Non-alcoholic steatohepatitis: clinical, laboratory, histopathologic evaluation and search for mutations in the HFE gene. Casuistic from a reference center

A esteato-hepatite não alcoólica (EHNA) consiste em esteatose e inflamação lobular hepática, em indivíduos não alcoolistas. Ocorre associada a obesidade, hiperlipidemia, diabetes mellitus, sexo feminino, medicamentos e ‘bypass’ jejunoileal. Recentemente, a sobrecarga de ferro, secundária a mutações no gene HFE da hemocromatose hereditária, também vem sendo evidenciada nos pacientes com EHNA do sexo masculino, não obesos e não diabéticos. O presente estudo, envolvendo pacientes com EHNA do Ambulatório de Gastroenterologia do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, teve como objetivos traçar seu perfil clínico, laboratorial e histopatológico, pesquisar a presença de mutações do gene HFE, buscar associações entre esses resultados e rever a literatura a respeito. Trinta e dois indivíduos foram caracterizados quanto a 14 aspectos clínicos, 12 parâmetros laboratoriais e 11 variáveis histopatológicas. Em 31 destes pesquisaram-se as mutações C282Y e H63D pela técnica de PCR-RFLP, utilizando-se as enzimas de restrição SnaB I e Bcl I, respectivamente. As idades variaram entre 32 e 76 anos, com média de 49,2 anos. Sexo feminino (59%), obesidade (50%), hiperlipidemia (53%) e diabetes mellitus (31%) ocorreram em taxas inferiores às das primeiras séries publicadas. Outras condições encontradas foram uso de amiodarona e prednisona, inalação de substâncias químicas industriais e enterectomia extensa. As etnias branca (72%) e asiática (12%) ocorreram em percentagens maiores que da população geral; ao contrário, a negra (ausente) e mulatos (12%), em menores. A fibrose perivenular ocorreu em todos os casos, proporcional ao grau de atividade necroinflamatória. Os hialinos de Mallory foram identificados em 78% dos casos, mas a siderose em apenas 9%. Cerca de dois terços da casuística não apresentou queixas relacionadas ao aparelho digestivo. Dentre as enzimas hepáticas, a ALT foi a que se alterou com maior freqüência e magnitude, e a relação AST/ALT foi menor que dois em todos os casos. As incidências das mutações pesquisadas corresponderam às da população geral. A sobrecarga de ferro em sangue periférico não se correlacionou estatisticamente com a agressão histológica, nem com a presença das mutações. EHNA é um diagnóstico que engloba múltiplas condições, mas, na população estudada, não houve associação com a sobrecarga de ferro hepático, tampouco com as mutações conhecidas do gene HFE.Non-alcoholic steatohepatitis (NASH) consists of steatosis and hepatic lobular inflammation in non-alcoholic individuals. It occurs in association to obesity, hyperlipidemia, diabetes mellitus, female sex, drug therapy and jejunoileal bypass. Recently, iron overload, secondary to mutations in the HFE gene in hereditary hemochromatosis has also been evidenced in nonobese, non-diabetic male patients with NASH. This study involves patients with NASH from the outpatient clinic of Hospital das Clinicas of the University of São Paulo School of Medicine, and its objective was to define patients’ clinical, laboratory and histological profiles and search for mutations in the HFE gene, compare results for associations and review the literature. Thirtytwo individuals were characterized for 14 clinical features, 12 laboratory parameters and 11 histopathological variables. The C282Y and H63D mutations in 31 of these individuals were searched using PCR-RFLP techniques, using restriction enzymes SnaB I and BcI I, respectively. Age varied from 32 to 76 yrs old, with an average of 49,2 yrs. Female sex (59%), obesity (50%), hyperlipidemia (53%) and diabetes mellitus (31%) had a lower incidence than those in the first series in the literature. Other features observed were amiodarone and prednisone use, inhalation of industrial chemical substances and extensive enterectomy. Its incidence was higher among Caucasians (72%) and Asians (12%) than in the general population, contrary to other ethnic types such as Black (absent) and Mulattos (12%) which presented lower incidences. Perivenular fibrosis was present in all cases, proportional to the degree of necroinflammatory activity. Mallory’s hyalines were identified in 78% of the cases, but hepatic siderosis was identified in only 9%. Around two-thirds of the casuistic did not have abdominal complaints. Among the hepatic enzymes, ALT was the most frequently altered with the highest magnitude and the AST/ALT ratio was < 2 in all cases. The incidence of the mutations studied was similar to those found in the general population. The iron overload in peripheral blood was neither statistically correlated to the histological aggression, nor to the presence of mutations. NASH diagnosis depends on multiple features, but in the population studied, there was no association with hepatic iron overload as well as with the known mutations in the HFE gene

