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Altered Body Weight Regulation in CK1ε Null and tau Mutant Mice on Regular Chow and High Fat Diets
by
Keith C. Summa
, Christopher Olker
, Martha H. Vitaterna
, Lili Zhou
, Fred W. Turek
in
Body temperature
/ Body weight
/ Body weight gain
/ Casein
/ Casein kinase I
/ Circadian rhythm
/ Circadian rhythms
/ Clock gene
/ Diet
/ Entrainment
/ Experiments
/ Food intake
/ Gene expression
/ High fat diet
/ Insulin
/ Kinases
/ Metabolism
/ Mutants
/ Mutation
/ Obesity
/ Proteins
2016
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Altered Body Weight Regulation in CK1ε Null and tau Mutant Mice on Regular Chow and High Fat Diets
by
Keith C. Summa
, Christopher Olker
, Martha H. Vitaterna
, Lili Zhou
, Fred W. Turek
in
Body temperature
/ Body weight
/ Body weight gain
/ Casein
/ Casein kinase I
/ Circadian rhythm
/ Circadian rhythms
/ Clock gene
/ Diet
/ Entrainment
/ Experiments
/ Food intake
/ Gene expression
/ High fat diet
/ Insulin
/ Kinases
/ Metabolism
/ Mutants
/ Mutation
/ Obesity
/ Proteins
2016
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Altered Body Weight Regulation in CK1ε Null and tau Mutant Mice on Regular Chow and High Fat Diets
by
Keith C. Summa
, Christopher Olker
, Martha H. Vitaterna
, Lili Zhou
, Fred W. Turek
in
Body temperature
/ Body weight
/ Body weight gain
/ Casein
/ Casein kinase I
/ Circadian rhythm
/ Circadian rhythms
/ Clock gene
/ Diet
/ Entrainment
/ Experiments
/ Food intake
/ Gene expression
/ High fat diet
/ Insulin
/ Kinases
/ Metabolism
/ Mutants
/ Mutation
/ Obesity
/ Proteins
2016
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Altered Body Weight Regulation in CK1ε Null and tau Mutant Mice on Regular Chow and High Fat Diets
Journal Article
Altered Body Weight Regulation in CK1ε Null and tau Mutant Mice on Regular Chow and High Fat Diets
2016
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Overview
Disruption of circadian rhythms results in metabolic dysfunction. Casein kinase 1 epsilon (CK1ε) is a canonical circadian clock gene. Null and tau mutations in CK1ε show distinct effects on circadian period. To investigate the role of CK1ε in body weight regulation under both regular chow (RC) and high fat (HF) diet conditions, we examined body weight on both RC and HF diets in CK1ε-/- and CK1εtau/tau mice on a standard 24 hr light-dark (LD) cycle. Given the abnormal entrainment of CK1εtau/tau mice on a 24 hr LD cycle, a separate set of CK1εtau/tau mice were tested under both diet conditions on a 20 hr LD cycle, which more closely matches their endogenous period length. On the RC diet, both CK1ε-/- and CK1εtau/tau mutants on a 24 hr LD cycle and CK1εtau/tau mice on a 20 hr LD cycle exhibited significantly lower body weights, despite similar overall food intake and activity levels. On the HF diet, CK1εtau/tau mice on a 20 hr LD cycle were protected against the development of HF diet-induced excess weight gain. These results provide additional evidence supporting a link between circadian rhythms and energy regulation at the genetic level, particularly highlighting CK1ε involved in the integration of circadian biology and metabolic physiology.
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