The Unfolded Protein Response Governs Integrity of the Haematopoietic Stem-cell Pool During Stress

Overview

Journal Nature

Specialty Science

Date 2014 Apr 30

PMID 24776803

Citations 181

Authors

Peter van Galen

Antonija Kreso

Nathan Mbong

David G Kent

Timothy Fitzmaurice

Joseph E Chambers

Stephanie Xie

Elisa Laurenti

Karin Hermans

Kolja Eppert

Stefan J Marciniak

Jane C Goodall

Anthony R Green

Bradly G Wouters

Erno Wienholds

John E Dick

Affiliations

Soon will be listed here.

Abstract

The blood system is sustained by a pool of haematopoietic stem cells (HSCs) that are long-lived due to their capacity for self-renewal. A consequence of longevity is exposure to stress stimuli including reactive oxygen species (ROS), nutrient fluctuation and DNA damage. Damage that occurs within stressed HSCs must be tightly controlled to prevent either loss of function or the clonal persistence of oncogenic mutations that increase the risk of leukaemogenesis. Despite the importance of maintaining cell integrity throughout life, how the HSC pool achieves this and how individual HSCs respond to stress remain poorly understood. Many sources of stress cause misfolded protein accumulation in the endoplasmic reticulum (ER), and subsequent activation of the unfolded protein response (UPR) enables the cell to either resolve stress or initiate apoptosis. Here we show that human HSCs are predisposed to apoptosis through strong activation of the PERK branch of the UPR after ER stress, whereas closely related progenitors exhibit an adaptive response leading to their survival. Enhanced ER protein folding by overexpression of the co-chaperone ERDJ4 (also called DNAJB9) increases HSC repopulation capacity in xenograft assays, linking the UPR to HSC function. Because the UPR is a focal point where different sources of stress converge, our study provides a framework for understanding how stress signalling is coordinated within tissue hierarchies and integrated with stemness. Broadly, these findings reveal that the HSC pool maintains clonal integrity by clearance of individual HSCs after stress to prevent propagation of damaged stem cells.

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