Analysis of differential expression of glycosyltransferases in healing corneas by glycogene microarrays

doi:10.1093/glycob/cwp133

Glycobiology Advance Access originally published online on September 7, 2009
Glycobiology 2010 20(1):13-23; doi:10.1093/glycob/cwp133

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Analysis of differential expression of glycosyltransferases in healing corneas by glycogene microarrays

Chandrassegar Saravanan^2,3, Zhiyi Cao³, Steven R Head⁴ and Noorjahan Panjwani¹^,2,3

² Program in Cell, Molecular and Developmental Biology, Sackler School of Graduate Biomedical Sciences
³ Department of Ophthalmology and The New England Eye Center, Tufts University School of Medicine, Boston, MA
⁴ The Scripps Research Institute, La Jolla, CA, USA

¹ To whom correspondence should be addressed: Tel: +1-617-636-6776; Fax: +1-617-636-0348; e-mail: noorjahan.panjwani{at}tufts.edu

Received on December 18, 2008; revised on August 9, 2009; accepted on August 28, 2009

It is generally accepted that the glycans on the cell surfaceand extracellular matrix proteins play a pivotal role in theevents that mediate re-epithelialization of wounds. Yet, theglobal alteration in the structure and composition of glycans,specifically occuring during corneal wound closure remains unknown.In this study, GLYCOv2 glycogene microarray technology was usedfor the first time to identify the differentially expressedglycosylation-related genes in healing mouse corneas. Of $~$ 2000glycogenes on the array, the expression of 11 glycosytransferaseand glycosidase enzymes was upregulated and that of 19 was downregulatedmore than 1.5-fold in healing corneas compared with the normal,uninjured corneas. Among them, notably, glycosyltransferases,β3GalT5, T-synthase, and GnTIVb, were all found to be inducedin the corneas in response to injury, whereas, GnTIII and manysialyltransferases were downregulated. Interestingly, it appearsthat the glycan structures on glycoproteins and glycolipids,expressed in healing corneas as a result of differential regulationof these glycosyltransferases, may serve as specific counter-receptorsfor galectin-3, a carbohydrate-binding protein, known to playa key role in re-epithelialization of corneal wounds. Additionally,many glycogenes including a proteoglycan, glypican-3, cell adhesionproteins dectin-1 and -2, and mincle, and mucin 1 were identifiedfor the first time to be differentially regulated during cornealwound healing. Results of glycogene microarray data were confirmedby qRT-PCR and lectin blot analyses. The differentially expressedglycogenes identified in the present study have not previouslybeen investigated in the context of wound healing and representnovel factors for investigating the role of carbohydrate-mediatedrecognition in corneal wound healing.

Key words: cornea / galectin-3 / glycosyltransferases / microarray / wound healing

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