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1	Psychopathology in Wilson's disease. Portala, Kamilla 1961- January 1900 (has links) Diss. (sammanfattning) Uppsala : Univ., 2001. / Härtill 5 uppsatser.
2	Molecular basis of Wilson's disease in Hong Kong Chinese. / CUHK electronic theses & dissertations collection January 2008 (has links) Mak, Miu. / "April 2008." / Thesis (Ph.D.)--Chinese University of Hong Kong, 2008. / Includes bibliographical references (p. 207-230). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Abstracts in English and Chinese. Hepatolenticular Degeneration Hepatolenticular Degeneration--Hong Kong
3	Avaliação do olfato em pacientes com doença de Wilson / Smell analysis in patients with Wilson\'s disease Carvalho, Margarete de Jesus 21 January 2016 (has links) A Doença de Wilson (DW) é uma moléstia hereditária, caracterizada pela deficiência de excreção do cobre pelo fígado devido à mutação do gene A TP7B. O distúrbio do olfato ocorre com frequência em doenças neurodegenerativas como na doença de Parkinson (DP) e na doença de Alzheimer (DA). A análise do olfato tem sido utilizada como um instrumento útil no diagnóstico diferencial das diversas formas de parkinsonismo degenerativo, e, especialmente, na diferenciação entre DP e tremor essencial. O diagnóstico precoce na DW é a chave para o sucesso do tratamento. Na hipótese de haver comprometimento do olfato em fases iniciais da doença, esse poderia ser um dado a mais para auxiliar no diagnóstico. Até o presente, há apenas um estudo relacionando a DW com a disfunção do olfato. O objetivo deste estudo foi avaliar o olfato em um grupo de pacientes com DW e confrontar com grupo- controle. No presente estudo, foram analisados 37 portadores de DW com manifestação neurológica, 24 portadores de DW sem manifestação neurológica e 59 controles. Todos os indivíduos foram analisados com relação à idade, ao gênero, ao grau de escolaridade, ao uso de tabaco e ao miniexame do estado mental (MEEM), e os portadores de DW foram avaliados quanto ao tempo de doença, tratamento medicamentoso e escore neurológico. O olfato foi avaliado por meio do teste de identificação de odor 8niffin\' 8ticks (88-16 canetas numeradas e quatro opções de resposta para cada uma). Vinte e quatro indivíduos eram pacientes da DW sem manifestação neurológica (45,83% do gênero feminino) e 37 pacientes apresentavam manifestações neurológicas (56,76% do gênero masculino). O qrupo-controle foi composto por 59 indivíduos, 35 (59,33%) do gênero masculino. As médias de- idade foram de 33,38 ± 9,79 anos no grupo de portadores de DW com manifestação neurológica; 29 ± 9,61 anos no grupo de portadores de DW sem manifestação neurológica e 33,81 ± 10,67 anos no grupo-controle. Todos os pacientes com DW estavam em tratamento: 47(77%) com penicilamina, 7 (11,5%) com trientine e 7 (11,5%) com sais de zinco. As médias de respostas corretas no teste de identificação do odor 88-16 foram: 12,03 ± 2, 21 no grupo de portadores de DW com manifestação neurológica, 12, 15 ± 2,07 no grupo de portadores de DW com manifestação hepática e 12,70 ± 2,03 para o grupo- controle. Na avaliação objetiva do olfato com o teste de identificação do odor SS-16, não foi evidenciada diferença significativa entre os três grupos analisados, mas observou-se que o MEEM e o grau de escolaridade influenciaram significativamente no escore do 88-16 na comparação do grupo de pacientes com DW com manifestação neurológica com os outros dois grupos (grupo-controle e o grupo de portadores de DW com manifestação hepática). No presente estudo, não foi evidenciada disfunção olfatória nos pacientes com DW, mas foi observada diminuição da percepção do olfato em alguns pacientes com DW (com e sem manifestação neurológica). Em relação à disfunção olfatória evidenciada em alguns pacientes com DW na presente análise, algumas considerações são pertinentes e poderiam ter influenciado na identificação do olfato neste grupo de pacientes com DW. O acúmulo de cobre e a produção de radicais livres no sistema nervoso central (SNC) podem desencadear processos de neurodegeneração em estruturas envolvidas no olfato, alterações metabólicas, acúmulo de substâncias neurotóxicas (amônia e manganês) e alterações de neurotransmissores, e contribuir para o surgimento da disfunção olfatória / Wilson\'s disease (WO) is a hereditary disease due to a mutation in ATP7B gene, characterized by deficiency of copper excretion by the liver. Smell disorders are frequently encountered in neurodegenerative diseases, such as Parkinson\'s disease (PO) and Alzheimer\'s disease (AO). Smell analysis has been a useful tool for the differential diagnosis of several forms of