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5. Audiological investigations in patients with late onset facioscapulohumeral muscular dystrophy (FSHD)

Author

Zhao F, Stephens D, Rogers MT, and Harper PS

Abstract

We have systematically tested the peripheral auditory system in 21 late-onset FSHD cases. The pure tone thresholds did not differ significantly at low and mid frequencies in either better ear or worse ear between FSHD subjects and controls. The patients with FSHD had significantly better hearing thresholds at 4 and 6 kHz than the normative data in the better and the worse ears. Transient evoked otoacoustic emissions (TEOAEs) were recorded as an objective and sensitive method for evaluating cochlear function. A significantly lower occurrence of TEOAEs was found in the FSHD patients with hearing thresholds better than 20 dB HL. Furthermore, this study provides evidence for the neuromuscular abnormalities of FSHD through its findings on the relaxation time of the acoustic stapedial reflex. A significantly longer relaxation time was found in patients with FSHD. No significant correlations were found between age and severity, or between duration and severity. Moreover, there were no significant correlations between hearing level and clinical severity in patients with FSHD. [ABSTRACT FROM AUTHOR]

Published
2004
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6. ABH secretor status of the fetus: a genetic marker identifiable by amniocentesis

Author

Harper Ps, W B Bias, J R Hutchinson, and Victor A. McKusick

Subjects
Amniotic fluid, ABO Blood-Group System, Antigen, Pregnancy, ABO blood group system, Genetics, medicine, Humans, Antigens, Saliva, Genetics (clinical), Fetus, medicine.diagnostic_test, business.industry, medicine.disease, Amniotic Fluid, Histocompatibility, Genetic marker, Immunology, Amniocentesis, Blood Group Antigens, Female, business, Research Article
Published
1971

8. Polycystic Kidney Disease Re-evaluated: A Population-based Study

Author

DAVIES, F, COLES, GA, HARPER, PS, WILLIAMS, AJ, EVANS, C, and COCHLIN, D

Abstract

A genetic register of all known cases of autosomal dominant polycystic kidney disease occurring in South and Mid-Wales has been established. In a population of 2.1 million, 209 families with affected members were identified, 303 of whom are currently alive, 70 on renal replacement therapy. An additional 551 cases would be predicted amongst family members at 50 per cent and 25 per cent risk, giving an apparent prevalence of 1:2459 in the general population. Five possible new mutations were seen where adults with phenotypic autosomal dominant polycystic kidney disease had both parents alive, age > 55 years with no cysts visible on ultrasound. The take-on rate for renal replacement therapy increased during 1970–79 but has apparently reached a plateau of 4.8 cases per million population per year over the last 8 years, despite a rapidly increasing acceptance of uraemic patients as a whole (72/106/year in 1988–89). Considerably more patients with autosomal dominant polycystic kidney disease aged over 50 years were started on treatment in 1980–89 than in 1970–79, but the survival overall improved with time. All cases of autosomal dominant polycystic kidney disease reaching end-stage renal disease are now being treated, but the apparent clinical prevalence of this condition in our region is less than half the supposed gene frequency, suggesting that undiagnosed cases have a benign prognosis.

Published
1991

9. Conversations with French medical geneticists. A personal perspective on the origins and early years of medical genetics in France.

Author

Harper PS

Subjects
Biomedical Research, France, History, 19th Century, History, 20th Century, History, 21st Century, Humans, Interviews as Topic, Medicine, Science, Education, Medical history, Education, Medical trends, Genetics, Medical education, Genetics, Medical history, Genetics, Medical legislation & jurisprudence, Genetics, Medical trends, Physicians, Research Personnel
Abstract

The history of the beginnings of medical genetics in France is discussed, based on the personal perspective provided by recorded interviews with 16 early French workers in the field. The weakness of French genetics overall up to the beginning of the Second World War meant that post-war medical genetics had to start from new, with its origins largely derived from the medical fields of child health and the prevention of genetic disorders, rather than from basic science. The key people responsible for initiating these developments were Robert Debré and Maurice Lamy at Hôpital Necker in Paris and those interviewed included a number of their colleagues and successors, including Jean Frézal, Pierre Maroteaux, Josué Feingold, André and Joelle Boué, and Jean-Claude Kaplan. A separate group of paediatricians, originally at Hôpital Trousseau under Raymond Turpin, including Jérôme Lejeune, Marthe Gautier and Roland Berger, was responsible for major advances in human cytogenetics. Outside Paris, workers were interviewed from Marseille, Strasbourg and Nancy, although not from Lyon, where Jacques-Michel Robert was an early pioneer, particularly of genetic counselling. Challenges in the development of medical genetics in France included the advent of prenatal diagnosis with its ethical issues, the emergence of medical genetics as a distinct specialty from paediatrics, and its spread from Paris across France. These and other aspects are described by those interviewed from their own experiences, given in Appendix S1, while the fully edited transcripts for most interviews are accessible on the Web: www.genmedhist.org/interviews., (© 2017 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2018
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12. Human genetics in troubled times and places.

Author

Harper PS

Subjects
Communism, Eugenics, Europe, Germany, History, 20th Century, Humans, National Socialism, Russia, Warfare, Genetics, Medical history
Abstract

The development of human genetics world-wide during the twentieth century, especially across Europe, has occurred against a background of repeated catastrophes, including two world wars and the ideological problems and repression posed by Nazism and Communism. The published scientific literature gives few hints of these problems and there is a danger that they will be forgotten. The First World War was largely indiscriminate in its carnage, but World War 2 and the preceding years of fascism were associated with widespread migration, especially of Jewish workers expelled from Germany, and of their children, a number of whom would become major contributors to the post-war generation of human and medical geneticists in Britain and America. In Germany itself, eminent geneticists were also involved in the abuses carried out in the name of 'eugenics' and 'race biology'. However, geneticists in America, Britain and the rest of Europe were largely responsible for the ideological foundations of these abuses. In the Soviet Union, geneticists and genetics itself became the object of persecution from the 1930s till as late as the mid 1960s, with an almost complete destruction of the field during this time; this extended also to Eastern Europe and China as part of the influence of Russian communism. Most recently, at the end of the twentieth century, China saw a renewal of government sponsored eugenics programmes, now mostly discarded. During the post-world war 2 decades, human genetics research benefited greatly from recognition of the genetic dangers posed by exposure to radiation, following the atomic bomb explosions in Japan, atmospheric testing and successive accidental nuclear disasters in Russia. Documenting and remembering these traumatic events, now largely forgotten among younger workers, is essential if we are to fully understand the history of human genetics and avoid the repetition of similar disasters in the future. The power of modern human genetic and genomic techniques now gives a greater potential for abuse as well as for beneficial use than has ever been seen in the past.

