Pin1 modulates p63α protein stability in regulation of cell survival, proliferation and tumor formation

Li, Chenshuang; Chang, Donny L.F.; Yang, Zemin; Qi, Jin; Liu, R; He, Hualong; Li, D; Xiao, Zhi

doi:10.1038/cddis.2013.468

Cited by 50 publications

(77 citation statements)

References 37 publications

(62 reference statements)

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“…Therefore, in keeping with very recent studies, 99 the Thr phosphorylation and the action of Pin1 on p63 directly regulates the physical recognition and interaction of Itch, similar to what has been described in the case of WWP1, 98,99,110 affecting the steady-state levels of the p63 protein. This could be also explained with a proline trans to cis isomerization of the p(T/S)P motif by Pin1.…”

Section: Effect Of the Phosphorylation And The Cis/trans Isomerizatiosupporting

confidence: 83%

“…[94][95][96][97] In order to understand the biochemical properties of the interaction between these 2 proteins, the interaction between the Itch-WW2 and the synthetic peptide pep63, including the PPxY recognition motif, has been monitored using spectroscopic techniques; the apparent dissociation constant value of the Itch-WW2-pep63 complex has been reported previously. 96 The presence of the consensus TP motif, close to the PPxY recognition motif, and also the recent studies on the Pin1/p63 interaction 98,99 led us to evaluate the effect of the threonine phosphorylation of the (T/S)PPPxY motif on the binding of the Itch-WW domains to the pep63 peptide. The measured apparent dissociation constants of Itch-WW2 with both pep63 and the phosphorylated Thr form Ppep63 were obtained from the intrinsic fluorescence of the domain upon addition of increasing amounts of the peptides, resulting in a value of 42.09 § 7.45 mM (for the WW2-pep63), which is in keeping with our previously reported value, 96 and 10.97 § 1.45 mM for the Itch-WW2-Ppep63 (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…107 As reported above, p(T/ S)P motif is a characteristic recognition binding motif of the WW domain of Pin1 proline isomerase and recent data have shown a catalytic action of Pin1 on p63. 99 Therefore we have investigated the effect of the cis/trans isomerization of the first proline on the binding of the Itch-WW-p(T/S)PPPxY motif. Firstly, the binding between Itch-WW2 and Ppep63, following a previous incubation of the Ppep63 with Pin1 aimed at creating a proline cis/trans isomerization, has been analyzed by fluorescence spectroscopy (Fig.…”

Section: Pro Cis/trans Isomerization Of Tp Motif Modulates the Itch-wmentioning

confidence: 99%

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p63 threonine phosphorylation signals the interaction with the WW domain of the E3 ligase Itch

et al. 2014

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Both in epithelial development as well as in epithelial cancers, the p53 family member p63 plays a crucial role acting as a master transcriptional regulator. P63 steady state protein levels are regulated by the E3 ubiquitin ligase Itch, via a physical interaction between the PPxY consensus sequence (PY motif) of p63 and one of the 4 WW domains of Itch; this substrate recognition process leads to protein-ubiquitylation and p63 proteasomal degradation. The interaction of the WW domains, a highly compact protein-protein binding module, with the short proline-rich sequences is therefore a crucial regulatory event that may offer innovative potential therapeutic opportunity. Previous molecular studies on the Itch-p63 recognition have been performed in vitro using the Itch-WW2 domain and the peptide interacting fragment of p63 (pep63), which includes the PY motif. Itch-WW2-pep63 interaction is also stabilized in vitro by the conformational constriction of the S-S cyclization in the p63 peptide. The PY motif of p63, as also for other proteins, is characterized by the nearby presence of a (T/S)P motif, which is a potential recognition site of the WW domain of the IV group present in the prolyl-isomerase Pin1. In this study, we demonstrate, by in silico and spectroscopical studies using both the linear pep63 and its cyclic form, that the threonine phosphorylation of the (T/S)PPPxY motif may represent a crucial regulatory event of the Itch-mediated p63 ubiquitylation, increasing the Itch-WW domains-p63 recognition event and stabilizing in vivo the Itch-WW-p63 complex. Moreover, our studies confirm that the subsequently trans/cis proline isomerization of (T/S)P motif by the Pin1 prolyl-isomerase, could modulate the E3-ligase interaction, and that the (T/S) p P trans PPxY motif represent the best conformer for the ItchWW-(T/S)PPPxY motif recognition.