degenerative parkinsonism, and especially for the differentiation between PO and essential tremor. Early diagnosis in WO is the key for a successful treatment. If there were smell impairment in the early stages of the illness, it could be used as another clue to help on its diagnosis. To the present date, there is only one study connecting WO with smell problems, the aim of this study was to evaluate smell function in a group of WO patients and compare them with a control group. We analyzed 37 WO patients with and 24 WO patients without neurologic symptoms, and 59 controls. Ali subjects were evaluated regarding age, gender, schooling, tobacco use, Mini Mental State Examination (MMSE), and the WO patients were also evaluated regarding duration of the illness, medication and neurologic scoring. Smell was analyzed by means of Sniffin\' Sticks smell identification test (SS-16 numbered pens and four options of answer for each pen). Twenty-four subjects with WO had no neurologic symptoms (45.83% female), and 37 patients had neurologic impairment (56,76% male). The control group was composed by 59 individuais, 35 (59,33%) male. Their age average were 33,38 ± 9,79 years for WO neurologic symptoms; 29 ± 9,61 years for WO without neurologic symptoms; and 33,81 ± 10,67 years for the control group. Ali WO patients were on treatment: 47(77%) with penicillamine, 7(11,5%) with trientine, and 7(11,5%) with zinc salt formulations. The average of correct answers in the SS-16 were: 12,03 ± 2,21 for the WO with neurologic symptoms group; 12,15 ± 2,07 for the WO without neurologic symptoms; and 12,70 ± 2,03 for the control group. In the smell testing with SS-16, there was no significant difference among the three groups, but the MMSE scoring and schooling had a significant influence over SS-16 score when comparing WO with neurologic symptoms patients with the other groups (WO patients without neurologic symptoms and control group). There was no smell dysfunction in WO patients in this study, but diminished smell perception was observed in some WO patients (either with or without neurologic impairment). Regarding smell impairment observed in some WO patients in the current analysis, some considerations must be made that could have influenced smell identification in these individuais. Copper accumulation and free radicais production in the central neNOUS system can trigger neurodegeneration processes in structures involved in srnell perception, metabolic impairment, building up of neurotoxic substances (such as ammonia and manganese), and neurotransmitter disorders, contributing to the emergence of srnell dysfunction Ceruloplasmina Ceruloplasmine Cobre Copper Degeneração hepatocecular Hepatolenticular degeneration Manifestações neurológicas Neurologic manifestations Olfato Penicilamina Penicillamine Smell
4	Manifestações neurológicas na doença de Wilson: estudo clínico e correlações genotípicas / Neurological manifestations in Wilson disease: clinical study and genotype correlations Machado, Alexandre Aluizio Costa 05 November 2008 (has links) A doença de Wilson, moléstia hereditária, caracteriza-se pela deficiência de excreção de cobre pelo fígado, originária da mutação do gene ATP7B. As manifestações neurológicas na doença de Wilson são pleomórficas, observando-se distúrbios do movimento com início insidioso e em idade variável - geralmente na segunda ou terceira décadas de vida. Este estudo, dividido em duas partes, descreve as manifestações neurológicas iniciais em 119 pacientes com doença de Wilson (93 casos-índice e 26 familiares acometidos), avaliados entre 1963 e 2004 dos quais 109 foram através de análise retrospectiva dos prontuários médicos, enquanto aos 10 pacientes restantes se dispensou avaliação clínica prospectiva, a partir de 2002. O início dos sintomas ocorreu na média etária dos 19,4 anos (7-37), e o tempo médio do surgimento dos sintomas ao diagnóstico de 1,1 +/- 1,2 anos (0-5 anos). Entre as manifestações neurológicas mais freqüentes, observaram-se: disartria (91%), distúrbios da marcha (75%), risus sardonicus (72%), distonia (69%), rigidez (66%), tremor (60%) e disfagia (50%). A incidência das manifestações coréia e atetose, 16% e 14%, respectivamente, foi baixa. Manifestações atípicas incluíram convulsões (4,2%) e sinais piramidais (3%). A segunda parte do estudo trata da investigação do genótipo ATP7B em 41 pacientes e suas possíveis correlações com o fenótipo neurológico. Encontraram-se 23 mutações distintas, a mais comum das quais (p.A1135fs) com freqüência alélica de 31,7%. Expressiva associação (p<0,05) se deu entre essa mutação e a manifestação disfagia, ainda que limitada por amostra restrita de pacientes. Também