Global Rhes knockout in the Q175 Huntington's disease mouse model.
Taneli HeikkinenTimo BraggeJuha KuosmanenTeija ParkkariSanna GustafssonMei KwanJose BeltranAfshin GhavamiSrinivasa SubramaniamNeelam ShahaniUri Nimrod Ramírez-JarquínLarry ParkIgnacio Muñoz-SanjuánDeanna M MarchioniniPublished in: PloS one (2021)
Huntington's disease (HD) results from an expansion mutation in the polyglutamine tract in huntingtin. Although huntingtin is ubiquitously expressed in the body, the striatum suffers the most severe pathology. Rhes is a Ras-related small GTP-binding protein highly expressed in the striatum that has been reported to modulate mTOR and sumoylation of mutant huntingtin to alter HD mouse model pathogenesis. Reports have varied on whether Rhes reduction is desirable for HD. Here we characterize multiple behavioral and molecular endpoints in the Q175 HD mouse model with genetic Rhes knockout (KO). Genetic RhesKO in the Q175 female mouse resulted in both subtle attenuation of Q175 phenotypic features, and detrimental effects on other kinematic features. The Q175 females exhibited measurable pathogenic deficits, as measured by MRI, MRS and DARPP32, however, RhesKO had no effect on these readouts. Additionally, RhesKO in Q175 mixed gender mice deficits did not affect mTOR signaling, autophagy or mutant huntingtin levels. We conclude that global RhesKO does not substantially ameliorate or exacerbate HD mouse phenotypes in Q175 mice.
Keyphrases
- mouse model
- wild type
- traumatic brain injury
- binding protein
- cell proliferation
- genome wide
- high fat diet induced
- magnetic resonance imaging
- mental health
- copy number
- oxidative stress
- computed tomography
- signaling pathway
- emergency department
- metabolic syndrome
- type diabetes
- contrast enhanced
- magnetic resonance
- endoplasmic reticulum stress
- skeletal muscle
- adipose tissue