomyelinating leukodystrophy. Recently, SMD-H has been associated with variants confined to a specific intra-genic locus involving Exon 7, suggesting that AIFM1 plays an important role in bone development and metabolism as well as cerebral myelination. Here we describe two further affected boys, one with a novel intronic variant associated with skipping of Exon 7 of AIFM1 and the other a synonymous variant within Exon 7 of AIFM1. We describe their clinical course and radiological and genetic findings, providing further insight into the natural history of this condition., (© 2021 Wiley Periodicals LLC.)

Published
2021
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19. The third case of TNFRSF11A-associated dysosteosclerosis with a mutation producing elongating proteins.

Author

Xue JY, Wang Z, Smithson SF, Burren CP, Matsumoto N, Nishimura G, Ikegawa S, and Guo L

Subjects
Child, Preschool, Female, Humans, Osteosclerosis genetics, Osteosclerosis metabolism, Prognosis, Exome Sequencing, Mutation, Osteosclerosis pathology, Receptor Activator of Nuclear Factor-kappa B genetics, Receptor Activator of Nuclear Factor-kappa B metabolism
Abstract

Dysosteosclerosis (DOS) is a distinct form of sclerosing bone disease characterized by platyspondyly and progressive osteosclerosis. DOS is genetically heterogeneous. Three causal genes, SLC29A3, CSF1R, and TNFRSF11A are reported. TNFRSF11A-associated DOS has been identified in two patients; however, TNFRSF11A is also a causal gene for osteopetrosis, autosomal recessive 7 (OP-AR7). Whole-exome sequencing in a patient with sclerosing bone disease identified novel compound heterozygous variants (c.414_427 + 7del, c.1664del) in TNFRSF11A. We examined the impact of the two variants on five splicing isoforms of TNFRSF11A by RT-PCR. We found that c.1664del resulted in elongated proteins (p.S555Cfs*121, etc.), while c.414_427 + 7del generated two aberrant splicing products (p.A139Wfs*19 and p.E132Dfs*19) that lead to nonsense mediated mRNA decay (NMD). In the previous two cases of TNFRSF11A-associated DOS, their mutations produced truncated TNFRSF11A protein isoforms. The mutations in all three cases thus contrast with TNFRSF11A mutations reported in OP-AR7, which does not generated truncated or elongated TNFRSF11A proteins. Thus, we identified the third case of TNFRSF11A-associated DOS and reinforced the genotype-phenotype correlation that aberrant protein-producing TNFRSF11A mutations cause DOS.

Published
2021
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20. Pathobiologic Mechanisms of Neurodegeneration in Osteopetrosis Derived From Structural and Functional Analysis of 14 ClC-7 Mutants.

Author

Di Zanni E, Palagano E, Lagostena L, Strina D, Rehman A, Abinun M, De Somer L, Martire B, Brown J, Kariminejad A, Balasubramaniam S, Baynam G, Gurrieri F, Pisanti MA, De Maggio I, Abboud MR, Chiesa R, Burren CP, Villa A, Sobacchi C, and Picollo A

Subjects
Animals, Chloride Channels genetics, Humans, Lysosomes, Mice, Mutation genetics, Osteoclasts, Bone Resorption, Osteopetrosis genetics
Abstract

ClC-7 is a chloride-proton antiporter of the CLC protein family. In complex with its accessory protein Ostm-1, ClC-7 localizes to lysosomes and to the osteoclasts' ruffled border, where it plays a critical role in acidifying the resorption lacuna during bone resorption. Gene inactivation in mice causes severe osteopetrosis, neurodegeneration, and lysosomal storage disease. Mutations in the human CLCN7 gene are associated with diverse forms of osteopetrosis. The functional evaluation of ClC-7 variants might be informative with respect to their pathogenicity, but the cellular localization of the protein hampers this analysis. Here we investigated the functional effects of 13 CLCN7 mutations identified in 13 new patients with severe or mild osteopetrosis and a known ADO2 mutation. We mapped the mutated amino acid residues in the homology model of ClC-7 protein, assessed the lysosomal colocalization of ClC-7 mutants and Ostm1 through confocal microscopy, and performed patch-clamp recordings on plasma-membrane-targeted mutant ClC-7. Finally, we analyzed these results together with the patients' clinical features and suggested a correlation between the lack of ClC-7/Ostm1 in lysosomes and severe neurodegeneration. © 2020 American Society for Bone and Mineral Research (ASBMR)., (© 2020 American Society for Bone and Mineral Research (ASBMR).)

Published
2021
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21. Challenges in long-term control of hypercalcaemia with denosumab after haematopoietic stem cell transplantation for TNFRSF11A osteoclast-poor autosomal recessive osteopetrosis.

Author

Taylor-Miller T, Sivaprakasam P, Smithson SF, Steward CG, and Burren CP

Abstract

Autosomal recessive osteopetrosis (ARO) is rare, involving increased bone density due to defective osteoclast differentiation or function, with several genetic subtypes., Case: This child with compound heterozygous novel loss-of-function TNFRSF11A pathogenic variants causing osteoclast-poor ARO underwent haematopoietic stem cell transplantation (HSCT) aged 3.1 years and experienced episodic severe hypercalcaemia over 2.5 years. She initially presented aged 8 months with craniosynostosis and visual impairment and underwent surgery; no increased bone density evident on skull imaging nor variants in genes associated with craniosynostosis identified. She was subsequently referred for investigation of poor linear growth and low alkaline phosphatase. Clinical abnormalities included asymmetric pectus carinatum, thickened anterior tibia and wrists, and markedly delayed dentition. Skeletal survey revealed generalised osteosclerosis with undertubulation., Management: She received haploidentical HSCT aged 3.1 years and developed hypercalcaemia (adjusted calcium 4.09mmol/L = 16.4mg/dL) Day 18 post-HSCT, unresponsive to hyperhydration and diuretics. Denosumab achieved normocalcaemia, which required 0.6mg/kg every 6 weeks long-term. The ensuing 2.75 years feature full donor engraftment, good HSCT graft function, skeletal remodelling with 2.5 years recurrent severe hypercalcaemia and nine fragility long bone fractures., Conclusion: This case illustrates challenges of bone and calcium management in ultrarare TNFRSF11A -related OP-ARO. Craniosynostosis was an early feature, evident pre-sclerosis in osteopetrosis. Following HSCT, restoration of osteoclast activity in the context of elevated bone mass produced severe and prolonged (2.5 years) hypercalcaemia. Denosumab was effective medium-term, but required concurrent long duration (11 months) zoledronic acid to manage recurrent hypercalcaemia. Fragility fractures brought appreciable additional morbidity in the post-HSCT phase., Competing Interests: None., (© 2020 The Authors.)

Published
2020
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22. Expanding the phenotypic spectrum of IFT81: Associated ciliopathy syndrome.

