Effects of genetic variations in the dystonia protein torsinA: identification of polymorphism at residue 216 as protein modifier

生物 突变体 遗传学 编码区 点突变 基因 等位基因 组氨酸 蛋白质结构 生物化学 氨基酸
作者
Norman Kock,Teresa V. Naismith,Heather Boston,Laurie J. Ozelius,David P. Corey,Xandra O. Breakefield,Phyllis I. Hanson
出处
期刊:Human Molecular Genetics [Oxford University Press]
卷期号:15 (8): 1355-1364 被引量:94
标识
DOI:10.1093/hmg/ddl055
摘要

Four naturally occurring sequence variations have been found in the coding region of the DYT1 gene encoding torsinA. One of these, a 3 bp (ΔGAG) deletion, underlies dominantly inherited cases of early-onset torsion dystonia. Others, including a single nucleotide polymorphism that replaces aspartic acid (D) at residue 216 with histidine (H) in 12% of normal alleles and two other rare deletions, have not been clearly associated with disease. To gain insight into how these sequence variations affect torsinA, we used the structure of the related protein ClpB to provide a model of torsinA's AAA+ domain. Motifs important for ATP hydrolysis—sensor 1 and sensor 2—were identified, mutagenized and used to validate predictions of this model. Inspection revealed that the ΔGAG deletion associated with dystonia removes one residue from an α-helix in the C-terminal portion of the AAA+ domain. The resulting distortion in torsinA structure may underlie this mutant's known tendency to produce ER-derived inclusions as well as its proposed loss of function. The D/H polymorphism at residue 216 falls in the N-terminal portion of the AAA+ domain near the sensor 1 motif. Surprisingly, cells expressing torsinA with the polymorphic histidine developed inclusions similar to those associated with ΔGAG-torsinA, indicating that this change may also affect torsinA structure. Introducing H216 into ΔGAG-torsinA reduced its tendency to form inclusions, suggesting that the two changes offset each other. Our findings point to a structural basis for the defects associated with the disease-linked ΔGAG deletion in torsinA. They also suggest possible connections between the allelic polymorphism at residue 216 and the penetrance of DYT1 dystonia, as well as a possible role for this polymorphism in related disease states.
最长约 10秒,即可获得该文献文件

科研通智能强力驱动
Strongly Powered by AbleSci AI
科研通是完全免费的文献互助平台,具备全网最快的应助速度,最高的求助完成率。 对每一个文献求助,科研通都将尽心尽力,给求助人一个满意的交代。
实时播报
3秒前
sunnyqqz完成签到,获得积分10
3秒前
林枫完成签到,获得积分10
5秒前
西瓜西瓜完成签到,获得积分10
5秒前
2275523154完成签到,获得积分10
6秒前
HH完成签到,获得积分10
17秒前
ding应助朱洪帆采纳,获得10
19秒前
19秒前
呀呀呀完成签到,获得积分10
21秒前
plant完成签到,获得积分10
22秒前
mm完成签到 ,获得积分10
22秒前
Song完成签到 ,获得积分10
23秒前
HuangShuting发布了新的文献求助10
23秒前
哆啦啦啦A梦完成签到 ,获得积分10
23秒前
26秒前
神勇的天问完成签到 ,获得积分10
27秒前
荣幸完成签到 ,获得积分10
29秒前
30秒前
双双完成签到,获得积分10
32秒前
随风沙ZYX完成签到 ,获得积分10
32秒前
33秒前
朱洪帆完成签到,获得积分20
33秒前
33秒前
Xue完成签到 ,获得积分10
34秒前
朱洪帆发布了新的文献求助10
36秒前
科研王子完成签到 ,获得积分10
37秒前
w0r1d完成签到 ,获得积分10
39秒前
cocofan完成签到 ,获得积分10
42秒前
务实白开水完成签到 ,获得积分10
46秒前
47秒前
47秒前
hj123完成签到,获得积分10
51秒前
沐偶发布了新的文献求助10
52秒前
59秒前
大模型应助科研通管家采纳,获得10
59秒前
Kao应助苹果松采纳,获得10
1分钟前
bill完成签到,获得积分0
1分钟前
Ws完成签到,获得积分10
1分钟前
qqq完成签到 ,获得积分0
1分钟前
yellow完成签到,获得积分10
1分钟前
高分求助中
Principles of Economics, 11th Edition 10000
University Physics with Modern Physics, 16th edition 10000
(应助此贴封号)【重要!!请各用户(尤其是新用户)详细阅读】【科研通的精品贴汇总】 10000
48V Low-voltage Power Distribution Network (PDN) Architecture Industry Report, 2024 800
ズームレンズの光学設計に関する研究 800
Fundamentals of Pharmaceutical and Biologics Regulations: A Global Perspective, Second Edition 700
Matrix Methods in Data Mining and Pattern Recognition Second Edition 610
热门求助领域 (近24小时)
化学 材料科学 医学 生物 纳米技术 工程类 有机化学 化学工程 生物化学 计算机科学 内科学 物理 复合材料 催化作用 细胞生物学 无机化学 光电子学 物理化学 电极 基因
热门帖子
关注 科研通微信公众号,转发送积分 7298296
求助须知:如何正确求助?哪些是违规求助? 8916642
关于积分的说明 18879477
捐赠科研通 6963240
什么是DOI,文献DOI怎么找? 3210642
关于科研通互助平台的介绍 2379958
邀请新用户注册赠送积分活动 2187125