Sadasivam Murali scite author profile

Lowering the efficacious dose of bone morphogenetic protein-2 (BMP-2) for the repair of critical-sized bone defects is highly desirable, as supra-physiological amounts of BMP-2 have an increased risk of side effects and a greater economic burden for the healthcare system. To address this need, we explored the use of heparan sulfate (HS), a structural analog of heparin, to enhance BMP-2 activity. We demonstrate that HS isolated from a bone marrow stromal cell line (HS5) and heparin each enhances BMP-2-induced osteogenesis in C2C12 myoblasts, through increased ALP activity and osteocalcin mRNA expression. Commercially available HS variants from porcine kidney and bovine lung failed to generate similar effects. Heparin and HS5 influence BMP-2 activity by (i) prolonging BMP-2 half-life, (ii) reducing interactions between BMP-2 with its antagonist noggin, and (iii) modulating BMP2 distribution on the cell surface. Importantly, long-term supplementation of HS5 but not heparin greatly enhances BMP-2-induced bone formation in vitro and in vivo. These results show that bone marrow-derived HS effectively support bone formation, and suggests its applicability in bone repair by selectively facilitating the delivery and bioavailability of BMP-2.

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Receptor-Ligand Interaction between Vitellogenin Receptor (VtgR) and Vitellogenin (Vtg), Implications on Low Density Lipoprotein Receptor and Apolipoprotein B/E

Li¹,

Murali

Ding

2003

Journal of Biological Chemistry

130

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Affinity-selected heparan sulfate for bone repair

et al. 2013

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