Abstract

In this project, studies are proposed to analyze organophosphate insecticides as toxicants, the consequences of organophosphate exposure, in terms of body burden and inhibition of the target acetylcholinesterase (AChE), and differences in individual susceptibility related to organophosphate target. Fluorescence detection using the AChE target itself will be explored as a means for developing remote sensing and portable detection devices. The disposition of organophosphates in the body will be analyzed by mass spectrometry to assess tissue distribution and conjugation at the active center of AChE. The latter approach enables us to detect inhibited AChE, inhibited and aged AChE and AChE that is spontaneously or oxime reactivated. Hence, a complete kinetic profile of reactions at the active center serine is possible. Because of malathion's prevalent use world-wide and locally, initial studies will involve this organophosphate which must be converted to malaoxon to become an active and toxic agent. Rates of conversion will be studied using animals with enhanced P450 activity which control the conversion of protoxicant to cholinesterase reactive entity. These studies of insecticide exposure will be buttressed by examining transgenic strains where the acetylcholinesterase gene, its alternatively spliced exons and regulatory regions of the gene have been modified. The modified genes enable us to express AChE in select tissues and in discrete cellular locations thereby allowing an analysis of the cellular basis of toxicity in the intact animal. Finally, the investigators have adopted a pharmacogenomic approach to detect single polynucleotide polymorphisms and, in turn, haplotypes to analyze differential sensitivity to cholinesterase inhibitors. Previous studies characterizing the AChE molecule and the single gene encoding the enzyme place the investigators in a strong position to analyze the target molecule of insecticide interaction and determine genetic relationships in individual susceptibility.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Hazardous Substances Basic Research Grants Program (NIEHS) (P42)
Project #
5P42ES010337-09
Application #
7598927
Study Section
Special Emphasis Panel (ZES1)
Project Start
Project End
Budget Start
2008-04-01
Budget End
2009-03-31
Support Year
9
Fiscal Year
2008
Total Cost
$256,038
Indirect Cost

  Institution

Name
University of California San Diego
Department
Type
DUNS #
804355790
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Que, Xuchu; Hung, Ming-Yow; Yeang, Calvin et al. (2018) Oxidized phospholipids are proinflammatory and proatherogenic in hypercholesterolaemic mice. Nature 558:301-306
Fan, Weiwei; He, Nanhai; Lin, Chun Shi et al. (2018) ERR? Promotes Angiogenesis, Mitochondrial Biogenesis, and Oxidative Remodeling in PGC1?/?-Deficient Muscle. Cell Rep 22:2521-2529
Brouha, Sharon S; Nguyen, Phirum; Bettencourt, Ricki et al. (2018) Increased severity of liver fat content and liver fibrosis in non-alcoholic fatty liver disease correlate with epicardial fat volume in type 2 diabetes: A prospective study. Eur Radiol 28:1345-1355
Hsu, Po-Kai; Takahashi, Yohei; Munemasa, Shintaro et al. (2018) Abscisic acid-independent stomatal CO2 signal transduction pathway and convergence of CO2 and ABA signaling downstream of OST1 kinase. Proc Natl Acad Sci U S A 115:E9971-E9980
Dhar, Debanjan; Antonucci, Laura; Nakagawa, Hayato et al. (2018) Liver Cancer Initiation Requires p53 Inhibition by CD44-Enhanced Growth Factor Signaling. Cancer Cell 33:1061-1077.e6
Febbraio, Mark A; Reibe, Saskia; Shalapour, Shabnam et al. (2018) Preclinical Models for Studying NASH-Driven HCC: How Useful Are They? Cell Metab :
Fujiwara, Ryoichi; Yoda, Emiko; Tukey, Robert H (2018) Species differences in drug glucuronidation: Humanized UDP-glucuronosyltransferase 1 mice and their application for predicting drug glucuronidation and drug-induced toxicity in humans. Drug Metab Pharmacokinet 33:9-16
Hartmann, Phillipp; Hochrath, Katrin; Horvath, Angela et al. (2018) Modulation of the intestinal bile acid/farnesoid X receptor/fibroblast growth factor 15 axis improves alcoholic liver disease in mice. Hepatology 67:2150-2166
Ganguly, Abantika; Guo, Lan; Sun, Lingling et al. (2018) Tdp1 processes chromate-induced single-strand DNA breaks that collapse replication forks. PLoS Genet 14:e1007595
Tripathi, Anupriya; Debelius, Justine; Brenner, David A et al. (2018) The gut-liver axis and the intersection with the microbiome. Nat Rev Gastroenterol Hepatol 15:397-411

Showing the most recent 10 out of 404 publications