Your search keyword '"Sebire N"' showing total 11 results

1. Evaluation of the feasibility, diagnostic yield, and clinical utility of rapid genome sequencing in infantile epilepsy (Gene-STEPS): an international, multicentre, pilot cohort study

Author

D'Gama, AM, Mulhern, S, Sheidley, BR, Boodhoo, F, Buts, S, Chandler, NJ, Cobb, J, Curtis, M, Higginbotham, E, Holland, J, Khan, T, Koh, J, Yliang, NS, Mcrae, L, Nesbitt, SE, Oby, BT, Paternoster, B, Patton, A, Rose, G, Scotchman, E, Valentine, R, Wiltrout, KN, Hayeems, RZ, Jain, P, Lunke, S, Marshall, CR, Rockowitz, S, Sebire, N, Stark, Z, White, SM, Chitty, LS, Cross, JH, Scheffer, IE, Chau, V, Costain, G, Poduri, A, Howell, KB, McTague, A, D'Gama, AM, Mulhern, S, Sheidley, BR, Boodhoo, F, Buts, S, Chandler, NJ, Cobb, J, Curtis, M, Higginbotham, E, Holland, J, Khan, T, Koh, J, Yliang, NS, Mcrae, L, Nesbitt, SE, Oby, BT, Paternoster, B, Patton, A, Rose, G, Scotchman, E, Valentine, R, Wiltrout, KN, Hayeems, RZ, Jain, P, Lunke, S, Marshall, CR, Rockowitz, S, Sebire, N, Stark, Z, White, SM, Chitty, LS, Cross, JH, Scheffer, IE, Chau, V, Costain, G, Poduri, A, Howell, KB, and McTague, A

Abstract

BACKGROUND: Most neonatal and infantile-onset epilepsies have presumed genetic aetiologies, and early genetic diagnoses have the potential to inform clinical management and improve outcomes. We therefore aimed to determine the feasibility, diagnostic yield, and clinical utility of rapid genome sequencing in this population. METHODS: We conducted an international, multicentre, cohort study (Gene-STEPS), which is a pilot study of the International Precision Child Health Partnership (IPCHiP). IPCHiP is a consortium of four paediatric centres with tertiary-level subspecialty services in Australia, Canada, the UK, and the USA. We recruited infants with new-onset epilepsy or complex febrile seizures from IPCHiP centres, who were younger than 12 months at seizure onset. We excluded infants with simple febrile seizures, acute provoked seizures, known acquired cause, or known genetic cause. Blood samples were collected from probands and available biological parents. Clinical data were collected from medical records, treating clinicians, and parents. Trio genome sequencing was done when both parents were available, and duo or singleton genome sequencing was done when one or neither parent was available. Site-specific protocols were used for DNA extraction and library preparation. Rapid genome sequencing and analysis was done at clinically accredited laboratories, and results were returned to families. We analysed summary statistics for cohort demographic and clinical characteristics and the timing, diagnostic yield, and clinical impact of rapid genome sequencing. FINDINGS: Between Sept 1, 2021, and Aug 31, 2022, we enrolled 100 infants with new-onset epilepsy, of whom 41 (41%) were girls and 59 (59%) were boys. Median age of seizure onset was 128 days (IQR 46-192). For 43 (43% [binomial distribution 95% CI 33-53]) of 100 infants, we identified genetic diagnoses, with a median time from seizure onset to rapid genome sequencing result of 37 days (IQR 25-59). Genetic diagnosis w

Published

2023

2. Lung metastases in low-risk gestational trophoblastic neoplasia: a retrospective cohort study

Author

Frijstein, M.M., Lok, C.A. (Christianne), Trommel, N.E. van, Kate-Booij, M.J. (Marianne) ten, Massuger, L.F. (Leon), Werkhoven, E.D. (E.) van, Short, D. (D.), Aguiar, X. (X.), Fisher, R.A. (R. A.), Kaur, B. (B.), Sarwar, N., Sebire, N. (Neil), Seckl, M.J., Frijstein, M.M., Lok, C.A. (Christianne), Trommel, N.E. van, Kate-Booij, M.J. (Marianne) ten, Massuger, L.F. (Leon), Werkhoven, E.D. (E.) van, Short, D. (D.), Aguiar, X. (X.), Fisher, R.A. (R. A.), Kaur, B. (B.), Sarwar, N., Sebire, N. (Neil), and Seckl, M.J.

