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Journal of Lipid Research, Vol 31, 995-1004, Copyright © 1990 by Lipid Research, Inc.
Cellular localization of apolipoprotein D and lecithin:cholesterol acyltransferase mRNA in rhesus monkey tissues by in situ hybridization
KM Smith, RM Lawn and JN Wilcox
Department of Cardiovascular Research, Genentech, Inc., So. San Francisco, CA 94080.
Apolipoprotein D (apoD) and lecithin:cholesterol acyl transferase (LCAT)
are found on high density lipoprotein particles (HDLs) and have been
postulated to form part of a complex involved in the transport of
cholesterol from peripheral tissues to the liver for excretion. We have
examined the sites of synthesis of the mRNAs for these two proteins in the
rhesus monkey by in situ hybridization. ApoD mRNA-containing cells were
widely distributed throughout peripheral tissues in interstitial and
connective tissue fibroblasts often associated with blood vessels or
capillaries. ApoD mRNA was also found localized in cells associated with
peripheral nerves, neuroglial cells, cells in the subarachnoid space on the
surface of the brain including the pial cells, perivascular cells, and
scattered neurons in the brain. LCAT demonstrated a much more restricted
pattern of synthesis and was found to be synthesized by hepatocytes, the
basal cell layer of the epidermis, and in brain cell populations distinct
from those that synthesize apoD. In the brain LCAT was synthesized by
scattered neurons, neuroglial cells, ependymal cells, as well as a discrete
cell layer in the cerebellum. ApoD has been shown to possess extensive
homology to retinol binding protein, which has a binding pocket for vitamin
A. We propose that apoD may also function to bind cholesterol or its
derivatives in compartments not in direct contact with the blood. The
findings of both apoD and LCAT synthesis in the brain suggest that they
play a significant role in lipid transport in the brain.

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Copyright © 1990 by the American Society for Biochemistry and Molecular Biology.
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