A Novel, Orally Bioavailable, Small-Molecule Inhibitor of PCSK9 With Significant Cholesterol-Lowering Properties In Vivo

Alexandra K Suchowerska; Geurt Stokman; James T Palmer; Phillip A Coghlan; Elsbet J Pieterman; Nanda Keijzer; Gilles Lambert; Kevin Chemello; Ali K Jaafar; Jasneet Parmar; Liping Yan; Yingtao Tong; Lin Mu; Hans M G Princen; James Bonnar; Benny J Evison

doi:10.1016/j.jlr.2022.100293

A Novel, Orally Bioavailable, Small-Molecule Inhibitor of PCSK9 With Significant Cholesterol-Lowering Properties In Vivo

J Lipid Res. 2022 Nov;63(11):100293. doi: 10.1016/j.jlr.2022.100293. Epub 2022 Oct 6.

Authors

Affiliations

¹ Nyrada Inc., Gordon, New South Wales, Australia.
² Metabolic Health Research, The Netherlands Organization of Applied Scientific Research, Leiden, The Netherlands.
³ Pharmaceutical Discovery Consultation, Warrandyte, Victoria, Australia.
⁴ i-Chem Consulting, Condell Park, New South Wales, Australia.
⁵ Laboratoire Inserm UMR 1188 DeTROI, Universite de la Reunion Plateforme CYROI, Sainte Clotilde, France.
⁶ DMPK/Exploratory Toxicology Department, Shanghai ChemPartner Co., Ltd., Shanghai, China.
⁷ Nyrada Inc., Gordon, New South Wales, Australia. Electronic address: benny.evison@nyrada.com.

Abstract

Proprotein convertase subtilisin kexin type 9 (PCSK9) inhibits the clearance of low-density lipoprotein (LDL) cholesterol (LDL-C) from plasma by directly binding with the LDL receptor (LDLR) and sending the receptor for lysosomal degradation. As the interaction promotes elevated plasma LDL-C levels, and therefore a predisposition to cardiovascular disease, PCSK9 has attracted intense interest as a therapeutic target. Despite this interest, an orally bioavailable small-molecule inhibitor of PCSK9 with extensive lipid-lowering activity is yet to enter the clinic. We report herein the discovery of NYX-PCSK9i, an orally bioavailable small-molecule inhibitor of PCSK9 with significant cholesterol-lowering activity in hyperlipidemic APOE∗3-Leiden.CETP mice. NYX-PCSK9i emerged from a medicinal chemistry campaign demonstrating potent disruption of the PCSK9-LDLR interaction in vitro and functional protection of the LDLR of human lymphocytes from PCSK9-directed degradation ex vivo. APOE∗3-Leiden.CETP mice orally treated with NYX-PCSK9i demonstrated a dose-dependent decrease in plasma total cholesterol of up to 57%, while its combination with atorvastatin additively suppressed plasma total cholesterol levels. Importantly, the majority of cholesterol lowering by NYX-PCSK9i was in non-HDL fractions. A concomitant increase in total plasma PCSK9 levels and significant increase in hepatic LDLR protein expression strongly indicated on-target function by NYX-PCSK9i. Determinations of hepatic lipid and fecal cholesterol content demonstrated depletion of liver cholesteryl esters and promotion of fecal cholesterol elimination with NYX-PCSK9i treatment. All measured in vivo biomarkers of health indicate that NYX-PCSK9i has a good safety profile. NYX-PCSK9i is a potential new therapy for hypercholesterolemia with the capacity to further enhance the lipid-lowering activities of statins.

Keywords: LDL; PCSK9; apolipoproteins; cardiovascular disease; drug therapy; hypercholesterolemia; lipoproteins; lysosomal degradation; small-molecule; statins.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Anticholesteremic Agents* / pharmacology
Apolipoproteins E
Cholesterol
Cholesterol, LDL
Humans
Hyperlipidemias* / drug therapy
Mice
PCSK9 Inhibitors* / pharmacology
Receptors, LDL* / genetics
Receptors, LDL* / metabolism

Substances

Apolipoproteins E
Cholesterol
Cholesterol, LDL
Receptors, LDL
PCSK9 Inhibitors
Anticholesteremic Agents