Author

Ashraf T, Vaina C, Giri D, Burren CP, James M, Offiah AC, Overton T, Baptista J, Ellard S, and Smithson SF

Subjects
Cilia pathology, Ciliopathies diagnosis, Ciliopathies physiopathology, Craniosynostoses diagnosis, Craniosynostoses physiopathology, Homozygote, Humans, Infant, Newborn, Male, Mutation genetics, Phenotype, Short Rib-Polydactyly Syndrome diagnosis, Short Rib-Polydactyly Syndrome physiopathology, Ciliopathies genetics, Craniosynostoses genetics, Muscle Proteins genetics, Short Rib-Polydactyly Syndrome genetics
Abstract

Short-rib polydactyly syndromes are a heterogeneous group of disorders characterized by narrow thorax with short ribs, polydactyly and often other visceral and skeletal malformations. To date there have only been six reported patients with homozygous and compound heterozygous variants in IFT81, causing a short-rib thoracic dysplasia, with, or without, polydactyly (SRTD19: OMIM 617895). IFT81 is a protein integral to the core of the intraflagellar transport complex B (IFT-B), which is involved in anterograde transport in the cilium. We describe the case of a male infant with compound heterozygous variants in IFT81, who presented with short long bones, a narrow thorax, polydactyly, and multiple malformations. Three novel clinical features are reported including complete situs inversus, micropenis, and rectal atresia, which have not previously been associated with variants in IFT81. We reviewed the literature and identified the most consistent clinical features associated with this rare ciliopathy syndrome. We postulate that dolichocephaly and sagittal craniosynostosis may be associated with this condition, and provide a clue to considering IFT81 as the causative gene when deciphering complex ciliopathies., (© 2020 Wiley Periodicals LLC.)

Published
2020
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23. Improvement in glycaemic parameters using SGLT-2 inhibitor and GLP-1 agonist in combination in an adolescent with diabetes mellitus and Prader-Willi syndrome: a case report.

Author

Candler T, McGregor D, Narayan K, Moudiotis C, and Burren CP

Subjects
Adolescent, Benzhydryl Compounds pharmacology, Blood Glucose drug effects, Blood Glucose metabolism, Child, Diabetes Mellitus blood, Diabetes Mellitus etiology, Drug Therapy, Combination, Female, Glucagon-Like Peptide 1 agonists, Glucosides pharmacology, Humans, Liraglutide pharmacology, Prader-Willi Syndrome blood, Prader-Willi Syndrome complications, Sodium-Glucose Transporter 2 Inhibitors administration & dosage, Sodium-Glucose Transporter 2 Inhibitors pharmacology, Treatment Outcome, Benzhydryl Compounds administration & dosage, Diabetes Mellitus drug therapy, Glucosides administration & dosage, Liraglutide administration & dosage, Prader-Willi Syndrome drug therapy
Abstract

Objectives Prader-Willi Syndrome (PWS) is characterised by hyperphagia often leading to obesity; a known risk factor for insulin resistance and type 2 (T2) diabetes. We present a prepubertal girl with PWS who developed diabetes. Case presentation Our case was diagnosed with PWS in infancy following investigation for profound central hypotonia and feeding difficulties. She commenced growth hormone (GH) aged 8 years for short stature and treatment improved linear growth. At age 12 years, she presented with polydipsia, polyuria and vulvovaginitis. She was overweight (BMI SDS +1.43). Diabetes was diagnosed (Blood glucose = 24.2 mmol/L, HbA1c = 121 mmol/mol or 13.2%). She was not acidotic and had negative blood ketones. Autoantibodies typical of type 1 diabetes were negative. She was initially treated with basal bolus insulin regime. GH was discontinued 3 months later due to concerns regarding GH-induced insulin resistance. Off GH, insulin requirements reduced to zero, allowing Metformin monotherapy. However off GH, she reported significant lethargy with static growth and increased weight. Combinations of Metformin with differing insulin regimes did not improve glucose levels. Liraglutide (GLP-1 agonist) and Metformin did not improve glucose levels nor her weight. Liraglutide and Empaglifozin (SGLT-2 inhibitor) therapy used in combination were well tolerated and demonstrated rapid normalisation of blood glucose and improvement in her HbA1c to within target (48 mmol/mol) which was sustained after 6 months of treatment. Conclusions Newer treatments for type 2 diabetes (e. g. GLP-1 agonists or SGLT-2 inhibitors) offer potential treatment options for those with diabetes and PWS when conventional treatments are ineffective.

Published
2020
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24. Post-mortem histology in transient receptor potential cation channel subfamily V member 6 (TRPV6) under-mineralising skeletal dysplasia suggests postnatal skeletal recovery: a case report.

Author

Mason AE, Grier D, Smithson SF, Burren CP, and Gradhand E

Subjects
Autopsy, Bone and Bones abnormalities, Calcification, Physiologic genetics, Calcium metabolism, Calcium Channels analysis, DNA Mutational Analysis, Female, Humans, Infant, Osteochondrodysplasias rehabilitation, Parturition physiology, TRPV Cation Channels analysis, Bone Development genetics, Bone and Bones pathology, Calcium Channels genetics, Child Development physiology, Osteochondrodysplasias genetics, Osteochondrodysplasias pathology, TRPV Cation Channels genetics
Abstract

Background: The calcium-selective channel TRPV6 (transient receptor potential cation channel subfamily V member 6) is crucial for maternal-fetal calcium transport across the placenta. TRPV6 mutations have recently been associated with an antenatally severe under-mineralising skeletal dysplasia accompanied by postnatal biochemical abnormalities. This is the first post-mortem report in a patient with TRPV6 skeletal dysplasia., Case Presentation: The female infant had severe antenatal and postnatal skeletal abnormalities by 20 weeks gestation and was ventilator-dependent from birth. These skeletal abnormalities were apparent at an earlier gestational age than in previous reported cases and a more severe clinical course ensued. Biochemical and skeletal abnormalities, including bone density, improved postnatally but cardiac arrest at 4 months of age led to withdrawal of intensive care. Compound heterozygous TRPV6 variants (c.1978G > C p.(Gly660Arg) and c.1528C > T p.(Arg510Ter)) were identified on exome sequencing. Post-mortem identified skeletal abnormalities but no specific abnormalities in other organ systems. No placental pathology was found, multi-organ histological features reflected prolonged intensive care only. Post-mortem macroscopic examination indicated reduced thoracic size and short, pale and pliable ribs. Histological examination identified reduced number of trabeculae in the diaphyses (away from the growth plates), whereas metaphyses showed adequate mineralisation and normal number of trabeculae, but with slightly enlarged reactive chondrocytes, indicating post-natal skeletal growth recovery. Post-mortem radiological findings demonstrated improved bone density, improved rib width, healed fractures, although ribs were still shorter than normal. Long bones (especially humerus and femur) had improved from initial poorly defined metaphyses and reduced bone density to sharply defined metaphyses, prominent growth restart lines in distal diaphyses and bone-in-bone appearance along diaphyses., Conclusions: This case provide bone histological confirmation that human skeletal development is compromised in the presence of TRPV6 pathogenic variants. Post-mortem findings were consistent with abnormal in utero skeletal mineralisation due to severe calcium deficit from compromised placental calcium transfer, followed by subsequent phenotypic improvement with adequate postnatal calcium availability. Significant skeletal recovery occurs in the early weeks of postnatal life in TRPV6 skeletal dysplasia.

