Pheromone binding by polymorphic mouse major urinary proteins
- 1 September 2002
- journal article
- Published by Wiley in Protein Science
- Vol. 11 (9), 2247-2256
- https://doi.org/10.1110/ps.0204202
Abstract
Mouse major urinary proteins (MUPs) have been proposed to play a role in regulating the release and capture of pheromones. Here, we report affinity measurements of five recombinant urinary MUP isoforms (MUPs-I, II, VII, VIII, and IX) and one recombinant nasal isoform (MUP-IV) for each of three pheromonal ligands, (+/-)-2-sec-butyl-4,5-dihydrothiazole (SBT), 6-hydroxy-6-methyl-3-heptanone (HMH), and (+/-)dehydro-exo-brevicomin (DHB). Dissociation constants for all MUP-pheromone pairs were determined by isothermal titration calorimetry, and data for SBT were corroborated by measurements of intrinsic protein fluorescence. We also report the isolation of MUP-IV protein from mouse nasal extracts, in which MUP-IV mRNA has been observed previously. The affinity of each MUP isoform for SBT (K(d) approximately 0.04 to 0.9 micro M) is higher than that for DHB (K(d) approximately 26 to 58 micro M), which in turn is higher than that for HMH (K(d) approximately 50 to 200 micro M). Isoforms I, II, VIII, and IX show very similar affinities for each of the ligands. MUP-VII has approximately twofold higher affinity for SBT but approximately twofold lower affinity for the other pheromones, whereas MUP-IV has approximately 23-fold higher affinity for SBT and approximately fourfold lower affinity for the other pheromones. The variations in ligand affinities of the MUP isoforms are consistent with structural differences in the binding cavities of the isoforms. The data indicate that the concentrations of available pheromones in urine may be influenced by changes in the expression levels of urinary MUPs or the excretion levels of other MUP ligands. The variation in pheromone affinities of the urinary MUP isoforms provides only limited support for the proposal that MUP heterogeneity plays a role in regulating profiles of available pheromones. However, the binding data support the proposed role of nasal MUPs in sequestering pheromones and possibly transporting them to their receptors.Keywords
This publication has 41 references indexed in Scilit:
- Individual recognition in mice mediated by major urinary proteinsNature, 2001
- NMR Mapping of the Recombinant Mouse Major Urinary Protein I Binding Site Occupied by the Pheromone 2-sec-Butyl-4,5-dihydrothiazoleBiochemistry, 1999
- Binding Kinetics of Engineered Mutants Provide Insight about the Pathway for Entering and Exiting the Intestinal Fatty Acid Binding ProteinBiochemistry, 1999
- Fatty Acid Interactions with a Helix-less Variant of Intestinal Fatty Acid-Binding ProteinBiochemistry, 1996
- Stereoselectivity in mammalian chemical communication: Male mouse pheromonesCellular and Molecular Life Sciences, 1995
- Sexual dimorphism and growth hormone induction of murine pheromone-binding proteinsJournal of Molecular Endocrinology, 1995
- Extraction, characterization, and binding analysis of two pheromonally active ligands associated with major urinary protein of house mouse (Mus musculus)Journal of Chemical Ecology, 1993
- A novel multigene family may encode odorant receptors: A molecular basis for odor recognitionCell, 1991
- Chemistry of male dominance in the house mouse,Mus domesticusCellular and Molecular Life Sciences, 1990
- Variation in mouse major urinary protein (MUP) genes and the MUP gene products within and between inbred linesGene, 1982