Published
2017
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13. The European Society of Human Genetics: beginnings, early history and development over its first 25 years.

Author

Harper PS

Abstract

The European Society of Human Genetics (ESHG) was founded on 15 March 1967, after preliminary discussions at the International Human Genetics Congress in Chicago the previous year and in Copenhagen in early 1967. Its initial meeting was held on 18-19 November 1967, also in Copenhagen, and annual meetings have been held from that time until the present, apart from years in which the International Congress of Human Genetics was also being held. The character of the Society during its early years was strongly influenced by its founding and permanent Secretary, Jan Mohr, head of the Copenhagen Institute of Medical Genetics, whose records are archived in the Tage Kemp/Jan Mohr Archive, now part of the Danish National Archives. These records show Jan Mohr's determination to keep the activities of the Society limited to the holding of an annual meeting to enhance contacts between European human geneticists, and to resist expansion to other activities. Pressures for a wider role of ESHG became irresistible in the late 1980s and a revised constitution, adopted in 1991, reshaped the Society into a more conventional and less restrictive structure. This has allowed it to play a wider and increasingly influential role in the development of human and medical genetics across Europe, with its own Journal, a range of committees covering different aspects of the field and a series of valuable reports on specific important topics, to be described in a forthcoming article on the Society's more recent history.European Journal of Human Genetics advance online publication, 10 May 2017; doi:10.1038/ejhg.2017.34.

Published
2017
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14. Some pioneers of European human genetics.

Author

Harper PS

Abstract

Some of the pioneers of human genetics across Europe are described, based on a series of 100 recorded interviews made by the author. These interviews, and the memories of earlier workers in the field recalled by interviewees, provide a vivid picture, albeit incomplete, of the early years of human and medical genetics. From small beginnings in the immediate post-World War 2 years, human genetics grew rapidly across many European countries, a powerful factor being the development of human cytogenetics, stimulated by concerns over the risks of radiation exposure. Medical applications soon followed, with the recognition of human chromosome abnormalities, the need for genetic counselling, the possibility of prenatal diagnosis and later, the applications of human molecular genetics. The evolution of the field has been strongly influenced by the characters and interests of the relatively small number of founding workers in different European countries, as well as by wider social, medical and scientific factors in the individual countries.European Journal of Human Genetics advance online publication, 10 May 2017; doi:10.1038/ejhg.2017.47.

Published
2017
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15. Recorded interviews with human and medical geneticists.

Author

Harper PS

Subjects
Databases, Genetic, History, 20th Century, History, 21st Century, Humans, Phylogeography, Genetics, Medical history, Interviews as Topic methods
Abstract

A series of 100 recorded interviews with human and medical geneticists has been carried out and some general results are reported here. Twenty countries across the world are represented, mostly European, with a particular emphasis on the United Kingdom. A priority was given to older workers, many of whom were key founders of human genetics in their own countries and areas of work, and over 20 of whom are now no longer living. The interviews also give valuable information on the previous generation of workers, as teachers and mentors of the interviewees, thus extending the coverage of human genetics back to the 1930s or even earlier. A number of prominent themes emerge from the interview series; notably the beginnings of human cytogenetics from the late 1950s, the development of medical genetics research and its clinical applications in the 1960s and 1970s, and more recently the beginnings and rapid growth of human molecular genetics. The interviews provide vivid personal portraits of those involved, and also show the effects of social and political issues, notably those arising from World War 2 and its aftermath, which affected not only the individuals involved but also broader developments in human genetics, such as research related to risks of irradiation. While this series has made a start in the oral history of this important field, extension and further development of the work is urgently needed to give a fuller picture of how human genetics has developed., Competing Interests: The author records no conflict of interest.

Published
2017
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16. Mary Lyon and the hypothesis of random X chromosome inactivation.

Author

Harper PS

Subjects
Animals, Female, History, 20th Century, Humans, Mice, X Chromosome Inactivation genetics, Biological Evolution, Developmental Biology history, Genetics history, Research history, X Chromosome Inactivation physiology
Abstract

The 50th anniversary of Mary Lyon's 1961 Nature paper, proposing random inactivation in early embryonic life of one of the two X chromosomes in the cells of mammalian females, provides an opportunity to remember and celebrate the work of those involved. While the hypothesis was initially put forward by Lyon based on findings in the mouse, it was founded on earlier studies, notably the work of Susumu Ohno; it was also suggested independently by Beutler and colleagues using experimental evidence from a human X-linked disorder, glucose-6-phosphate dehydrogenase deficiency, and has proved to be of as great importance for human and medical genetics as it has for general mammalian genetics. Alongside the hypothesis itself, previous cytological studies of mouse and human chromosomes, and the observations on X-linked mutants in both species deserve recognition for their essential role in underpinning the hypothesis of random X-inactivation, while subsequent research on the X-inactivation centre and the molecular mechanisms underlying the inactivation process represent some of the most outstanding contributions to human and wider mammalian genetics over the past 50 years.

Published
2011
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17. Paul Polani and the development of medical genetics.

Author

Harper PS

Subjects
History, 20th Century, History, 21st Century, Italy, London, Genetics, Medical history
Abstract

Paul Polani (1914-2006) was one of the key figures internationally in the beginnings and development of medical genetics. Best remembered scientifically for his highly original work on the basis of human sex chromosome disorders, notably Turner syndrome, he pioneered the application of basic biological research to clinical genetic problems. The unit that he founded in 1960, at Guys Hospital, London, provided an unparalleled model for combined research and service in medical genetics across a wide range of laboratory areas and helped to establish medical genetics as a specific discipline.

Published
2007
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18. The discovery of the human chromosome number in Lund, 1955-1956.

Author

Harper PS

Subjects
Chromosome Disorders diagnosis, Chromosome Disorders genetics, Cytogenetic Analysis methods, History, 20th Century, Humans, Karyotyping, Sweden, Chromosomes, Human genetics, Cytogenetic Analysis history, Genetics, Medical history
Abstract

The correct determination of the human diploid chromosome number as 46, by J-H Tjio and A Levan, at the University of Lund, Sweden, occurred 50 years ago, in December 1955; the finding was published in April 1956, ending a period of more than 30 years when the number had been thought to be 48. The background to the discovery and the surrounding factors are reassessed, as are the reasons why previous investigators persistently misidentified the precise number. The necessity for multiple technological advances, the power of previously accepted conclusions in influencing the interpretation of later results, and the importance of other work already undertaken in Lund, are all relevant factors for the occurrence of this discovery, the foundation for modern human cytogenetics, at this particular time and place.

