Fumarate hydratase is a critical metabolic regulator of hematopoietic stem cell functions

Pollard, P. J.; So, C. W.; O'Carroll, D.; Vernimmen, D.; Rodrigues, N. P.; Morton, N. M.; Kranc, K. R.; Finch, A.; Guitart, A. V.; Panagopoulou, T. I.; Villacreces, A.; Vukovic, M.; Sepulveda, C.; Allen, L.; Carter, R. N.; van de Lagemaat, L. N.; Morgan, M.; Giles, P.; Sas, Z.; Gonzalez, M. V.; Lawson, H.; Paris, J.; Edwards-Hicks, J.; Schaak, K.; Subramani, C.; Gezer, D.; Armesilla-Diaz, A.; Wills, J.; Easterbrook, A.; Coman, D.

Please use this identifier to cite or link to this item: https://dora.health.qld.gov.au/qldresearchjspui/handle/1/3064

Title:	Fumarate hydratase is a critical metabolic regulator of hematopoietic stem cell functions
Authors:	Pollard, P. J. So, C. W. O'Carroll, D. Vernimmen, D. Rodrigues, N. P. Morton, N. M. Kranc, K. R. Finch, A. Guitart, A. V. Panagopoulou, T. I. Villacreces, A. Vukovic, M. Sepulveda, C. Allen, L. Carter, R. N. van de Lagemaat, L. N. Morgan, M. Giles, P. Sas, Z. Gonzalez, M. V. Lawson, H. Paris, J. Edwards-Hicks, J. Schaak, K. Subramani, C. Gezer, D. Armesilla-Diaz, A. Wills, J. Easterbrook, A. Coman, D.
Issue Date:	2017
Source:	214, (3), 2017, p. 719-735
Pages:	719-735
Journal:	The Journal of experimental medicine
Abstract:	Strict regulation of stem cell metabolism is essential for tissue functions and tumor suppression. In this study, we investigated the role of fumarate hydratase (Fh1), a key component of the mitochondrial tricarboxylic acid (TCA) cycle and cytosolic fumarate metabolism, in normal and leukemic hematopoiesis. Hematopoiesis-specific Fh1 deletion (resulting in endogenous fumarate accumulation and a genetic TCA cycle block reflected by decreased maximal mitochondrial respiration) caused lethal fetal liver hematopoietic defects and hematopoietic stem cell (HSC) failure. Reexpression of extramitochondrial Fh1 (which normalized fumarate levels but not maximal mitochondrial respiration) rescued these phenotypes, indicating the causal role of cellular fumarate accumulation. However, HSCs lacking mitochondrial Fh1 (which had normal fumarate levels but defective maximal mitochondrial respiration) failed to self-renew and displayed lymphoid differentiation defects. In contrast, leukemia-initiating cells lacking mitochondrial Fh1 efficiently propagated Meis1/Hoxa9-driven leukemia. Thus, we identify novel roles for fumarate metabolism in HSC maintenance and hematopoietic differentiation and reveal a differential requirement for mitochondrial Fh1 in normal hematopoiesis and leukemia propagation.L6178868502017-08-23
DOI:	10.1084/jem.20161087
Resources:	https://www.embase.com/search/results?subaction=viewrecord&id=L617886850&from=exporthttp://dx.doi.org/10.1084/jem.20161087 \|
Keywords:	C57BL mouse;female;hematopoiesis;hematopoietic stem cell;acute myeloid leukemia;metabolism;mitochondrion;mouse;oxygen consumption;physiology;transcription factor Nrf2;Nfe2l2 protein, mouse;histone;fumarate hydratasefumaric acid derivative;animal
Type:	Article
Appears in Sites:	Children's Health Queensland Publications

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