Abstract

Objective: Presence of lung metastases in low-risk gestational trophoblastic neoplasia (GTN) is generally considered not to influence prognosis. However, in a recent study in the Netherlands, GTN patients with lung metastases had a higher recurrence rate and more disease-specific deaths compared with patients without metastases. The aim of the present study was to validate these findings in a different country. Design: Historical cohort study. Setting: Charing Cross Hospital, United Kingdom. Population: A total of 1040 low-risk GTN patients treated with methotrexate (MTX) between 2002 and 2016 were identified: 65 with lung metastases (group 1) and 975 without metastases (group 2). Methods: Baseline characteristics, MTX resistance, survival and recurrence rates were recorded and compared between both groups. Main outcome measures: MTX resistance, recurrence rate and survival. Results: The occurrence of MTX resistance and median number of MTX courses to achieve remission was significantly higher in patients with lung metastases than patients without metastases (60% versus 38.9%, P = 0.001; and nine versus six courses, P < 0.001). All choriocarcinoma patients (n = 4) with lung metastases developed MTX resistance. The recurrence rate was also higher in group I (9.2% versus 2.7%; P = 0.012). Disease-specific survival was 100% in both groups. Conclusions: The presence of lung metastases at the start of MTX therapy is associated with increased incidence of MTX resistance and recurrence in low-risk GTN without affecting overall survival, which remains 100%. However, individuals with low-risk choriocarcinoma with lung metastases are likely to become resistant to MTX and primary multi-agent chemotherapy should be considered. Tweetable abstract: The presence of lung metastases appears to increase the risk of recurrence in low-risk GTN, but does not affect overall cure rates and survival.

Published

2019

3. Dutch Risk Classification and FIGO 2000 for Gestational Trophoblastic Neoplasia Compared

Author

Eysbouts, Y.K., Massuger, L.F., Thomas, C., Ottevanger, P.B., Short, D., Harvey, R., Sebire, N., Kaur, B., Naveed, S., Sweep, C.G.J., Seckl, M., Eysbouts, Y.K., Massuger, L.F., Thomas, C., Ottevanger, P.B., Short, D., Harvey, R., Sebire, N., Kaur, B., Naveed, S., Sweep, C.G.J., and Seckl, M.

Abstract

Contains fulltext : 172368.pdf (publisher's version ) (Closed access), OBJECTIVE: Over the years, there has been a wide variety of classification systems in use worldwide to stratify patients between single-agent versus multi-agent chemotherapy, hindering comparison of international research results. The study presents a retrospective comparison of the International Federation of Gynecology and Obstetrics 2000 and Dutch risk classification system for gestational trophoblastic neoplasia. METHODS AND MATERIALS: All patients diagnosed with gestational trophoblastic neoplasia between January 2003 and December 2012 at the trophoblastic disease centre in London were retrospectively scored according to the Dutch classification system (N = 813). RESULTS: An extensive overlap between both scoring systems was seen, even though items and relative value of items were quite distinct. The Dutch system seems to be simpler and easier to apply in all situation; a degree of overtreatment can however be presumed with the use of either system. CONCLUSIONS: Although it is likely that outcome is indeed affected by the individual factors used in both systems, many factors relate to tumor bulk and may not be independently prognostic. We therefore believe that further refinement of the classification systems and their underlying prognostic items plus any new items that seem promising would be useful.