sugestiva foi a associação entre a mutação p.A1135fs e quadros neurológicos precoces e graves. Este é o primeiro estudo a comparar o genótipo ATP7B com as manifestações neurológicas na doença de Wilson / Wilson disease, a rare inborn metabolic error, is characterized by deficient hepatic copper excretion, due to mutations in ATP7B gene. Neurological manifestations may vary, although there is commonly a movement disorder starting in the second or third decade of life. This study is divided in two parts, and it describes the neurological manifestations in 119 patients with Wilson disease (93 index cases and 26 affected family members), which were seen between 1963 and 2004 a retrospective analysis in 109 medical records and prospective clinical evaluation in 10 patients since 2002. The average age of symptoms onset was 19.4 years (ranging from 7 - 37 years), and the mean time between the first symptom and diagnosis was 1, 1 +/- 1, 2 years. The most frequent neurological manifestations observed were: dysarthria (91%), gait disturbance (75%), risus sardonicus (72%), dystonia (69%), rigidity (66%), tremor (60%), and dysphagia (50%). Less frequent manifestations were chorea (16%), and athetosis (14%). Rare neurological presentations were seizures (4,2%), and pyramidal signs (3%). In the second part of this study, we ascertain ATP7B genotype correlations with distinct neurological phenotypes in 41 Wilson disease patients. A total of 23 distinct mutations were detected, and the p.A1135fs frameshift had the highest allelic frequency (31.7%). An association between a p.A1135fs mutation and dysphagia was detected (p<0, 05), but the limited number of patients restricts valuable conclusions. This analysis also suggests an association between this mutation and early and severe neurological presentation. This present study is the first one to evaluate an ATP7B genotype correlation with specific neurological profile in Wilson disease Degeneração hepatolenticular Genótipo Genotype Hepatolenticular degeneration Manifestações neurológicas Mutação Mutation Neurologic manifestations
5	Genetical and clinical studies in Wilson's disease / Waldenström, Erik, January 2007 (has links) Diss. (sammanfattning) Uppsala : Uppsala universitet, 2007. / Härtill 5 uppsatser.
6	Avaliação do olfato em pacientes com doença de Wilson / Smell analysis in patients with Wilson\'s disease Margarete de Jesus Carvalho 21 January 2016 (has links) A Doença de Wilson (DW) é uma moléstia hereditária, caracterizada pela deficiência de excreção do cobre pelo fígado devido à mutação do gene A TP7B. O distúrbio do olfato ocorre com frequência em doenças neurodegenerativas como na doença de Parkinson (DP) e na doença de Alzheimer (DA). A análise do olfato tem sido utilizada como um instrumento útil no diagnóstico diferencial das diversas formas de parkinsonismo degenerativo, e, especialmente, na diferenciação entre DP e tremor essencial. O diagnóstico precoce na DW é a chave para o sucesso do tratamento. Na hipótese de haver comprometimento do olfato em fases iniciais da doença, esse poderia ser um dado a mais para auxiliar no diagnóstico. Até o presente, há apenas um estudo relacionando a DW com a disfunção do olfato. O objetivo deste estudo foi avaliar o olfato em um grupo de pacientes com DW e confrontar com grupo- controle. No presente estudo, foram analisados 37 portadores de DW com manifestação neurológica, 24 portadores de DW sem manifestação neurológica e 59 controles. Todos os indivíduos foram analisados com relação à idade, ao gênero, ao grau de escolaridade, ao uso de tabaco e ao miniexame do estado mental (MEEM), e os portadores de DW foram avaliados quanto ao tempo de doença, tratamento medicamentoso e escore neurológico. O olfato foi avaliado por meio do teste de identificação de odor 8niffin\' 8ticks (88-16 canetas numeradas e quatro opções de resposta para cada uma). Vinte e quatro indivíduos eram pacientes da DW sem manifestação neurológica (45,83% do gênero feminino) e 37 pacientes apresentavam manifestações neurológicas (56,76% do gênero masculino). O qrupo-controle foi composto por 59 indivíduos, 35 (59,33%) do gênero masculino. As médias de- idade foram de 33,38 ± 9,79 anos no grupo de portadores de DW com manifestação neurológica; 29 ± 9,61 anos no grupo de portadores de DW sem manifestação neurológica e 33,81 ± 10,67 anos no grupo-controle. Todos os pacientes com DW estavam em tratamento: 47(77%) com penicilamina, 7 (11,5%) com trientine e 7 (11,5%) com sais de zinco. As médias de respostas corretas no teste de identificação do odor 88-16 foram: 12,03 ± 2, 21 no grupo de portadores de DW com manifestação neurológica, 12, 15 ± 2,07 no