Published
2020
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25. Challenges of delivery of dental care and dental pathologies in children and young people with osteogenesis imperfecta.

Author

Clark R, Burren CP, and John R

Subjects
Adolescent, Child, Dental Care, Diphosphonates, Humans, Dental Caries, Dentinogenesis Imperfecta, Osteogenesis Imperfecta
Abstract

Background: Osteogenesis imperfecta (OI) is the most common inherited disorder of bone fragility in children, increasing fracture risk 100-fold and can feature dental and facial bone involvement causing additional morbidities., Aim: To assess the utilisation of tertiary dental services by children and young people with OI attending a supra-regional multi-disciplinary OI service and review of the pathology identified and interventions undertaken., Design: Case notes review of the current caseload of children and young people (0-18 years) with OI at a large regional OI specialist centre (n = 92). Primary outcome was whether an initial dental assessment was arranged in a tertiary dental centre and the corresponding attendance., Results: 49% had a tertiary dental assessment arranged, of whom 82% attended (one quarter requiring several appointments) and 18% did not attend (DNA).Those travelling > 100 miles had a DNA rate of 47%. Assessed children had dentinogenesis imperfecta (24%, 50% in Type III OI), radiographs (95%), caries (41%), required extraction under general anaesthesia (38%) and malocclusion (30%). 48% of the total cohort received bisphosphonates., Conclusion: Tertiary dental assessment encountered barriers to uptake of recommended referral in all patients, often due to geographic factors of travel distance, yet when implemented did identify pathology in a large proportion and many resulted in dental intervention. These emphasise the relevance of specialist dental assessment in OI, particularly in the modern context of increased use of bisphosphonates. This is challenging to achieve and several models of delivery of care may need to be considered in this chronic childhood condition.

Published
2019
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27. TRPV6 compound heterozygous variants result in impaired placental calcium transport and severe undermineralization and dysplasia of the fetal skeleton.

Author

Burren CP, Caswell R, Castle B, Welch CR, Hilliard TN, Smithson SF, and Ellard S

Subjects
Alleles, Calcium Channels chemistry, Comparative Genomic Hybridization, Exome, Female, Humans, Models, Molecular, Placenta metabolism, Pregnancy, Protein Conformation, Radiography, Severity of Illness Index, Structure-Activity Relationship, TRPV Cation Channels chemistry, Exome Sequencing, Bone Diseases, Developmental diagnosis, Bone Diseases, Developmental genetics, Calcium Channels genetics, Genetic Association Studies methods, Genetic Predisposition to Disease, Genetic Variation, Heterozygote, TRPV Cation Channels genetics
Abstract

Transient receptor potential vanilloid 6 (TRPV6) functions in tetramer form for calcium transport. Until now, TRPV6 has not been linked with skeletal development disorders. An infant with antenatal onset thoracic insufficiency required significant ventilatory support. Skeletal survey showed generalized marked undermineralization, hypoplastic fractured ribs, metaphyseal fractures, and extensive periosteal reaction along femoral, tibial, and humeral diaphyses. Parathyroid hormone (PTH) elevation (53.4-101 pmol/L) initially suggested PTH signaling disorders. Progressively, biochemical normalization with radiological mineralization suggested recovery from in utero pathophysiology. Genomic testing was undertaken and in silico protein modeling of variants. No abnormalities in antenatal CGH array or UPD14 testing. Postnatal molecular genetic analysis found no causative variants in CASR, GNA11, APS21, or a 336 gene skeletal dysplasia panel investigated by whole exome sequencing. Trio exome analysis identified compound heterozygous TRPV6 likely pathogenic variants: novel maternally inherited missense variant, c.1978G > C p.(Gly660Arg), and paternally inherited nonsense variant, c.1528C > T p.(Arg510Ter), confirming recessive inheritance. p.(Gly660Arg) generates a large side chain protruding from the C-terminal hook into the interface with the adjacent TRPV6 subunit. In silico protein modeling suggests steric clashes between interface residues, decreased C-terminal hook, and TRPV6 tetramer stability. The p.(Gly660Arg) variant is predicted to result in profound loss of TRPV6 activity. This first case of a novel dysplasia features severe but improving perinatal abnormalities. The TRPV6 compound heterozygous variants appear likely to interfere with fetoplacental calcium transfer crucial for in utero skeletal development. Astute clinical interpretation of evolving perinatal abnormalities remains valuable in complex calcium and bone pathophysiology and informs exome sequencing interpretation., (© 2018 Wiley Periodicals, Inc.)

Published
2018
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28. Diagnostic and management challenges from childhood, puberty through to transition in severe insulin resistance due to insulin receptor mutations.

Author

Wei C and Burren CP

Subjects
Child, Female, Humans, Hyperinsulinism drug therapy, Hyperinsulinism genetics, Hypoglycemic Agents therapeutic use, Insulin Resistance genetics, Antigens, CD genetics, Hyperinsulinism complications, Puberty, Receptor, Insulin genetics
Abstract

Two Caucasian girls, both of normal weight and body mass indices, were diagnosed with type A insulin resistance (IR) in childhood. Case 1 presented with premature adrenarche aged 7 years, then by age 12 years had hirsutism, acne, acanthosis nigricans, and asymptomatic diabetes. Subsequent investigation revealed raised adiponectin (15.3 mg/L) and heterozygous p.Pro1205Leu mutation in the INSR gene encoding the insulin receptor. She experienced postprandial hypoglycaemia on metformin; acarbose was trialled and discontinued aged 16 years, as she became normoglycaemic. Hirsutism was treated with topical eflornithine, oral spironolactone and flutamide, and laser therapy. Unfortunately, diabetes reemerged in young adulthood with obesity. Case 2: during an emergency admission for acute abdominal pain aged 11 years, hyperglycaemia was noted which led to further investigation. An oral glucose tolerance test showed diabetes and ultrasound showed polycystic ovaries. Further investigations revealed raised adiponectin (18 mg/L) and compound heterozygous mutations in the INSR gene: p.Pro1263Ala and p.Ser748Leu (latter probable normal variant). She was treated with metformin and experienced postprandial hypoglycaemia. Symptoms of hyperandrogenism were controlled by flutamide. She maintained a healthy weight and reassessment at young adulthood showed resolution of diabetes. Type A IR may present in childhood with overlapping features of common endocrine entities such as premature adrenarche and polycystic ovarian syndrome. Patients with abnormal glucose tolerance yet normal weight merit screening with adiponectin; raised adiponectin levels prompt insulin receptor mutational analysis. Postprandial hypoglycaemia is characteristic. Management includes optimization of glycaemic control with oral hypoglycaemic agents and maintenance of healthy weight, and controlling the effects of hyperandrogenism., (© 2017 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2017
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29. Pamidronate "zebra lines": A treatment timeline.