Published
2006
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19. A case of multiple cutaneous schwannomas; schwannomatosis or neurofibromatosis type 2?

Author

Murray AJ, Hughes TA, Neal JW, Howard E, Evans DG, and Harper PS

Subjects
Diagnosis, Differential, Genes, Neurofibromatosis 2, Hand, Humans, Male, Middle Aged, Mosaicism, Neoplasms, Multiple Primary genetics, Neurilemmoma genetics, Neurofibromatosis 2 genetics, Point Mutation genetics, Skin Neoplasms genetics, Neoplasms, Multiple Primary diagnosis, Neurilemmoma diagnosis, Neurofibromatosis 2 diagnosis, Skin Neoplasms diagnosis
Abstract

A 54 year old man presented with numerous cutaneous schwannomas, cranial nerve lesions, and spinal cord lesions, but no evidence of vestibular nerve involvement. There was no family history of neurocutaneous lesions. To help discriminate between the various possible diagnoses in this patient, molecular analysis of two cutaneous schwannomas was undertaken. An identical point mutation in the NF2 gene in the two anatomically distinct tumours was found, confirming this as a case of NF2 mosaicism.

Published
2006
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20. William Bateson, human genetics and medicine.

Author

Harper PS

Subjects
Genetic Diseases, Inborn genetics, History, 19th Century, History, 20th Century, Metabolism, Inborn Errors genetics, Societies, United Kingdom, Genetics, Medical history
Abstract

The importance of human genetics in the work of William Bateson (1861-1926) and in his promotion of Mendelism in the decade following the 1900 rediscovery of Mendel's work is described. Bateson had close contacts with clinicians interested in inherited disorders, notably Archibald Garrod, to whom he suggested the recessive inheritance of alkaptonuria, and the ophthalmologist Edward Nettleship, and he lectured extensively to medical groups. Bateson's views on human inheritance were far sighted and cautious. Not only should he be regarded as one of the founders of human genetics, but human genetics itself should be seen as a key element of the foundations of mendelian inheritance, not simply a later development from knowledge gained by study of other species.

Published
2005
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21. Julia Bell and the Treasury of Human Inheritance.

Author

Harper PS

Subjects
History, 20th Century, London, Reference Books, Medical, Genetics, Medical history
Abstract

The Treasury of Human Inheritance represents the most extensive, and one of the earliest series of documentations and analyses of human genetic disorders. Published between 1909 and 1958, from The Galton Laboratory, London, most of the numerous sections were written by Julia Bell, who represents a key figure in the development of human and medical genetics. Her combination of mathematical training, genetic knowledge and clinical expertise yielded numerous important insights into human inheritance first appearing in the Treasury; it remains a valuable scientific as well as an historical record of the genetics of a range of important inherited disorders.

Published
2005
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23. Population based study of late onset cerebellar ataxia in south east Wales.

Author

Muzaimi MB, Thomas J, Palmer-Smith S, Rosser L, Harper PS, Wiles CM, Ravine D, and Robertson NP

Subjects
Adult, Age of Onset, Aged, Aged, 80 and over, Cerebellar Ataxia genetics, Epidemiologic Studies, Female, Geography, Humans, Male, Middle Aged, Needs Assessment, Phenotype, Prevalence, Wales epidemiology, Cerebellar Ataxia epidemiology, Cerebellar Ataxia pathology, Registries statistics & numerical data
Abstract

Objective: To determine the prevalence and causation of late onset cerebellar ataxia (LOCA) in south east Wales, United Kingdom., Methods: A population based study of LOCA was conducted in a defined geographical region with a total population of 742,400. Multiple sources of ascertainment were used to identify all cases prevalent on 1 January 2001. The inclusion criteria were: a predominantly progressive cerebellar ataxia with onset of symptoms at age > or = 18 years; and disease duration of > or = 1 year. Cases with known acquired ataxias, ataxic syndromes with associated prominent autonomic dysfunction and/or atypical parkinsonism suggestive of multiple system atrophy and disorders with ataxia as a minor feature were excluded., Results: We identified 76 index cases of LOCA, of whom 63 were sporadic, idiopathic LOCA (ILOCA) and 13 were familial LOCA, of whom six had either spinocerebellar ataxia type 6, Friedreich's ataxia or dominant episodic ataxia. The mean annual incidence rate for the period 1999-2001 was 0.3/100,000 population/year. The crude prevalence rates were 8.4 per 100,000 (95% CI 7.2 to 11.6) for ILOCA and 1.8 per 100,000 (95% CI 0.8 to 2.7) for inherited LOCA. Of the 54/63 (85.7%) patients with ILOCA who were assessed, mean (SD) age at onset of symptoms was 53.8 (14.1) years (range 19 to 78) with a male:female ratio of 2.1:1. The mean disease duration was 8.7 (6.3) years (range 1 to 31). The most frequent presenting complaint was disturbance in gait (90.7%). One-third had a relatively pure cerebellar syndrome (33.3%) and two-thirds (66.7%) had additional extracerebellar neurological features. The majority (92%) were ambulant but only 9.3% were independently self-caring., Conclusion: This population based study provides insight into LOCA within a defined region and will inform decisions about the rational use of healthcare resources for patients with LOCA.

Published
2004
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24. Genetic testing and Huntington's disease: issues of employment.

Author

Harper PS, Gevers S, de Wert G, Creighton S, Bombard Y, and Hayden MR

Subjects
Employment, Family Health, Humans, Huntington Disease diagnosis, Huntington Disease epidemiology, Genetic Counseling legislation & jurisprudence, Genetic Testing legislation & jurisprudence, Genetic Testing methods, Huntington Disease genetics, Molecular Diagnostic Techniques
Published
2004
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25. Familial motor neurone disease with dementia: phenotypic variation and cerebellar pathology.

