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XB-ART-47480
J Biol Chem 2013 Nov 08;28845:32809-32820. doi: 10.1074/jbc.M113.512962.
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Stabilization of speckle-type POZ protein (Spop) by Daz interacting protein 1 (Dzip1) is essential for Gli turnover and the proper output of Hedgehog signaling.

Schwend T , Jin Z , Jiang K , Mitchell BJ , Jia J , Yang J .


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The Hedgehog (Hh) pathway is essential for embryonic development and adult tissue homeostasis. The Gli/Cubitus interruptus (Ci) family of transcription factors acts at the downstream end of the pathway to mediate Hh signaling. Both Hh-dependent and -independent Gli regulatory mechanisms are important for the output of Hh signaling. Daz interacting protein 1 (Dzip1) has bipartite positive and negative functions in the Hh pathway. The positive Hh regulatory function appears to be attributed to a requirement for Dzip1 during ciliogenesis. The mechanism by which Dzip1 inhibits Hh signaling, however, remains largely unclear. We recently found that Dzip1 is required for Gli turnover, which may account for its inhibitory function in Hh signaling. Here, we report that Dzip1 regulates Gli/Ci turnover by preventing degradation of speckle-type POZ protein (Spop), a protein that promotes proteasome-dependent turnover of Gli proteins. We provide evidence that Dzip1 regulates the stability of Spop independent of its function in ciliogenesis. Partial knockdown of Dzip1 to levels insufficient for perturbing ciliogenesis, sensitized Xenopus embryos to Hh signaling, leading to phenotypes that resemble activation of Hh signaling. Importantly, overexpression of Spop was able to restore proper Gli protein turnover and rescue phenotypes in Dzip1-depleted embryos. Consistently, depletion of Dzip1 in Drosophila S2 cells destabilized Hh-induced BTB protein (HIB), the Drosophila homolog of Spop, and increased the level of Ci. Thus, Dzip1-dependent stabilization of Spop/HIB is evolutionarily conserved and essential for proper regulation of Gli/Ci proteins in the Hh pathway.

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Species referenced: Xenopus laevis
Genes referenced: dzip1 foxa2 gli1 gli2 ift88 myc nkx2-2 odc1 pax2 pax6 pou4f4 ptch1 rax shh smo spop sufu tuba4b
???displayArticle.antibodies??? FLAG Ab1 Myc Ab2 Myh7 Ab5 Spop AB1 Tuba4b Ab4 Tubb3 Ab2 Ubiquitin Ab1
???displayArticle.morpholinos??? dzip1 MO1 dzip1 MO2 gli1 MO1 gli2 MO1 ift88 MO2


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References [+] :
Aza-Blanc, Proteolysis that is inhibited by hedgehog targets Cubitus interruptus protein to the nucleus and converts it to a repressor. 1997, Pubmed