Author

Loizidou A, Andronikou S, and Burren CP

Abstract

Osteogenesis imperfecta is a hereditary bone dysplasia characterized by bone fragility, deformity, and short stature. Treatment focuses on preventing bone fractures and symptom relief. Pamidronate, a second-generation bisphosphonate drug that minimizes bone loss, is the chosen treatment in osteogenesis imperfecta. Radiologically, each cycle of pamidronate treatment is depicted as a line of sclerosed nondecalcified cartilage at the metaphysis, termed a pamidronate line. In this case report, we demonstrate that a treatment timeline can be visualized on plain radiographs as the number and spacing of pamidronate lines reflects the number and timing of treatment cycles. The educational value of this is to reassure physicians of the benign nature of "zebra lines," to demonstrate that the pamidronate lines migrate and fade with bone growth, and alert physicians that the lack of expected pamidronate lines during treatment may reflect a change in the patient's condition that reduces the effectiveness of bisphosphonate infusions.

Published
2017
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30. Gonadotrophin abnormalities in an infant with Lowe syndrome.

Author

Warner BE, Inward CD, and Burren CP

Abstract

Summary: This case, presenting with bilateral impalpable testes, illustrates the relevance of a broad differential disorders of sex development case management. It provides new insights on hypothalamic-pituitary-gonadal (HPG) axis and testicular function abnormalities in the multisystem disorder of Lowe syndrome. Lowe syndrome, also known as oculocerebrorenal syndrome, is a rare disorder characterised by eye abnormalities, central nervous system involvement and proximal renal tubular acidosis. There are a handful of reports of pubertal delay, infertility and cryptorchidism in Lowe syndrome. Biochemistry aged 72 h: testosterone 6.4 nmol/L, LH <0.5 IU/L and FSH <0.5 IU/L. Gonadotropin-releasing hormone stimulation test identified significantly raised baseline LH = 45.4 IU/L (contrasts with earlier undetectable LH), with a 20% increase on stimulation, while baseline FSH = 4.3 IU/L with no increase on stimulation. Day 14 HCG stimulation test produced an acceptable 50% increase in testosterone. The constellation of further abnormalities suggested Lowe syndrome: hypotonia, bilateral cataracts (surgical extraction and intraocular lens implantation) and renal tubular acidosis (microscopic haematuria, hypercalciuria, proteinuria, generalised aminoaciduria, hypophosphataemia and metabolic acidosis). DNA sequencing identified de novo hemizygous frameshift mutation OCRL c.2409&#95;2410delCT in exon 22. Interpretation of initial and repeat GnRH and HCG testing indicates the likelihood of testicular failure. Partial testicular descent occurred but left orchidopexy was required. Improving long-term gonadal function in Lowe syndrome assumes increased importance for current cohorts as advances in renal replacement therapy have greatly improved life expectancy. Noting HPG axis abnormalities in Lowe syndrome in infancy can identify cases requiring increased surveillance of pubertal progress for earlier detection and management., Learning Points: Clinical endocrine problems in Lowe syndrome has been reported, but has focused on abnormalities in adolescence and young adulthood: pubertal delay and infertility.We present an infant with isolated LH elevation at baseline and on GnRH stimulation testing who also had bilateral impalpable testes.Early testing of the HPG axis in patients with Lowe syndrome may help predict gonadal abnormalities from a younger age, which will enhance the overall case management into adolescence.

Published
2017
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31. Hartsfield syndrome associated with a novel heterozygous missense mutation in FGFR1 and incorporating tumoral calcinosis.

Author

Prasad R, Brewer C, and Burren CP

Subjects
Humans, Infant, Newborn, Male, Cleft Lip genetics, Cleft Palate genetics, Fingers abnormalities, Hand Deformities, Congenital genetics, Heterozygote, Holoprosencephaly genetics, Intellectual Disability genetics, Mutation, Missense, Receptor, Fibroblast Growth Factor, Type 1 genetics
Published
2016
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32. Germline or somatic GPR101 duplication leads to X-linked acrogigantism: a clinico-pathological and genetic study.

Author

Iacovazzo D, Caswell R, Bunce B, Jose S, Yuan B, Hernández-Ramírez LC, Kapur S, Caimari F, Evanson J, Ferraù F, Dang MN, Gabrovska P, Larkin SJ, Ansorge O, Rodd C, Vance ML, Ramírez-Renteria C, Mercado M, Goldstone AP, Buchfelder M, Burren CP, Gurlek A, Dutta P, Choong CS, Cheetham T, Trivellin G, Stratakis CA, Lopes MB, Grossman AB, Trouillas J, Lupski JR, Ellard S, Sampson JR, Roncaroli F, and Korbonits M

Subjects
Acromegaly complications, Acromegaly genetics, Acromegaly pathology, Adenoma complications, Adenoma genetics, Adenoma pathology, Adolescent, Child, Child, Preschool, Female, Germ-Line Mutation, Gigantism complications, Gigantism pathology, Gigantism therapy, Humans, Infant, Intracellular Signaling Peptides and Proteins genetics, Male, Pituitary Neoplasms complications, Pituitary Neoplasms genetics, Pituitary Neoplasms pathology, Treatment Outcome, Young Adult, Gene Duplication, Gigantism genetics, Receptors, G-Protein-Coupled genetics
Abstract

Non-syndromic pituitary gigantism can result from AIP mutations or the recently identified Xq26.3 microduplication causing X-linked acrogigantism (XLAG). Within Xq26.3, GPR101 is believed to be the causative gene, and the c.924G > C (p.E308D) variant in this orphan G protein-coupled receptor has been suggested to play a role in the pathogenesis of acromegaly.We studied 153 patients (58 females and 95 males) with pituitary gigantism. AIP mutation-negative cases were screened for GPR101 duplication through copy number variation droplet digital PCR and high-density aCGH. The genetic, clinical and histopathological features of XLAG patients were studied in detail. 395 peripheral blood and 193 pituitary tumor DNA samples from acromegaly patients were tested for GPR101 variants.We identified 12 patients (10 females and 2 males; 7.8 %) with XLAG. In one subject, the duplicated region only contained GPR101, but not the other three genes in found to be duplicated in the previously reported patients, defining a new smallest region of overlap of duplications. While females presented with germline mutations, the two male patients harbored the mutation in a mosaic state. Nine patients had pituitary adenomas, while three had hyperplasia. The comparison of the features of XLAG, AIP-positive and GPR101&AIP-negative patients revealed significant differences in sex distribution, age at onset, height, prolactin co-secretion and histological features. The pathological features of XLAG-related adenomas were remarkably similar. These tumors had a sinusoidal and lobular architecture. Sparsely and densely granulated somatotrophs were admixed with lactotrophs; follicle-like structures and calcifications were commonly observed. Patients with sporadic of familial acromegaly did not have an increased prevalence of the c.924G > C (p.E308D) GPR101 variant compared to public databases.In conclusion, XLAG can result from germline or somatic duplication of GPR101. Duplication of GPR101 alone is sufficient for the development of XLAG, implicating it as the causative gene within the Xq26.3 region. The pathological features of XLAG-associated pituitary adenomas are typical and, together with the clinical phenotype, should prompt genetic testing.

