Heparin Characterization: Challenges and Solutions

Author:

Jones Christopher J.1,Beni Szabolcs12,Limtiaco John F.K.1,Langeslay Derek J.1,Larive Cynthia K.1

Affiliation:

1. Department of Chemistry, University of California, Riverside, California 92521;, , , ,

2. Department of Pharmaceutical Chemistry, Semmelweis University, H-1092 Budapest, Hungary

Abstract

Although heparin is an important and widely prescribed pharmaceutical anticoagulant, its high degree of sequence microheterogeneity and size polydispersity make molecular-level characterization challenging. Unlike nucleic acids and proteins that are biosynthesized through template-driven assembly processes, heparin and the related glycosaminoglycan heparan sulfate are actively remodeled during biosynthesis through a series of enzymatic reactions that lead to variable levels of O- and N-sulfonation and uronic acid epimers. As summarized in this review, heparin sequence information is determined through a bottom-up approach that relies on depolymerization reactions, size- and charge-based separations, and sensitive mass spectrometric and nuclear magnetic resonance experiments to determine the structural identity of component oligosaccharides. The structure-elucidation process, along with its challenges and opportunities for future analytical improvements, is reviewed and illustrated for a heparin-derived hexasaccharide.

Publisher

Annual Reviews

Subject

Analytical Chemistry

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