Your search keyword '"Helena Kemp"' showing total 6 results

1. Incidental Detection of Classical Galactosemia through Newborn Screening for Phenylketonuria: A 10-Year Retrospective Audit to Determine the Efficacy of This Approach

Author

Nathan W. P. Cantley, Robert Barski, Helena Kemp, Sarah L. Hogg, Hoi Yee Teresa Wu, Ann Bowron, Catherine Collingwood, Jennifer Cundick, Claire Hart, Lynette Shakespeare, Mary Anne Preece, Helen Aitkenhead, Sarah Smith, Rachel S. Carling, and Stuart J. Moat

Subjects

classical galactosaemia, newborn screening, phenylketonuria, phenylalanine, tyrosine, Pediatrics, RJ1-570

Abstract

In the UK, Classical Galactosaemia (CG) is identified incidentally from the Newborn Screening (NBS) for phenylketonuria (PKU) using an “Other disorder suspected” (ODS) pathway when phenylalanine (Phe) and tyrosine (Tyr) concentrations are increased. We aimed to determine the efficacy of CG detection via NBS and estimate the incidence of CG in live births in the UK. A survey was sent to all UK NBS laboratories to collate CG cases diagnosed in the UK from 2010 to 2020. Cases of CG diagnosed were determined if detected clinically, NBS, or by family screening, as well as age at diagnosis. Cases referred via the ODS pathway were also collated, including the final diagnosis made. Responses were obtained from 13/16 laboratories. Between 2010 and 2020, a total of 6,642,787 babies were screened, and 172 cases of CG were identified. It should be noted that 85/172 presented clinically, 52/172 were identified by NBS, and 17/172 came from family screening. A total of 117 referrals were made via the ODS pathway, and 45/117 were subsequently diagnosed with CG. Median (interquartile range) age at diagnosis by NBS and clinically was 8 days (7–11) and 10 days (7–16), respectively (Mann–Whitney U test, U = 836.5, p-value = 0.082). The incidence of CG is 1:38,621 live births. The incidence of CG in the UK is comparable with that of other European/western countries. No statistical difference was seen in the timing of diagnosis between NBS and clinical presentation based on the current practice of sampling on day 5. Bringing forward the day of NBS sampling to day 3 would increase the proportion diagnosed with CG by NBS from 52/172 (30.2%) to 66/172 (38.4%).

Published

2023

2. Treating the placenta to prevent adverse effects of gestational hypoxia on fetal brain development

Author

Tom J. Phillips, Hannah Scott, David A. Menassa, Ashleigh L. Bignell, Aman Sood, Jude S. Morton, Takami Akagi, Koki Azuma, Mark F. Rogers, Catherine E. Gilmore, Gareth J. Inman, Simon Grant, Yealin Chung, Mais M. Aljunaidy, Christy-Lynn Cooke, Bruno R. Steinkraus, Andrew Pocklington, Angela Logan, Gavin P. Collett, Helena Kemp, Peter A. Holmans, Michael P. Murphy, Tudor A. Fulga, Andrew M. Coney, Mitsuru Akashi, Sandra T. Davidge, and C. Patrick Case

Subjects

Medicine, Science

Abstract

Abstract Some neuropsychiatric disease, including schizophrenia, may originate during prenatal development, following periods of gestational hypoxia and placental oxidative stress. Here we investigated if gestational hypoxia promotes damaging secretions from the placenta that affect fetal development and whether a mitochondria-targeted antioxidant MitoQ might prevent this. Gestational hypoxia caused low birth-weight and changes in young adult offspring brain, mimicking those in human neuropsychiatric disease. Exposure of cultured neurons to fetal plasma or to secretions from the placenta or from model trophoblast barriers that had been exposed to altered oxygenation caused similar morphological changes. The secretions and plasma contained altered microRNAs whose targets were linked with changes in gene expression in the fetal brain and with human schizophrenia loci. Molecular and morphological changes in vivo and in vitro were prevented by a single dose of MitoQ bound to nanoparticles, which were shown to localise and prevent oxidative stress in the placenta but not in the fetus. We suggest the possibility of developing preventative treatments that target the placenta and not the fetus to reduce risk of psychiatric disease in later life.

