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Published February 2007 | public
Journal Article

Profiling the sulfation specificities of glycosaminoglycan interactions with growth factors and chemotactic proteins using microarrays

Abstract

We report a carbohydrate microarray-based approach for the rapid, facile analysis of glycosaminoglycan-protein interactions. The key structural determinants responsible for protein binding, such as sulfate groups that participate in the interactions, were elucidated. Specificities were also readily compared across protein families or functional classes, and comparisons among glycosaminoglycan subclasses provided a more comprehensive understanding of protein specificity. To validate the approach, we showed that fibroblast growth factor family members have distinct sulfation preferences. We also demonstrated that heparan sulfate and chondroitin sulfate interact in a sulfation-dependent manner with various axon guidance proteins, including slit2, netrin1, ephrinA1, ephrinA5, and semaphorin5B. We anticipate that these microarrays will accelerate the discovery of glycosaminoglycan-binding proteins and provide a deeper understanding of their roles in regulating diverse biological processes.

Additional Information

© 2007 Elsevier Ltd. Received: August 30, 2006; Revised: December 13, 2006; Accepted: December 28, 2006; Published: February 23, 2007. We thank Dr. J.L. Riechmann, Director of the Millard and Muriel Jacobs Genetics and Genomics Laboratory at the California Institute of Technology, for assistance with printing the microarrays, and Dr. S.E. Tully, C.J. Rogers, and Dr. M.C. Bryan for helpful discussions. We also thank M. Ward, Professor Y. Rao, and Professor J. Wu for the slit2 and netrin1 cell lines and for training in neuronal migration and coculture techniques. We thank Professor A. Kolodkin and R. Matsuoka for the generous gift of sema5B. This research was supported by a National Science Foundation Minority Postdoctoral Fellowship (E.L.S.), the National Institutes of Health (RO1 NS045061), the American Cancer Society (RSG-05-106-01-CDD), and the Tobacco-Related Disease Research Program (14RT-0034).

Additional details

Created:
August 19, 2023
Modified:
October 23, 2023