Published
2016
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33. Attitudes to Exercise and Diabetes in Young People with Type 1 Diabetes Mellitus: A Qualitative Analysis.

Author

Ryninks K, Sutton E, Thomas E, Jago R, Shield JP, and Burren CP

Subjects
Adolescent, Child, Diabetes Mellitus, Type 1 psychology, Exercise Therapy, Female, Focus Groups, Humans, Life Style, Male, Qualitative Research, Surveys and Questionnaires, Attitude to Health, Diabetes Mellitus, Type 1 physiopathology, Exercise
Abstract

Aims: To investigate young people's attitudes to, and understanding of, physical activity on glycaemic control in Type 1 Diabetes Mellitus., Methods: Four focus groups with 11-14 and 15-16 year olds were conducted with twelve young people with Type 1 Diabetes, from within a larger study investigating physical activity and fitness. Qualitative analysis of the focus group data was performed using Interpretative Phenomenological Analysis., Results: Four superordinate themes were identified: Benefits of Exercise, Knowledge and Understanding, Information and Training and "You can do anything". Young people felt that exercising helped them to manage their diabetes and had a beneficial psychological and physical impact on their bodies. They reported a lack of knowledge and understanding about diabetes among school staff and other young people. The overwhelming sense from young people was that although diabetes impacts upon their lives, with preparation, physical activity can take place as normal., Conclusions: Whilst young people had an awareness of the physical and psychological benefits of exercise in managing their diabetes, they experienced difficulties at school. Professional support and discussions with young people, giving tailored strategies for managing Type 1 Diabetes during exercise are needed. Healthcare teams should ensure that the support and educational needs of school staff are met. Providing more opportunities to empower young people to take on the responsibility for their Type 1 Diabetes care is merited. Young people felt diabetes did not stop them from participating in activities; it is simply a part of them that needs managing throughout life.

Published
2015
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34. Risedronate in children with osteogenesis imperfecta: a randomised, double-blind, placebo-controlled trial.

Author

Bishop N, Adami S, Ahmed SF, Antón J, Arundel P, Burren CP, Devogelaer JP, Hangartner T, Hosszú E, Lane JM, Lorenc R, Mäkitie O, Munns CF, Paredes A, Pavlov H, Plotkin H, Raggio CL, Reyes ML, Schoenau E, Semler O, Sillence DO, and Steiner RD

Subjects
Administration, Oral, Adolescent, Alkaline Phosphatase metabolism, Analysis of Variance, Bone Density drug effects, Bone Density Conservation Agents adverse effects, Child, Child, Preschool, Collagen metabolism, Double-Blind Method, Drug Administration Schedule, Etidronic Acid administration & dosage, Etidronic Acid adverse effects, Female, Humans, Male, Osteogenesis Imperfecta physiopathology, Risedronic Acid, Treatment Outcome, Bone Density Conservation Agents administration & dosage, Etidronic Acid analogs & derivatives, Osteogenesis Imperfecta drug therapy
Abstract

Background: Children with osteogenesis imperfecta are often treated with intravenous bisphosphonates. We aimed to assess the safety and efficacy of risedronate, an orally administered third-generation bisphosphonate, in children with the disease., Methods: In this multicentre, randomised, parallel, double-blind, placebo-controlled trial, children aged 4-15 years with osteogenesis imperfecta and increased fracture risk were randomly assigned by telephone randomisation system in a 2:1 ratio to receive either daily risedronate (2·5 or 5 mg) or placebo for 1 year. Study treatment was masked from patients, investigators, and study centre personnel. Thereafter, all children received risedronate for 2 additional years in an open-label extension. The primary efficacy endpoint was percentage change in lumbar spine areal bone mineral density (BMD) at 1 year. The primary efficacy analysis was done by ANCOVA, with treatment, age group, and pooled centre as fixed effects, and baseline as covariate. Analyses were based on the intention-to-treat population, which included all patients who were randomly assigned and took at least one dose of assigned study treatment. The trial is registered with ClinicalTrials.gov, number NCT00106028., Findings: Of 147 patients, 97 were randomly assigned to the risedronate group and 50 to the placebo group. Three patients from the risedronate group and one from the placebo group did not receive study treatment, leaving 94 and 49 in the intention-to-treat population, respectively. The mean increase in lumbar spine areal BMD after 1 year was 16·3% in the risedronate group and 7·6% in the placebo group (difference 8·7%, 95% CI 5·7-11·7; p<0·0001). After 1 year, clinical fractures had occurred in 29 (31%) of 94 patients in the risedronate group and 24 (49%) of 49 patients in the placebo group (p=0·0446). During years 2 and 3 (open-label phase), clinical fractures were reported in 46 (53%) of 87 patients in the group that had received risedronate since the start of the study, and 32 (65%) of 49 patients in the group that had been given placebo during the first year. Adverse event profiles were otherwise similar between the two groups, including frequencies of reported upper-gastrointestinal and selected musculoskeletal adverse events., Interpretation: Oral risedronate increased areal BMD and reduced the risk of first and recurrent clinical fractures in children with osteogenesis imperfecta, and the drug was generally well tolerated. Risedronate should be regarded as a treatment option for children with osteogenesis imperfecta., Funding: Alliance for Better Bone Health (Warner Chilcott and Sanofi)., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published
2013
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35. Authors' reply to Nussey.

Author

Arundel P, Ahmed SF, Allgrove J, Bishop NJ, Burren CP, Jacobs B, Mughal MZ, Offiah AC, and Shaw NJ

Subjects
Humans, Vitamin D Deficiency
Published
2013
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36. British Paediatric and Adolescent Bone Group's position statement on vitamin D deficiency.