Published

2017

3. Treating the placenta to prevent adverse effects of gestational hypoxia on fetal brain development

Author

Hannah Scott, Bruno R. Steinkraus, C. Patrick Case, Ashleigh L. Bignell, Jude S. Morton, Gareth J. Inman, Andrew M. Coney, Tudor A. Fulga, Peter Holmans, Andrew Pocklington, David A. Menassa, Michael P. Murphy, Mark F. Rogers, Helena Kemp, Gavin Collett, Simon Grant, Mais M. Aljunaidy, Yealin Chung, Takami Akagi, Sandra T. Davidge, Thomas J. Phillips, Catherine E. Gilmore, Mitsuru Akashi, Christy-Lynn M. Cooke, Koki Azuma, Angela Logan, Aman Sood, Scott, Hannah [0000-0002-2497-549X], Pocklington, Andrew [0000-0002-2137-0452], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Organogenesis, Placenta, Gene Expression, medicine.disease_cause, Antioxidants, Fetal Development, chemistry.chemical_compound, 0302 clinical medicine, Pregnancy, Hypoxia, Microscopy, Confocal, Multidisciplinary, Brain, 3. Good health, Experimental models of disease, medicine.anatomical_structure, embryonic structures, Medicine, Female, medicine.symptom, medicine.medical_specialty, Offspring, Science, Article, 03 medical and health sciences, Fetus, Internal medicine, medicine, Animals, MitoQ, Disease model, business.industry, Trophoblast, Hypoxia (medical), medicine.disease, R1, Rats, Pregnancy Complications, Oxidative Stress, 030104 developmental biology, Endocrinology, chemistry, Schizophrenia, Reactive Oxygen Species, business, Biomarkers, 030217 neurology & neurosurgery, Oxidative stress

Abstract

Some neuropsychiatric disease, including schizophrenia, may originate during prenatal development, following periods of gestational hypoxia and placental oxidative stress. Here we investigated if gestational hypoxia promotes damaging secretions from the placenta that affect fetal development and whether a mitochondria-targeted antioxidant MitoQ might prevent this. Gestational hypoxia caused low birth-weight and changes in young adult offspring brain, mimicking those in human neuropsychiatric disease. Exposure of cultured neurons to fetal plasma or to secretions from the placenta or from model trophoblast barriers that had been exposed to altered oxygenation caused similar morphological changes. The secretions and plasma contained altered microRNAs whose targets were linked with changes in gene expression in the fetal brain and with human schizophrenia loci. Molecular and morphological changes in vivo and in vitro were prevented by a single dose of MitoQ bound to nanoparticles, which were shown to localise and prevent oxidative stress in the placenta but not in the fetus. We suggest the possibility of developing preventative treatments that target the placenta and not the fetus to reduce risk of psychiatric disease in later life.

Published

2017

4. Bohring-Opitz (Oberklaid-Danks) syndrome: clinical study, review of the literature, and discussion of possible pathogenesis

Author

Sahar Mansour, Peter Lunt, Bregje W.M. van Bon, Kay Metcalfe, Hanne Hove, Catherine Murdoch-Davis, Gabriele Gillessen-Kaesbach, Marlène Rio, Sarah F. Smithson, Mary Ray, Ruth Newbury-Ecob, Helena Kemp, Helen Kingston, John Tolmie, Jan-Maarten Cobben, Dagmar Wieczorek, Peter D. Turnpenny, Judith A. Goodship, Rob Hastings, Ruth McGowan, Susanne Kjaergaard, Department of Clinical Genetics, Leicester Royal Infirmary, and University Hospitals Leicester-University Hospitals Leicester

Subjects

Male, Medizin, Trigonocephaly, Biology, Bioinformatics, Article, Pathogenesis, Craniosynostoses, 03 medical and health sciences, Intellectual Disability, Bohring-Opitz, Intellectual disability, Genetics, medicine, Humans, Genetics (clinical), 030304 developmental biology, Comparative Genomic Hybridization, 0303 health sciences, trigonocephaly, Oberklaid-Danks, 030305 genetics & heredity, Infant, medicine.disease, 3. Good health, Natural history, Cholesterol, Child, Preschool, Etiology, Female, Bohring–Opitz syndrome, Congenital disorder, Comparative genomic hybridization

Abstract

International audience; Bohring-Opitz syndrome (BOS) is a rare congenital disorder of unknown etiology diagnosed on the basis of distinctive clinical features. We suggest diagnostic criteria for this condition, describe ten previously unreported patients and update the natural history of four previously reported patients. This is the largest series reported to date, providing a unique opportunity to document the key clinical features and course through childhood. Investigations undertaken to try and elucidate the underlying pathogenesis of BOS using array comparative genomic hybridization and tandem mass spectrometry of cholesterol precursors did not demonstrate any pathogenic changes responsible.

Published

2011

5. Bloodspot assay using HPLC-tandem mass spectrometry for detection of Barth syndrome

Author

Frédéric M. Vaz, Henk van Lenthe, Janet E. Stone, Femke S. Stet, Colin G. Steward, Willem Kulik, Ronald J.A. Wanders, Helena Kemp, Riekelt H. Houtkooper, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Adolescent, Cardiolipins, Clinical Biochemistry, Tafazzin, Tandem mass spectrometry, High-performance liquid chromatography, Sensitivity and Specificity, chemistry.chemical_compound, Tandem Mass Spectrometry, Cardiolipin, medicine, Screening method, Humans, Child, Chromatography, High Pressure Liquid, Blood Specimen Collection, Chromatography, biology, Monolysocardiolipin, Biochemistry (medical), Selected reaction monitoring, Infant, Newborn, Infant, Barth syndrome, Genetic Diseases, X-Linked, Syndrome, medicine.disease, chemistry, Child, Preschool, biology.protein, Lysophospholipids

