Potent and Selective Human Neutrophil Elastase Inhibitors with Novel Equatorial Ring Topology: in Vivo Efficacy of the Polar Pyrimidopyridazine BAY-8040 in a Pulmonary Arterial Hypertension Rat Model

Overview

Journal ChemMedChem

Specialties Chemistry
Pharmacology

Date 2015 Sep 4

PMID 26333652

Citations 12

Authors

Franz von Nussbaum

Volkhart M Li

Daniel Meibom

Sonja Anlauf

Martin Bechem

Martina Delbeck

Michael Gerisch

Axel Harrenga

Dagmar Karthaus

Dieter Lang

Klemens Lustig

Joachim Mittendorf

Martina Schafer

Stefan Schafer

Jens Schamberger

Affiliations

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Abstract

Human neutrophil elastase (HNE) is a key driver of inflammation in many cardiopulmonary and systemic inflammatory and autoimmune conditions. Overshooting high HNE activity is the consequence of a disrupted protease-antiprotease balance. Accordingly, there has been an intensive search for potent and selective HNE inhibitors with suitable pharmacokinetics that would allowing oral administration in patients. Based on the chemical probe BAY-678 and the clinical candidate BAY 85-8501 we explored further ring topologies along the equator of the parent pyrimidinone lead series. Novel ring systems were annulated in the east, yielding imidazolo-, triazolo-, and tetrazolopyrimidines in order to ensure additional inhibitor-HNE contacts beyond the S1 and the S2 pocket of HNE. The western annulation of pyridazines led to the polar pyrimidopyridazine BAY-8040, which combines excellent potency and selectivity with a promising pharmacokinetic profile. In vivo efficacy with regard to decreasing cardiac remodeling and amelioration of cardiac function was shown in a monocrotaline-induced rat model for pulmonary arterial hypertension. This demonstrated in vivo proof of concept in animals.

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