Wilson's disease in southern Brazil: a 40-year follow-up study

BACKGROUND: Long-term data on the clinical follow-up and the treatment effectiveness of Wilson's disease are limited because of the low disease frequency. This study evaluated a retrospective cohort of Wilson's disease patients from southern Brazil during a 40-year follow-up period. METHODS: Thirty-six Wilson's disease patients, diagnosed from 1971 to 2010, were retrospectively evaluated according to their clinical presentation, epidemiological and social features, response to therapy and outcome. RESULTS: Examining the patients' continental origins showed that 74.5% had a European ancestor. The mean age at the initial symptom presentation was 23.3 ± 9.3 years, with a delay of 27.5 ± 41.9 months until definitive diagnosis. At presentation, hepatic symptoms were predominant (38.9%), followed by mixed symptoms (hepatic and neuropsychiatric) (30.6%) and neuropsychiatric symptoms (25%). Kayser-Fleischer rings were identified in 55.6% of patients, with a higher frequency among those patients with neuropsychiatric symptoms (77.8%). Eighteen patients developed neuropsychiatric features, most commonly cerebellar syndrome. Neuroradiological imaging abnormalities were observed in 72.2% of these patients. Chronic liver disease was detected in 68% of the patients with hepatic symptoms. 94.2% of all the patients were treated with D-penicillamine for a mean time of 129.9 ± 108.3 months. Other treatments included zinc salts, combined therapy and liver transplantation. After initiating therapy, 78.8% of the patients had a stable or improved outcome, and the overall survival rate was 90.1%. CONCLUSION: This study is the first retrospective description of a population of Wilson's disease patients of mainly European continental origin who live in southern Brazil. Wilson's disease is treatable if correctly diagnosed, and an adequate quality of life can be achieved, resulting in a long overall survival

Doença de Wilson no sul do Brasil: correlação genotípica-fenotípica\ud e a descrição de duas novas mutações no gene ATP7B

OBJECTIVE:\ud \ud Wilson's disease (WD) is an inborn error of metabolism caused by abnormalities of the copper-transporting protein encoding gene ATP7B. In this study, we examined ATP7B for mutations in a group of patients living in southern Brazil.\ud \ud METHODS:\ud \ud 36 WD subjects were studied and classified according to their clinical and epidemiological data. In 23 subjects the ATP7B gene was analyzed.\ud \ud RESULTS:\ud \ud Fourteen distinct mutations were detected in at least one of the alleles. The c.3207C>A substitution at exon 14 was the most common mutation (allelic frequency=37.1%) followed by the c.3402delC at exon 15 (allelic frequency=11.4%). The mutations c.2018-2030del13 at exon 7 and c.4093InsT at exon 20 are being reported for the first time.\ud \ud CONCLUSION:\ud \ud The c.3207C>A substitution at exon 14, was the most common mutation, with an allelic frequency of 37.1%. This mutation is the most common mutation described in Europe.OBJETIVO:\ud \ud A doença de Wilson (DW) é um erro inato do metabolismo causado por abnormalidades no gene ATP7B, que codifica uma proteína transportadora de cobre. Neste estudo, avaliamos as mutações do gene ATP7B em um grupo de pacientes do sul do Brasil.\ud \ud MÉTODOS:\ud \ud Foram estudados 36 pacientes com DW e classificados do ponto de vista clínico e epidemiológico. Em 23 pacientes, o gene ATP7B foi analisado.\ud \ud RESULTADOS:\ud \ud A substituição c.3207C>A no éxon 14 foi a mutação mais comum seguida pela mutação c.3402delC no éxon 15 . A mutação c.2018-2030del13 no éxon 7 e a c.4093InsT no éxon 20 são relatadas pela primeira vez na literatura.\ud \ud CONCLUSÃO:\ud \ud A mutação do gene ATP7B, com a substituição c.3207C>A no éxon 14 foi a mais frequente. Esta mutação é a mais comumente encontrada em pacientes europeus

Wilson disease : demographic and phenotypic aspects related to ATP7B genotype and haplotype analysis in carriers of the L708P mutation

