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在一个因EGR2突变导致1型夏科-马里-图斯病神经病的家族中,PMP22缺失的修饰作用。

The modifying effect a PMP22 deletion in a family with Charcot-Marie-Tooth type 1 neuropathy due to an EGR2 mutation.

作者信息

Reményi Viktória, Inczédy-Farkas Gabriella, Gál Anikó, Bereznai Benjamin, Pál Zsuzsanna, Karcagi Veronica, Mechler Ferenc, Molnár Mária Judit

出版信息

Ideggyogy Sz. 2014 Nov 30;67(11-12):420-5.

Abstract

BACKGROUND

Mutations of both the PMP22 and EGR2 genes cause Charcot-Marie-Tooth (CMT) disease type 1. Deletion of the PMP22 gene, results in hereditary neuropathy with liability to pressure palsies. More publications exist about the interaction of PMP22 duplication and other CMT-causing gene mutations. In these cases the intrafamiliar discordant phenotypes draw the attention to the possible role of modifying genes. The gene-gene interactions between the PMP22 and EGR2 genes are not well understood.

CASE REPORT

We report two brothers with late onset CMT1 due to a c. 1142 G>A (Arg381His) heterozygous substitution in the EGR2 gene. Additionally, the older brother with the less severe symptoms harbored the PMP22 gene deletion also.

CONCLUSION

The coexistence of the two genetic alterations did not aggravate the clinical symptoms. Moreover, the PMP22 deletion appeared to have a beneficial modifying effect, thus implying potential gene-gene interaction of PMP22 and EGR2. PMP22 deletion may increase Schwann cells proliferation and compensate the dominant-negative effect of the Arg381 His substitution in the EGR2 gene.

摘要

背景

PMP22和EGR2基因的突变都会导致1型夏科-马里-图斯(CMT)病。PMP22基因的缺失会导致遗传性压迫易感性神经病。关于PMP22基因重复与其他导致CMT的基因突变之间的相互作用,有更多的文献报道。在这些病例中,家族内不一致的表型引起了人们对修饰基因可能作用的关注。PMP22和EGR2基因之间的基因-基因相互作用尚未完全了解。

病例报告

我们报告了两兄弟,由于EGR2基因中发生c.1142 G>A(Arg381His)杂合替代,导致迟发性CMT1。此外,症状较轻的哥哥还存在PMP22基因缺失。

结论

两种基因改变的共存并未加重临床症状。此外,PMP22基因缺失似乎具有有益的修饰作用,这意味着PMP22和EGR2之间可能存在基因-基因相互作用。PMP22基因缺失可能会增加雪旺细胞的增殖,并补偿EGR2基因中Arg381His替代的显性负效应。

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