FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2022791592> ?p ?o ?g. }

• W2022791592 endingPage "1105" @default.
• W2022791592 startingPage "1095" @default.
• W2022791592 abstract "Huntington disease (HD), an autosomal dominant neurodegenerative disorder caused by an abnormal expansion of CAG trinucleotide repeat in the Huntingtin (HTT) gene, is characterized by extensive neurodegeneration of striatum and cortex and severe diffuse atrophy at MRI. The expression of genes involved in the cholesterol biosynthetic pathway and the amount of cholesterol, lanosterol, lathosterol and 24S-hydroxycholesterol were reduced in murine models of HD. In case of HD-patients, the decrease of plasma 24OHC follows disease progression proportionally to motor and neuropsychiatric dysfunction and MRI brain atrophy, together with lanosterol and lathosterol (markers of cholesterol synthesis), and 27-hydroxycholesterol. A significant reduction of total plasma cholesterol was observed only in advanced stages. It is likely that mutant HTT decreases the maturation of SREBP and the up-regulation LXR and LXR-targeted genes (SREBP, ABCG1 and ABCG4, HMGCoA reductase, ApoE) resulting into a lower synthesis and transport of cholesterol from astrocytes to neurons via ApoE. In primary oligodendrocytes, mutant HTT inhibited the regulatory effect of PGC1α on cholesterol metabolism and on the expression of MBP. HTT seems to play a regulatory role in lipid metabolism. The impairment of the cholesterol metabolism was found to be proportional to the CAG repeat length and to the load of mutant HTT. A dysregulation on PGC1α and mitochondria dysfunction may be involved in an overall reduction of acetyl-CoA and ATP synthesis, contributing to the cerebral and whole body cholesterol impairment. This article is part of a Special Issue entitled Brain Lipids." @default.
• W2022791592 created "2016-06-24" @default.
• W2022791592 creator A5034637504 @default.
• W2022791592 creator A5061201309 @default.
• W2022791592 date "2015-08-01" @default.
• W2022791592 modified "2023-10-03" @default.
• W2022791592 title "The impairment of cholesterol metabolism in Huntington disease" @default.
• W2022791592 cites W133038330 @default.
• W2022791592 cites W13351788 @default.
• W2022791592 cites W1496189784 @default.
• W2022791592 cites W1518741841 @default.
• W2022791592 cites W1580279589 @default.
• W2022791592 cites W1602494991 @default.
• W2022791592 cites W166972436 @default.
• W2022791592 cites W1831632254 @default.
• W2022791592 cites W1943560076 @default.
• W2022791592 cites W1963578022 @default.
• W2022791592 cites W1965703692 @default.
• W2022791592 cites W1970541648 @default.
• W2022791592 cites W1972769378 @default.
• W2022791592 cites W1973094968 @default.
• W2022791592 cites W1973747307 @default.
• W2022791592 cites W1975639206 @default.
• W2022791592 cites W1977207564 @default.
• W2022791592 cites W1982493902 @default.
• W2022791592 cites W1992262127 @default.
• W2022791592 cites W1993976809 @default.
• W2022791592 cites W1998510870 @default.
• W2022791592 cites W2000462578 @default.
• W2022791592 cites W2006161539 @default.
• W2022791592 cites W2006534012 @default.
• W2022791592 cites W2006760403 @default.
• W2022791592 cites W2007960303 @default.
• W2022791592 cites W2008823657 @default.
• W2022791592 cites W2009230396 @default.
• W2022791592 cites W2009959558 @default.
• W2022791592 cites W2010404670 @default.
• W2022791592 cites W2013889250 @default.
• W2022791592 cites W2015896899 @default.
• W2022791592 cites W2016068173 @default.
• W2022791592 cites W2016988002 @default.
• W2022791592 cites W2022192094 @default.
• W2022791592 cites W2022991915 @default.
• W2022791592 cites W2025379166 @default.
• W2022791592 cites W2025872849 @default.
• W2022791592 cites W2028410644 @default.
• W2022791592 cites W2031340288 @default.
• W2022791592 cites W2035247878 @default.
• W2022791592 cites W2037640340 @default.
• W2022791592 cites W2038083025 @default.
• W2022791592 cites W2041214350 @default.
• W2022791592 cites W2041392266 @default.
• W2022791592 cites W2043166587 @default.
• W2022791592 cites W2046855179 @default.
• W2022791592 cites W2048822173 @default.
• W2022791592 cites W2048958063 @default.
• W2022791592 cites W2052496080 @default.
• W2022791592 cites W2055998713 @default.
• W2022791592 cites W2057249336 @default.
• W2022791592 cites W2057365200 @default.
• W2022791592 cites W2058930537 @default.
• W2022791592 cites W2059097153 @default.
• W2022791592 cites W2059698256 @default.
• W2022791592 cites W2062416372 @default.
• W2022791592 cites W2067064610 @default.
• W2022791592 cites W2068320007 @default.
• W2022791592 cites W2069638209 @default.
• W2022791592 cites W2071145481 @default.
• W2022791592 cites W2076615525 @default.
• W2022791592 cites W2078976507 @default.
• W2022791592 cites W2079124378 @default.
• W2022791592 cites W2079407277 @default.
• W2022791592 cites W2080518662 @default.
• W2022791592 cites W2081722421 @default.
• W2022791592 cites W2082056883 @default.
• W2022791592 cites W2083719092 @default.
• W2022791592 cites W2089651715 @default.
• W2022791592 cites W2089653224 @default.
• W2022791592 cites W2090996828 @default.
• W2022791592 cites W2091896743 @default.
• W2022791592 cites W2092177215 @default.
• W2022791592 cites W2093810123 @default.
• W2022791592 cites W2093851813 @default.
• W2022791592 cites W2098723544 @default.
• W2022791592 cites W2101504245 @default.
• W2022791592 cites W2105216461 @default.
• W2022791592 cites W2106009748 @default.
• W2022791592 cites W2106515170 @default.
• W2022791592 cites W2110395308 @default.
• W2022791592 cites W2111214545 @default.
• W2022791592 cites W2112939466 @default.
• W2022791592 cites W2114806174 @default.
• W2022791592 cites W2117842413 @default.
• W2022791592 cites W2120218847 @default.
• W2022791592 cites W2121261412 @default.
• W2022791592 cites W2121642311 @default.
• W2022791592 cites W2121760835 @default.
• W2022791592 cites W2121926054 @default.

• next