Author

Polvikoski TM, Murray A, Harper PS, and Neal JW

Subjects
Adult, Basal Ganglia pathology, Brain Stem pathology, Dementia genetics, Female, Humans, Male, Middle Aged, Motor Neuron Disease genetics, Pedigree, Phenotype, Ubiquitin analysis, Cerebellum pathology, Cerebral Cortex pathology, Dementia etiology, Motor Neuron Disease complications, Motor Neuron Disease psychology
Abstract

Objectives: To characterise the neuropathological phenotypes of two affected individuals from a family with an unusual clinical phenotype resembling motor neurone disease and dementia., Methods: Histological sections of cerebral cortex, basal ganglia, brain stem, cerebellum, and spinal cord were stained with haematoxylin-eosin, luxol fast blue, silver stains, anti-tau, anti-ubiquitin, anti-alpha-synuclein, and anti-neurofilament., Results: Numerous ubiquitin positive, tau and alpha-synuclein negative intraneuronal inclusions were present in the cerebral cortex (particularly within the dentate gyrus), cerebellar cortex, brain stem, and spinal cord. The cerebellar ubiquitinated inclusions were located in the proximal dendrite of the Purkinje cells. Loss of Purkinje cells and occasional silver and neurofilament positive axonal swellings (torpedoes) were also seen within the cerebellar cortex. The main difference between the two cases was the severity of the spinal cord involvement: no significant pathology was present within one, but obvious motor neurone disease within the other., Conclusions: The clinical and neuropathological findings in this family are best described as an example of familial motor neurone disease with dementia. Intraneuronal ubiquitin inclusions together with agyrophilic, neurofilament positive torpedoes were present within the cerebellar cortex, both previously unrecognised findings in this group of diseases.

Published
2003
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26. Confirmation of the type 2 myotonic dystrophy (CCTG)n expansion mutation in patients with proximal myotonic myopathy/proximal myotonic dystrophy of different European origins: a single shared haplotype indicates an ancestral founder effect.

Author

Bachinski LL, Udd B, Meola G, Sansone V, Bassez G, Eymard B, Thornton CA, Moxley RT, Harper PS, Rogers MT, Jurkat-Rott K, Lehmann-Horn F, Wieser T, Gamez J, Navarro C, Bottani A, Kohler A, Shriver MD, Sallinen R, Wessman M, Zhang S, Wright FA, and Krahe R

Subjects
Base Sequence, Chromosome Mapping, Europe ethnology, Female, Haplotypes, Humans, In Situ Hybridization, Fluorescence, Male, Models, Genetic, Molecular Sequence Data, Myotonic Dystrophy classification, Pedigree, Polymerase Chain Reaction methods, United States, Chromosomes, Human, Pair 3, Founder Effect, Microsatellite Repeats genetics, Myotonic Dystrophy genetics, Polymorphism, Single Nucleotide
Abstract

Myotonic dystrophy (DM), the most common form of muscular dystrophy in adults, is a clinically and genetically heterogeneous neuromuscular disorder. DM is characterized by autosomal dominant inheritance, muscular dystrophy, myotonia, and multisystem involvement. Type 1 DM (DM1) is caused by a (CTG)(n) expansion in the 3' untranslated region of DMPK in 19q13.3. Multiple families, predominantly of German descent and with clinically variable presentation that included proximal myotonic myopathy (PROMM) and type 2 DM (DM2) but without the DM1 mutation, showed linkage to the 3q21 region and were recently shown to segregate a (CCTG)(n) expansion mutation in intron 1 of ZNF9. Here, we present linkage to 3q21 and mutational confirmation in 17 kindreds of European origin with PROMM and proximal myotonic dystrophy, from geographically distinct populations. All patients have the DM2 (CCTG)(n) expansion. To study the evolution of this mutation, we constructed a comprehensive physical map of the DM2 region around ZNF9. High-resolution haplotype analysis of disease chromosomes with five microsatellite and 22 single-nucleotide polymorphism markers around the DM2 mutation identified extensive linkage disequilibrium and a single shared haplotype of at least 132 kb among patients from the different populations. With the exception of the (CCTG)(n) expansion, the available markers indicate that the DM2 haplotype is identical to the most common haplotype in normal individuals. This situation is reminiscent of that seen in DM1. Taken together, these data suggest a single founding mutation in DM2 patients of European origin. We estimate the age of the founding haplotype and of the DM2 (CCTG) expansion mutation to be approximately 200-540 generations.

Published
2003
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27. Clinical and genetic heterogeneity in peroneal muscular atrophy associated with vocal cord weakness.

Author

McEntagart M, Dunstan M, Bell C, Boltshauser E, Donaghy M, Harper PS, Williams N, Teare MD, and Rahman N

Subjects
Charcot-Marie-Tooth Disease classification, Charcot-Marie-Tooth Disease diagnosis, Chromosome Mapping, Chromosomes, Human, Pair 2, DNA Mutational Analysis, Deafness classification, Deafness diagnosis, Deafness genetics, Female, Genetic Markers genetics, Genetic Testing, Humans, Lod Score, Male, Muscle Weakness classification, Muscle Weakness diagnosis, Pedigree, Vocal Cord Paralysis classification, Vocal Cord Paralysis diagnosis, Charcot-Marie-Tooth Disease genetics, Genetic Heterogeneity, Muscle Weakness genetics, Vocal Cord Paralysis genetics
Abstract

Background: The peroneal muscular atrophy syndrome is the most common inherited disorder of the peripheral nervous system and has extensive clinical and genetic heterogeneity. Cranial nerve involvement is rare, though there are distinct peroneal muscular atrophy syndromes in which vocal cord paralysis is a characteristic feature. Among these dHMN-VII and HMSN-IIC are clinically similar but are differentiated by sensory involvement in HMSN-IIC. The gene for dHMN-VII, designated DHMNVP, has been localised to chromosome 2q14, but the location of the gene for HMSN-IIC is currently unknown. It has been suggested that dHMN-VII and HMSN II-C are allelic disorders., Objective: To assess the contribution of the dHMN-VII predisposition gene to peroneal muscular atrophy syndromes associated with vocal cord weakness., Methods: Linkage analysis of microsatellite markers at chromosome 2q14 was undertaken on two families, one affected by HMSN-IIC and a second manifesting vocal cord paralysis and sensorineural deafness in addition to distal muscular atrophy., Results: Two-point LOD scores at chromosome 2q14 markers encompassing the DHMNVP gene were negative in both families., Conclusions: These results suggest that at least one further gene predisposing to distal muscular weakness in association with vocal cord paralysis is likely to exist, and that dHMN-VII and HMSN-IIC are unlikely to be allelic disorders. Analyses of further HMSN-IIC families are required to confirm this.

Published
2002
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29. Absence of hearing impairment in adult onset facioscapulohumeral muscular dystrophy.

