Binding of vasoactive intestinal polypeptide (VIP) by human blood monocytes: demonstration of specific binding sites |
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Authors: | Pål Wiik Per K. Opstad Arne Bøyum |
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Affiliation: | Norwegian Defence Research Institute, Division for Environmental Toxicology, P.O. Box 25, N-2007 Kjeller, Norway |
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Abstract: | Vasoactive intestinal polypeptide (VIP) interaction with a 94% pure preparation of monocytes isolated from human peripheral blood was studied by direct binding technique using 3-[125I]tyrosyl-VIP as a tracer ligand. Scatchard analysis of binding data was compatible with two classes of binding sites, one with Kd = 0.25 nM and maximal binding capacity of 16 fmol/10(6) cells, and another one with Kd = 25 nM and maximal binding capacity of 180 fmol/10(6) cells. The binding was time-, temperature-, and pH-dependent and was saturable, reversible, and specific. This study has demonstrated that human monocytes have high affinity/low capacity as well as low affinity/high capacity binding sites for VIP. No specific VIP binding was found in pure preparations of human granulocytes, platelets or erythrocytes. |
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Keywords: | VIP-receptor human monocytes |
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