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7 research outputs found

Optimization of Potent Hepatitis C Virus NS3 Helicase Inhibitors Isolated from the Yellow Dyes Thioflavine S Primuline

Author: Aubé Jeffrey
Belon Craig A.
Blagg Brian S. J.
Frankowski Kevin J.
Frick David N.
Hanson Alicia M.
Li Kelin
Ndjomou Jean
Neuenswander Benjamin
Schoenen Frank J.
Shanahan Matthew A.
Publication venue: 'American Chemical Society (ACS)'
Publication date: 12/04/2012
Field of study

A screen for hepatitis C virus (HCV) NS3 helicase inhibitors revealed that the commercial dye thioflavine S was the most potent inhibitor of NS3-catalyzed DNA and RNA unwinding in the 827-compound National Cancer Institute Mechanistic Set. Thioflavine S and the related dye primuline were separated here into their pure components, all of which were oligomers of substituted benzothiazoles. The most potent compound (P4), a benzothiazole tetramer, inhibited unwinding >50% at 2±1 μM, inhibited the subgenomic HCV replicon at 10 μM, and was not toxic at 100 μM. Because P4 also interacted with DNA, more specific analogs were synthesized from the abundant dimeric component of primuline. Some of the 29 analogs prepared retained ability to inhibit HCV helicase but did not appear to interact with DNA. The most potent of these specific helicase inhibitors (compound 17) was active against the replicon and inhibited the helicase more than 50% at 2.6±1 μM

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PubMed Central

Possibilities and challenges for physical and social environment research in Brazil: a systematic literature review on health behaviors

Author: Alexander A
Amorim TC
Ana Paula Belon
Aveyard H
Ball K
Bandoni DH
Bandoni DH
Barros MV
Bengoechea GE
Boscatto EC
Brownson RC
Brug J
Candace Nykiforuk
Cardoso LO
Caspi CE
Cassou ACN
Cerin E
Clark MI
Cockerham WC
Corseuil MW
Craig CL
Dambros DD
Diez-Roux AV
Ding D
Duncan MJ
Farias Júnior JC
Florindo AA
Florindo AA
Florindo AA
Foster S
Gauthier E
Giles-Corti B
Gobbi S
Gomes GAO
Guedes DP
Hallal PC
Hallal PC
Hino AA
Hino AAF
Hoehner CM
how CK
Humpel N
Jaime PC
Kuntsche E
Liberati A
Lovato CY
Macintyre S
Macintyre S
Malavasi LM
Martins MO
Matsudo SM
Matsudo V
McCormack G
McCormack GR
Mendonça BC
Montemurro GR
Papas MA
Parra DC
Parra DC
Petroski EL
Proietti FA
Raine K
Reis RS
Reis RS
Rydin Y
Saelens BE
Sallis JF
Sallis JF
Sallis JF
Salvador EP
Salvador EP
Santos MS
Santos MS
Scarinci IC
Schmidt MI
Silva DAS
Silva KS
Silva SG
Simões EJ
Swinburn B
van Lenthe FJ
Waddington H
Publication venue: 'FapUNIFESP (SciELO)'
Publication date
Field of study

Crossref

Monitoring helicase activity with molecular beacons

Author: Craig A. Belon
David N. Frick
Frick D.N.
Matson S.W.
Wong I.
Publication venue: 'Future Science Ltd'
Publication date
Field of study

Crossref

Helicase inhibitors as specifically targeted antiviral therapy for hepatitis C

Author: Boguszewska-Chachulska
Borowski
Craig A Belon
David N Frick
Falck-Ytter
Frick
Grakoui
Hicham
Hu
Hwang
Kyono
McHutchison
Murphy
Prabhu
Walker
Wohnsland
Publication venue: 'Future Medicine Ltd'
Publication date
Field of study

Crossref

Optimization of Potent Hepatitis C Virus NS3 Helicase Inhibitors Isolated from the Yellow Dyes Thioflavine S and Primuline

Crossref

Optimization of Potent Hepatitis C Virus NS3 Helicase Inhibitors Isolated from the Yellow Dyes Thioflavine S and Primuline

Author: Alicia M. Hanson (835456)
Ben Neuenswander (2093521)
Brian S. J. Blagg (1316115)
Craig A. Belon (2093524)
David N. Frick (835458)
Frank J. Schoenen (1545445)
Jean Ndjomou (369916)
Jeffrey Aubé (1314141)
Kelin Li (1545454)
Kevin J. Frankowski (1514284)
Matthew A. Shanahan (2093518)
Publication venue
Publication date
Field of study

A screen for hepatitis C virus (HCV) NS3 helicase inhibitors revealed that the commercial dye thioflavine S was the most potent inhibitor of NS3-catalyzed DNA and RNA unwinding in the 827-compound National Cancer Institute Mechanistic Set. Thioflavine S and the related dye primuline were separated here into their pure components, all of which were oligomers of substituted benzothiazoles. The most potent compound (P4), a benzothiazole tetramer, inhibited unwinding >50% at 2 ± 1 μM, inhibited the subgenomic HCV replicon at 10 μM, and was not toxic at 100 μM. Because P4 also interacted with DNA, more specific analogues were synthesized from the abundant dimeric component of primuline. Some of the 32 analogues prepared retained ability to inhibit HCV helicase but did not appear to interact with DNA. The most potent of these specific helicase inhibitors (compound 17) was active against the replicon and inhibited the helicase more than 50% at 2.6 ± 1 μM

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Fuel Specificity of the Hepatitis C Virus NS3 Helicase

Author: Ali
Boguszewska-Chachulska
Carroll
Cho
Craig A. Belon
David N. Frick
Delagoutte
Dumont
Frick
Frick
Frick
Frick
Gwack
Hahm
Heck
Howe
Jennings
Kim
Kim
Kolykhalov
Kyono
Lam
Lam
Lam
Lanzetta
Levin
Levin
Levin
Locatelli
Luo
Mandelkow
Matson
McHutchison
Morris
Murakami
Myong
Neumann-Haefelin
Porter
Preugschat
Quinkert
Serebrov
Sigel
Sikora
Suzich
Tai
Vale
Vamvakopoulos
Wardell
Wu
Yao
Publication venue: 'Elsevier BV'
Publication date
Field of study

Crossref