Author

Arundel P, Ahmed SF, Allgrove J, Bishop NJ, Burren CP, Jacobs B, Mughal MZ, Offiah AC, and Shaw NJ

Subjects
Adolescent, Child, Child, Preschool, Humans, Infant, Infant, Newborn, Biomarkers blood, Dietary Supplements, Vitamin D analogs & derivatives, Vitamin D blood, Vitamin D therapeutic use, Vitamins therapeutic use, Practice Guidelines as Topic, Vitamin D Deficiency blood, Vitamin D Deficiency diagnosis, Vitamin D Deficiency drug therapy
Published
2012
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37. How does physical activity and fitness influence glycaemic control in young people with Type 1 diabetes?

Author

Cuenca-García M, Jago R, Shield JP, and Burren CP

Subjects
Adolescent, Adolescent Behavior, Body Composition, Case-Control Studies, Child, Child Behavior, Cross-Sectional Studies, Diabetes Mellitus, Type 1 epidemiology, England epidemiology, Female, Humans, Insulin therapeutic use, Male, Puberty, Siblings, Blood Glucose metabolism, Diabetes Mellitus, Type 1 metabolism, Exercise, Glycated Hemoglobin metabolism, Insulin metabolism
Abstract

Aims: To assess physical activity and fitness levels of young people with Type 1 diabetes compared with siblings without diabetes, and to investigate the association between physical activity, physical fitness and glycaemic control (HbA(1c)) in those young people with diabetes., Methods: The study consisted of 97 young people aged 8 to 16 years (62% male) from a Paediatric Diabetes Service in South West England. Sixty participants (67% male) had Type 1 diabetes and 37 participants (54% male) were siblings without diabetes (control group). We measured weight, height and waist circumference, calculated BMI and waist-height ratio and recorded pubertal status, blood pressure and current insulin regimen information. We assessed physical activity by accelerometry, from which we calculated light and moderate-to-vigorous intensity activity. We measured physical fitness by multistage sub-maximal bicycle ergometer test. We obtained HbA(1c) by venipuncture., Results: There were no differences between the young people with diabetes and siblings without diabetes in body composition, blood pressure, physical activity and fitness. Moderate-to-vigorous physical activity was associated with better glycaemic control, accounting for 30-37% (R(2) = 0.295-0.374) of the variance for HbA(1c). Physical fitness was not associated with HbA(1c)., Conclusions: Moderate-to-vigorous physical activity was associated with better glycaemic control while fitness was not. Findings suggest that developing strategies to increased moderate-to-vigorous physical activity may prove an effective method of improving glycaemic control in young people with diabetes., (© 2012 The Authors. Diabetic Medicine © 2012 Diabetes UK.)

Published
2012
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38. Evaluation and management of bone health in children with epilepsy on long-term antiepileptic drugs: United Kingdom survey of paediatric neurologists.

Author

Fong CY, Mallick AA, Burren CP, and Patel JS

Subjects
Anticonvulsants administration & dosage, Bone Diseases diagnosis, Bone Diseases physiopathology, Bone and Bones diagnostic imaging, Bone and Bones pathology, Child, Health Care Surveys methods, Humans, Neurology standards, Pediatrics standards, Pilot Projects, Practice Patterns, Physicians' trends, Preventive Health Services methods, Preventive Health Services trends, Radiography, Surveys and Questionnaires standards, Treatment Outcome, United Kingdom epidemiology, Anticonvulsants adverse effects, Bone Diseases chemically induced, Bone and Bones drug effects, Epilepsy drug therapy, Neurology methods, Pediatrics methods
Abstract

Background and Objective: Current evidence indicates long-term use of antiepileptic drugs (AEDs) is associated with impaired childhood bone health. The objective of this study was to ascertain the current clinical practice of paediatric neurologists managing children with epilepsy on long-term (>2 years) AED therapy, particularly against the UK Medicines and Healthcare products Regulatory Agency (MHRA) current recommendation of vitamin D supplementation in patients on long-term AEDs at-risk of impaired bone health., Methods: An internet-based survey of UK paediatric neurologists who routinely see children with epilepsy (n = 95) covered clinicians' epilepsy case-load and reflection on their current clinical practice with estimation of the frequency with which they considered various bone health issues. Responses were graded as 'frequent'(≥50%), 'sometimes'(25%-50%) and 'infrequent'(<25%)., Results: Overall response rate was 72/95 (76%). 3% frequently recommend prophylactic calcium and vitamin D supplementation, 6% frequently perform bone screening investigations, 7% frequently give bone health advice and 10% frequently enquire about skeletal risk factors. Clinical practices were not associated with epilepsy caseload (p-values 0.44-1). 84% infrequently performed bone health screening investigations. 54% of respondents indicated that, if performed, 100% would undertake bone profile, 64% 25(OH) Vitamin D, 18% PTH, 49% dual energy X-ray absorptiometry (DEXA) scan and 13% bone X-ray., Conclusions: The majority of paediatric neurologists do not routinely consider bone health related issues in children on long-term AEDs. Greater emphasis should be placed on vitamin D supplementation in these children., (Copyright © 2011 European Paediatric Neurology Society. Published by Elsevier Ltd. All rights reserved.)

Published
2011
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40. The continuum of growth hormone-IGF-I axis defects causing short stature: diagnostic and therapeutic challenges.

Author

Savage MO, Burren CP, and Rosenfeld RG

Subjects
Adult, Algorithms, Diagnostic Techniques, Endocrine, Growth Disorders genetics, Humans, Signal Transduction genetics, Treatment Outcome, Body Height genetics, Growth Disorders diagnosis, Growth Disorders therapy, Human Growth Hormone genetics, Insulin-Like Growth Factor I genetics
Abstract

The growth hormone (GH)-IGF-I axis is essential for normal foetal and childhood growth. Defects at different sites in the axis frequently result in short stature which may compromise adult height. We describe a continuum of clinically relevant abnormalities from GH deficiency through to GH resistance and discuss the implementation and interpretation of investigations. We consider appropriate therapy for patients with abnormal auxology and subnormal adult height prognosis, highlighting new data to clarify therapeutic choices leading to optimal clinical outcome.

Published
2010
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41. Backache in a Duchenne boy.

Author

Kinali M, Robinson R, Manzur AY, Burren CP, and Robb SA

Subjects
Child, Humans, Male, Muscular Dystrophy, Duchenne pathology, Radiography, Scoliosis diagnostic imaging, Back Pain etiology, Muscular Dystrophy, Duchenne physiopathology
Published
2007
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42. Variable phenotypes associated with aromatase (CYP19) insufficiency in humans.

