NEDD4 and NEDD4L regulate Wnt signalling and intestinal stem cell priming by degrading LGR5 receptor.

Laura Novellasdemunt,Helmuth Gehart,Cara Jamieson,Anna Kucharska,Anna Baulies,Pedro Antas,Maria Prange‐Barczynska,Vivian Sw Li,Jelte Van Der Vaart,Madelon M Maurice

doi:10.15252/embj.2019102771

Laura Novellasdemunt, Helmuth Gehart + Show 8 more

Open Access

https://doi.org/10.15252/embj.2019102771

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Abstract

The intestinal stem cell (ISC) marker LGR5 is a receptor for R‐spondin (RSPO) that functions to potentiate Wnt signalling in the proliferating crypt. It has been recently shown that Wnt plays a priming role for ISC self‐renewal by inducing RSPO receptor LGR5 expression. Despite its pivotal role in homeostasis, regeneration and cancer, little is known about the post‐translational regulation of LGR5. Here, we show that the HECT‐domain E3 ligases NEDD4 and NEDD4L are expressed in the crypt stem cell regions and regulate ISC priming by degrading LGR receptors. Loss of Nedd4 and Nedd4l enhances ISC proliferation, increases sensitivity to RSPO stimulation and accelerates tumour development in Apcmin mice with increased numbers of high‐grade adenomas. Mechanistically, we find that both NEDD4 and NEDD4L negatively regulate Wnt/β‐catenin signalling by targeting LGR5 receptor and DVL2 for proteasomal and lysosomal degradation. Our findings unveil the previously unreported post‐translational control of LGR receptors via NEDD4/NEDD4L to regulate ISC priming. Inactivation of NEDD4 and NEDD4L increases Wnt activation and ISC numbers, which subsequently enhances tumour predisposition and progression.

Highlights

The intestinal epithelium is constantly self-renewed through a small population of stem cells localised at the bottom of the crypts that continuously regenerate new epithelial cells (Cheng & Leblond, 1974)
The bona fide intestinal stem cell (ISC) marker leucine-rich repeat containing G protein-coupled receptor 5 (LGR5) is expressed exclusively at the intestinal crypt base under tight regulation, while LGR5+ ISCs are indispensable for regeneration and tumourigenesis (Metcalfe et al, 2014; de Sousa e Melo et al, 2017)
This is the first study describing the post-translational modification of LGR5 receptors via the E3 ubiquitin ligases NEDD4 and NEDD4L

Summary

Introduction

The intestinal epithelium is constantly self-renewed through a small population of stem cells localised at the bottom of the crypts that continuously regenerate new epithelial cells (Cheng & Leblond, 1974) These ISCs are maintained by a Wnt gradient at the intestinal crypts during homeostasis. Wnt signalling pathway plays central role in multiple cellular processes such as stem cell maintenance and cell fate decision (Clevers & Nusse, 2012) Perturbation of this pathway impairs tissue homeostasis, leading to many diseases including cancer and metabolic disorders (MacDonald et al, 2009; Clevers & Nusse, 2012; Novellasdemunt et al, 2015). Little is known about the post-translational regulation of LGR5 protein stability

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