Dihydroquinazoline and Triazinedione Derivatives as Prok1 and Prok2 receptor antagonists in HEK-293 transfected cells

BALBONI, GIANFRANCO;CONGIU, CENZO;DEPLANO, ALESSANDRO;DEMURTAS, MONICA;
2015-01-01

Abstract

Prokineticin were originally identified as potent agents mediating gut motility, but were later shown to promote angiogenesis in steroidogenic glands, heart and reproductive system. They also modulate neurogenesis, circadian rhythms, nociception, haematopoiesis as well as immune response.[1] Prokineticin are thought to be associated with pathologies of the reproductive systems,[2] myocardial infarction,[3] and tumorigenesis.[4,5] Consequently, antagonism of the prokineticins functions may have utility in the treatment of disorders or diseases including gastrointestinal motility, angiogenesis, haematopoiesis, diabetes and pain. Here we report the identification and pharmacological characterization of a new prototype (KYS-05090) in comparison with our reference prokineticin receptor antagonist (PC-7), [6, 7] (Figure 1). Figure 1. Prokineticin receptor antagonists
2015
Inglese
XXIII National Meeting on Medicinal Chemistry Abstract Book
97
97
1
XXIII National Meeting on Medicinal Chemistry
Comitato scientifico
September 6-9, 2015
Salerno
internazionale
scientifica
4 Contributo in Atti di Convegno (Proceeding)::4.1 Contributo in Atti di convegno
Balboni, Gianfranco; Congiu, Cenzo; Deplano, Alessandro; Demurtas, Monica; Buyn, Joon Seok; Sohn, Joo Mi; Lee, Jae Yeol; Sbai, Oualid; Rondard, Philippe; Onnis, Valentina
273
10
4.1 Contributo in Atti di convegno
open
info:eu-repo/semantics/conferencePaper
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