[摘要] Apolipoprotein (apo) A-I, the major structural protein of high-density lipoprotein (HDL), is present in human and mouse cerebrospinal fluid (CSF) despite its lack of expression in brain cells. To identify the origin of apoA-I in CSF, we generated intestine-specific and liver-specific Apoa1 knockout mice ( Apoa1 ΔInt and Apoa1 Δliv mice, respectively). Lipoprotein profiles of Apoa1 ΔInt and Apoa1 ΔLiv mice resembled those of control littermates, whereas knockout of Apoa1 in both intestine and liver ( Apoa1 ΔIntΔLiv ) resulted in a 60-percent decrease in HDL-cholesterol levels, thus strongly mimicking the Apoa1 −/− mice. Immunoassays revealed that mouse apoA-I was not present in the CSF of the Apoa1 ΔIntΔLiv mice. Furthermore, apoA-I levels in CSF were highly correlated with plasma spherical HDL levels, which were regulated by ABCA1 and LCAT. Collectively, these results suggest that apoA-I protein in CSF originates in liver and small intestine and is taken up from the plasma.