Abstract

Background: Barth syndrome (BTHS) is a serious X-linked, metabolic, multisystem disorder characterized by cardiomyopathy, neutropenia, myopathy, and growth delay. Because early diagnosis and appropriate treatment are of key importance for the survival of affected boys, we developed a biochemical BTHS screening method based on analysis of the monolysocardiolipin:cardiolipin ratio in bloodspots. Methods: We performed chloroform/methanol extraction on quarter-inch punches of dried bloodspots on Guthrie cards from BTHS patients and controls. Extracts were dried (60 °C, N2) and reconstituted in CHCl3/methanol/H2O [50:45:5 vol/vol/vol, 0.1% NH3 (25%)]. HPLC–tandem mass spectrometry analysis was performed with a normal-phase HPLC column and multiple reaction monitoring transitions for monolysocardiolipin (MLCL) and cardiolipin (CL) with a total run time of 10 min. The ratio of MLCL and CL was used as screening parameter. Results: All BTHS patients (n = 31) had monolysocardiolipin:cardiolipin ratios >0.40 and all controls (n = 215) had monolysocardiolipin:cardiolipin ratios 1 year without affecting the test outcome. Three neonatal Guthrie cards of BTHS patients taken 3.6 to 5.8 years previously were correctly identified as positive for BTHS. Conclusions: HPLC–tandem mass spectrometry analysis of dried bloodspots is an unambiguous screening test for BTHS with potential for rapid screening of neonates suspected of having BTHS, making remote and retrospective diagnosis accessible for a disease that is almost certainly underdiagnosed.

Published

2008

6. Isolation of human genomic DNA for genetic analysis from premature neonates: a comparison between newborn dried blood spots, whole blood and umbilical cord tissue

Author

Shavanthi Rajatileka, Karen Luyt, Manal El-Bokle, Anikó Váradi, Elek Molnár, Helena Kemp, and Maggie Williams

Subjects

Time Factors, Genotype, Genomic DNA, Gestational Age, Biology, Sample storage, Umbilical cord, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Umbilical Cord, Premature newborns, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, medicine, Genetics, Humans, Genetics(clinical), 030212 general & internal medicine, Genetic Testing, Genotyping, Genetics (clinical), Alleles, 030304 developmental biology, Whole blood, Dried Blood Spot Testing, 0303 health sciences, Genome, Human, Methodology Article, Infant, Newborn, Pyrosequencing, DNA, Sequence Analysis, DNA, Molecular biology, Newborn dried blood spots, 3. Good health, Dried blood spot, Single nucleotide polymorphism, genomic DNA, medicine.anatomical_structure, Genetic Techniques, Premature Birth, Sample collection, Blood sampling

Abstract

Background Genotyping requires biological sample collection that must be reliable, convenient and acceptable for patients and clinicians. Finding the most optimal procedure of sample collection for premature neonates who have a very limited blood volume is a particular challenge. The aim of the current study was to evaluate the use of umbilical cord (UC) tissue and newborn dried blood spot (DBS)-extracted genomic DNA (gDNA) as an alternative to venous blood-derived gDNA from premature neonates for molecular genetic analysis. All samples were obtained from premature newborn infants between 24-32 weeks of gestation. Paired blood and UC samples were collected from 31 study participants. gDNA was extracted from ethylenediaminetetraacetic acid (EDTA) anticoagulant-treated blood samples (~500 μl) and newborn DBSs (n = 723) using QIAamp DNA Micro kit (Qiagen Ltd., Crawley, UK); and from UC using Qiagen DNAeasy Blood and Tissue kit (Qiagen Ltd., Crawley, UK). gDNA was quantified and purity confirmed by measuring the A260:A280 ratio. PCR amplification and pyrosequencing was carried out to determine suitability of the gDNA for molecular genetic analysis. Minor allele frequency of two unrelated single nucleotide polymorphisms (SNPs) was calculated using the entire cohort. Results Both whole blood samples and UC tissue provided good quality and yield of gDNA, which was considerably less from newborn DBS. The gDNA purity was also reduced after 3 years of storage of the newborn DBS. PCR amplification of three unrelated genes resulted in clear products in all whole blood and UC samples and 86%-100% of newborn DBS. Genotyping using pyrosequencing showed 100% concordance in the paired UC and whole blood samples. Minor allele frequencies of the two SNPs indicated that no maternal gDNA contamination occurred in the genotyping of the UC samples. Conclusions gDNAs from all three sources are suitable for standard PCR and pyrosequencing assays. Given that UC provide good quality and quantity gDNA with 100% concordance in the genetic analysis with whole blood, it can replace blood sampling from premature infants. This is likely to reduce the stress and potential side effects associated with invasive sample collection and thus, greatly facilitate participant recruitment for genetic studies.