Galectin-7 modulates the length of the primary cilia and wound repair in polarized kidney epithelial cells

Author:

Rondanino Christine1,Poland Paul A.1,Kinlough Carol L.1,Li Hui1,Rbaibi Youssef1,Myerburg Michael M.2,Al-bataineh Mohammad M.1,Kashlan Ossama B.1,Pastor-Soler Nuria M.13,Hallows Kenneth R.13,Weisz Ora A.13,Apodaca Gerard13,Hughey Rebecca P.13

Affiliation:

1. Renal-Electrolyte Division and

2. Pulmonary Division, Department of Medicine, and

3. Department of Cell Biology and Physiology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania

Abstract

Galectins (Gal) are β-galactoside-binding proteins that function in epithelial development and homeostasis. An overlapping role for Gal-3 and Gal-7 in wound repair was reported in stratified epithelia. Although Gal-7 was thought absent in simple epithelia, it was reported in a proteomic analysis of cilia isolated from cultured human airway, and we recently identified Gal-7 transcripts in Madin-Darby canine kidney (MDCK) cells (Poland PA, Rondanino C, Kinlough CL, Heimburg-Molinaro J, Arthur CM, Stowell SR, Smith DF, Hughey RP. J Biol Chem 286: 6780–6790, 2011). We now report that Gal-7 is localized exclusively on the primary cilium of MDCK, LLC-PK1(pig kidney), and mpkCCDc14(mouse kidney) cells as well as on cilia in the rat renal proximal tubule. Gal-7 is also present on most cilia of multiciliated cells in human airway epithelia primary cultures. Interestingly, exogenous glutathione S-transferase (GST)-Gal-7 bound the MDCK apical plasma membrane as well as the cilium, while the lectin Ulex europeaus agglutinin, with glycan preferences similar to Gal-7, bound the basolateral plasma membrane as well as the cilium. In pull-down assays, β1-integrin isolated from either the basolateral or apical/cilia membranes of MDCK cells was similarly bound by GST-Gal-7. Selective localization of Gal-7 to cilia despite the presence of binding sites on all cell surfaces suggests that intracellular Gal-7 is specifically delivered to cilia rather than simply binding to surface glycoconjugates after generalized secretion. Moreover, depletion of Gal-7 using tetracycline-induced short-hairpin RNA in mpkCCDc14cells significantly reduced cilia length and slowed wound healing in a scratch assay. We conclude that Gal-7 is selectively targeted to cilia and plays a key role in surface stabilization of glycoconjugates responsible for integrating cilia function with epithelial repair.

Publisher

American Physiological Society

Subject

Physiology

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