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Binding of squalene, lanosterol, desmosterol, and cholesterol to proteins in brain and liver 105,000 g supernatant fractions: Evidence for specific binding sites
Author(s) -
Johnson Ronald C.,
Shah Shantilal N.
Publication year - 1976
Publication title -
lipids
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.601
H-Index - 120
eISSN - 1558-9307
pISSN - 0024-4201
DOI - 10.1007/bf02532881
Subject(s) - lanosterol , desmosterol , squalene , biochemistry , chemistry , binding site , cholesterol , sterol , biology
The binding of squalene, lanosterol, desmosterol, and cholesterol to proteins in 105,000 g supernatant fraction (S 105 ) from brain and liver of rats was investigated. The S 105 fractions from both tissues contain specific binding sites for sterols, which are sensitive to trypsin. The dissociation constants for squalene and sterol protein complexes were in the range of 10 −6 M and were not appreciably different for proteins in brain and liver S 105 . Competition studies revealed that both brain and liver S 105 contain one receptor protein which binds lanosterol and is specific for methyl sterols, and a second receptor which binds both desmosterol and cholesterol. Binding of 7‐dehydrocholesterol reported by others must occur at a third independent site since this compound does not interfere with the binding of lanosterol, desmosterol, or cholesterol. Although binding of squalene to proteins in brain and liver S 105 does occur, we were unable to show the specificity of squalene binding. The concentration of desmosterol and cholesterol binding sites, which ranged from 6 to 10 nmol/mg protein, was 3‐ to 5‐fold higher than the concentration of squalene and lanosterol binding sites (1.6–2.3 nmol/mg protein). The brain S 105 from suckling rats contained fewer binding sites for desmosterol and cholesterol than the brain S 105 from weaned rats. However, the concentration of lanosterol binding sites in brain S 105 did not show an age‐dependent change. The receptor proteins in brain and liver appear to be identical.

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