Analytical comparison of a US generic enoxaparin with the originator product: The focus on comparative assessment of antithrombin-binding components

Pierre A J Mourier; Fréderic Herman; Philippe Sizun; Christian Viskov

doi:10.1016/j.jpba.2016.07.033

Analytical comparison of a US generic enoxaparin with the originator product: The focus on comparative assessment of antithrombin-binding components

J Pharm Biomed Anal. 2016 Sep 10:129:542-550. doi: 10.1016/j.jpba.2016.07.033. Epub 2016 Jul 28.

Authors

Pierre A J Mourier¹, Fréderic Herman², Philippe Sizun³, Christian Viskov⁴

Affiliations

¹ Sanofi R&D, Centre de Recherche Vitry-sur-Seine, 13, Quai Jules Guesde, 94403 Vitry-sur Seine, France. Electronic address: Pierre.Mourier@sanofi.com.
² Sanofi R&D, Centre de Recherche Vitry-sur-Seine, 13, Quai Jules Guesde, 94403 Vitry-sur Seine, France. Electronic address: Frederic.Herman@sanofi.com.
³ Sanofi R&D, Centre de Recherche Vitry-sur-Seine, 13, Quai Jules Guesde, 94403 Vitry-sur Seine, France. Electronic address: Philippe.Sizun@sanofi.com.
⁴ Sanofi R&D, Centre de Recherche Vitry-sur-Seine, 13, Quai Jules Guesde, 94403 Vitry-sur Seine, France. Electronic address: Christian.Viskov@sanofi.com.

PMID: 27497655
DOI: 10.1016/j.jpba.2016.07.033

Abstract

Enoxaparin sodium, a low-molecular-weight heparin (LMWH) prepared from porcine intestinal heparin, is widely used for the prevention and treatment of venous thromboembolism. The antithrombotic activity of heparin is mediated mainly through its activation of antithrombin (AT) and subsequent inhibition of coagulation factors. Heparin is a complex heteropolymer and the sulfation pattern of its alternating uronic acid and glucosamine sugar units is a major factor influencing its biological activity. The manufacturing process itself is associated with the introduction of exogenous microheterogeneities that may further affect its biological efficacy. This is important since enoxaparin is prepared by depolymerizing the heparin with the aim of optimizing its biological activity and safety. Changes during its manufacture could thus affect its biological activity and safety. The current study was performed to assess potential differences between the originator enoxaparin and a new generic enoxaparin commercialized by Teva. Heparinase digestion, AT affinity chromatography, gel permeation chromatography, anion exchange chromatography, and nuclear magnetic resonance methodologies were used. The results indicated differences in oligosaccharides related to the cleavage selectivity around the heparin AT-binding sequences of the Teva Enoxaparin Sodium Injection, USP and the originator Sanofi enoxaparin. These differences influence the strength of the AT-binding affinity of the individual oligosaccharides, their ability to activate AT and, therefore, the inhibitory potency on the proteases of the coagulation cascade. This study, together with other published analytical reports, describes specific compositional differences between generics and originator LWMHs. However, it is yet to be established whether such variations might have any clinical relevance.

Keywords: Analytical comparability; Antithrombin affine oligosaccharides; Disaccharide quantification; Enoxaparin sodium; Generic.

Publication types

Comparative Study

MeSH terms

Anticoagulants / chemistry
Antithrombins / chemistry*
Antithrombins / pharmacology*
Chromatography, Affinity / methods
Chromatography, Gel / methods
Drugs, Generic / chemistry*
Enoxaparin / chemistry*
Enoxaparin / pharmacology*
Heparin, Low-Molecular-Weight / chemistry
Magnetic Resonance Spectroscopy / methods
Oligosaccharides / chemistry

Substances

Anticoagulants
Antithrombins
Drugs, Generic
Enoxaparin
Heparin, Low-Molecular-Weight
Oligosaccharides