A doença de Wilson é um distúrbio da excreção biliar de cobre devido a um defeito na proteína ATP7B. Em caráter pioneiro na América do Sul, seqüenciou-se o gene ATP7B em 60 pacientes brasileiros pertencentes a 46 famílias; os resultados foram relacionados com aspectos demográficos e fenotípicos. Detectaram-se 25 mutações, 12 das quais novas. A 3402delC (34,8%) e a L708P (14,1%) ocorreu em 58,3% das famílias de São Paulo e em 44,4% das de Minas Gerais, respectivamente. As substituições novas, pesquisadas por RFLP ou PCR alelo-específica, não ocorreram em 60 indivíduos controle; portanto, não são polimorfismos comuns. O estudo comparativo de haplótipos dos portadores da L708P da coorte atual e de Gran Canaria sugeriu um efeito-fundador comum para ambos os grupos. O fenótipo variou amplamente para genótipos idênticosATP7B protein. As the first study of its kind in South America, the ATP7B gene was sequenced and the results were related to demographic and phenotypic aspects of 60 Brazilian patients, from 46 distinct families. Twenty-five mutations were detected, 12 of which are novel. The 3402delC (34.8%) and the L708P (14.1%) occurred in 58.3% of the families from Sao Paulo and in 44.4% of those from Minas Gerais, respectively. The novel substitutions were shown not to be common polymorphisms by RFLP or allele-specific PCR studies performed in 60 control subjects. Haplotype analysis comparing carriers of the L708P from this cohort study with patients from Gran Canary suggests the same founder-effect for both groups. Phenotype varied widely for identic genotypes

Non-alcoholic steatohepatitis: clinical, laboratory, histopathologic evaluation and search for mutations in the HFE gene: casuistic from a reference center.

A esteato-hepatite não alcoólica (EHNA) consiste em esteatose e inflamação lobular hepática, em indivíduos não alcoolistas. Ocorre associada a obesidade, hiperlipidemia, diabetes mellitus, sexo feminino, medicamentos e bypass jejunoileal. Recentemente, a sobrecarga de ferro, secundária a mutações no gene HFE da hemocromatose hereditária, também vem sendo evidenciada nos pacientes com EHNA do sexo masculino, não obesos e não diabéticos. O presente estudo, envolvendo pacientes com EHNA do Ambulatório de Gastroenterologia do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo, teve como objetivos traçar seu perfil clínico, laboratorial e histopatológico, pesquisar a presença de mutações do gene HFE, buscar associações entre esses resultados e rever a literatura a respeito. Trinta e dois indivíduos foram caracterizados quanto a 14 aspectos clínicos, 12 parâmetros laboratoriais e 11 variáveis histopatológicas. Em 31 destes pesquisaram-se as mutações C282Y e H63D pela técnica de PCR-RFLP, utilizando-se as enzimas de restrição SnaB I e Bcl I, respectivamente. As idades variaram entre 32 e 76 anos, com média de 49,2 anos. Sexo feminino (59%), obesidade (50%), hiperlipidemia (53%) e diabetes mellitus (31%) ocorreram em taxas inferiores às das primeiras séries publicadas. Outras condições encontradas foram uso de amiodarona e prednisona, inalação de substâncias químicas industriais e enterectomia extensa. As etnias branca (72%) e asiática (12%) ocorreram em percentagens maiores que da população geral; ao contrário, a negra (ausente) e mulatos (12%), em menores. A fibrose perivenular ocorreu em todos os casos, proporcional ao grau de atividade necroinflamatória. Os hialinos de Mallory foram identificados em 78% dos casos, mas a siderose em apenas 9%. Cerca de dois terços da casuística não apresentou queixas relacionadas ao aparelho digestivo. Dentre as enzimas hepáticas, a ALT foi a que se alterou com maior freqüência e magnitude, e a relação AST/ALT foi menor que dois em todos os casos. As incidências das mutações pesquisadas corresponderam às da população geral. A sobrecarga de ferro em sangue periférico não se correlacionou estatisticamente com a agressão histológica, nem com a presença das mutações. EHNA é um diagnóstico que engloba múltiplas condições, mas, na população estudada, não houve associação com a sobrecarga de ferro hepático, tampouco com as mutações conhecidas do gene HFE.Non-alcoholic steatohepatitis (NASH) consists of steatosis and hepatic lobular inflammation in non-alcoholic individuals. It occurs in association to obesity, hyperlipidemia, diabetes mellitus, female sex, drug therapy and jejunoileal bypass. Recently, iron overload, secondary to mutations in the HFE gene in hereditary hemochromatosis has also been evidenced in nonobese, non-diabetic male patients with NASH. This study involves patients with NASH from the outpatient clinic of Hospital das Clinicas of the University of São Paulo School of Medicine, and its objective was to define patients clinical, laboratory and histological profiles and search for mutations in the HFE gene, compare results for associations and review the literature. Thirtytwo individuals were characterized for 14 clinical features, 12 laboratory parameters and 11 histopathological variables. The C282Y and H63D mutations in 31 of these individuals were searched using PCR-RFLP techniques, using restriction enzymes SnaB I and BcI I, respectively. Age varied from 32 to 76 yrs old, with an average of 49,2 yrs. Female sex (59%), obesity (50%), hyperlipidemia (53%) and diabetes mellitus (31%) had a lower incidence than those in the first series in the literature. Other features observed were amiodarone and prednisone use, inhalation of industrial chemical substances and extensive enterectomy. Its incidence was higher among Caucasians (72%) and Asians (12%) than in the general population, contrary to other ethnic types such as Black (absent) and Mulattos (12%) which presented lower incidences. Perivenular fibrosis was present in all cases, proportional to the degree of necroinflammatory activity. Mallorys hyalines were identified in 78% of the cases, but hepatic siderosis was identified in only 9%. Around two-thirds of the casuistic did not have abdominal complaints. Among the hepatic enzymes, ALT was the most frequently altered with the highest magnitude and the AST/ALT ratio was < 2 in all cases. The incidence of the mutations studied was similar to those found in the general population. The iron overload in peripheral blood was neither statistically correlated to the histological aggression, nor to the presence of mutations. NASH diagnosis depends on multiple features, but in the population studied, there was no association with hepatic iron overload as well as with the known mutations in the HFE gene

