Abstract

EXCEEDTHE SPACE PROVIDED. There has been mounting evidence that estrogens express neuroprotective effects by the suppression of neurotoxic stimuli largely via their direct radical-scavenging activity. The objective of this grant application is to understand this activity by focusing on the underlying chemistry in which the molecular mechanism of the process and the chemical nature and fate of the products derived from the radical-scavenging reaction are considered the key elements. Our hypotheses center on the role of estrogen-derived quinols as specific reaction products whose involvement has been implicated by preliminary data. By systematically varying substituents in the 2- and/or 4-positions of the phenolic A-ring compounds, we should gain insight into the influence of phenoxy-radical (ArO*) stability, electron density of ArO' at the C-10 position and, thus, its reactivity towards hydroxyl radical (*OH). The Fenton-reaction, which leads to *OH formation, will be employed as a chemical model. We hypothesize that hydroxylation will be involved upon *OH exposure as an important process that produces non-radical products from estrogens. In the model system that will be used to study the fate of the synthetic estrogens obtained by the systematic modification of the endogenous compounds, only one type of (mono)hydroxylated species, of a quinol structure, is anticipated via a two-step hydroxyl-radical scavenging mechanism. The rate of quinol formation is expected to correlate not only with the steric and electronic elements of the steroidal compounds, but also with their neuroprotective effect. The phenol to quinol pathway may augment the estrogens' free- radical scavenging efficacy, and make a pivotal contribution to neuroprotection. A reductive quinol to phenol transformation (hence, estrogen 'recycling') that prevents the depletion of the available neuroprotective estrogens in vivo will also be investigated. This reactivation (in terms of kinetics and influence by the A-ring substituents) will be studied in vitro in cell-free and cellular system, and by in vivo microdialysis in experimental animals. Support will be sought to the hypothesis that the reduction of quinols is not accompanied by an increased formation of reactive oxygen species. By using glutamate-induced oxidative stress in HT22 cells as an experimental paradigm, we will study the neuroprotective effects of the phenolic A-ring derivatives of estrogens. In addition to structure - activity relationship studies, a correlation between the propensity of the compound to form its quinol product upon *OH exposure and its effective dose in this model system for neuroprotection will be sought. It is anticipated that the new estrogen analogs selected based on mechanistic studies and in vitro screening will show in vivo neuroprotective effects in a transient middle cerebral artery occlusion, a model for cerebral ischemia. Hence, they will serve as new lead compounds for the development of neuroprotective agents with improved efficacy. PERFORMANCE SITE ========================================Section End===========================================

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
7R01NS044765-04
Application #
7127400
Study Section
Special Emphasis Panel (ZRG1-MDCN-2 (03))
Program Officer
Jacobs, Tom P
Project Start
2003-01-15
Project End
2006-12-31
Budget Start
2005-08-01
Budget End
2005-12-31
Support Year
4
Fiscal Year
2005
Total Cost
$186,489
Indirect Cost

  Institution

Name
University of North Texas
Department
Microbiology/Immun/Virology
Type
Other Domestic Higher Education
DUNS #
110091808
City
Fort Worth
State
TX
Country
United States
Zip Code
76107

  Publications

Prokai, Laszlo; Nguyen, Vien; Szarka, Szabolcs et al. (2015) The prodrug DHED selectively delivers 17?-estradiol to the brain for treating estrogen-responsive disorders. Sci Transl Med 7:297ra113
Prokai-Tatrai, Katalin; Prokai, Laszlo; Simpkins, James W et al. (2009) Phenolic compounds protect cultured hippocampal neurons against ethanol-withdrawal induced oxidative stress. Int J Mol Sci 10:1773-87
Prokai, Laszlo; Stevens Jr, Stanley M; Rauniyar, Navin et al. (2009) Rapid label-free identification of estrogen-induced differential protein expression in vivo from mouse brain and uterine tissue. J Proteome Res 8:3862-71
Nguyen, V; Bonds, D V; Prokai, L (2008) Measurement of Hydroxyl-Radical Formation in the Rat Striatum by In Vivo Microdialysis and GC-MS. Chromatographia 68:s57-s62
Prokai-Tatrai, Katalin; Perjesi, Pal; Rivera-Portalatin, Nilka M et al. (2008) Mechanistic investigations on the antioxidant action of a neuroprotective estrogen derivative. Steroids 73:280-8
Prokai, Laszlo; Simpkins, James W (2007) Structure-nongenomic neuroprotection relationship of estrogens and estrogen-derived compounds. Pharmacol Ther 114:1-12
Rivera-Portalatin, Nilka M; Vera-Serrano, Jose L; Prokai-Tatrai, Katalin et al. (2007) Comparison of estrogen-derived ortho-quinone and para-quinol concerning induction of oxidative stress. J Steroid Biochem Mol Biol 105:71-5
Prokai, Laszlo; Zharikova, Alevtina D; Stevens Jr, Stanley M (2005) Effect of chronic morphine exposure on the synaptic plasma-membrane subproteome of rats: a quantitative protein profiling study based on isotope-coded affinity tags and liquid chromatography/mass spectrometry. J Mass Spectrom 40:169-75
Prokai-Tatrai, Katalin; Prokai, Laszlo (2005) Impact of metabolism on the safety of estrogen therapy. Ann N Y Acad Sci 1052:243-57
Simpkins, James W; Wang, Jian; Wang, Xiaofei et al. (2005) Mitochondria play a central role in estrogen-induced neuroprotection. Curr Drug Targets CNS Neurol Disord 4:69-83

Showing the most recent 10 out of 13 publications