Author

Rogers MT, Zhao F, Harper PS, and Stephens D

Subjects
Adolescent, Adult, Age of Onset, Analysis of Variance, Audiometry, Auditory Threshold, Female, Humans, Male, Middle Aged, Muscular Dystrophy, Facioscapulohumeral genetics, Prevalence, Severity of Illness Index, Hearing, Hearing Loss, Sensorineural epidemiology, Muscular Dystrophy, Facioscapulohumeral epidemiology
Abstract

Hearing impairment has long been associated with the rarer forms of severe childhood and infantile facioscapulohumeral muscular dystrophy. Recent studies have suggested a high prevalence in classic, adult or adolescent, onset cases as well. We undertook detailed pure tone audiometric examination of 21 adult onset facioscapulohumeral muscular dystrophy cases. Patient results were compared with normative data obtained from the (United Kingdom) National Study of Hearing (The prevalence and distribution of hearing impairment and reported hearing disability in the MRC Institute of Hearing Research's National Study of Hearing, Whurr, 1995). There was no significant difference in the prevalence of hearing impairment in facioscapulohumeral muscular dystrophy patients at any single or averaged frequency tested. In this group of patients, pure tone audiometric thresholds were consistently better in the facioscapulohumeral muscular dystrophy patients, although these reached statistical significance only at 4 and 6 kHz. Age of onset, disease duration, clinical severity, degree of facial weakness and double-digest fragment size made no significant difference to mean hearing thresholds. We conclude that hearing impairment is not more common in adult onset facioscapulohumeral muscular dystrophy, and according to this data, may even, be less prevalent than in the normal population.

Published
2002
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30. Three proteins, MBNL, MBLL and MBXL, co-localize in vivo with nuclear foci of expanded-repeat transcripts in DM1 and DM2 cells.

Author

Fardaei M, Rogers MT, Thorpe HM, Larkin K, Hamshere MG, Harper PS, and Brook JD

Subjects
Alternative Splicing, Amino Acid Sequence, Humans, Molecular Sequence Data, Nuclear Proteins metabolism, Phylogeny, RNA, Messenger metabolism, Sequence Alignment, Drosophila Proteins, Myotonic Dystrophy genetics, Nuclear Proteins genetics, Trinucleotide Repeat Expansion genetics, Zinc Fingers physiology
Abstract

Myotonic dystrophy is a complex neuromuscular disorder associated with DNA expansion mutations in two different genes. In DM1 a CTG repeat in the 3'-untranslated region of DMPK is expanded, whereas in DM2 an intronic CCTG expansion occurs in the gene ZNF9. Transcripts containing expanded repeats form foci in the nuclei of DM1 and DM2 cells. Recent work using antibodies has shown that proteins related to Drosophila muscleblind co-localize with repeat foci in DM1 and DM2 cells. We show that rather than there being a single human muscleblind gene producing multiple proteins through alternative splicing, there are in fact three different muscleblind genes, MBNL, MBLL and MBXL, which map to chromosomes 3, 13 and X, respectively, and which show extensive alternative splicing. Two of the genes, MBNL and MBLL, are expressed in many adult tissues whereas MBXL is expressed predominantly in the placenta. Green fluorescent protein-tagged versions of MBNL, MBLL and MBXL co-localize with nuclear foci in DM1 and DM2 cells, suggesting that all three proteins may play a role in DM pathophysiology.

Published
2002
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31. Presymptomatic testing in myotonic dystrophy: genetic counselling approaches.

Author

Fokstuen S, Myring J, Evans C, and Harper PS

Subjects
Adolescent, Adult, Child, Preschool, DNA Mutational Analysis methods, Female, Humans, Infant, Male, Myotonin-Protein Kinase, Phenotype, Pregnancy, Prenatal Diagnosis methods, Wales, Genetic Counseling methods, Genetic Testing, Mutation genetics, Myotonic Dystrophy diagnosis, Myotonic Dystrophy genetics, Protein Serine-Threonine Kinases genetics, Trinucleotide Repeat Expansion genetics
Published
2001
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32. Eight years' experience of direct molecular testing for myotonic dystrophy in Wales.

Author

Fokstuen S, Myring J, Meredith L, Ravine D, and Harper PS

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Alleles, DNA Mutational Analysis, Female, Genetics, Medical, Humans, Male, Middle Aged, Mutation genetics, Myotonin-Protein Kinase, Neurology, Pediatrics, Pedigree, Prenatal Diagnosis, Time Factors, Wales, Genetic Testing, Myotonic Dystrophy diagnosis, Myotonic Dystrophy genetics, Protein Serine-Threonine Kinases genetics, Trinucleotide Repeat Expansion genetics
Published
2001
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33. Mutational analysis in X-linked spondyloepiphyseal dysplasia tarda.

Author

Christie PT, Curley A, Nesbit MA, Chapman C, Genet S, Harper PS, Keeling SL, Wilkie AO, Winter RM, and Thakker RV

Subjects
Codon, Nonsense, Exons, Female, Frameshift Mutation, Gene Deletion, Genetic Linkage, Humans, Male, Mutation, Pedigree, Proteins genetics, DNA Mutational Analysis, Osteochondrodysplasias genetics, X Chromosome
Abstract

Spondyloepiphyseal dysplasia tarda (SEDT) is an X-linked recessive disorder characterized by short stature due to defective growth of the vertebral bodies. In addition, deformities of the femoral heads result in early onset secondary osteoarthritis of the hips. The disorder affects males only with heterozygous female carriers showing no consistent abnormalities. The gene causing SEDT, which is located on Xp22.12-p22.31, consists of 6 exons of which only exons 3, 4, 5, and 6 are translated to yield an 140 amino acid protein, referred to as SEDLIN. SEDLIN mutations have been observed in SEDT patients, and we have undertaken studies to characterize such mutations in four unrelated SEDT kindreds by DNA sequence analysis. We identified two nonsense and two intragenic deletional frameshift mutations. The nonsense mutations occurred in exons 4 (TGG-->TGA, Trp70Stop) and 6 (CGA-->TGA, Arg122Stop). Both of the intragenic deletions, which were approximately 750 bp and 1300-1445 bp in size, involved intron 5 and part of exon 6 and resulted in frameshifts that lead to premature termination (Stop) signals. Thus, all four mutations are predicted to result in truncated proteins. The results of our study expand the spectrum of SEDLIN mutations associated with SEDT, and this will help to elucidate further the role of this novel protein in the etiology of this form of osteochondrodysplasia.

