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Refining frontotemporal dementia with parkinsonism linked to chromosome 17: introducing FTDP-17 (MAPT) and FTDP-17 (PGRN).细化与17号染色体相关的额颞叶痴呆伴帕金森综合征:引入FTDP-17(微管相关蛋白tau)和FTDP-17(原纤维蛋白)
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IVS10+16、IVS10+3、N279K、S305N、P301L和V337M MAPT突变的萎缩模式

Atrophy patterns in IVS10+16, IVS10+3, N279K, S305N, P301L, and V337M MAPT mutations.

作者信息

Whitwell J L, Jack C R, Boeve B F, Senjem M L, Baker M, Ivnik R J, Knopman D S, Wszolek Z K, Petersen R C, Rademakers R, Josephs K A

机构信息

Department of Radiology, Mayo Clinic, Rochester, MN 55905, USA.

出版信息

Neurology. 2009 Sep 29;73(13):1058-65. doi: 10.1212/WNL.0b013e3181b9c8b9.

DOI:10.1212/WNL.0b013e3181b9c8b9
PMID:19786698
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2754325/
Abstract

OBJECTIVE

To use a case-control study to assess and compare patterns of gray matter loss across groups of subjects with different mutations in the microtubule-associated protein tau (MAPT) gene.

METHODS

We identified all subjects from Mayo Clinic, Rochester, Minnesota, that screened positive for mutations in MAPT and had a head MRI (n = 22). Voxel-based morphometry was used to assess patterns of gray matter atrophy in groups of subjects with the IVS10+16, IVS10+3, N279K, S305N, P301L, and V337M mutations compared with age- and sex-matched controls.

RESULTS

All MAPT groups showed gray matter loss in the anterior temporal lobes, with varying degrees of involvement of the frontal and parietal lobes. Within the temporal lobe, the subjects with IVS10+16, IVS10+3, N279K, and S305N mutations (mutations that influence the alternative splicing of tau pre-messenger RNA) all showed gray matter loss focused on the medial temporal lobes. In contrast to these groups, the subjects with P301L or V337M mutations (mutations that affect the structure of the tau protein) both showed gray matter loss focused on the lateral temporal lobes, with a relative sparing of the medial temporal lobe.

CONCLUSION

There seem to be differences in patterns of temporal lobe atrophy across the MAPT mutations, which may aid in the differentiation of the different mutation carriers. Furthermore, there seems to be a possible association between mutation function and pattern of temporal lobe atrophy.

摘要

目的

采用病例对照研究,评估和比较微管相关蛋白tau(MAPT)基因不同突变的受试者组间灰质丢失模式。

方法

我们从明尼苏达州罗切斯特市梅奥诊所确定了所有筛查MAPT突变呈阳性且进行了头部MRI检查的受试者(n = 22)。与年龄和性别匹配的对照组相比,基于体素的形态学测量用于评估携带IVS10 + 16、IVS10 + 3、N279K、S305N、P301L和V337M突变的受试者组的灰质萎缩模式。

结果

所有MAPT组均显示颞叶前部灰质丢失,额叶和顶叶受累程度各异。在颞叶内,携带IVS10 + 16、IVS10 + 3、N279K和S305N突变(影响tau前体信使RNA可变剪接的突变)的受试者均显示灰质丢失集中在内侧颞叶。与这些组不同,携带P301L或V337M突变(影响tau蛋白结构的突变)的受试者均显示灰质丢失集中在外侧颞叶,内侧颞叶相对 spared。

结论

MAPT突变之间颞叶萎缩模式似乎存在差异,这可能有助于区分不同的突变携带者。此外,突变功能与颞叶萎缩模式之间似乎存在可能的关联。