2013
DOI: 10.1172/jci71488
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LRIG1 inhibits STAT3-dependent inflammation to maintain corneal homeostasis

Abstract: Corneal integrity and transparency are indispensable for good vision. Cornea homeostasis is entirely dependent upon corneal stem cells, which are required for complex wound-healing processes that restore corneal integrity following epithelial damage. Here, we found that leucine-rich repeats and immunoglobulin-like domains 1 (LRIG1) is highly expressed in the human holoclone-type corneal epithelial stem cell population and sporadically expressed in the basal cells of ocular-surface epithelium. In murine models,… Show more

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Cited by 54 publications
(61 citation statements)
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“…Many putative corneal epithelial stem cell markers (e.g. p63, ABCG2, Integrin a9, Keratin 15, N-cadherin, NGF/TrkA, Integrin a6/CD71, Hes1, p75, Nectin 3, Importin 13, Nucleostemin, CD38/157, Lrig1, ABCB5, WNT7A) have been reported worldwide (Di Girolamo et al, 2008;Hayashi et al, 2008Hayashi et al, , 2007Horenstein et al, 2009;Kawashima et al, 2009;Ksander et al, 2014;Kusanagi et al, 2009;Nakamura et al, 2014Nakamura et al, , 2008aOuyang et al, 2014;Pajoohesh-Ganji et al, 2006;Pellegrini et al, 2001;Qi et al, 2008;Wang et al, 2009;Watanabe et al, 2004;Yoshida et al, 2006) (Fig. 10).…”
Section: Candidate Limbal Stem Cell Markersmentioning
confidence: 99%
“…Many putative corneal epithelial stem cell markers (e.g. p63, ABCG2, Integrin a9, Keratin 15, N-cadherin, NGF/TrkA, Integrin a6/CD71, Hes1, p75, Nectin 3, Importin 13, Nucleostemin, CD38/157, Lrig1, ABCB5, WNT7A) have been reported worldwide (Di Girolamo et al, 2008;Hayashi et al, 2008Hayashi et al, , 2007Horenstein et al, 2009;Kawashima et al, 2009;Ksander et al, 2014;Kusanagi et al, 2009;Nakamura et al, 2014Nakamura et al, , 2008aOuyang et al, 2014;Pajoohesh-Ganji et al, 2006;Pellegrini et al, 2001;Qi et al, 2008;Wang et al, 2009;Watanabe et al, 2004;Yoshida et al, 2006) (Fig. 10).…”
Section: Candidate Limbal Stem Cell Markersmentioning
confidence: 99%
“…We next studied the expression of EGFR and CD44v3 in these clusters, since CD44v3 has been shown to modulate EGFR signaling [6,7,8]. Two human skin serial sections from the scalp and from the retroauricular area were stained with antibodies directed against the human form of Lrig1 [1,9,10], EGFR (Cell Signaling, #4267, Danvers, Mass., USA) and CD44v3 (BMS144, Bender MedSystems, Vienna, Austria). The previously described clusters of Lrig1+ cells in the IFE were detected in the basal layer, and these clusters were negative for EGFR (fig.…”
Section: Figmentioning
confidence: 99%
“…It contains 19 β-strands with 16 LRRs (numbered [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15][16]. There are 15 complete LRRs [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15], each with 23-27 residues, where 11 LRRs have the 24-residue repeat [LxxLxLxxNxLxxLxxxx(Hφ)xx(Hφ)xx, where Hφ is any hydrophobic amino acid residue]. LRR16 is only a partial repeat with a new pattern LxxLxIxSxxFx, where Ser appears to replace Asn in the consensus repeat (LxxLxLxxNxLxx).…”
Section: Crystal Structure Of Lrig1-lrr Domainmentioning
confidence: 99%
“…In the last decade, LRIG1 has been reported to interact with many receptor tyrosine kinases, GDNF/c-Ret [11], E-cadherin [12], JAK/STAT [13], c-Met [14,15], and the EGFR family [7,9] signalling systems. In some cases, LRIG1 is reported to reduce receptor levels by increasing the rates of degradation [7]; in other reports, LRIG1 appears to bind directly to the receptor kinase (e.g., the EGFR) [9].…”
mentioning
confidence: 99%