Abstract

Several projects are proposed to further the ability of researchers to determine the transition-state structure of bioorganic reactions. The biomedical significance of the research is the improvements it offers in understanding the fundamental principles underlying efforts in rational drug design. Many disease processes are the result of an enzyme functioning out of control. The enzymes are controlled using drugs that act as inhibitors of the enzyme. Antipathogenic agents are also often specific inhibitors of key metabolic enzymes of a particular pathogen. Understanding transition-state structure is central to the rational design of medicines that act as enzyme inhibitors.
The specific aims of the project are: 1. To define the role that hydrogen bonds play in determining the reactivity of bases in model reactions for enzymes. Solvent isotope effects, substrate isotope effects, and isotope effects on isotope effect will be used to study the extent of base desolvation in the transition state for a proton transfer from a carbon acid. The degree to which solvent motions around the base are coupled to the proton transfer event will also be determined. 2. To develop methods for calculating isotopic fractionation factors of strong hydrogen bonds thought to be important in enzymic catalysis. Several researchers have proposed recently new theories about he origins of enzymic catalytic power. The stabilizing effects of short, strong hydrogen bonds are thought to be central features of the mechanisms used by enzymes to reduce the barrier heights for chemical reactions. The present proposal is a plan to develop methods for model calculations which can be used to test and further refine theories of enzymic catalysis. 3. To use carbon isotope effects to determine transition state structures in enzymic decarboxylations. A new laser-based technique for high- precision measurements of isotope ratios will be developed and tested for use in studying the mechanisms of reactions catalyzed by enzymes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
5S06GM008223-15
Application #
6271679
Study Section
Project Start
1998-07-01
Project End
1999-12-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
15
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Rutgers University
Department
Type
DUNS #
130029205
City
Newark
State
NJ
Country
United States
Zip Code
07102

  Publications

Baykal, Ahmet; Chakraborty, Sumit; Dodoo, Afua et al. (2006) Synthesis with good enantiomeric excess of both enantiomers of alpha-ketols and acetolactates by two thiamin diphosphate-dependent decarboxylases. Bioorg Chem 34:380-93
Mattson, Brandi J; Williams, Sharon E; Rosenblatt, Jay S et al. (2003) Preferences for cocaine- or pup-associated chambers differentiates otherwise behaviorally identical postpartum maternal rats. Psychopharmacology (Berl) 167:1-8
Gilchrist, Alan L; Annan Jr, Vidal (2002) Articulation effects in lightness: historical background and theoretical implications. Perception 31:141-50
Vathy, Ilona; Komisaruk, Barry R (2002) Differential effects of prenatal morphine exposure on analgesia produced by vaginocervical stimulation or systemic morphine administration in adult rats. Pharmacol Biochem Behav 72:165-70
Mattson, B J; Williams, S; Rosenblatt, J S et al. (2001) Comparison of two positive reinforcing stimuli: pups and cocaine throughout the postpartum period. Behav Neurosci 115:683-94
Duque, A; Balatoni, B; Detari, L et al. (2000) EEG correlation of the discharge properties of identified neurons in the basal forebrain. J Neurophysiol 84:1627-35
Komisaruk, B R; Rosenblatt, J S; Barona, M L et al. (2000) Combined c-fos and 14C-2-deoxyglucose method to differentiate site-specific excitation from disinhibition: analysis of maternal behavior in the rat. Brain Res 859:262-72
Caba, M; Komisaruk, B R; Beyer, C (1998) Analgesic synergism between AP5 (an NMDA receptor antagonist) and vaginocervical stimulation in the rat. Pharmacol Biochem Behav 61:45-8
Sansone, G R; Bianca, R; Cueva-Rolon, R et al. (1997) Cardiovascular responses to vaginocervical stimulation in the spinal cord-transected rat. Am J Physiol 273:R1361-6
Burroughs, L F; Fiber, J M; Swann, J M (1996) Neuropeptide Y in hamster limbic nuclei: lack of colocalization with substance P. Peptides 17:1053-62

Showing the most recent 10 out of 15 publications