New PIN1 inhibitors identified through a pharmacophore-driven, hierarchical consensus docking strategy

Giulio Poli; Miriana Di Stefano; Joan Arias Estevez; Filippo Minutolo; Carlotta Granchi; Antonio Giordano; Salvatore Parisi; Matteo Mauceri; Vincenzo Canzonieri; Marco Macchia; Isabella Caligiuri; Tiziano Tuccinardi; Flavio Rizzolio

doi:10.1080/14756366.2021.1979970

Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2022)

New PIN1 inhibitors identified through a pharmacophore-driven, hierarchical consensus docking strategy

Giulio Poli,
Miriana Di Stefano,
Joan Arias Estevez,
Filippo Minutolo,
Carlotta Granchi,
Antonio Giordano,
Salvatore Parisi,
Matteo Mauceri,
Vincenzo Canzonieri,
Marco Macchia,
Isabella Caligiuri,
Tiziano Tuccinardi,
Flavio Rizzolio

Affiliations

Giulio Poli: Department of Pharmacy, University of Pisa
Miriana Di Stefano: Department of Pharmacy, University of Pisa
Joan Arias Estevez: Department of Pharmacy, University of Pisa
Filippo Minutolo: Department of Pharmacy, University of Pisa
Carlotta Granchi: Department of Pharmacy, University of Pisa
Antonio Giordano: Sbarro Institute for Cancer Research and Molecular Medicine, Center for Biotechnology, College of Science and Technology, Temple University
Salvatore Parisi: Pathology Unit, CRO Aviano, National Cancer Institute, IRCCS
Matteo Mauceri: Pathology Unit, CRO Aviano, National Cancer Institute, IRCCS
Vincenzo Canzonieri: Pathology Unit, CRO Aviano, National Cancer Institute, IRCCS
Marco Macchia: Department of Pharmacy, University of Pisa
Isabella Caligiuri: Pathology Unit, CRO Aviano, National Cancer Institute, IRCCS
Tiziano Tuccinardi: Department of Pharmacy, University of Pisa
Flavio Rizzolio: Pathology Unit, CRO Aviano, National Cancer Institute, IRCCS

DOI: https://doi.org/10.1080/14756366.2021.1979970
Journal volume & issue: Vol. 37, no. 1
pp. 145 – 150

Abstract

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PIN1 is considered as a therapeutic target for a wide variety of tumours. However, most of known inhibitors are devoid of cellular activity despite their good enzyme inhibitory profile. Hence, the lack of effective compounds for the clinic makes the identification of novel PIN1 inhibitors a hot topic in the medicinal chemistry field. In this work, we reported a virtual screening study for the identification of new promising PIN1 inhibitors. A receptor-based procedure was applied to screen different chemical databases of commercial compounds. Based on the whole workflow, two compounds were selected and biologically evaluated. Both ligands, compounds VS1 and VS2, showed a good enzyme inhibitory activity and VS2 also demonstrated a promising antitumoral activity in ovarian cancer cells. These results confirmed the reliability of our in silico protocol and provided a structurally novel ligand as a valuable starting point for the development of new PIN1 inhibitors.

Published in Journal of Enzyme Inhibition and Medicinal Chemistry

ISSN: 1475-6366 (Print); 1475-6374 (Online)
Publisher: Taylor & Francis Group
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: https://www.tandfonline.com/journals/ienz

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