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亨廷顿舞蹈症突变的外显率降低。

Reduced penetrance of the Huntington's disease mutation.

作者信息

McNeil S M, Novelletto A, Srinidhi J, Barnes G, Kornbluth I, Altherr M R, Wasmuth J J, Gusella J F, MacDonald M E, Myers R H

机构信息

Molecular Neurogenetics Unit, Massachusetts General Hospital, Harvard Medical School, Boston 02114, USA.

出版信息

Hum Mol Genet. 1997 May;6(5):775-9. doi: 10.1093/hmg/6.5.775.

Abstract

Controversy persists concerning the significance of Huntington disease (HD) alleles in the 36-39 repeat range. Although some clinically affected persons have been documented with repeats in this range, elderly unaffected individuals have also been reported. We examined 10 paternal transmissions of HD alleles of 37-39 repeats in collateral branches of families with de novo HD. All 10 descendants, including many who are elderly, are without symptoms of HD. Forty percent of the transmissions were unstable, although none varied by more than one repeat. The observation that individuals with alleles of 37-39 repeats may survive unaffected beyond common life expectancy supports the presence of reduced penetrance for HD among some persons with repeat sizes which overlap the clinical range. Non-penetrance may be increased in the collateral branches of de novo mutation families when compared to penetrance estimates from patient series. There was no CAA-->CAG mutation for the penultimate glutamine in either a de novo expanded 42 repeat allele or the corresponding non-penetrant 38 repeat allele in a family with fresh mutation to HD.

摘要

关于亨廷顿舞蹈病(HD)等位基因在36 - 39次重复范围内的意义,争议仍然存在。虽然有记录显示一些临床患者的重复次数在此范围内,但也有报道称未受影响的老年人也存在这种情况。我们研究了新发HD家族旁系分支中10例37 - 39次重复的HD等位基因的父系传递情况。所有10名后代,包括许多老年人,均无HD症状。40%的传递是不稳定的,尽管没有一个变化超过一次重复。37 - 39次重复等位基因的个体可能在超过正常预期寿命的情况下仍未受影响,这一观察结果支持了在一些重复大小与临床范围重叠的人群中,HD的外显率降低。与患者系列的外显率估计相比,新发突变家族的旁系分支中非外显率可能会增加。在一个新发HD突变家族中,一个新发扩展的42次重复等位基因或相应的非外显的38次重复等位基因中,倒数第二个谷氨酰胺均未发生CAA→CAG突变。

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