Published November 27, 2020 | Version 1
Dataset Open

MSN (Moesin); A Target Enabling Package

Creators

  • 1. Structural Genomics Consortium
  • 2. Department of Pharmacology & Chemical Biology, Emory University

Description

Moesin (MSN; membrane-organizing extension spike protein) contains a FERM domain (Four-point-1, Ezrin, Radixin, Moesin) that links transmembrane receptors such as CD44 to the actin cytoskeleton, in a manner regulated by phosphorylation and PIP2. A proteomic, post-mortem analysis of >400 brains identified a protein co-expression module that is highly correlated with pathological and cognitive measures of Alzheimer’s disease (AD). Moesin and CD44 have emerged as key drivers in the module. MSN is highly expressed in microglia and brain endothelium (as well as several non-brain tissues). This TEP targets the CD44-MSN interaction, to test the hypothesis that inhibiting the CD44-MSN interaction would reverse harmful activities of microglia and provide beneficial outcomes for AD patients.

Notes

This document represents version 1 of the TEP datasheet and includes all updates on the project as of November 2020. For more information about TEPs and the TEP Programme, please visit https://thesgc.org/tep.

Files

MSN TEP_v1.pdf

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Additional details

Related works

Is part of
https://www.thesgc.org/tep (URL)

Funding

A UK Hub to Catalyse Open Target Discovery. 106169
Wellcome Trust