胆固醇
生物
痴呆
内科学
神经病理学
阿尔茨海默病
内分泌学
颞叶皮质
神经科学
医学
疾病
作者
Hitesh Mistry,Christopher D. Richardson,Adrian Higginbottom,Bridget Ashford,SYasmeen Ahamed,Zhuzhi Moore,Fiona E. Matthews,Carol Brayne,JE Simpson,Stephen B. Wharton
标识
DOI:10.1016/j.neures.2024.01.003
摘要
Altered cholesterol metabolism is implicated in brain ageing and Alzheimer’s disease. We examined whether key genes regulating cholesterol metabolism and levels of brain cholesterol are altered in dementia and Alzheimer’s disease neuropathological change (ADNC). Temporal cortex (n=99) was obtained from the Cognitive Function and Ageing Study. Expression of the cholesterol biosynthesis rate-limiting enzyme HMG-CoA reductase (HMGCR) and its regulator, SREBP2, were detected using immunohistochemistry. Expression of HMGCR, SREBP2, CYP46A1 and ABCA1 were quantified by qPCR in samples enriched for astrocyte and neuronal RNA following laser-capture microdissection. Total cortical cholesterol was measured using the Amplex Red assay. HMGCR and SREBP2 proteins were predominantly expressed in pyramidal neurones, and in glia. Neuronal HMGCR did not vary with ADNC, oxidative stress, neuroinflammation or dementia status. Expression of HMGCR neuronal mRNA decreased with ADNC (p=0.022) and increased with neuronal DNA damage (p=0.049), whilst SREBP2 increased with ADNC (p=0.005). High or moderate tertiles for cholesterol levels were associated with increased dementia risk (OR 1.44, 1.58). APOE ε4 allele was not associated with cortical cholesterol levels. ADNC is associated with gene expression changes that may impair cholesterol biosynthesis in neurones but not astrocytes, whilst levels of cortical cholesterol show a weak relationship to dementia status.
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