grupo de portadores de DW com manifestação hepática e 12,70 ± 2,03 para o grupo- controle. Na avaliação objetiva do olfato com o teste de identificação do odor SS-16, não foi evidenciada diferença significativa entre os três grupos analisados, mas observou-se que o MEEM e o grau de escolaridade influenciaram significativamente no escore do 88-16 na comparação do grupo de pacientes com DW com manifestação neurológica com os outros dois grupos (grupo-controle e o grupo de portadores de DW com manifestação hepática). No presente estudo, não foi evidenciada disfunção olfatória nos pacientes com DW, mas foi observada diminuição da percepção do olfato em alguns pacientes com DW (com e sem manifestação neurológica). Em relação à disfunção olfatória evidenciada em alguns pacientes com DW na presente análise, algumas considerações são pertinentes e poderiam ter influenciado na identificação do olfato neste grupo de pacientes com DW. O acúmulo de cobre e a produção de radicais livres no sistema nervoso central (SNC) podem desencadear processos de neurodegeneração em estruturas envolvidas no olfato, alterações metabólicas, acúmulo de substâncias neurotóxicas (amônia e manganês) e alterações de neurotransmissores, e contribuir para o surgimento da disfunção olfatória / Wilson\'s disease (WO) is a hereditary disease due to a mutation in ATP7B gene, characterized by deficiency of copper excretion by the liver. Smell disorders are frequently encountered in neurodegenerative diseases, such as Parkinson\'s disease (PO) and Alzheimer\'s disease (AO). Smell analysis has been a useful tool for the differential diagnosis of several forms of degenerative parkinsonism, and especially for the differentiation between PO and essential tremor. Early diagnosis in WO is the key for a successful treatment. If there were smell impairment in the early stages of the illness, it could be used as another clue to help on its diagnosis. To the present date, there is only one study connecting WO with smell problems, the aim of this study was to evaluate smell function in a group of WO patients and compare them with a control group. We analyzed 37 WO patients with and 24 WO patients without neurologic symptoms, and 59 controls. Ali subjects were evaluated regarding age, gender, schooling, tobacco use, Mini Mental State Examination (MMSE), and the WO patients were also evaluated regarding duration of the illness, medication and neurologic scoring. Smell was analyzed by means of Sniffin\' Sticks smell identification test (SS-16 numbered pens and four options of answer for each pen). Twenty-four subjects with WO had no neurologic symptoms (45.83% female), and 37 patients had neurologic impairment (56,76% male). The control group was composed by 59 individuais, 35 (59,33%) male. Their age average were 33,38 ± 9,79 years for WO neurologic symptoms; 29 ± 9,61 years for WO without neurologic symptoms; and 33,81 ± 10,67 years for the control group. Ali WO patients were on treatment: 47(77%) with penicillamine, 7(11,5%) with trientine, and 7(11,5%) with zinc salt formulations. The average of correct answers in the SS-16 were: 12,03 ± 2,21 for the WO with neurologic symptoms group; 12,15 ± 2,07 for the WO without neurologic symptoms; and 12,70 ± 2,03 for the control group. In the smell testing with SS-16, there was no significant difference among the three groups, but the MMSE scoring and schooling had a significant influence over SS-16 score when comparing WO with neurologic symptoms patients with the other groups (WO patients without neurologic symptoms and control group). There was no smell dysfunction in WO patients in this study, but diminished smell perception was observed in some WO patients (either with or without neurologic impairment). Regarding smell impairment observed in some WO patients in the current analysis, some considerations must be made that could have influenced smell identification in these individuais. Copper accumulation and free radicais production in the central neNOUS system can trigger neurodegeneration processes in structures involved in srnell perception, metabolic impairment, building up of neurotoxic substances (such as ammonia and manganese), and neurotransmitter disorders, contributing to the emergence of srnell dysfunction Ceruloplasmina Cobre Degeneração hepatocecular Manifestações neurológicas Olfato Penicilamina Ceruloplasmine Copper Hepatolenticular degeneration Neurologic manifestations Penicillamine Smell
