新发性变异与儿童期发病的烟雾病和弥漫性闭塞性血管病的关联。

Association of De Novo Variants With Childhood Onset Moyamoya Disease and Diffuse Occlusive Vasculopathy.

机构信息

From the Department of Internal Medicine (A.P., A.C.C., M.A., D.G., D.M.M.), McGovern Medical School, University of Texas Health Science Center at Houston; Maritime Medical Genetics Service (A.L.R., S.P., M.A.V.), Division of Neurosurgery (M.D.J.F., P.D.M., S.W.) and Department of Pediatrics (M.A.V.), Division of Medical Genetics, Dalhousie University, IWK Health Centre Halifax, Nova Scotia Canada; Department of Pediatrics (S.C.N.), Division of Child Neurology, and Department of Genetics (A.C.E.H.), University of Alabama at Birmingham; Department of Pediatrics (M.J.B., A.M.V.), Division of Genetics Medicine and Department of Genome Sciences (M.J.B., D.A.N.), University of Washington, Seattle; and Department of Pediatrics (S.M.F.), Division of Child Neurology, University of Texas McGovern Medical School.

出版信息

Neurology. 2021 Mar 30;96(13):e1783-e1791. doi: 10.1212/WNL.0000000000011653. Epub 2021 Feb 10.

DOI:10.1212/WNL.0000000000011653

PMID:33568546

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8055312/

Abstract

OBJECTIVE

To test the hypothesis that de novo genetic variants are responsible for moyamoya disease (MMD) in children with unaffected relatives, we performed exome sequencing of 28 affected children and their unaffected parents.

METHODS

Exome sequencing was performed on 28 trios of affected patients with MMD and unaffected parents.

RESULTS

We identified 3 novel rare de novo variants, 1 in the RING domain and 2 in a highly conserved region distal to the RING domain (4,114-4,120). These de novo cases of MMD present at a young age with aggressive MMD and uniquely have additional occlusive vascular lesions, including renal artery stenosis. Two previously reported cases had de novo variants in the same limited region and presented young with aggressive MMD, and 1 case had narrowing of the inferior abdominal aorta.

CONCLUSIONS

These results indicate a novel syndrome associated with rare variants defined by de novo mutations disrupting highly conserved amino acids in the RING domain and a discrete region distal to the RING domain delimited by amino acids 4,114 to 4,120 leading to onset of severe MMD before 3 years of age and occlusion of other arteries, including the abdominal aorta, renal, iliac, and femoral arteries.

摘要

目的

为了验证新出现的遗传变异是导致无亲缘关系的儿童烟雾病（MMD）的假说，我们对 28 名受影响的儿童及其未受影响的父母进行了外显子组测序。

方法

对 28 个受 MMD 影响的患者及其未受影响的父母的三联体进行外显子组测序。

结果

我们发现了 3 个新的罕见的新生突变，1 个在 RING 结构域，2 个在 RING 结构域远端的高度保守区域（4,114-4,120）。这些新发的 MMD 病例在年轻时表现为侵袭性 MMD，且独特地伴有其他闭塞性血管病变，包括肾动脉狭窄。之前有 2 例报道的病例在相同的有限区域存在新生突变，且在年轻时表现为侵袭性 MMD，1 例病例存在下腹部主动脉狭窄。

结论

这些结果表明一种新的综合征与新生突变导致的 RING 结构域高度保守氨基酸和 RING 结构域远端的离散区域（由氨基酸 4,114 至 4,120 定义的）破坏有关，导致严重的 MMD 在 3 岁之前发病，并导致其他动脉闭塞，包括腹主动脉、肾动脉、髂动脉和股动脉。

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