亨廷顿蛋白 HTT1a 在人类组织中以 CAG 重复长度依赖性方式产生。
Huntingtin HTT1a is generated in a CAG repeat-length-dependent manner in human tissues.
机构信息
Department of Neurology, University Hospital Ulm, 89081, Ulm, Germany.
Huntington's Disease Centre, Department of Neurodegenerative Disease, Queen Square Institute of Neurology, University College London, WC1N 3BG, London, UK.
出版信息
Mol Med. 2024 Mar 8;30(1):36. doi: 10.1186/s10020-024-00801-2.
BACKGROUND
The disease-causing mutation in Huntington disease (HD) is a CAG trinucleotide expansion in the huntingtin (HTT) gene. The mutated CAG tract results in the production of a small RNA, HTT1a, coding for only exon 1 of HTT. HTT1a is generated by a block in the splicing reaction of HTT exon 1 to exon 2 followed by cleavage in intron 1 and polyadenylation. Translation of HTT1a leads to the expression of the highly toxic HTT exon 1 protein fragment. We have previously shown that the levels of HTT1a expression in mouse models of HD is dependent on the CAG repeat length. However, these data are lacking for human tissues.
METHODS
To answer this question, we developed highly sensitive digital PCR assays to determine HTT1a levels in human samples. These assays allow the absolute quantification of transcript numbers and thus also facilitate the comparison of HTT1a levels between tissues, cell types and across different studies. Furthermore, we measured CAG repeat sizes for every sample used in the study. Finally, we analysed our data with ANOVA and linear modelling to determine the correlation of HTT1a expression levels with CAG repeat sizes.
RESULTS
In summary, we show that HTT1a is indeed expressed in a CAG repeat-length-dependent manner in human post mortem brain tissues as well as in several peripheral cell types. In particular, PBMCs show a statistically significant positive correlation of HTT1a expression with CAG repeat length, and elevated HTT1a expression levels even in the adult-onset CAG repeat range.
CONCLUSIONS
Our results show that HTT1a expression occurs throughout a wide range of tissues and likely with all CAG lengths. Our data from peripheral sample sources demonstrate that HTT1a is indeed generated throughout the body in a CAG repeat-length-dependent manner. Therefore, the levels of HTT1a might be a sensitive marker of disease state and/or progression and should be monitored over time, especially in clinical trials targeting HTT expression.
背景
亨廷顿病(HD)的致病突变是亨廷顿(HTT)基因中的 CAG 三核苷酸扩展。突变的 CAG 片段导致小 RNA HTT1a 的产生,仅编码 HTT 的外显子 1。HTT1a 的产生是由于 HTT 外显子 1 到外显子 2 的剪接反应受阻,然后在内含子 1 中切割并多聚腺苷酸化。HTT1a 的翻译导致高度毒性的 HTT 外显子 1 蛋白片段的表达。我们之前已经表明,HD 小鼠模型中 HTT1a 的表达水平取决于 CAG 重复长度。然而,这些数据在人体组织中缺乏。
方法
为了回答这个问题,我们开发了高度敏感的数字 PCR 测定法来确定人类样本中的 HTT1a 水平。这些测定法允许对转录物数量进行绝对定量,从而还便于比较组织、细胞类型和不同研究之间的 HTT1a 水平。此外,我们还为研究中使用的每个样本测量了 CAG 重复大小。最后,我们使用方差分析和线性建模分析我们的数据,以确定 HTT1a 表达水平与 CAG 重复大小的相关性。
结果
总之,我们表明,HTT1a 确实以 CAG 重复长度依赖的方式在人类死后脑组织以及几种外周细胞类型中表达。特别是,PBMC 显示 HTT1a 表达与 CAG 重复长度呈统计学上显著的正相关,并且即使在成人发病的 CAG 重复范围内也存在升高的 HTT1a 表达水平。
结论
我们的结果表明,HTT1a 在广泛的组织中表达,并且可能与所有 CAG 长度都存在。我们来自外周样本来源的数据表明,HTT1a 确实以 CAG 重复长度依赖的方式在整个体内产生。因此,HTT1a 的水平可能是疾病状态和/或进展的敏感标志物,应随时间进行监测,特别是在针对 HTT 表达的临床试验中。
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