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Phenotypes associated with this allele
Allele Symbol
Allele Name
Allele ID 		Usp20em1Gpt
endonuclease-mediated mutation 1, GemPharmatech Co., Ltd
MGI:6515593
Summary 2 genotypes
Jump to Allelic Composition Genetic Background Genotype ID
cn1
 		Usp20em1Gpt/Usp20em1Gpt
Speer6-ps1Tg(Alb-cre)21Mgn/Speer6-ps1+ 		involves: C57BL/6JGpt * DBA MGI:6515651
cn2
 		Hmgcrem1Bcgen/Hmgcrem1Bcgen
Usp20em1Gpt/Usp20em1Gpt
Speer6-ps1Tg(Alb-cre)21Mgn/Speer6-ps1+ 		involves: C57BL/6JGpt * DBA MGI:6515654


Genotype
MGI:6515651
cn1
Allelic
Composition		 Usp20em1Gpt/Usp20em1Gpt
Speer6-ps1Tg(Alb-cre)21Mgn/Speer6-ps1+
Genetic
Background		 involves: C57BL/6JGpt * DBA
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Speer6-ps1Tg(Alb-cre)21Mgn mutation (6 available); any Speer6-ps1 mutation (4 available)
Usp20em1Gpt mutation (0 available); any Usp20 mutation (49 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
homeostasis/metabolism
homeostasis/metabolism phenotype ( J:299971 )
N
• mice fed a high-fat and high-sucrose diet exhibit normal respiratory exchange ratio
decreased circulating glucose level ( J:299971 )
• in fasted and refed mice
decreased fasting circulating glucose level ( J:299971 )
• in fasted and refed mice
decreased circulating insulin level ( J:299971 )
• in refed mice
• however, fasted mice exhibit normal levels
decreased circulating cholesterol level ( J:299971 )
• in fasted and refed mice
• treatment with GSK2643943A does not alter cholesterol levels
• however, adenoviral expression of HMGCR with the point mutation K248R exhibit rescued phenotype
decreased circulating HDL cholesterol level ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
decreased circulating LDL cholesterol level ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
decreased circulating triglyceride level ( J:299971 )
• in fasted and refed mice
• treatment with GSK2643943A does not alter triglyceride levels
• however, adenoviral expression of HMGCR with the point mutation K248R exhibit rescued phenotype
decreased circulating VLDL triglyceride level ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
increased body surface temperature ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
increased energy expenditure ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
• treatment with GSK2643943A does not ameliorate energy expenditure
• however, adenoviral expression of HMGCR with the point mutation K248R exhibit rescued phenotype
abnormal enzyme/coenzyme level ( J:299971 )
• increased liver levels of HMG-CoA and succinate
• decreased liver levels of succinyl-CoA
abnormal circulating enzyme level ( J:299971 )
• doubled serum succinate levels
increased oxygen consumption ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
improved glucose tolerance ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
• treatment with GSK2643943A does not alter glucose clearance
• however, adenoviral expression of HMGCR with the point mutation K248R exhibit rescued phenotype
increased insulin sensitivity ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
decreased liver cholesterol level ( J:299971 )
• in fasted and refed mice
decreased liver triglyceride level ( J:299971 )
• in fasted and refed mice
• decreased VLDL, LDL, and HDL

liver/biliary system
abnormal liver morphology ( J:299971 )
• reduced fat accumulation when mice are fed a high-fat and high-sucrose diet
decreased liver cholesterol level ( J:299971 )
• in fasted and refed mice
decreased liver triglyceride level ( J:299971 )
• in fasted and refed mice
• decreased VLDL, LDL, and HDL
decreased liver weight ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet

growth/size/body
decreased body fat mass ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
• however, adenoviral expression of HMGCR with the point mutation K248R exhibit rescued phenotype
decreased body weight ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
• however, lean body mass to body weight is normal

behavior/neurological
behavior/neurological phenotype ( J:299971 )
N
• mice fed a high-fat and high-sucrose diet exhibit normal physical activity

adipose tissue
decreased body fat mass ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet
• however, adenoviral expression of HMGCR with the point mutation K248R exhibit rescued phenotype
decreased fat cell size ( J:299971 )
• reduced area
decreased white adipose tissue mass ( J:299971 )
• when mice are fed a high-fat and high-sucrose diet




Genotype
MGI:6515654
cn2
Allelic
Composition		 Hmgcrem1Bcgen/Hmgcrem1Bcgen
Usp20em1Gpt/Usp20em1Gpt
Speer6-ps1Tg(Alb-cre)21Mgn/Speer6-ps1+
Genetic
Background		 involves: C57BL/6JGpt * DBA
Find Mice Using the International Mouse Strain Resource (IMSR)
Mouse lines carrying:
Hmgcrem1Bcgen mutation (0 available); any Hmgcr mutation (59 available)
Speer6-ps1Tg(Alb-cre)21Mgn mutation (6 available); any Speer6-ps1 mutation (4 available)
Usp20em1Gpt mutation (0 available); any Usp20 mutation (49 available)
phenotype observed in females
phenotype observed in males
N normal phenotype
homeostasis/metabolism
homeostasis/metabolism phenotype ( J:299971 )
N
• mice fed a high-fat and high-sucrose diet exhibit normal total cholesterol levels in fasted and refed mice, oxygen consumption, and glucose tolerance
increased circulating triglyceride level ( J:299971 )
• in fasted and refed mice fed a high-fat and high-sucrose diet




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Send questions and comments to User Support. 		last database update
04/23/2024
MGI 6.23 		The Jackson Laboratory