Author

Lin L, Ercan O, Raza J, Burren CP, Creighton SM, Auchus RJ, Dattani MT, and Achermann JC

Subjects
Adolescent, Amino Acid Sequence, Animals, Base Sequence, COS Cells, Chlorocebus aethiops, DNA Mutational Analysis, Female, Humans, Male, Models, Molecular, Molecular Sequence Data, Mutant Proteins genetics, Pedigree, Phenotype, Sequence Homology, Amino Acid, Transfection, Virilism genetics, Aromatase deficiency, Aromatase genetics
Abstract

Context: The P450 enzyme aromatase (CYP19) plays a crucial role in the endocrine and paracrine biosynthesis of estrogens from androgens in many diverse estrogen-responsive tissues. Complete aromatase deficiency has been reported in a small number of 46,XX girls with genital ambiguity and absent pubertal development, but it is unknown whether nonclassic phenotypes exist., Objective: The objective of this study was to determine whether variant forms of aromatase insufficiency can occur in humans., Patients and Methods: Four patients (46,XX) from three kindreds with variable degrees of androgenization and pubertal failure were studied using mutational analysis of CYP19 and assay of enzyme activity., Results: Aromatase insufficiency resulting in genital ambiguity at birth, but with variable breast development at puberty (B2-B4), occurred in 46,XX patients from two kindreds who harbored point mutations or single codon deletions (R435C, F234del). Absent puberty with minimal androgenization at birth was found in one girl with a deletion involving exon 5 of CYP19 (exon5del), which would be predicted to lead to an in-frame deletion of 59 amino acids from the enzyme. Functional studies revealed low residual aromatase activity in the cases in which breast development occurred., Conclusions: These studies demonstrate that aromatase mutations can produce variable or "nonclassic" phenotypes in humans. Low residual aromatase activity may be sufficient for breast and uterine development to occur at puberty, despite significant androgenization in utero. Such phenotypic variability may be influenced further by modifying factors such as nonclassic pathways of estrogen synthesis, variability in coregulators, or differences in androgen responsiveness.

Published
2007
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43. A family with autosomal dominant hypocalcaemia with hypercalciuria (ADHH): mutational analysis, phenotypic variability and treatment challenges.

Author

Burren CP, Curley A, Christie P, Rodda CP, and Thakker RV

Subjects
Adolescent, Adult, Child, DNA Mutational Analysis, Dimerization, Family Health, Female, Genetic Variation, Humans, Hypocalcemia therapy, Male, Middle Aged, Nephrocalcinosis genetics, Nephrocalcinosis prevention & control, Pedigree, Phenotype, Receptors, Calcium-Sensing chemistry, Receptors, Calcium-Sensing metabolism, Genes, Dominant, Hypocalcemia genetics, Mutation, Missense, Receptors, Calcium-Sensing genetics
Abstract

Autosomal dominant hypocalcaemia with hypercalciuria (ADHH) is an intriguing syndrome, in which activating mutations of the calcium sensing receptor (CaSR) have recently been recognised. We describe a kindred with seven affected individuals across three generations, including patients affected in the first decade of life. Age at diagnosis varied from birth to 50 years. Affected members had hypocalcaemia (1.53-1.85 mmol/l), hypercalciuria, low but detectable parathyroid hormone (PTH) and hypomagnesaemia. Four of seven affected individuals were symptomatic (seizures, abdominal pains and paraesthesias), unrelated to severity of hypocalcaemia. Additional complications include nephrocalcinosis (n = 3) and basal ganglia calcification, identified by CT scanning in all five individuals. Symptomatic individuals were treated with calcium and calcitriol to reduce the risk of hypocalcaemic seizures. DNA sequence analysis, identified a mutation in exon 3, codon 129 (TGC-->TAC) of the CaSR gene of seven affected family members, resulting in loss of a conserved cysteine residue, potentially disrupting CaSR receptor dimerisation. Thus, a novel mutation was identified in this family, who demonstrate variability of ADHH phenotype and also illustrate the complexities of clinical management. Optimal management of ADHH is difficult and we recommend judicious treatment to avoid an increased risk of nephrocalcinosis.

Published
2005
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45. Phenotypic variability in growth hormone insensitivity.

Author

Savage MO, Blair JC, Burren CP, Camacho-Hübner C, Woods KA, Metherell L, and Clark AJ

Subjects
Body Height, Carrier Proteins blood, Humans, Phenotype, Growth Disorders genetics, Growth Hormone pharmacology, Mutation, Receptors, Somatotropin genetics
Published
2002

46. IGF generation in short stature.

Author

Buckway CK, Selva KA, Burren CP, Pratt KL, Tjoeng E, Guevara-Aguirre J, and Rosenfeld RG

Subjects
Female, Growth Disorders diagnosis, Growth Hormone pharmacology, Humans, Male, Body Height, Growth Disorders metabolism, Insulin-Like Growth Factor Binding Protein 3 biosynthesis, Insulin-Like Growth Factor I biosynthesis
Published
2002

47. The IGF-I generation test revisited: a marker of GH sensitivity.

Author

Buckway CK, Guevara-Aguirre J, Pratt KL, Burren CP, and Rosenfeld RG

Subjects
Adolescent, Adult, Biomarkers, Body Height, Child, Ecuador, Female, Growth Disorders genetics, Heterozygote, Human Growth Hormone deficiency, Human Growth Hormone genetics, Humans, Male, Reference Values, Sex Characteristics, Human Growth Hormone physiology, Insulin-Like Growth Factor I analysis
Abstract

IGF-I generation tests were developed over 20 yr ago and are currently used in differentiating GH insensitivity (GHI) from other disorders characterized by low serum IGF-I. Nevertheless, generation tests have never been adequately characterized, and insufficient normative data are available. One hundred and ninety-eight subjects [including normal subjects; subjects with GHI, GH deficiency (GHD), and idiopathic short stature (ISS); and heterozygotes for the E180 splice GH receptor mutation] were randomized to self-administration of either a high (0.05 mg/kg x d) or a low (0.025 mg/kg x d) dose of GH for 7 d. After a 2-wk washout period, they received the alternate dose. Samples were collected on d 1, 5, and 8 of each treatment period. In normal individuals, IGF-I generation was GH dependent at all ages, and little advantage was observed in using the higher dose of GH or extending beyond the d 5 sample. Some GHD patients had IGF-I levels, both baseline and stimulated, that overlapped levels in the verified GHI patients. Subjects heterozygous for the E180 GH receptor splice mutation did not show a decreased responsiveness to GH. ISS patients had low-normal IGF-I levels that did not stimulate beyond the baseline normative ranges for age. These data provide the first large scale effort to provide preliminary normative IGF generation data and evaluate the GH sensitivity of patients with GHI, GHD, and ISS.

Published
2001
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48. Growth hormone insensitivity: pathophysiology, diagnosis, clinical variation and future perspectives.

