Cross-linkable short-chain phosphatidylcholines with thiols at the chain terminus have been synthesized and characterized. These micelle-forming species were used to investigate two water-soluble phospholipases. When reduced, the thiol lipids were excellent substrates for phospholipase A2. Once cross-linked, they became extremely poor substrates. This is consistent with a mechanism in which a key step is the partial extraction of the substrate phosphatidylcholine from an aggregate. In contrast, phospholipase C activity was slightly enhanced if the product diglyceride was tethered to the aggregate through disulfide formation. For this enzyme such a kinetic effect is consistent with the hydrophobic diglyceride biasing the enzyme to the interface.
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REVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USAREVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USA
SUTHERLAND, CA
WHYZMUZIS, C
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REVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USAREVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USA
WHYZMUZIS, C
AMIN, D
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REVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USAREVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USA
AMIN, D
KHANDWALA, A
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REVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USAREVLON HLTH CARE GRP, DIV RES & DEV, DEPT BIOCHEM RES, TUCKAHOE, NY 10707 USA