The Infantile Myofibromatosis NOTCH3 L1519P Mutation Leads to Hyperactivated Ligand-independent Notch Signaling and Increased PDGFRB Expression

Overview

Journal Dis Model Mech

Specialty General Medicine

Date 2021 Jan 29

PMID 33509954

Citations 7

Authors

Dan Wu

Sailan Wang

Daniel V Oliveira

Francesca Del Gaudio

Michael Vanlandewijck

Thibaud Lebouvier

Christer Betsholtz

Jian Zhao

Shaobo Jin

Urban Lendahl

Helena Karlstrom

Affiliations

Soon will be listed here.

Abstract

Infantile myofibromatosis (IMF) is a benign tumor form characterized by the development of nonmetastatic tumors in skin, bone, muscle and sometimes viscera. Autosomal dominant forms of IMF are caused by mutations in the gene, but a family carrying a L1519P mutation in the gene has also recently been identified. In this report, we address the molecular consequences of the NOTCH3 mutation and the relationship between the NOTCH and PDGFRB signaling in IMF. The NOTCH3 receptor generates enhanced downstream signaling in a ligand-independent manner. Despite the enhanced signaling, the NOTCH3 receptor is absent from the cell surface and instead accumulates in the endoplasmic reticulum. Furthermore, the localization of the NOTCH3 receptor in the bipartite, heterodimeric state is altered, combined with avid secretion of the mutated extracellular domain from the cell. Chloroquine treatment strongly reduces the amount of secreted NOTCH3 extracellular domain and decreases signaling. Finally, NOTCH3 upregulates PDGFRB expression in fibroblasts, supporting a functional link between Notch and PDGF dysregulation in IMF. Collectively, our data define a NOTCH3-PDGFRB axis in IMF, where an IMF-mutated NOTCH3 receptor elevates PDGFRB expression. The functional characterization of a ligand-independent gain-of-function NOTCH3 mutation is important for Notch therapy considerations for IMF, including strategies aimed at altering lysosome function.

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