Issue 40, 2020
From the journal:

Chemical Communications

Uncovering the pathological functions of Ser404 phosphorylation by semisynthesis of a phosphorylated TDP-43 prion-like domain

Qian-Qian Li,a   Yu-Qing Liu,a   Yun-Yi Luo,a   Ting-Ting Chu,a   Na Gao,a   Pu-Guang Chen,a   Yong-Xiang Chen ORCID logo a  and  Yan-Mei Li ORCID logo *ab  

* Corresponding authors

a Key Lab of Bioorganic Phosphorus Chemistry & Chemical Biology, Department of Chemistry, Center for Synthetic & Systems Biology, Tsinghua University, Beijing 100084, P. R. China
E-mail: liym@mail.tsinghua.edu.cn

b Beijing Institute for Braifn Disorders, Beijing 100069, P. R. China

Abstract

Herein, we have successfully semi-synthesized a TDP-43 prion-like domain with Ser404 phosphorylation. We have demonstrated that Ser404 phosphorylation could accelerate the amyloid aggregation of the TDP-43 prion-like domain and aggravate its cytotoxicity.

Graphical abstract: Uncovering the pathological functions of Ser404 phosphorylation by semisynthesis of a phosphorylated TDP-43 prion-like domain

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Article information

DOI
https://doi.org/10.1039/D0CC01409E
Article type
Communication
Submitted
23 Feb 2020
Accepted
30 Mar 2020
First published
30 Mar 2020

Chem. Commun., 2020,56, 5370-5373

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Uncovering the pathological functions of Ser404 phosphorylation by semisynthesis of a phosphorylated TDP-43 prion-like domain

Q. Li, Y. Liu, Y. Luo, T. Chu, N. Gao, P. Chen, Y. Chen and Y. Li, Chem. Commun., 2020, 56, 5370 DOI: 10.1039/D0CC01409E

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