2009
DOI: 10.1128/mcb.01620-08
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Glis3 Is Associated with Primary Cilia and Wwtr1/TAZ and Implicated in Polycystic Kidney Disease

Abstract: In this study, we describe the generation and partial characterization of Krüppel-like zinc finger protein Glis3 mutant (Glis3 zf/zf ) mice. These mice display abnormalities very similar to those of patients with neonatal diabetes and hypothyroidism syndrome, including the development of diabetes and polycystic kidney disease. We demonstrate that Glis3 localizes to the primary cilium, suggesting that Glis3 is part of a cilium-associated signaling pathway. Although Glis3 zf/zf mice form normal primary cilia, re… Show more

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Cited by 82 publications
(113 citation statements)
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“…SUFU has been shown to co-localize to the primary cilium with Gli proteins, and although the functional consequence of their co-localization is still far from being understood, both primary cilium-dependent and -independent regulation of Gli proteins by SUFU have been reported (32,33,41,42). In this context it is interesting to note that Glis2 and Glis3 have also been localized to the primary cilium (7,10,44). One might speculate that SUFU-Glis3 interaction might be linked functionally to the primary cilium and possibly involved in the regulation of Glis3 activity.…”
Section: Discussionmentioning
confidence: 99%
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“…SUFU has been shown to co-localize to the primary cilium with Gli proteins, and although the functional consequence of their co-localization is still far from being understood, both primary cilium-dependent and -independent regulation of Gli proteins by SUFU have been reported (32,33,41,42). In this context it is interesting to note that Glis2 and Glis3 have also been localized to the primary cilium (7,10,44). One might speculate that SUFU-Glis3 interaction might be linked functionally to the primary cilium and possibly involved in the regulation of Glis3 activity.…”
Section: Discussionmentioning
confidence: 99%
“…We reported previously that Glis3 robustly activates transcription of murine Ins2 via its proximal promoter, which contains two functional Glis-responsive elements (7,8). To assess the potential role of the Glis3 N terminus in modulating Glis3 transcriptional activity, we examined the effect of various N-terminal deletions on the activation of the Ins2 promoter.…”
Section: Resultsmentioning
confidence: 99%
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