Published

2016

4. Pathogenetics of alveolar capillary dysplasia with misalignment of pulmonary veins

Author

Szafranski, P., Gambin, T., Dharmadhikari, A.V., Akdemir, K.C., Jhangiani, S.N., Schuette, J., Godiwala, N., Yatsenko, S.A., Sebastian, J., Madan-Khetarpal, S., Surti, U., Abellar, R.G., Bateman, D.A., Wilson, A.L., Markham, M.H., Slamon, J., Santos-Simarro, F., Palomares, M., Nevado, J., Lapunzina, P., Chung, B.H., Wong, W.L., Chu, Y.W., Mok, G.T., Kerem, E., Reiter, J., Ambalavanan, N., Anderson, S.A., Kelly, D.R., Shieh, J., Rosenthal, T.C., Scheible, K., Steiner, L., Iqbal, M.A., McKinnon, M.L., Hamilton, S.J., Schlade-Bartusiak, K., English, D., Hendson, G., Roeder, E.R., DeNapoli, T.S., Littlejohn, R.O., Wolff, D.J., Wagner, C.L., Yeung, A., Francis, D., Fiorino, E.K., Edelman, M., Fox, J., Hayes, D.A., Janssens, S., Baere, E. De, Menten, B., Loccufier, A., Vanwalleghem, L., Moerman, P., Sznajer, Y., Lay, A.S., Kussmann, J.L., Chawla, J., Payton, D.J., Phillips, G.E., Brosens, E., Tibboel, D., Klein, A., Maystadt, I., Fisher, R., Sebire, N., Male, A., Chopra, M., Pinner, J., Malcolm, G., Peters, G., Arbuckle, S., Lees, M., Mead, Z., Quarrell, O., Sayers, R., Owens, M., Shaw-Smith, C., Lioy, J., McKay, E., Leeuw, N. de, Feenstra, I., Spruijt, L., Elmslie, F., Thiruchelvam, T., Bacino, C.A., Langston, C., Lupski, J.R., Sen, P., Popek, E., Stankiewicz, P., Szafranski, P., Gambin, T., Dharmadhikari, A.V., Akdemir, K.C., Jhangiani, S.N., Schuette, J., Godiwala, N., Yatsenko, S.A., Sebastian, J., Madan-Khetarpal, S., Surti, U., Abellar, R.G., Bateman, D.A., Wilson, A.L., Markham, M.H., Slamon, J., Santos-Simarro, F., Palomares, M., Nevado, J., Lapunzina, P., Chung, B.H., Wong, W.L., Chu, Y.W., Mok, G.T., Kerem, E., Reiter, J., Ambalavanan, N., Anderson, S.A., Kelly, D.R., Shieh, J., Rosenthal, T.C., Scheible, K., Steiner, L., Iqbal, M.A., McKinnon, M.L., Hamilton, S.J., Schlade-Bartusiak, K., English, D., Hendson, G., Roeder, E.R., DeNapoli, T.S., Littlejohn, R.O., Wolff, D.J., Wagner, C.L., Yeung, A., Francis, D., Fiorino, E.K., Edelman, M., Fox, J., Hayes, D.A., Janssens, S., Baere, E. De, Menten, B., Loccufier, A., Vanwalleghem, L., Moerman, P., Sznajer, Y., Lay, A.S., Kussmann, J.L., Chawla, J., Payton, D.J., Phillips, G.E., Brosens, E., Tibboel, D., Klein, A., Maystadt, I., Fisher, R., Sebire, N., Male, A., Chopra, M., Pinner, J., Malcolm, G., Peters, G., Arbuckle, S., Lees, M., Mead, Z., Quarrell, O., Sayers, R., Owens, M., Shaw-Smith, C., Lioy, J., McKay, E., Leeuw, N. de, Feenstra, I., Spruijt, L., Elmslie, F., Thiruchelvam, T., Bacino, C.A., Langston, C., Lupski, J.R., Sen, P., Popek, E., and Stankiewicz, P.

