Bacon B R, Olynyk J K, Brunt E M, Britton R S, Wolff R K
Saint Louis University School of Medicine, Missouri, USA.
Ann Intern Med. 1999 Jun 15;130(12):953-62. doi: 10.7326/0003-4819-130-12-199906150-00002.
Hereditary hemochromatosis is a common inherited disorder of iron metabolism. The gene HFE, which contains two missense mutations (C282Y and H63D), was recently identified.
To determine how HFE genotyping for the C282Y and H63D mutations contributes to the diagnosis of hemochromatosis and to determine the prevalence of HFE mutations in a group of patients with liver disease.
Cross-sectional study.
Academic medical center.
66 patients with hereditary hemochromatosis and 132 referred patients with other liver diseases.
At initial diagnosis, fasting transferrin saturation, ferritin level, routine chemistry panel, and complete blood count were determined. Percutaneous liver biopsy was done on all patients for histologic analysis and measurement of hepatic iron concentration and hepatic iron index. HFE genotyping for the C282Y and H63D mutations was done on all patients by using genomic DNA samples.
Of the 66 patients with hemochromatosis diagnosed on the basis of serum iron studies and liver biopsy findings, 60 (91%) were C282Y homozygotes, 2 (3%) were compound heterozygotes, 1 (1.5%) was a C282Y heterozygote, 2 (3%) were H63D heterozygotes, and 1 (1.5%) was negative for both mutations. Of the 132 patients with liver disease, 6 (5%) were C282Y homozygotes, 8 (6%) were compound heterozygotes, 6 (5%) were C282Y heterozygotes, 5 (4%) were H63D homozygotes, 20 (15%) were H63D heterozygotes, and 87 (66%) were negative for both mutations. All 66 C282Y homozygotes had an elevated hepatic iron concentration, and 65 of the 66 patients (98%) had a transferrin saturation of at least 45%. Ten of the 66 patients (15% [95% CI, 7.5% to 26%]) had a hepatic iron index less than 1.9 mmol/kg per year; hemochromatosis was not suspected in 6 of the 10 patients before genotyping. Cirrhosis or substantial hepatic fibrosis was not seen in any (0% [CI, 0% to 18%]) of the 19 patients younger than 40 years of age who were homozygous for the C282Y mutation.
All 66 patients homozygous for the C282Y mutation of HFE had an elevated hepatic iron concentration, but approximately 15% of these patients did not meet a previous diagnostic criterion for hemochromatosis (hepatic iron index > 1.9 mmol/kg per year). Determination of HFE genotype is clinically useful in patients with liver disease and suspected iron overload and may lead to identification of otherwise unsuspected C282Y homozygotes.
遗传性血色素沉着症是一种常见的铁代谢遗传性疾病。最近发现了包含两个错义突变(C282Y和H63D)的HFE基因。
确定针对C282Y和H63D突变的HFE基因分型对血色素沉着症诊断的贡献,并确定一组肝病患者中HFE突变的患病率。
横断面研究。
学术医疗中心。
66例遗传性血色素沉着症患者和132例转诊的其他肝病患者。
在初次诊断时,测定空腹转铁蛋白饱和度、铁蛋白水平、常规化学检查和全血细胞计数。对所有患者进行经皮肝活检,用于组织学分析以及测量肝铁浓度和肝铁指数。通过使用基因组DNA样本对所有患者进行C282Y和H63D突变的HFE基因分型。
在根据血清铁研究和肝活检结果诊断为血色素沉着症的66例患者中,60例(91%)为C282Y纯合子,2例(3%)为复合杂合子,1例(1.5%)为C282Y杂合子,2例(3%)为H63D杂合子,1例(1.5%)两种突变均为阴性。在132例肝病患者中,6例(5%)为C282Y纯合子,8例(6%)为复合杂合子,6例(5%)为C282Y杂合子,5例(4%)为H63D纯合子,20例(15%)为H63D杂合子,87例(66%)两种突变均为阴性。所有66例C282Y纯合子的肝铁浓度均升高,66例患者中的65例(98%)转铁蛋白饱和度至少为45%。66例患者中有10例(15%[95%CI,7.5%至26%])肝铁指数低于1.9 mmol/kg每年;在基因分型前,这10例患者中有6例未被怀疑患有血色素沉着症。在19例年龄小于40岁的C282Y突变纯合子患者中,无一例(0%[CI,0%至18%])出现肝硬化或严重肝纤维化。
所有66例HFE基因C282Y突变纯合子患者的肝铁浓度均升高,但其中约15%的患者不符合先前血色素沉着症的诊断标准(肝铁指数>1.9 mmol/kg每年)。对于患有肝病且怀疑铁过载的患者,测定HFE基因型在临床上有用,可能会发现其他未被怀疑的C282Y纯合子。
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