Arginine methylation by PRMT5 at a naturally occurring mutation site Is critical for liver metabolic regulation by small heterodimer partner

Keyphrases

• Liver 100%
• Metabolic Regulation 100%
• Naturally Occurring mutations 100%
• Mutation Sites 100%
• Small Heterodimer Partner 100%
• Arginine Methylation 100%
• Protein Arginine Methyltransferase 5 (PRMT5) 100%
• Methylation 21%
• Metabolic Syndrome 14%
• Bile Acids 14%
• Post-translational Modification 7%
• Overexpression 7%
• Gene Expression 7%
• Transcription Factor 7%
• Human Disease 7%
• Glucose Metabolism 7%
• Biological Processes 7%
• Adenovirus 7%
• Metabolic Genes 7%
• Therapeutic Strategies 7%
• Lipid Metabolism 7%
• Triglyceride Level 7%
• Infertility 7%
• Post-translational 7%
• Hepatic Fat 7%
• Glucose Tolerance 7%
• Histone Deacetylase 1 (HDAC1) 7%
• Natural mutation 7%
• Metabolic Outcomes 7%
• Partner Interaction 7%
• MSin3A 7%
• Metabolic Targets 7%

Biochemistry, Genetics and Molecular Biology

• Methylation 100%
• Metabolic Regulation 100%
• Protein Arginine Methyltransferase 5 100%
• Arginine 100%
• Bile Acid 33%
• Gene Expression 16%
• Transcription Factors 16%
• Posttranslational Modification 16%
• Glucose Metabolism 16%
• Biological Phenomena and Functions Concerning the Entire Organism 16%
• Lipid Metabolism 16%
• Triacylglycerol Level 16%
• HDAC1 16%
• Adenoviridae 16%