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首页> 外文期刊>Clinical Chemistry: Journal of the American Association for Clinical Chemists >Molecular diagnosis of Charcot-Marie-Tooth 1A disease and hereditary neuropathy with liability to pressure palsies by quantifying CMT1A-REP sequences: consequences of recombinations at variant sites on chromosomes 17p11.2-12.
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Molecular diagnosis of Charcot-Marie-Tooth 1A disease and hereditary neuropathy with liability to pressure palsies by quantifying CMT1A-REP sequences: consequences of recombinations at variant sites on chromosomes 17p11.2-12.

机译:通过定量CMT1A-REP序列的分子诊断Charcot-Marie-Tooth 1A疾病和遗传性神经病,并伴有压力性麻痹:17p11.2-12号染色体变异位点的重组结果。

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The most frequent form of Charcot-Marie-Tooth disease (CMT1A; OMIM118.220) is the result of a duplication on chromosome 17 in pll.2-p12. This region contains PMP22, a gene expressed in peripheral myelin. The mutation results from an unequal crossing-over involving repeated sequences, CMT1A-REP, located on both sides of the duplicated region. The reciprocal product of this recombination is a deletion of the same region, which is associated with hereditary neuropathy with liability to pressure palsies (HNPP; OMIM162.500). Proximal and distal CMT1A-REP sequences can be distinguished by the presence of a variant EcoRI site. We quantified the number of these repeat sequences in 36 CMT1A and 40 HNPP patients. CMT1A-REP sequences are involved in almost all of the mutations. The majority of recombination breakpoints occur distally from the variant EcoRI site. However, a few have a breakpoint proximal to this site, which creates the risk of misinterpretation with respect to a duplicated/deleted status.
机译:Charcot-Marie-Tooth病(CMT1A; OMIM118.220)是最常见的形式,是pll.2-p12中17号染色​​体重复的结果。该区域含有在外周髓磷脂中表达的基因PMP22。突变是由不重复的重复序列CMT1A-REP(位于重复区域的两侧)引起的。这种重组的相互产物是同一区域的缺失,这与遗传性神经病有关,并伴有压力性麻痹(HNPP; OMIM162.500)。近端和远端CMT1A-REP序列可以通过存在一个变异的EcoRI位点来区分。我们量化了36名CMT1A和40名HNPP患者中这些重复序列的数量。 CMT1A-REP序列几乎参与了所有突变。大多数重组断点发生在变异EcoRI位点的远端。但是,有一些在此站点附近有一个断点,这会产生关于重复/删除状态的误解的风险。

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