Modeling Phenotypic Heterogeneity of Glycogen Storage Disease Type 1a Liver Disease in Mice by Somatic CRISPR/CRISPR-associated protein 9–Mediated Gene Editing
Rutten, Martijn G S; Derks, Terry G J; Huijkman, Nicolette C A; Bos, Trijnie; Kloosterhuis, Niels J; van de Kolk, Kees C W A; Wolters, Justina C; Koster, Mirjam H; Bongiovanni, Laura; Thomas, Rachel E; de Bruin, Alain; van de Sluis, Bart; Oosterveer, Maaike H
(2021) Hepatology, volume 74, issue 5, pp. 2491 - 2507
(Article)
Abstract
Background and Aims: Patients with glycogen storage disease type 1a (GSD-1a) primarily present with life-threatening hypoglycemia and display severe liver disease characterized by hepatomegaly. Despite strict dietary management, long-term complications still occur, such as liver tumor development. Variations in residual glucose-6-phosphatase (G6PC1) activity likely contribute to phenotypic heterogeneity in biochemical
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symptoms and complications between patients. However, lack of insight into the relationship between G6PC1 activity and symptoms/complications and poor understanding of the underlying disease mechanisms pose major challenges to provide optimal health care and quality of life for GSD-1a patients. Currently available GSD-1a animal models are not suitable to systematically investigate the relationship between hepatic G6PC activity and phenotypic heterogeneity or the contribution of gene-gene interactions (GGIs) in the liver. Approach and Results: To meet these needs, we generated and characterized a hepatocyte-specific GSD-1a mouse model using somatic CRISPR/CRISPR-associated protein 9 (Cas9)–mediated gene editing. Hepatic G6pc editing reduced hepatic G6PC activity up to 98% and resulted in failure to thrive, fasting hypoglycemia, hypertriglyceridemia, hepatomegaly, hepatic steatosis (HS), and increased liver tumor incidence. This approach was furthermore successful in simultaneously modulating hepatic G6PC and carbohydrate response element-binding protein, a transcription factor that is activated in GSD-1a and protects against HS under these conditions. Importantly, it also allowed for the modeling of a spectrum of GSD-1a phenotypes in terms of hepatic G6PC activity, fasting hypoglycemia, hypertriglyceridemia, hepatomegaly and HS. Conclusions: In conclusion, we show that somatic CRISPR/Cas9-mediated gene editing allows for the modeling of a spectrum of hepatocyte-borne GSD-1a disease symptoms in mice and to efficiently study GGIs in the liver. This approach opens perspectives for translational research and will likely contribute to personalized treatments for GSD-1a and other genetic liver diseases.
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Keywords: Hepatology
ISSN: 0270-9139
Publisher: John Wiley and Sons Ltd
Note: Funding Information: We thank S. de Neck, Y.T. van der Veen, J. van der Krogt, T.H. van Dijk, R. Havinga, F. Kuipers, I.A. Martini, M. Koehorst, V.W. Bloks, A. de Haan, A. Bleeker, J.A. Hoogerland, K.A. Krishnamurthy, M. Vos, A.J.C. Tol, and A.H. Heida for excellent technical assistance. We thank J. Chou (NIH) for providing us with the protocols for the microsomal preparations and phosphohydrolase assays and M.J. Lizak (NIH) for support with MRI procedures. We thank W.H. Lamers (Academic Medical Center) for providing us with the CK19 antibody. Funding Information: Supported by a VIDI grant (91717373) from the Dutch Scientific Organization and by the UMCG Cancer Research Foundation. M.H.O holds a Rosalind Franklin Fellowship from the University of Groningen. Publisher Copyright: © 2021 The Authors. Hepatology published by Wiley Periodicals LLC on behalf of American Association for the Study of Liver Diseases.
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