Abstract

Noroviruses (NIAID category B priority pathogens) are a leading cause of food- or water-borne gastroenteritis outbreaks, responsible for an estimated 23 million cases annually in the US. However, currently there are no commercially available vaccines or antivirals against noroviruses. We have initiated a comprehensive plan aimed at developing anti-noroviral therapeutics in cooperation with medicinal chemists and virologists from various institutes. Using a novel cell-based Norwalk virus (NV) replication system, we have identified viral proteinase (Pro) and cellular acyl-coenzyme Axholesterol acyltransferase (ACAT) as potential therapeutic targets and have furthermore demonstrated that two classes of compounds significantly reduced virus replication, presumably via the inhibition of viral Pro and ACAT, respectively. Since NV Pro and ACAT play a critical role in viral replication, the hypothesis is advanced that agents capable of inhibiting these enzymes selectively are of potential therapeutic value. Thus, the long term goal of this program is the development of novel small molecule therapeutics against human noroviruses by advancing the active compounds through the stage prior to filing an IND application with the FDA. We have established the following specific aims for advancing our hit compounds into a drug candidate for preclinical development.
Specific Aim 1 : Utilize medicinal/combinatorial chemistry and molecular modeling to optimize two classes of compounds. The goal of this aim is to identify lead compounds that meet potency, selectivity, c log P, bioavailability, and other relevant parameters for drug development.
Aim 2. Conduct in vitro studies to establish the mechanism of action of two classes of compounds. We will also evaluate viral resistance to lead compounds by long-term treatment.
Aim 3. Conduct ADME/TOX and oral bioavailability studies to optimize the phamacokinetic parameters of selected lead compounds.
Aim 4. Demonstrate in vivo efficacy of lead compounds using the gnotobiotic pig model of human norovirus infection. Accomplishment of these specific aims will set the stage for conducting IND-enabling studies, including large-scale GMP synthesis of lead compounds, pharmacokinetics, GLP toxicology and safety pharmacology.

Public Health Relevance

Human noroviruses are now the leading cause of food- or water-borne gastroenteritis illnesses, but currently there are no commercially available vaccines or antivirals against them. Our studies aim at advancing our hit compounds into a drug candidate for preclinical development, which will have a significant impact on norovirus research and public health.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01AI081891-04
Application #
8213750
Study Section
Special Emphasis Panel (ZAI1-MMT-M (J2))
Program Officer
Cassels, Frederick J
Project Start
2009-03-15
Project End
2014-02-28
Budget Start
2012-03-01
Budget End
2013-02-28
Support Year
4
Fiscal Year
2012
Total Cost
$952,801
Indirect Cost
$142,646

  Institution

Name
Kansas State University
Department
Veterinary Sciences
Type
Schools of Veterinary Medicine
DUNS #
929773554
City
Manhattan
State
KS
Country
United States
Zip Code
66506

  Publications

Weerasekara, Sahani; Prior, Allan M; Hua, Duy H (2016) Current tools for norovirus drug discovery. Expert Opin Drug Discov 11:529-41
Kim, Yunjeong; Shivanna, Vinay; Narayanan, Sanjeev et al. (2015) Broad-spectrum inhibitors against 3C-like proteases of feline coronaviruses and feline caliciviruses. J Virol 89:4942-50
Shivanna, Vinay; Kim, Yunjeong; Chang, Kyeong-Ok (2014) The crucial role of bile acids in the entry of porcine enteric calicivirus. Virology 456-457:268-78
Jung, Kwonil; Scheuer, Kelly A; Zhang, Zhenwen et al. (2014) Pathogenesis of GIII.2 bovine norovirus, CV186-OH/00/US strain in gnotobiotic calves. Vet Microbiol 168:202-7
Prior, Allan M; Gunaratna, Medha J; Kikuchi, Daisuke et al. (2014) Syntheses of 3-[(Alkylamino)methylene]-6-methylpyridine-2,4(1H,3H)-diones, 3-Substituted 7-Methyl-2H-pyrano[3,2-c]pyridine-2,5(6H)-dione Fluorescence Probes, and Tetrahydro-1H,9H-2,10-dioxa-9-azaanthracen-1-ones. Synthesis (Stuttg) 46:2179-2190
Prior, Allan M; Zhang, Man; Blakeman, Nina et al. (2014) Inhibition of long chain fatty acyl-CoA synthetase (ACSL) and ischemia reperfusion injury. Bioorg Med Chem Lett 24:1057-61
Shivanna, Vinay; Kim, Yunjeong; Chang, Kyeong-Ok (2014) Endosomal acidification and cathepsin L activity is required for calicivirus replication. Virology 464-465:287-295
Prior, Allan M; Kim, Yunjeong; Weerasekara, Sahani et al. (2013) Design, synthesis, and bioevaluation of viral 3C and 3C-like protease inhibitors. Bioorg Med Chem Lett 23:6317-20
Zhang, Yuchen; Hays, Amanda; Noblett, Alexander et al. (2013) Transport by OATP1B1 and OATP1B3 enhances the cytotoxicity of epigallocatechin 3-O-gallate and several quercetin derivatives. J Nat Prod 76:368-73
Kim, Yunjeong; Mandadapu, Sivakoteswara Rao; Groutas, William C et al. (2013) Potent inhibition of feline coronaviruses with peptidyl compounds targeting coronavirus 3C-like protease. Antiviral Res 97:161-8

Showing the most recent 10 out of 32 publications