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遗传性粪卟啉病:一个大家族中分子与生化研究的比较

Hereditary coproporphyria: comparison of molecular and biochemical investigations in a large family.

作者信息

Allen K R, Whatley S D, Degg T J, Barth J H

机构信息

Department of Clinical Biochemistry, Leeds Teaching Hospitals, Leeds, UK.

出版信息

J Inherit Metab Dis. 2005;28(5):779-85. doi: 10.1007/s10545-005-0092-z.

Abstract

Hereditary coproporphyria (HCP) is the least common of the three autosomal dominant acute porphyrias. To compare the sensitivity of metabolite measurements for the identification of asymptomatic HCP, we carried out a molecular and biochemical investigation of a large family in which HCP is caused by a previously unreported frameshift mutation (c.119delA). Thirteen of 19 asymptomatic family members, aged 10-72 years, were shown by mutational analysis to have HCP. The faecal coproporphyrin isomer III:I ratio was increased in all of these 13 family members; faecal total porphyrin concentration and urinary porphyrin excretion were increased in 11 and 8 of them, respectively. Plasma porphyrin concentrations were marginally increased in three individuals and plasma fluorescence emission scanning showed a porphyrin peak at 618 nm in two of these. Our results add to the evidence that an increased faecal porphyrin coproporphyrin III:I ratio is a highly sensitive test for the detection of clinically latent HCP in individuals over the age of 10 years; its sensitivity below this age remains uncertain. They also show that plasma fluorescence emission scanning is not useful for the investigation of families with HCP.

摘要

遗传性粪卟啉病(HCP)是三种常染色体显性急性卟啉病中最不常见的一种。为了比较代谢物检测对无症状HCP的识别敏感性,我们对一个大家庭进行了分子和生化研究,该家庭中的HCP由一个此前未报道的移码突变(c.119delA)引起。在19名年龄在10至72岁之间的无症状家庭成员中,经突变分析显示有13人患有HCP。这13名家庭成员的粪便粪卟啉异构体III:I比值均升高;其中11人粪便总卟啉浓度升高,8人尿卟啉排泄增加。3人的血浆卟啉浓度略有升高,其中2人的血浆荧光发射扫描显示在618nm处有一个卟啉峰。我们的结果进一步证明,粪便卟啉粪卟啉III:I比值升高是检测10岁以上个体临床潜伏性HCP的一项高度敏感的检测方法;其在该年龄以下的敏感性仍不确定。研究结果还表明,血浆荧光发射扫描对HCP家族的调查并无帮助。

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