Novel oral nano-hepatic targeted anti-PCSK9 in hypercholesterolemia

Taher A Salaheldin; Kavitha Godugu; Dhruba J Bharali; Kazutoshi Fujioka; Nabil Elshourbagy; Shaker A Mousa

doi:10.1016/j.nano.2021.102480

Novel oral nano-hepatic targeted anti-PCSK9 in hypercholesterolemia

Nanomedicine. 2022 Feb:40:102480. doi: 10.1016/j.nano.2021.102480. Epub 2021 Nov 5.

Authors

Taher A Salaheldin¹, Kavitha Godugu¹, Dhruba J Bharali¹, Kazutoshi Fujioka¹, Nabil Elshourbagy², Shaker A Mousa³

Affiliations

¹ The Pharmaceutical Research Institute, Albany College of Pharmacy and Health Sciences, Rensselaer, NY, USA.
² Shifa Biomedical Corporation, Malvern, PA, USA.
³ The Pharmaceutical Research Institute, Albany College of Pharmacy and Health Sciences, Rensselaer, NY, USA. Electronic address: shaker.mousa@acphs.edu.

PMID: 34748962
DOI: 10.1016/j.nano.2021.102480

Abstract

Proprotein convertase subtilisin/kexin type 9 is a protease enzyme secreted by liver that downregulates hepatic low-density lipoprotein receptor (LDLR) by binding and chaperoning LDLR to lysosomes for degradation, causing hypercholesteremia. The development of anti-PCSK9 therapeutics attracted considerable attention for the management of cardiovascular disease risk. However, only subcutaneous injectable PCSK9 monoclonal antibodies have been FDA approved. Oral administration of small-molecule PCSK9 inhibitors has the potential to become a practical therapeutic option if achievable. In the present work, we used nanotechnological approaches to develop the first small oral molecule nano-hepatic targeted anti-PCSK9. Using high-throughput optimization and a series of evaluations, a stable water-dispersible 150-200 nm nano-encapsulated drug (named P-4) conjugated with hepatic targeting moiety was synthesized and characterized (named P-21). Pharmacodynamic (PD), pharmacokinetic (PK) and bioavailability studies were conducted using a high fat diet nutritionally induced hypercholesterolemia mouse model to evaluate the efficacy of P-21 as an anti-PCSK9 LDL-cholesterol lowering hepatic targeted nanodrug. The PD results demonstrate that P-21 in a dose-dependent manner is highly effective in lowering LDL-C by 50-90%. PK results show the maximum plasma concentration (C_max) of P-4 was observed after 30 min of administration with 31% oral bioavailability and had a sustained longer half-life up to 24 h. In vivo safety studies in rats showed no apparent adverse effects, normal chemical biomarkers and normal histopathological findings in all P-21 treated groups at different escalating doses. Compared to the FDA-approved monoclonal antibodies, P-21 offers a more efficient, and practical treatment protocol for targeting uncontrolled hypercholesterolemia in reducing the risk of cardiovascular diseases. The present study introduced a nano-targeted drug delivery approaches for PCSK9/LDLR antagonist.

Keywords: Anti-PCSK9; Cardiovascular diseases; Dyslipidemia; Hepatic targeting; Hypercholesterolemia; Nano-encapsulation; PCSK9/LDLR.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cholesterol, LDL / metabolism
Cholesterol, LDL / therapeutic use
Hypercholesterolemia* / drug therapy
Hypercholesterolemia* / metabolism
Liver / metabolism
Mice
Proprotein Convertase 9* / metabolism
Proprotein Convertase 9* / therapeutic use
Rats
Receptors, LDL / metabolism

Substances

Cholesterol, LDL
Receptors, LDL
PCSK9 protein, human
Proprotein Convertase 9

Grants and funding

R44 HL137449/HL/NHLBI NIH HHS/United States