Antioxidants and Redox Signaling

, volume 19 , issue 11 , pages 1149-1165

Identification of Michael acceptor-centric pharmacophores with substituents that yield strong thioredoxin reductase inhibitory character correlated to antiproliferative activity.

Fei-Fei Gan ¹

Kamila K. Kaminska ¹

Hong Yang ¹

Chin-Yee Liew ¹

Pay Chin Leow ¹

Choon-Leng So ¹

Lan N.L. Tu ¹

Amrita Roy ¹

Chun Wei Yap ¹

Tse Siang Kang ¹

Wai Keung Chui ¹

Eng Hui Chew ¹

Hide authors affiliations Show authors affiliations: 1 affiliation

Department of Pharmacy, National University of Singapore, Singapore, Republic of Singapore. |

Publication type: Journal Article

Publication date: 2013-01-11

Mary Ann Liebert

Antioxidants and Redox Signaling

scimago Q1

wos Q1

SJR: 1.951

CiteScore: 14.5

Impact factor: 6.1

ISSN: 15230864, 15577716

DOI: 10.1089/ars.2012.4909

Copy DOI

PubMed ID: 23311917

Biochemistry

Molecular Biology

Cell Biology

Clinical Biochemistry

Physiology

Abstract

AIMS The role of thioredoxin reductase (TrxR) in tumorigenesis has made it an attractive anticancer target. A systematic approach for development of novel compounds as TrxR inhibitors is currently lacking. Structurally diversified TrxR inhibitors share in common electrophilic propensities for the sulfhydryl groups, among which include the Michael reaction acceptors containing an α,β-unsaturated carbonyl moiety. We aimed to identify features among structurally diversified Michael acceptor-based compounds that would yield a strong TrxR inhibitory character. RESULTS Structurally dissimilar Michael acceptor-based natural compounds such as isobutylamides, zerumbone, and shogaols (SGs) were found to possess a poor TrxR inhibitory activity, indicating that a sole Michael acceptor moiety was insufficient to produce TrxR inhibition. The 1,7-diphenyl-hept-3-en-5-one pharmacophore in 3-phenyl-3-SG, a novel SG analog that possessed comparable TrxR inhibitory and antiproliferative potencies as 6-SG, was modified to yield 1,5-diphenyl-pent-1-en-3-one (DPPen) and 1,3-diphenyl-pro-1-en-3-one (DPPro, also known as chalcone) pharmacophores. These Michael acceptor-centric pharmacophores, when substituted with the hydroxyl and fluorine groups, gave rise to analogs displaying a TrxR inhibitory character positively correlated to their antiproliferative potencies. Lead analogs 2,2'-diOH-5,5'-diF-DPPen and 2-OH-5-F-DPPro yielded a half-maximal TrxR inhibitory concentration of 9.1 and 10.5 μM, respectively, after 1-h incubation with recombinant rat TrxR, with the C-terminal selenocysteine residue found to be targeted. INNOVATION Identification of Michael acceptor-centric pharmacophores among diversified compounds demonstrates that a systematic approach to discover and develop Michael acceptor-based TrxR inhibitors is feasible. CONCLUSION A strong TrxR inhibitory character correlated to the antiproliferative potency is attributed to structural features that include an α,β-unsaturated carbonyl moiety centered in a DPPen or DPPro pharmacophore bearing hydroxyl and fluorine substitutions.

Found

1 citation

Izmest'ev Alexei

PhD in Chemistry

33 publications, 313 citations

h-index: 12

N.D. Zelinsky Institute of Organic Chemistry of the Russian Academy of Sciences

1 citation

Bunev Alexander

🥼 🤝

83 publications, 469 citations, 307 reviews

h-index: 12

Togliatti State University

Research interests

Medicinal Chemistry

1 citation

Bakulina Olga

66 publications, 516 citations, 11 reviews

h-index: 13

Saint Petersburg State University

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GOST |

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GOST Copy

Gan F. et al. Identification of Michael acceptor-centric pharmacophores with substituents that yield strong thioredoxin reductase inhibitory character correlated to antiproliferative activity. // Antioxidants and Redox Signaling. 2013. Vol. 19. No. 11. pp. 1149-1165.

GOST all authors (up to 50) Copy

Gan F., Kaminska K. K., Yang H., Liew C., Leow P. C., So C., Tu L. N., Roy A., Yap C. W., Kang T. S., Chui W. K., Chew E. H. Identification of Michael acceptor-centric pharmacophores with substituents that yield strong thioredoxin reductase inhibitory character correlated to antiproliferative activity. // Antioxidants and Redox Signaling. 2013. Vol. 19. No. 11. pp. 1149-1165.

RIS |

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RIS Copy

TY - JOUR

DO - 10.1089/ars.2012.4909

UR - https://doi.org/10.1089/ars.2012.4909

TI - Identification of Michael acceptor-centric pharmacophores with substituents that yield strong thioredoxin reductase inhibitory character correlated to antiproliferative activity.

T2 - Antioxidants and Redox Signaling

AU - Gan, Fei-Fei

AU - Kaminska, Kamila K.

AU - Yang, Hong

AU - Liew, Chin-Yee

AU - Leow, Pay Chin

AU - So, Choon-Leng

AU - Tu, Lan N.L.

AU - Roy, Amrita

AU - Yap, Chun Wei

AU - Kang, Tse Siang

AU - Chui, Wai Keung

AU - Chew, Eng Hui

PY - 2013

DA - 2013/01/11

PB - Mary Ann Liebert

SP - 1149-1165

IS - 11

VL - 19

PMID - 23311917

SN - 1523-0864

SN - 1557-7716

ER -

BibTex |

Cite this

BibTex (up to 50 authors) Copy

@article{2013_Gan,

author = {Fei-Fei Gan and Kamila K. Kaminska and Hong Yang and Chin-Yee Liew and Pay Chin Leow and Choon-Leng So and Lan N.L. Tu and Amrita Roy and Chun Wei Yap and Tse Siang Kang and Wai Keung Chui and Eng Hui Chew},

title = {Identification of Michael acceptor-centric pharmacophores with substituents that yield strong thioredoxin reductase inhibitory character correlated to antiproliferative activity.},

journal = {Antioxidants and Redox Signaling},

year = {2013},

volume = {19},

publisher = {Mary Ann Liebert},

month = {jan},

url = {https://doi.org/10.1089/ars.2012.4909},

number = {11},

pages = {1149--1165},

doi = {10.1089/ars.2012.4909}

}

MLA

Cite this

MLA Copy

Gan, Fei-Fei, et al. “Identification of Michael acceptor-centric pharmacophores with substituents that yield strong thioredoxin reductase inhibitory character correlated to antiproliferative activity..” Antioxidants and Redox Signaling, vol. 19, no. 11, Jan. 2013, pp. 1149-1165. https://doi.org/10.1089/ars.2012.4909.

Publisher

Mary Ann Liebert

Journal

Antioxidants and Redox Signaling

scimago Q1

wos Q1

SJR

1.951

CiteScore

14.5

Impact factor

6.1

ISSN

15230864 (Print)

15577716 (Electronic)