7	Manifestações neurológicas na doença de Wilson: estudo clínico e correlações genotípicas / Neurological manifestations in Wilson disease: clinical study and genotype correlations Alexandre Aluizio Costa Machado 05 November 2008 (has links) A doença de Wilson, moléstia hereditária, caracteriza-se pela deficiência de excreção de cobre pelo fígado, originária da mutação do gene ATP7B. As manifestações neurológicas na doença de Wilson são pleomórficas, observando-se distúrbios do movimento com início insidioso e em idade variável - geralmente na segunda ou terceira décadas de vida. Este estudo, dividido em duas partes, descreve as manifestações neurológicas iniciais em 119 pacientes com doença de Wilson (93 casos-índice e 26 familiares acometidos), avaliados entre 1963 e 2004 dos quais 109 foram através de análise retrospectiva dos prontuários médicos, enquanto aos 10 pacientes restantes se dispensou avaliação clínica prospectiva, a partir de 2002. O início dos sintomas ocorreu na média etária dos 19,4 anos (7-37), e o tempo médio do surgimento dos sintomas ao diagnóstico de 1,1 +/- 1,2 anos (0-5 anos). Entre as manifestações neurológicas mais freqüentes, observaram-se: disartria (91%), distúrbios da marcha (75%), risus sardonicus (72%), distonia (69%), rigidez (66%), tremor (60%) e disfagia (50%). A incidência das manifestações coréia e atetose, 16% e 14%, respectivamente, foi baixa. Manifestações atípicas incluíram convulsões (4,2%) e sinais piramidais (3%). A segunda parte do estudo trata da investigação do genótipo ATP7B em 41 pacientes e suas possíveis correlações com o fenótipo neurológico. Encontraram-se 23 mutações distintas, a mais comum das quais (p.A1135fs) com freqüência alélica de 31,7%. Expressiva associação (p<0,05) se deu entre essa mutação e a manifestação disfagia, ainda que limitada por amostra restrita de pacientes. Também sugestiva foi a associação entre a mutação p.A1135fs e quadros neurológicos precoces e graves. Este é o primeiro estudo a comparar o genótipo ATP7B com as manifestações neurológicas na doença de Wilson / Wilson disease, a rare inborn metabolic error, is characterized by deficient hepatic copper excretion, due to mutations in ATP7B gene. Neurological manifestations may vary, although there is commonly a movement disorder starting in the second or third decade of life. This study is divided in two parts, and it describes the neurological manifestations in 119 patients with Wilson disease (93 index cases and 26 affected family members), which were seen between 1963 and 2004 a retrospective analysis in 109 medical records and prospective clinical evaluation in 10 patients since 2002. The average age of symptoms onset was 19.4 years (ranging from 7 - 37 years), and the mean time between the first symptom and diagnosis was 1, 1 +/- 1, 2 years. The most frequent neurological manifestations observed were: dysarthria (91%), gait disturbance (75%), risus sardonicus (72%), dystonia (69%), rigidity (66%), tremor (60%), and dysphagia (50%). Less frequent manifestations were chorea (16%), and athetosis (14%). Rare neurological presentations were seizures (4,2%), and pyramidal signs (3%). In the second part of this study, we ascertain ATP7B genotype correlations with distinct neurological phenotypes in 41 Wilson disease patients. A total of 23 distinct mutations were detected, and the p.A1135fs frameshift had the highest allelic frequency (31.7%). An association between a p.A1135fs mutation and dysphagia was detected (p<0, 05), but the limited number of patients restricts valuable conclusions. This analysis also suggests an association between this mutation and early and severe neurological presentation. This present study is the first one to evaluate an ATP7B genotype correlation with specific neurological profile in Wilson disease Degeneração hepatolenticular Genótipo Manifestações neurológicas Mutação Genotype Hepatolenticular degeneration Mutation Neurologic manifestations
8	Genetic Analysis of Wilson Disease in a South Indian Population and Molecular Characterization of 13 Novel ATP7B Mutations Singh, Nivedita January 2017 (has links) Wilson disease (WD) is an autosomal recessive disorder characterized by deposition of copper in the body, mainly in the liver and brain. WD patients present with hepatic, neurological, and psychiatric problems. The diagnosis of WD is very challenging, and is performed by taking into account both clinical and biochemical parameters. The treatment of WD exists, which aims at initial chelation therapy followed by maintenance therapy. WD is caused by mutations in the ATP7B gene. Till date, more than 600 mutations in ATP7B have already been described from many countries, including India. However, there are a very few large cohort studies which are reported from Indian population. In this study, we have attempted to perform mutation analysis of ATP7B in a large cohort of WD families from Bangalore, south India, and further look into the molecular consequences of the novel mutations identified in the present study. Wilson Disease TRIM36 ATP7B Mutations PLA2G6 Molecular Reproduction
