Synthesis of bioengineered heparin chemically and biologically similar to porcine-derived products and convertible to low MW heparin

肝素 化学 抗凝剂 药理学 生物化学 医学 外科
作者
Marc Douaisi,Elena E. Paskaleva,Li Fu,Navdeep Grover,Charity McManaman,Sony Varghese,Paul R. Brodfuehrer,James M. Gibson,Ian de Joode,Ke Xia,Matthew Brier,Trevor J. Simmons,P.K. Datta,Fuming Zhang,Akihiro Onishi,Makoto Hirakane,Daisuke Mori,Robert J. Linhardt,Jonathan S. Dordick
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:121 (14) 被引量:4
标识
DOI:10.1073/pnas.2315586121
摘要

Heparins have been invaluable therapeutic anticoagulant polysaccharides for over a century, whether used as unfractionated heparin or as low molecular weight heparin (LMWH) derivatives. However, heparin production by extraction from animal tissues presents multiple challenges, including the risk of adulteration, contamination, prion and viral impurities, limited supply, insecure supply chain, and significant batch-to-batch variability. The use of animal-derived heparin also raises ethical and religious concerns, as well as carries the risk of transmitting zoonotic diseases. Chemoenzymatic synthesis of animal-free heparin products would offer several advantages, including reliable and scalable production processes, improved purity and consistency, and the ability to produce heparin polysaccharides with molecular weight, structural, and functional properties equivalent to those of the United States Pharmacopeia (USP) heparin, currently only sourced from porcine intestinal mucosa. We report a scalable process for the production of bioengineered heparin that is biologically and compositionally similar to USP heparin. This process relies on enzymes from the heparin biosynthetic pathway, immobilized on an inert support and requires a tailored N -sulfoheparosan with N -sulfo levels similar to those of porcine heparins. We also report the conversion of our bioengineered heparin into a LMWH that is biologically and compositionally similar to USP enoxaparin. Ultimately, we demonstrate major advances to a process to provide a potential clinical and sustainable alternative to porcine-derived heparin products.
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