Hepatocyte-specific Dyrk1a gene transfer rescues plasma apolipoprotein A-I levels and aortic Akt/GSK3 pathways in hyperhomocysteinemic mice |
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| Authors: | Asma Tlili Frank Jacobs Leanne de Koning Sirine Mohamed Linh-Chi Bui Julien Dairou Nicole Belin Véronique Ducros Thierry Dubois Jean-Louis Paul Jean-Maurice Delabar Bart De Geest Nathalie Janel |
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| Institution: | 1. Univ Paris Diderot, Sorbonne Paris Cité, Unit of Functional and Adaptative Biology (BFA), EAC-CNRS 4413, 75013 Paris, France;2. Center for Molecular and Vascular Biology, University of Leuven, Campus Gasthuisberg, 3000 Leuven, Belgium;3. RPPA Platform, Institut Curie Department of Translational Research, 75248 Paris cedex 05, France;4. BioProfiler-UFLC Facilities, Univ Paris Diderot, Sorbonne Paris Cité, BFA, EAC-CNRS 4413, 75013 Paris, France;5. Département de Biochimie Toxicologie & Pharmacologie, IBP-CHU de Grenoble, 38043 Grenoble cedex 9, France;6. Breast Cancer Biology Group, Institut Curie Department of Translational Research, 75248 Paris cedex 05, France;7. AP-HP, Hôpital Européen Georges Pompidou, Service de Biochimie, 75015 Paris, France;8. Univ Paris-Sud, EA 4529, UFR de Pharmacie, 92296 Châtenay-Malabry, France |
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| Abstract: | Hyperhomocysteinemia, characterized by high plasma homocysteine levels, is recognized as an independent risk factor for cardiovascular diseases. The increased synthesis of homocysteine, a product of methionine metabolism involving B vitamins, and its slower intracellular utilization cause increased flux into the blood. Plasma homocysteine level is an important reflection of hepatic methionine metabolism and the rate of processes modified by B vitamins as well as different enzyme activity. Lowering homocysteine might offer therapeutic benefits. However, approximately 50% of hyperhomocysteinemic patients due to cystathionine-beta-synthase deficiency are biochemically responsive to pharmacological doses of B vitamins. Therefore, effective treatments to reduce homocysteine levels are needed, and gene therapy could provide a novel approach. We recently showed that hepatic expression of DYRK1A, a serine/threonine kinase, is negatively correlated with plasma homocysteine levels in cystathionine-beta-synthase deficient mice, a mouse model of hyperhomocysteinemia. Therefore, Dyrk1a is a good candidate for gene therapy to normalize homocysteine levels. We then used an adenoviral construct designed to restrict expression of DYRK1A to hepatocytes, and found decreased plasma homocysteine levels after hepatocyte-specific Dyrk1a gene transfer in hyperhomocysteinemic mice. The elevation of pyridoxal phosphate was consistent with the increase in cystathionine-beta-synthase activity. Commensurate with the decreased plasma homocysteine levels, targeted hepatic expression of DYRK1A resulted in elevated plasma paraoxonase-1 activity and apolipoprotein A-I levels, and rescued the Akt/GSK3 signaling pathways in aorta of mice, which can prevent homocysteine-induced endothelial dysfunction. These results demonstrate that hepatocyte-restricted Dyrk1a gene transfer can offer a useful therapeutic targets for the development of new selective homocysteine lowering therapy. |
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