Abstract

Contains fulltext : 168023.pdf (publisher's version ) (Closed access), Alveolar capillary dysplasia with misalignment of pulmonary veins (ACDMPV) is a lethal lung developmental disorder caused by heterozygous point mutations or genomic deletion copy-number variants (CNVs) of FOXF1 or its upstream enhancer involving fetal lung-expressed long noncoding RNA genes LINC01081 and LINC01082. Using custom-designed array comparative genomic hybridization, Sanger sequencing, whole exome sequencing (WES), and bioinformatic analyses, we studied 22 new unrelated families (20 postnatal and two prenatal) with clinically diagnosed ACDMPV. We describe novel deletion CNVs at the FOXF1 locus in 13 unrelated ACDMPV patients. Together with the previously reported cases, all 31 genomic deletions in 16q24.1, pathogenic for ACDMPV, for which parental origin was determined, arose de novo with 30 of them occurring on the maternally inherited chromosome 16, strongly implicating genomic imprinting of the FOXF1 locus in human lungs. Surprisingly, we have also identified four ACDMPV families with the pathogenic variants in the FOXF1 locus that arose on paternal chromosome 16. Interestingly, a combination of the severe cardiac defects, including hypoplastic left heart, and single umbilical artery were observed only in children with deletion CNVs involving FOXF1 and its upstream enhancer. Our data demonstrate that genomic imprinting at 16q24.1 plays an important role in variable ACDMPV manifestation likely through long-range regulation of FOXF1 expression, and may be also responsible for key phenotypic features of maternal uniparental disomy 16. Moreover, in one family, WES revealed a de novo missense variant in ESRP1, potentially implicating FGF signaling in the etiology of ACDMPV.

Published

2016

5. No evidence for mutations in NLRP7, NLRP2 or KHDC3L in women with unexplained recurrent pregnancy loss or infertility

Author

Aghajanova, Lusine, Mahadevan, S, Altmäe, Signe, Stavreus-Evers, Anneli, Regan, L, Sebire, N, Dixon, P, Fisher, R A, Van den Veyver, I B, Aghajanova, Lusine, Mahadevan, S, Altmäe, Signe, Stavreus-Evers, Anneli, Regan, L, Sebire, N, Dixon, P, Fisher, R A, and Van den Veyver, I B

Abstract

STUDY QUESTION: Are mutations in NLRP2/7 (NACHT, LRR and PYD domains-containing protein 2/7) or KHDC3L (KH Domain Containing 3 Like) associated with recurrent pregnancy loss (RPL) or infertility? SUMMARY ANSWER: We found no evidence for mutations in NLRP2/7 or KHDC3L in unexplained RPL or infertility. WHAT IS KNOWN ALREADY: Mutations in NLRP7 and KHDC3L are known to cause biparental hydatidiform moles (BiHMs), a rare form of pregnancy loss. NLRP2, while not associated with the BiHM pathology, is known to cause recurrent Beckwith Weidemann Syndrome (BWS). STUDY DESIGN, SIZE, AND DURATION: Ninety-four patients with well characterized, unexplained infertility were recruited over a 9-year period from three IVF clinics in Sweden. Blood samples from 24 patients with 3 or more consecutive miscarriages of unknown etiology were provided by the Recurrent Miscarriage Clinic at St Mary's Hospital, London, UK. PARTICIPANTS/MATERIALS, SETTING, METHODS: Patients were recruited into both cohorts following extensive clinical studies. Genomic DNA was isolated from peripheral blood and subject to Sanger sequencing of NLRP2, NLRP7 and KHDC3L. Sequence electropherograms were analyzed by Sequencher v5.0 software and variants compared with those observed in the 1000 Genomes, single nucleotide polymorphism database (dbSNP) and HapMap databases. Functional effects of non-synonymous variants were predicted using Polyphen-2 and sorting intolerant from tolerant (SIFT). MAIN RESULTS AND THE ROLE OF CHANCE: No disease-causing mutations were identified in NLRP2, NLRP7 and KHDC3L in our cohorts of unexplained infertility and RPL. LIMITATIONS, REASONS FOR CAUTION: Due to the limited patient size, it is difficult to conclude if the low frequency single nucleotide polymorphisms observed in the present study are causative of the phenotype. The design of the present study therefore is only capable of detecting highly penetrant mutations. WIDER IMPLICATIONS OF THE FINDINGS: The present study supports th