Published
2001
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34. Localization of the gene for distal hereditary motor neuronopathy VII (dHMN-VII) to chromosome 2q14.

Author

McEntagart M, Norton N, Williams H, Teare MD, Dunstan M, Baker P, Houlden H, Reilly M, Wood N, Harper PS, Futreal PA, Williams N, and Rahman N

Subjects
Chromosome Mapping, Female, Founder Effect, Genes, Dominant genetics, Haplotypes genetics, Homeodomain Proteins genetics, Humans, Lod Score, Male, Microsatellite Repeats genetics, Muscular Atrophy, Spinal physiopathology, Pedigree, Peptides genetics, Vocal Cords metabolism, Vocal Cords physiopathology, Wales, Chromosomes, Human, Pair 2 genetics, Genetic Linkage genetics, Muscular Atrophy, Spinal genetics
Abstract

Distal hereditary motor neuronopathy type VII (dHMN-VII) is an autosomal dominant disorder characterized by distal muscular atrophy and vocal cord paralysis. We performed a genomewide linkage search in a large Welsh pedigree with dHMN-VII and established linkage to chromosome 2q14. Analyses of a second family with dHMN-VII confirmed the location of the gene and provided evidence for a founder mutation segregating in both pedigrees. The maximum three-point LOD score in the combined pedigree was 7.49 at D2S274. Expansion of a polyalanine tract in Engrailed-1, a transcription factor strongly expressed in the spinal cord, was excluded as the cause of dHMN-VII.

Published
2001
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35. Prenatal testing for Huntington's disease: experience within the UK 1994-1998.

Author

Simpson SA and Harper PS

Subjects
Attitude, DNA Mutational Analysis, Female, Genetic Predisposition to Disease genetics, Genetic Testing methods, Genetic Testing psychology, Humans, Huntington Disease epidemiology, Male, Pregnancy, Pregnancy Outcome, Prenatal Diagnosis methods, Prenatal Diagnosis psychology, United Kingdom epidemiology, Genetic Testing statistics & numerical data, Huntington Disease diagnosis, Huntington Disease genetics, Prenatal Diagnosis statistics & numerical data
Published
2001
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37. The frequency of inherited disorders database: prevalence of Huntington disease.

Author

Al-Jader LN, Harper PS, Krawczak M, and Palmer SR

Abstract

A database of the frequency of human inherited disorders is being established for use in a clinical context, in medical research, for epidemiological studies, and in the planning of genetic services. Each entry includes the disease name categorized by organ system, an Online Mendelian Inheritance in Man (OMIM) number, the mode of inheritance, the population origin, a prevalence and/or incidence rate and a literature reference. The Frequency of Inherited Disorders Database (FIDD) currently contains 1,580 entries relating to 280 different Mendelian disorders. FIDD will be prospectively maintained and can be accessed at http://www.uwcm.ac.uk/uwcm/mg/fidd/. A more refined and systematic literature search that will serve to expand the size, scope and scale of the database is currently in progress. The coverage of neurological and neuromuscular disorders is however considered to be nearly complete. In this first description of FIDD, Huntington disease was used to illustrate the structure and scope of the database as well as its potential scientific utility. A total of 100 published articles on the prevalence of Huntington disease were appraised. Prevalence and incidence rates varied between different ethnic groups and between different countries. Possible reasons for this variation are discussed.

Published
2001
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38. Variation in the vitreous phenotype of Stickler syndrome can be caused by different amino acid substitutions in the X position of the type II collagen Gly-X-Y triple helix.

Author

Richards AJ, Baguley DM, Yates JR, Lane C, Nicol M, Harper PS, Scott JD, and Snead MP

Subjects
Abnormalities, Multiple pathology, Abnormalities, Multiple physiopathology, Amino Acid Sequence, Base Sequence, Biopolymers metabolism, Child, Child, Preschool, Collagen chemistry, DNA Mutational Analysis, Deafness physiopathology, Female, Genetic Linkage genetics, Genotype, Glycine metabolism, Humans, Infant, Infant, Newborn, Male, Myopia pathology, Myopia physiopathology, Pedigree, Phenotype, Retinal Detachment pathology, Retinal Detachment physiopathology, Syndrome, Abnormalities, Multiple genetics, Amino Acid Substitution genetics, Collagen genetics, Deafness genetics, Genetic Variation genetics, Myopia genetics, Retinal Detachment genetics
Abstract

Stickler syndrome is a dominantly inherited disorder characterized by arthropathy, midline clefting, hearing loss, midfacial hypoplasia, myopia, and retinal detachment. These features are highly variable both between and within families. Mutations causing the disorder have been found in the COL2A1 and COL11A1 genes. Premature termination codons in COL2A1 that result in haploinsufficiency of type II collagen are a common finding. These produce a characteristic congenital "membranous" anomaly of the vitreous of all affected individuals. Experience has shown that vitreous slit-lamp biomicroscopy can distinguish between patients with COL2A1 mutations and those with dominant negative mutations in COL11A1, who produce a different "beaded" vitreous phenotype. Here we characterize novel dominant negative mutations in COL2A1 that result in Stickler syndrome. Both alter amino acids in the X position of the Gly-X-Y triple-helical region. A recurrent R365C mutation occurred in two unrelated sporadic cases and resulted in the membranous vitreous anomaly associated with haploinsufficiency. In a large family with linkage to COL2A1, with a LOD score of 2.8, a unique L467F mutation produced a novel "afibrillar" vitreous gel devoid of all normal lamella structure. These data extend the mutation spectrum of the COL2A1 gene and help explain the basis for the different vitreous phenotypes seen in Stickler syndrome.

Published
2000
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39. Ten years of presymptomatic testing for Huntington's disease: the experience of the UK Huntington's Disease Prediction Consortium.

Author

Harper PS, Lim C, and Craufurd D

Subjects
Female, Humans, Male, Predictive Value of Tests, United Kingdom, Genetic Testing, Huntington Disease diagnosis, Huntington Disease genetics
Abstract

Data on all presymptomatic genetic tests for Huntington's disease (HD) in the UK have been collected over the 10 year period since testing became available as a service. A total of 2937 completed tests have been performed up to the end of 1997, 2502 based on specific mutation testing, feasible since late 1993.A total of 93.1% of these were at 50% prior risk, with a significant excess of females (58.3%); 41.4% of results were abnormal or high risk, including 29.4% in subjects aged 60 or over. The trend in test numbers has currently levelled out at around 500 per year. Almost all presymptomatic tests are carried out in National Health Service genetics centres, with a defined genetic counselling protocol and with availability now in all regions of the UK. The introduction and establishment of HD presymptomatic testing shows that this form of predictive medicine for Mendelian disorders can be successfully incorporated into National Health Service structures. The comprehensive collection of simple data allows trends in demand and outcomes to be monitored and has also been the foundation for more detailed specific studies. A comparable approach to data collection in other genetic disorders will be important as presymptomatic testing becomes more generally feasible.

