Truncation of mutant huntingtin in knock-in mice demonstrates exon1 huntingtin is a key pathogenic form

Huiming Yang; Su Yang; Liang Jing; Luoxiu Huang; Luxiao Chen; Xianxian Zhao; Weili Yang; Yongcheng Pan; Peng Yin; Zhaohui S. Qin; Shihua Li; Xiao-Jiang Li

doi:https://doi.org/10.1038/s41467-020-16318-1

doi.org/10.1038/s41467-020-16318-1

Truncation of mutant huntingtin in knock-in mice demonstrates exon1 huntingtin is a key pathogenic form

,

,

..., Xiao-Jiang Li

67

Nature Communications16.60

Volume: 11, Issue: 1

Published: May 22, 2020

Abstract

Polyglutamine expansion in proteins can cause selective neurodegeneration, although the mechanisms are not fully understood. In Huntington's disease (HD), proteolytic processing generates toxic N-terminal huntingtin (HTT) fragments that preferentially kill striatal neurons. Here, using CRISPR/Cas9 to truncate full-length mutant HTT in HD140Q knock-in (KI) mice, we show that exon 1 HTT is stably present in the brain, regardless of truncation...

Paper Fields

Paper Details

Title

Truncation of mutant huntingtin in knock-in mice demonstrates exon1 huntingtin is a key pathogenic form

DOI

doi.org/10.1038/s41467-020-16318-1

Published Date

May 22, 2020

Journal

Nature Communications

Volume

11

Issue

1

Citation AnalysisPro

You’ll need to upgrade your plan to Pro

Looking to understand the true influence of a researcher’s work across journals & affiliations?

Scinapse’s Top 10 Citation Journals & Affiliations graph reveals the quality and authenticity of citations received by a paper.
Discover whether citations have been inflated due to self-citations, or if citations include institutional bias.

Learn more

Notes

History