Published

2015

6. Small noncoding differentially methylated copy-number variants, including IncRNA genes, cause a lethal lung developmental disorder

Author

Szafranski, P. (Przemyslaw), Dharmadhikari, A.V. (Avinash), Brosens, E. (Erwin), Gurha, P. (Priyatansh), Kołodziejska, K.E. (Katarzyna), Zhishuo, O. (Ou), Dittwald, P. (Piotr), Majewski, J. (Jacek), Mohan, K.N. (K. Naga), Chen, B.P.C. (Benjamin), Person, A.D. (Anthony), Tibboel, D. (Dick), Klein, J.E.M.M. (Annelies) de, Pinner, J. (Jason), Chopra PhD, M. (Mickey), Malcolm, G. (Girvan), Peters, G., Arbuckle, S. (Susan), Guiang III, S.F. (Sixto), Hustead, V.A. (Virginia), Jessurun, J. (Jose), Hirsch, R. (Russel), Witte, D. (David), Maystadt, I. (Isabelle), Sebire, N. (Neil), Fisher, R. (Rachel), Langston, C. (Claire), Sen, P. (Partha), Stankiewicz, P. (Paweł), Szafranski, P. (Przemyslaw), Dharmadhikari, A.V. (Avinash), Brosens, E. (Erwin), Gurha, P. (Priyatansh), Kołodziejska, K.E. (Katarzyna), Zhishuo, O. (Ou), Dittwald, P. (Piotr), Majewski, J. (Jacek), Mohan, K.N. (K. Naga), Chen, B.P.C. (Benjamin), Person, A.D. (Anthony), Tibboel, D. (Dick), Klein, J.E.M.M. (Annelies) de, Pinner, J. (Jason), Chopra PhD, M. (Mickey), Malcolm, G. (Girvan), Peters, G., Arbuckle, S. (Susan), Guiang III, S.F. (Sixto), Hustead, V.A. (Virginia), Jessurun, J. (Jose), Hirsch, R. (Russel), Witte, D. (David), Maystadt, I. (Isabelle), Sebire, N. (Neil), Fisher, R. (Rachel), Langston, C. (Claire), Sen, P. (Partha), and Stankiewicz, P. (Paweł)

Abstract

An unanticipated and tremendous amount of the noncoding sequence of the human genome is transcribed. Long noncoding RNAs (IncRNAs) constitute a significant fraction of non-protein-coding transcripts; however, their functions remain enigmatic. We demonstrate that deletions of a small noncoding differentially methylated region at 16q24.1, including IncRNA genes, cause a lethal lung developmental disorder, alveolar capillary dysplasia with misalignment of pulmonary veins (ACD/MPV), with parent-of-origin effects. We identify overlapping deletions 250 kb upstream of FOXF1 in nine patients with ACD/MPV that arose de novo specifically on the maternally inherited chromosome and delete lung-specific IncRNAgenes. These deletions define a distant cis-regulatory region that harbors, besides lncRNAgenes, also a differentially methylated CpGisland, binds GLI2 depending on the methylation status of this CpG island, and physically interacts with and up-regulates the FOXF1 promoter. Wesuggest that lung-transcribed 16q24.1 IncRNAs may contribute to long-range regulation of FOXF1 by GLI2 and other transcription factors. Perturbation of IncRNA-mediated chromatin interactions may, in general, be responsible for position effect phenomena and potentially cause many disorders of human development.

Published

2013

7. Squamous cell carcinoma in a child with Clericuzio-type poikiloderma with neutropenia.

Author

Rodgers, W, Rodgers, W, Ancliff, P, Ponting, CP, Sanchez-Pulido, L, Burns, S, Hayman, M, Kimonis, V, Sebire, N, Bulstrode, N, Harper, JI, Rodgers, W, Rodgers, W, Ancliff, P, Ponting, CP, Sanchez-Pulido, L, Burns, S, Hayman, M, Kimonis, V, Sebire, N, Bulstrode, N, and Harper, JI

Published

2013

8. Development of the minimally invasive paediatric & perinatal autopsy

Author

Hutchinson, John Ciaran, Sebire, N., and Arthurs, O.