Author

Savage MO, Burren CP, Blair JC, Woods KA, Metherell L, Clark AJ, and Camacho-Hübner C

Subjects
Body Height physiology, Drug Resistance, Genetic Variation, Growth Disorders etiology, Humans, Syndrome, Human Growth Hormone physiology
Abstract

The study of genetic growth hormone (GH) insensitivity is an evolving field. GH insensitivity syndrome (GHIS), otherwise known as Laron syndrome, is a heterogeneous disorder. Biochemical features consist of severe insulin-like growth factor I (IGF-I) and IGF-binding protein 3 (IGFBP-3) deficiency and elevated GH secretion. In a heterogeneous 'European' cohort of GHIS patients, features varied from classical to moderate abnormalities of phenotype and endocrine disturbance. A study of facial features within this series showed that a mild subgroup existed with normal facies, mild short stature and moderate biochemical abnormalities. Overlap with idiopathic short stature (ISS) exists, with heterozygous mutations of the GH receptor demonstrated to cause impaired growth. This 'partial' GHIS has not yet been defined endocrinologically. GH sensitivity, measured by IGF-I and IGFBP-3 responses in the IGF-I generation test, may reveal abnormalities in ISS, although it is likely that the dose of recombinant human GH and frequency of sampling in the test need to be modified., (Copyright 2001 S. Karger AG, Basel)

Published
2001
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49. Clinical and endocrine characteristics in atypical and classical growth hormone insensitivity syndrome.

Author

Burren CP, Woods KA, Rose SJ, Tauber M, Price DA, Heinrich U, Gilli G, Razzaghy-Azar M, Al-Ashwal A, Crock PA, Rochiccioli P, Yordam N, Ranke MB, Chatelain PG, Preece MA, Rosenfeld RG, and Savage MO

Subjects
Body Height, Child, Female, Growth Disorders genetics, Growth Disorders physiopathology, Human Growth Hormone blood, Humans, Insulin-Like Growth Factor Binding Protein 2 blood, Insulin-Like Growth Factor Binding Protein 3 blood, Insulin-Like Growth Factor Binding Protein 3 metabolism, Insulin-Like Growth Factor I metabolism, Male, Phenotype, Syndrome, Growth Disorders classification, Growth Disorders diagnosis, Human Growth Hormone metabolism
Abstract

Objective: Classical growth hormone insensitivity syndrome (GHIS) comprises a dysmorphic phenotype, extreme short stature (height SDS < 3), normal GH and low IGF-I and IGFBP-3. Wide clinical variation is recognised with classical and atypical forms. We aimed to delineate features of the milder "atypical" GHIS phenotype, and to determine whether this correlates with milder auxological and biochemical features., Methods: Fifty-nine patients from a European series of 82 patients with GHIS, with strict diagnostic criteria of GHIS, were studied and assigned to classical or atypical GHIS groups according to facial phenotype, i.e. "classical" required 2 of 3 recognized GHIS features (frontal bossing, mid-facial hypoplasia and depressed nasal bridge), "atypical" required 0 or 1 of these facial features. Classical and atypical GHIS groups were compared in terms of (1) phenotypic features, including high-pitched voice, sparse hair, blue sclera, hypoglycaemia, microphallus, (2) birth length, height SDS, and (3) basal IGF-I, IGF-II, IGFBP-1, IGFBP-3, GHBP and increase in IGF-I on IGF-I generation testing., Results: Fifty patients [24 males, 26 females, aged 8.6 +/- 4.6 years (mean +/- SD)] had "classical GHIS", 9 patients (7 males, 2 females, aged 7.8 +/- 4.1 years) had "atypical GHIS", 7 with normal facies. Atypical GHIS patients had lesser height deficit (Ht SDS -4.0 +/- 1.4) compared to classical GHIS (-6.7 +/- 1.4), less reduction in IGFBP-3 SDS (atypical -5.5 +/- 3.3; classical -8.6 +/- 2.4), and more had normal GHBP (>10% binding). Other variables were also less frequent in atypical GHIS patients: high-pitched voice 11% (70% classical), sparse hair 11% (42% classical), blue sclera 0% (38% classical), hypoglycaemia 11% (42% classical), and microphallus 14% (1 of 7 males), compared to 79% of classical (19 of 24 males)., Conclusions: Atypical GHIS patients, with relatively normal facial appearance, demonstrate less height defect and biochemical abnormalities compared to classical patients. GH insensitivity may be present in children with short stature and an otherwise normal appearance., (Copyright 2001 S. Karger AG, Basel)

Published
2001
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50. Binding properties and distribution of insulin-like growth factor binding protein-related protein 3 (IGFBP-rP3/NovH), an additional member of the IGFBP Superfamily.

Author

Burren CP, Wilson EM, Hwa V, Oh Y, and Rosenfeld RG

Subjects
Amino Acid Sequence genetics, Animals, Antibodies immunology, Cell Line, Connective Tissue Growth Factor, Epitopes, Female, Growth Substances, Humans, Immediate-Early Proteins, Insulin-Like Growth Factor Binding Protein 3 genetics, Insulin-Like Growth Factor Binding Protein 3 immunology, Molecular Sequence Data, Nephroblastoma Overexpressed Protein, Oligopeptides, Peptides, Pregnancy, RNA, Messenger metabolism, Rabbits, Recombinant Proteins, Sequence Tagged Sites, Tissue Distribution physiology, Insulin-Like Growth Factor Binding Protein 3 metabolism, Intercellular Signaling Peptides and Proteins
Abstract

The protein product of the novH oncogene, a member of the CCN family, is structurally related to the insulin-like growth factor (IGF) binding proteins (IGFBPs). We have characterized aspects of structure, function, and distribution of this protein, which, as IGFBP-related protein 3 (IGFBP-rP3), is a proposed member of the IGFBP Superfamily. Affinity cross-linking experiments performed with baculovirus synthesized recombinant human IGFBP-rP3 established that rhIGFBP-rP3 binds IGF-I, IGF-II, and insulin with low affinity. Specificity of binding was shown by competitive cross-linking experiments; binding to IGF-I and -II was also demonstrated by nondenaturing Western ligand blots. Northern blot analysis indicated the presence of IGFBP-rP3 messenger RNA (mRNA) in a broad range of human tissues. Western immunoblotting studies, using a polyclonal rabbit anti-rhIGFBP-rP3 antibody, demonstrated that IGFBP-rP3 protein is synthesized in vitro by several breast and prostate cancer cell lines: Hs578T, PC3, P69, and LNCaP cells. Western immunoblotting studies of human biological fluids identified that IGFBP-rP3 was present in normal serum, pregnancy serum, serum from patients with growth hormone receptor deficiency, cerebrospinal fluid, amniotic fluid, peritoneal fluid, and follicular fluid, while IGFBP-rP3 fragments were identified in cerebrospinal fluid, amniotic fluid, and prepubertal and pubertal urine samples. Our studies demonstrate that IGFBP-rP3 exhibits IGF binding, albeit at low affinity, and IGFBP-rP3 thus merits inclusion in the IGFBP Superfamily. The low affinity IGF binding suggests that IGFBP-rP3 may act primarily independently of the IGFs. The synthesis of IGFBP-rP3 by several malignant cell lines and its presence in human biological fluids suggest that this protein possesses other interesting roles, potentially in cell growth regulation.

Published
1999
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