Published
2000
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40. Psychological Model for Presymptomatic Test Interviews: Lessons Learned from Huntington Disease.

Author

Soldan J, Street E, Gray J, Binedell J, and Harper PS

Abstract

This paper reflects on experience gained from presymptomatic testing for Huntington disease. An approach is presented which considers the role of the clinician and aims of the interview. Irrespective of the disease being tested for, it is suggested that the psychological aim of presymptomatic testing is to foster emotional insight and understanding that will help clients in their decision-making process about testing and their subsequent adjustment to the result. Based on these aims the process of presymptomatic testing, counseling is considered in terms of clarification, consideration, education, and reflection, followed by decision making. Practical approaches are discussed and illustrated with clinical examples.

Published
2000
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41. Aberrant interactions of transcriptional repressor proteins with the Huntington's disease gene product, huntingtin.

Author

Boutell JM, Thomas P, Neal JW, Weston VJ, Duce J, Harper PS, and Jones AL

Subjects
Acetyltransferases metabolism, Amino Acid Sequence, Animals, Brain metabolism, Escherichia coli metabolism, Histone Acetyltransferases, Histone Deacetylases, Humans, Huntingtin Protein, Huntington Disease genetics, Immunohistochemistry, Molecular Sequence Data, Nerve Tissue Proteins genetics, Nuclear Proteins genetics, Nuclear Receptor Co-Repressor 1, Rats, Recombinant Proteins metabolism, Sequence Alignment, Transcription Factors metabolism, Yeasts, Nerve Tissue Proteins metabolism, Nuclear Proteins metabolism, Repressor Proteins metabolism, Saccharomyces cerevisiae Proteins
Abstract

We detected an interaction of the N-terminus of huntingtin (htt171) with the C-terminal region of the nuclear receptor co-repressor (N-CoR) using the yeast two-hybrid system. This interaction was repeat length dependent and specific to htt171; the co-repressor did not interact with the repeat carrying a section of atrophin 1 nor with the androgen receptor or polyglutamine alone. The interaction was confirmed using His-tagged Escherichia coli -expressed C-terminal human and rat co-repressor protein which pulled full-length huntingtin out of homogenized rat brain and in pull-down assays. The N-CoR represses transcription from sequence-specific ligand-activated receptors such as the retinoid X-thyroid hormone receptor dimers and other nuclear receptors including Mad-Max receptor dimers. The mechanism of this repression appears to be through the formation of a complex of repressor proteins including the N-CoR, mSin3 and histone deacetylases. We have used N-CoR and mSin3A antibodies in immunohistochemical studies and find that in Huntington's disease (HD) cortex and caudate, the cellular localization of these proteins is exclusively cytoplasmic whilst in control brain they are localized in the nucleus as well as the cytoplasm; mSin3A immunoreactivity also occurred in a subset of huntingtin positive intranuclear inclusions. The relocalization of repressor proteins in HD brain may alter transcription and be involved in the pathology of the disease.

Published
1999
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43. Huntington's disease: a clinical, genetic and molecular model for polyglutamine repeat disorders.

Author

Harper PS

Subjects
Brain pathology, Chromosome Mapping, Chromosomes, Human, Pair 1, Eponyms, History, 19th Century, History, 20th Century, Humans, Huntingtin Protein, Huntington Disease pathology, Nerve Tissue Proteins genetics, Nuclear Proteins genetics, Repetitive Sequences, Amino Acid, Huntington Disease genetics, Huntington Disease history, Peptides genetics
Published
1999
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44. Localization of rabbit huntingtin using a new panel of monoclonal antibodies.

Author

Wilkinson FL, Nguyen TM, Manilal SB, Thomas P, Neal JW, Harper PS, Jones AL, and Morris GE

Subjects
Animals, Bacteriophages, Blotting, Western, Brain Chemistry genetics, Cross Reactions, Epitopes immunology, Gene Library, Huntingtin Protein, Huntington Disease genetics, Langerhans Cells chemistry, Mice, Mice, Inbred BALB C, Nerve Tissue Proteins genetics, Nuclear Proteins genetics, Pyramidal Cells chemistry, Rabbits, Recombinant Fusion Proteins immunology, Trinucleotide Repeats, Antibodies, Monoclonal pharmacology, Antibody Specificity, Huntington Disease diagnosis, Nerve Tissue Proteins analysis, Nerve Tissue Proteins immunology, Nuclear Proteins analysis, Nuclear Proteins immunology
Abstract

Huntington's disease (HD) is an autosomal dominant neurodegenerative disorder caused by the expansion of a CAG repeat which is expressed as a polyglutamine tract near the N-terminus of the gene product, huntingtin. N-terminal huntingtin fragments form intranuclear aggregates in HD patients and these may be involved in the pathogenesis. Monoclonal antibodies (mAbs) against three different regions of huntingtin (amino acids 997-1276, 1844-2131 and 2703-2911) have been produced and two of the epitopes have been identified using phage displayed peptide libraries. All mAbs reacted with 350 kDa huntingtin on Western blots and one mAb from each region was selected for further study by strong immunoreactivity with neurons in different regions of rabbit brain and by ability to immunoprecipitate native huntingtin. Subcellular fractionation and sucrose density centrifugation of rabbit brain extract showed that most of the huntingtin exists as a high molecular weight complex in the cytoplasm. Two outstanding problems have been addressed; the location of huntingtin in tissues outside the central nervous system and whether huntingtin is present in the nucleus of normal cells. We conclude that huntingtin is present at low levels in most non-neuronal cells though we have identified an interstitial cell type in skin with very high immunoreactivity. Using both immunolocalization and nuclear purification methods, we were unable to exclude the possibility that a small proportion of full-length huntingtin is present in the nucleus., (Copyright 1999 Elsevier Science B.V.)

Published
1999
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45. Daytime somnolence in myotonic dystrophy.