Subjects

618

Abstract

Introduction Perinatal autopsy contributes useful clinical information to patient management in approximately 40% of cases but remains poorly accepted due to parental concerns regarding disfigurement. Post-mortem imaging is an alternative, but 1.5 T MRI lacks resolution below 18 gestational weeks. Additionally, the Royal College of Pathologists autopsy guidelines recommend extensive tissue sampling as part of the investigation of fetal loss, which imaging alone cannot provide. Possible mitigating strategies include micro-CT for phenotyping small fetuses and laparoscopic techniques to obtain tissue samples. Interrogation of the evidence base for tissue sampling in different clinical scenarios is necessary to develop evidence-based practice and recommendations. Methods Minimally Invasive Autopsy with Laparoscopy (MinImAL) was performed in 103 cases. Micro-CT was optimised in extracted organs and the diagnostic accuracy evaluated in 20 fetuses. The Great Ormond Street Autopsy Database was retrospectively interrogated to investigate the yield of internal examination and visceral histology to the cause of death in 5,311 cases. Results MinImAL examination is reliable (97.8% successfully completed, 91/93) with good tissue sampling success rates (100% in lung, kidney, heart). Micro-CT offers an accurate method of scanning small fetuses (97.5% agreement with autopsy, 95% CI, 96.6-98.4) with fewer non-diagnostic indices than standard autopsy in < 14 weeks gestation (22/440 vs 48/348 respectively; p<0.001). Histology of macroscopically normal viscera is valuable in the investigation of infant and childhood deaths. However, it provides almost no useful information relevant to cause of death or main diagnosis (<1%) in fetal cases. Conclusions MinImAL examination offers a reliable method of internal examination and tissue sampling, which may be acceptable when standard autopsy is declined. Micro-CT provides an accurate, non-invasive method for phenotyping early gestation fetal anatomy. Histological sampling of macroscopically normal visceral organs is valuable when investigating infant or child deaths but of limited value in fetal loss and hence should not be routinely performed.

Published

2019

9. Autopsy investigation in stillbirth

Author

Man, J. A. and Sebire, N. J.

Subjects

618.92

Abstract

The UK has the highest rate of stillbirth in the developed world and there are more than three million stillbirths worldwide each year. With over 30 different classification systems, the rate of unexplained stillbirth varies from 15-60% despite postmortem investigation being undertaken in a number of cases. The primary aims of this project were to use a unique autopsy database to examine a large well characterised series of stillbirth autopsies to assess specific causes of death, relationships between fetal maceration, intrauterine and postmortem interval on cause of death and fetal intrauterine growth restriction as well as producing evidence based guidelines for autopsy practise and investigating the potential role of novel techniques in future stillbirth autopsy. The analysis of more than 1000 intrauterine and intrapartum fetal deaths revealed that two thirds had an unexplained cause of death. Internal examination of the fetuses provided a definitive cause of death in 1% of cases; 19% of the overall causes of death could have been diagnosed from review of the clinical circumstances and a further 18% by placental macroscopic and microscopic examination. Significant associations were found between increasing maceration and Small for Gestational Age (SGA) fetuses and that using birthweight or bodyweight alone erroneously overestimate the role of SGA as an underlying factor in stillbirth causation. Other investigations such as modified organ weight ratios may contribute to determining cause of death. Proteomic experiments proved that in principle significantly different amounts and types proteins could be successfully extracted from formalin fixed paraffin embedded stillbirth fetal tissue in different case groups, suggesting a possible future investigation into the causation of stillbirth.

Published

2016

10. Novel investigations in Sudden Unexpected Death in Infancy (SUDI)

Author

Pryce, J. W., Sebire, N. J., and Klein, N.