Wilson disease : demographic and phenotypic aspects related to ATP7B genotype and haplotype analysis in carriers of the L708P mutation

A doença de Wilson é um distúrbio da excreção biliar de cobre devido a um defeito na proteína ATP7B. Em caráter pioneiro na América do Sul, seqüenciou-se o gene ATP7B em 60 pacientes brasileiros pertencentes a 46 famílias; os resultados foram relacionados com aspectos demográficos e fenotípicos. Detectaram-se 25 mutações, 12 das quais novas. A 3402delC (34,8%) e a L708P (14,1%) ocorreu em 58,3% das famílias de São Paulo e em 44,4% das de Minas Gerais, respectivamente. As substituições novas, pesquisadas por RFLP ou PCR alelo-específica, não ocorreram em 60 indivíduos controle; portanto, não são polimorfismos comuns. O estudo comparativo de haplótipos dos portadores da L708P da coorte atual e de Gran Canaria sugeriu um efeito-fundador comum para ambos os grupos. O fenótipo variou amplamente para genótipos idênticosATP7B protein. As the first study of its kind in South America, the ATP7B gene was sequenced and the results were related to demographic and phenotypic aspects of 60 Brazilian patients, from 46 distinct families. Twenty-five mutations were detected, 12 of which are novel. The 3402delC (34.8%) and the L708P (14.1%) occurred in 58.3% of the families from Sao Paulo and in 44.4% of those from Minas Gerais, respectively. The novel substitutions were shown not to be common polymorphisms by RFLP or allele-specific PCR studies performed in 60 control subjects. Haplotype analysis comparing carriers of the L708P from this cohort study with patients from Gran Canary suggests the same founder-effect for both groups. Phenotype varied widely for identic genotypes

Mania as the first manifestation of Wilson`s disease

Background: Although mental changes are frequent in Wilson`s disease, severe psychiatric disorders occur uncommonly and usually accompany the neurological picture. There are few reports in the literature of Wilson`s disease patients with typical bipolar affective disorder (BPAD). Case report: The authors report the case of a patient with Wilson`s disease whose initial manifestation was a manic episode followed by depression. Tremor in the upper limbs appeared one year after the onset of symptoms. The diagnosis of Wilson`s disease was established three years after the first symptoms appeared, based on the neuropsychiatric picture, the detection of Kayser-Fleischer rings and the results of diagnostic tests indicating chronic liver disease and copper excess. ATP7B genotyping and magnetic resonance imaging of the brain with proton spectroscopy study were also performed. The patient became asymptomatic two years after starting treatment with penicillamine and remained non-symptomatic controlled during the eight-year follow-up period, without any specific treatment for the BPAD. Conclusions: To our knowledge, this is a singular report of a case of Wilson`s disease in which a manic episode preceded the onset of neurological symptoms. The association between Wilson`s disease and bipolar disorder is discussed

Neurological manifestations and ATP7B mutations in Wilson`s disease

Wilson`s disease (WD) is a rare inborn metabolic error characterized by deficient biliary copper excretion secondary to ATP7B gene mutations. Neurological presentations are variable in respect to both pattern and age of onset; commonly a movement disorder presents in the second or third decade. The aim of this study was to ascertain genotype correlations with distinct neurological manifestations in 41 WD patients in a Brazilian center for WD. A total of 23 distinct mutations were detected, and the frameshift 3402de1C had the highest allelic frequency (31.7%). An association between 3402de1C and dysphagia was detected (p = 0.01) but the limited number of patients is insufficient to allow one to draw conclusions. Both clinical studies analyzing larger cohorts and basic research on ATP7B protein function could potentially shed more light on our understanding of WD. (c) 2007 Elsevier Ltd. All rights reserved