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Section: Effect Of the Phosphorylation And The Cis/trans Isomerizatiosupporting

confidence: 83%

Section: Resultsmentioning

confidence: 99%

Section: Pro Cis/trans Isomerization Of Tp Motif Modulates the Itch-wmentioning

confidence: 99%

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p63 threonine phosphorylation signals the interaction with the WW domain of the E3 ligase Itch

et al. 2014

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“…These sites are absent in the p63g isoforms. Recent evidence shows that Pin1 stabilizes the a isoforms, but not the g variants (Li et al, 2013). This supports that the six Pin1-binding sites in the C-terminal region may play a critical role in p63a stability.…”

Section: P63: Regulationmentioning

confidence: 64%

“…The peptidyl-prolyl isomerase Pin1 may modulate p63 activity. This in turn affects cell survival/proliferation and tumorigenesis (Li et al, 2013). Pin1 consists of an N-terminal WW domain and a C-terminal peptidyl-prolyl cis/trans isomerase (PPIase) domain.…”

Section: P63: Regulationmentioning

confidence: 99%

P63 in health and cancer

Gonfloni

Caputo²,

Iannizzotto³

2015

Int. J. Dev. Biol.

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TP63 is the most ancient member of the p53 gene family. The p53 family comprises three transcription factors (p53/p63/p73). They share a high degree of homology and similar domain structure. Yet, they can exist as truncated isoforms. Alternative promoters and splicing sites lead to the generation of several molecules. P53/p63/p73 are important to maintain cell homeostasis. P63 and p73 regulate many p53 target genes. This is due to their common structural features. Both proteins may compensate the loss of p53. This is a common event occurring in more than 50% of malignancies. Yet, p63 (or p73) has its own role. Studies from p63-null mice have shown the key role of p63 in embryo development. Several reports have supported the p63 role in epidermal development and in skin homeostasis. P63 involvement in heart development is currently being researched. Recent studies have found p63 to be "the guardian of human reproduction". In addition, p63 has an important, even controversial, role in cancer. Here, we provide a general overview of p63 regulation and activity. We discuss emerging concepts about its role in germ line protection, metabolism and cancer.

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Cullin3/KCTD5 induces monoubiquitination of ΔNp63α and impairs its activity

Peng

Fan

et al. 2018

FEBS Letters

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Potassium channel tetramerization domain containing 5 (KCTD5) was previously documented as a component of the Cullin3-RING ligase (CRL3). It has been reported that KCTD5 can induce enrichment of polyubiquitinated proteins, and KCTD5-based CRL3 destabilizes several proteins. In our present study, we report that KCTD5 may physically interact with ΔNp63α, which is a member of the p53 family. Our further investigation revealed that Cullin3/KCTD5 can induce monoubiquitination of ΔNp63α. Cullin3/KCTD5 downregulates the DNA-binding affinity of ΔNp63α, impairing either its transactivity or its transinhibitory activity. Functionally, Cullin3/KCTD5 abates the proproliferation activity of ΔNp63α. These findings suggest that KCTD5-based CRL3 may mediate monoubiquitination and is a novel regulator of ΔNp63α.

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Pin1 modulates p63α protein stability in regulation of cell survival, proliferation and tumor formation

Cited by 50 publications

References 37 publications

p63 threonine phosphorylation signals the interaction with the WW domain of the E3 ligase Itch

p63 threonine phosphorylation signals the interaction with the WW domain of the E3 ligase Itch

P63 in health and cancer

Cullin3/KCTD5 induces monoubiquitination of ΔNp63α and impairs its activity

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