Subjects

618.92

Abstract

Unexplained Sudden Unexpected Death in Infancy (SUDI) is a diagnosis where a definitive cause of death cannot be ascertained. It remains the most common diagnosis in infant death at autopsy, despite the performance of a range of investigations including histology, microbiology and chemical pathology. Of all infant deaths with a demonstrable cause, infection is the most common finding. Recent research has shown that in some cases of unexplained SUDI, there is supportive evidence of an infectious process. Recent advances in diagnostic pathology include immunohistochemistry on formalin-fixed, paraffin-embedded (FFPE) tissue, proteomics and metabolomics. However, there are few techniques, which have transitioned from clinical practice into use during autopsy. Current techniques used at autopsy in cases of sudden infant death were assessed to see whether there was support for an infectious process. This included a retrospective analysis of all infant autopsies performed at a single centre over a fourteen-year period. Also, current consensus opinion was evaluated to determine areas of diagnostic difficulty. Cohort groups of infant deaths were selected for the application of novel immunohistochemical staining and proteomic analysis from FFPE tissues. The findings indicate that infection remains the commonest identifiable cause of death in SUDI, even over a 100 year time period, supported by recent demographic data. Unexplained SUDI cases were confirmed as having an increased incidence of positive blood cultures for infections of uncertain significance, including Staphylococcus aureus and Escherichia Coli. Evaluation of organ weights at autopsy demonstrated no significant associations, although the thymus was smaller in cases of infectious deaths. Blood/bile acylcarnitine levels showed differential expression in 3 different cohorts. Immunohistochemical staining revealed infectious deaths had a characteristic profile of expression including upregulated C Reactive Protein and ICAM-1. Protein expression was investigated with development of an applicable technique for usage in autopsy FFPE tissue. Subsequently, a pilot study of the utilisation of proteomics in the diagnosis of SUDI was performed with effective extraction of peptides and the identification of bacterial proteins in different cohorts. This thesis has demonstrated new techniques for the investigation of SUDI with establishment of supportive evidence for infectious deaths which are applicable for future use in autopsy cases.

Published

2013

11. Studies of congenital melanocytic naevi

Author

Kinsler, V. A., Moore, G. E., Sebire, N. J., and Healy, E.

Subjects

576.5

Abstract

Congenital melanocytic naevi (CMN) are pigmented birthmarks, known to be associated with an increased risk of neurological abnormalities and malignant melanoma. Current treatments for the cutaneous lesions and complications are limited for severely affected individuals, driving the research within this thesis into the aetiopathogenesis of this condition. The potential offered by studying rare diseases is also relevant to this project, particularly on the background of the rising incidence of melanoma in young people in the UK. The aims of this research were to expand the clinical description of the condition, to look for predisposing genetic alterations in the germline, to identify possible biomarkers for risk of complications and to investigate the lineage of naevus cells. To these ends we studied a large population of affected children to expand the phenotypic associations, investigating facial features, endocrinological status, pigmentary phenotype and growth, we undertook histopathological phenotyping of cutaneous and neurological lesions using immunohistochemistry and electron microscopy and employed array comparative genomic hybridisation and next generation sequencing for screening of germline haplotypes and mutations. Typical facial features were described in the majority of children with CMN, and the term CMN syndrome was proposed to encompass these. Post-natal growth was found to be rapid, leading to significantly increased BMI compared to the current UK population. Skewed anterior pituitary hormone measurements and increased parental thyroid abnormalities were suggestive of central hormonal dysfunction, however hormonal production from the cutaneous lesions could not be excluded. Histological phenotyping inferred that the primary abnormality underlying CMN may affect a population of stem cells, not necessarily destined to be melanocytes. An association between MC1R genotype and presence and severity of CMN was found using a candidate gene approach, and other germline candidates were identified. The results in this thesis have improved our understanding of the clinical and histological phenotype of CMN, and have identified genetic factors involved in the pathogenesis of the condition.

Published

2012