9	Genetical and Clinical Studies in Wilson's Disease Waldenström, Erik January 2007 (has links) <p>Wilson’s disease is a rare inborn error of metabolism caused by a defect in ATP7B, a protein necessary for proper copper excretion into bile. It is characterised by copper accumulation with hepatic and central nervous system dysfunction.</p><p>We investigated 24 Swedish families with Wilson’s disease by sequencing the entire coding sequence using a new technique called manifold sequencing. Disease causing mutations were found in 44 out of 48 alleles.</p><p>From data obtained in the first study, the two most common mutations (C3207A and C2930T) were sought in 2640 anonymous DNA samples from a Swedish population, using a pooling strategy and solid-phase minisequencing. Four C3207A and one C2930T were found. From the number of C3207A, a prevalence of Wilson’s disease in Sweden of about 1 in 110,000 could be estimated.</p><p>Four groups with three patients each had four different genotypes concerning mutations in ATP7B. The patients’ psychopathological symptoms were investigated, using the Karolinska Scales of Personality rating (KSP) and Comprehensive Psychopathological Rating Scale (CPRS). A trend towards lower CPRS scores was seen in the groups with mutations known to render ATP7B completely without activity.</p><p>Using <sup>61</sup>Cu liver PET in patients homozygous for mutations in ATP7B, heterozygotes, normal individuals and two patients with alcoholic liver cirrhosis, significantly slower uptake was seen in the homozygotes as compared to the heterozygotes and normal individuals. The patients with cirrhosis had values in between. This implies that <sup>61</sup>Cu liver PET might be used as an additional rapid and little invasive diagnostic tool in Wilson’s disease.</p><p>In a retrospectively studied cohort consisting of 363 patients followed in Sweden and the UK, nine cases of aggressive intra-abdominal malignancies were seen, which is more than expected. Caution should be taken in the follow-up of Wilson’s disease patients.</p> Internal medicine copper radioisotopes DNA sequence analyses genotype hepatolenticular degeneration neoplasms phenotype positron-emission tomography psychopathology Invärtesmedicin
10	Genetical and Clinical Studies in Wilson's Disease Waldenström, Erik January 2007 (has links) Wilson’s disease is a rare inborn error of metabolism caused by a defect in ATP7B, a protein necessary for proper copper excretion into bile. It is characterised by copper accumulation with hepatic and central nervous system dysfunction. We investigated 24 Swedish families with Wilson’s disease by sequencing the entire coding sequence using a new technique called manifold sequencing. Disease causing mutations were found in 44 out of 48 alleles. From data obtained in the first study, the two most common mutations (C3207A and C2930T) were sought in 2640 anonymous DNA samples from a Swedish population, using a pooling strategy and solid-phase minisequencing. Four C3207A and one C2930T were found. From the number of C3207A, a prevalence of Wilson’s disease in Sweden of about 1 in 110,000 could be estimated. Four groups with three patients each had four different genotypes concerning mutations in ATP7B. The patients’ psychopathological symptoms were investigated, using the Karolinska Scales of Personality rating (KSP) and Comprehensive Psychopathological Rating Scale (CPRS). A trend towards lower CPRS scores was seen in the groups with mutations known to render ATP7B completely without activity. Using 61Cu liver PET in patients homozygous for mutations in ATP7B, heterozygotes, normal individuals and two patients with alcoholic liver cirrhosis, significantly slower uptake was seen in the homozygotes as compared to the heterozygotes and normal individuals. The patients with cirrhosis had values in between. This implies that 61Cu liver PET might be used as an additional rapid and little invasive diagnostic tool in Wilson’s disease. In a retrospectively studied cohort consisting of 363 patients followed in Sweden and the UK, nine cases of aggressive intra-abdominal malignancies were seen, which is more than expected. Caution should be taken in the follow-up of Wilson’s disease patients. Internal medicine copper radioisotopes DNA sequence analyses genotype hepatolenticular degeneration neoplasms phenotype positron-emission tomography psychopathology Invärtesmedicin

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