Author

Phillips MF, Steer HM, Soldan JR, Wiles CM, and Harper PS

Subjects
Adult, Deglutition, Depressive Disorder etiology, Disabled Persons, Female, Humans, Male, Middle Aged, Myotonic Dystrophy psychology, Consciousness, Myotonic Dystrophy complications, Quality of Life, Sleep Wake Disorders etiology
Abstract

Somnolence in myotonic dystrophy (DM) has not been measured using a reliable daytime somnolence scale. The aim of this study was to compare somnolence in DM patients with healthy controls and Charcot-Marie-Tooth disease (CMT) patients using such a scale and to compare this with potential contributory factors. We investigated 35 subjects with adult-onset DM, 16 healthy controls and 13 CMT controls. The Epworth Sleepiness Scale (ESS) was the principal measurement of daytime somnolence. Nocturnal sleep was assessed using a sleep diary. Other assessments measured daytime respiratory function, cognitive function, motor impairment, disability, swallowing capacity and depression. DM and CMT patients had greater daytime sleepiness than unaffected controls. In the DM group significant correlations were found between somnolence and measures of disability, sleep quality and some measures of depression. It was concluded that there is an abnormal level of daytime somnolence in DM, which is partially associated with disability.

Published
1999
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46. Age of onset in Huntington disease: sex specific influence of apolipoprotein E genotype and normal CAG repeat length.

Author

Kehoe P, Krawczak M, Harper PS, Owen MJ, and Jones AL

Subjects
Anticipation, Genetic, Female, Genetic Variation, Genotype, Humans, Male, Models, Statistical, Sex Factors, Survival, Age of Onset, Apolipoproteins E genetics, Huntington Disease genetics, Trinucleotide Repeats
Abstract

Age of onset (AO) of Huntington disease (HD) is known to be correlated with the length of an expanded CAG repeat in the HD gene. Apolipoprotein E (APOE) genotype, in turn, is known to influence AO in Alzheimer disease, rendering the APOE gene a likely candidate to affect AO in other neurological diseases too. We therefore determined APOE genotype and normal CAG repeat length in the HD gene for 138 HD patients who were previously analysed with respect to CAG repeat length. Genotyping for APOE was performed blind to clinical information. In addition to highlighting the effect of the normal repeat length upon AO in maternally inherited HD and in male patients, we show that the APOE epsilon2epsilon3 genotype is associated with significantly earlier AO in males than in females. Such a sex difference in AO was not apparent for any of the other APOE genotypes. Our findings suggest that subtle differences in the course of the neurodegeneration in HD may allow interacting genes to exert gender specific effects upon AO.

Published
1999

47. Predictive testing for Huntington's disease: II. Qualitative findings from a study of uptake in South Wales.

Author

Binedell J, Soldan JR, and Harper PS

Subjects
Adult, Communication, Decision Making, Female, Health Knowledge, Attitudes, Practice, Humans, Male, Predictive Value of Tests, Risk Factors, Wales, Huntington Disease psychology
Abstract

Semi-structured interviews were conducted with a cohort of 22 test applicants who requested Huntington's disease (HD) predictive testing in South Wales, and a random sample of 32 non-requesters, drawn from the South Wales HD register. Apart from identifying differences between the groups, the study afforded the opportunity to listen, at length, to at-risk individuals' accounts of living at risk and their thoughts about predictive testing and genetic services. Emergent themes included difficulties in family communication and the uncertainties inherent in being at risk and undergoing testing. Important factors in decision making about testing were: moral imperatives to clarify one's genetic status: views about the controllability of the future; family attitudes and norms; and the impact of a test result on family members. At-risk individuals' perceptions of the genetics service were that contact with the service would result in pressure to be tested and a need for test applicants to present a favourable view of coping capacities to secure testing. In addition, there was an expectation of ongoing contact with HD families at the initiative of the service providers. Implications of the findings for the way in which predictive testing services are structured and introduced to the at-risk population are discussed.

Published
1998
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48. Predictive testing for Huntington's disease: I. Predictors of uptake in South Wales.

Author

Binedell J, Soldan JR, and Harper PS

Subjects
Adult, Decision Making, Female, Health Knowledge, Attitudes, Practice, Humans, Huntington Disease therapy, Male, Predictive Value of Tests, Risk, Stress, Physiological therapy, Wales, Huntington Disease psychology
Abstract

In Wales, predictive testing for Huntington's disease (HD) has not been offered proactively to families and uptake of testing is low in comparison to other centres. Little is known of those not requesting testing, particularly those not in direct contact with the genetics service. This study examined differences between a cohort of 22 test applicants and a random group of 32 'non-requesters', drawn from the South Wales HD register. Respondents were interviewed by means of a semi-structured schedule in their own homes. The study groups differed significantly on a number of variables including: knowledge of the availability of testing; perceived attitudes of family members and significant others to testing; length of knowledge and perceived stressfulness of being at risk; and perceived ability to cope with an unfavourable result. Overall, knowledge of testing procedures was poor and at-risk individuals' understanding of genetic terminology was at odds with scientific distinctions. Discussion focuses on the organisational and psychological factors associated with lack of knowledge of the availability of testing and the interpretation of reported coping capacities.

Published
1998
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49. PROMM: the expanding phenotype. A family with proximal myopathy, myotonia and deafness.

Author

Phillips MF, Rogers MT, Barnetson R, Braun C, Harley HG, Myring J, Stevens D, Wiles CM, and Harper PS

Subjects
Adult, Aged, Audiometry, Cataract genetics, Cataract pathology, Deafness genetics, Deafness pathology, Electromyography, Family Health, Female, Genes, Dominant genetics, Humans, Male, Middle Aged, Muscular Diseases genetics, Muscular Diseases pathology, Myotonia pathology, Pedigree, Phenotype, Myotonia genetics
Abstract

We describe a family with a proximal myopathy, subclinical EMG myotonia, cataracts and deafness. Transmission through two generations and down the male line confirms autosomal dominant inheritance. There was no abnormal expansion of the CTG triplet repeat in the last exon of the dystrophia myotonica protein kinase (DMPK) gene associated with myotonic dystrophy. Heteroduplex analysis of all but the promoter region of the DMPK gene has excluded point mutations in this gene as an underlying cause for this myotonic disorder. The family was not sufficiently informative to exclude linkage to the sodium channel gene SCN4A or the chloride channel gene CLC1. This family clearly fulfils the recently established diagnostic criteria for PROMM (proximal myotonic myopathy) and in addition shows consistent severe deafness as a hitherto undescribed feature of PROMM. We discuss the diagnostic criteria of PROMM in relation to this family and other recent papers, all of which would now fulfil the aforementioned diagnostic criteria for PROMM.

Published
1998
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