Post-Translational Processing of B-Endorphin - William Millington

Abstract

Funding Agency

Agency: National Institute of Health (NIH)
Institute: National Institute on Drug Abuse (NIDA)
Type: First Independent Research Support & Transition (FIRST) Awards (R29)
Project #: 5R29DA004598-04
Application #: 3461069
Study Section: Special Emphasis Panel (SRCD (26))

Project Start: 1989-11-01
Project End: 1994-01-31
Budget Start: 1991-02-01
Budget End: 1992-01-31
Support Year: 4
Fiscal Year: 1991
Total Cost
Indirect Cost

Institution

Name: University of Missouri Kansas City
Department
Type: Schools of Medicine
DUNS #: 800772162

City: Kansas City
State: MO
Country: United States
Zip Code: 64110

Related projects


NIH 1993 R29 DA	Post-Translational Processing of B-Endorphin Millington, William R. / University of Missouri Kansas City
NIH 1992 R29 DA	Post-Translational Processing of B-Endorphin Millington, William R. / University of Missouri Kansas City
NIH 1991 R29 DA	Post-Translational Processing of B-Endorphin Millington, William R. / University of Missouri Kansas City
NIH 1990 R29 DA	Post-Translational Processing of B-Endorphin Millington, William R. / University of Missouri Kansas City
NIH 1989 R29 DA	Post-Translational Processing of B-Endorphin Millington, William R. / Henry M. Jackson Fdn for the Adv Mil/Med
NIH 1989 R29 DA	Post-Translational Processing of B-Endorphin Millington, William R. / University of Missouri Kansas City

Publications

Evans, V R; Manning, A B; Bernard, L H et al. (1994) Alpha-melanocyte-stimulating hormone and N-acetyl-beta-endorphin immunoreactivities are localized in the human pituitary but are not restricted to the zona intermedia. Endocrinology 134:97-106

Gehlert, D R; Gackenheimer, S L; Millington, W R et al. (1994) Localization of neuropeptide Y immunoreactivity and [125I]peptide YY binding sites in the human pituitary. Peptides 15:651-6

Unal, C B; Owen, M D; Millington, W R (1994) Beta-endorphin-induced cardiorespiratory depression is inhibited by glycyl-L-glutamine, a dipeptide derived from beta-endorphin processing. J Pharmacol Exp Ther 271:952-8

Chronwall, B M; Dickerson, D S; Huerter, B S et al. (1994) Regulation of heterogeneity in D2 dopamine receptor gene expression among individual melanotropes in the rat pituitary intermediate lobe. Mol Cell Neurosci 5:35-45

Manning, A B; Chronwall, B M; Millington, W R (1993) POMC-derived peptide immunoreactivity in neural lobe axons of the human pituitary. Peptides 14:857-60

Millington, W R; Evans, V R; Forman, L J et al. (1993) Characterization of beta-endorphin- and alpha-MSH-related peptides in rat heart. Peptides 14:1141-7

Lavigne, G J; Millington, W R; Mueller, G P (1992) The CCK-A and CCK-B receptor antagonists, devazepide and L-365,260, enhance morphine antinociception only in non-acclimated rats exposed to a novel environment. Neuropeptides 21:119-29

Millington, W R; Dybdal, N O; Mueller, G P et al. (1992) N-acetylation and C-terminal proteolysis of beta-endorphin in the anterior lobe of the horse pituitary. Gen Comp Endocrinol 85:297-307

Millington, W R; Mueller, G P; Lavigne, G J (1992) Cholecystokinin type A and type B receptor antagonists produce opposing effects on cholecystokinin-stimulated beta-endorphin secretion from the rat pituitary. J Pharmacol Exp Ther 261:454-61

Millington, W R; Smith, D L (1991) The posttranslational processing of beta-endorphin in human hypothalamus. J Neurochem 57:775-81

Showing the most recent 10 out of 11 publications

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