ΔNp63α regulates keratinocyte proliferation by controlling PTEN expression and localization

Leonard, Mary K.; Kommagani, Ramakrishna; Payal, Vandana; Mayo, Lindsey D.; Shamma, H. Nicholas; Kadakia, Madhavi

doi:10.1038/cdd.2011.73

Cited by 54 publications

(72 citation statements)

References 36 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Cells were grown, treated and either lysed and analyzed by western blot or immunofluorescence as described previously. 21 For all figures, except Figure S2, PTEN was detected with mouse monoclonal anti-PTEN 6H2.1 antibody in PBS-NGS (1:50 for H1299 cells or 1:25 for all other cells from Cascade Bioscience). Confirmation of PTEN localization by immunofluorescence was shown in Figure S2 with rabbit monoclonal anti-PTEN (#9559) at a dilution of 1:25 (Cell Signaling).…”

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

The PTEN-Akt pathway impacts the integrity and composition of mitotic centrosomes

Leonard

Hill²,

Bubulya³

et al. 2013

Cell Cycle

View full text Add to dashboard Cite

Loss of the tumor suppressor PTEN is observed in many human cancers that display increased chromosome instability and aneuploidy. The subcellular fractions of PTEN are associated with different functions that regulate cell growth, invasion and chromosome stability. In this study, we show a novel role for PTEN in regulating mitotic centrosomes. PTEN localization at mitotic centrosomes peaks between prophase and metaphase, paralleling the centrosomal localization of PLK-1 and γ-tubulin and coinciding with the time frame of centrosome maturation. In primary keratinocytes, knockdown of PTEN increased whole-cell levels of γ-tubulin and PLK-1 in an Akt-dependent manner and had little effect on recruitment of either protein to mitotic centrosomes. Conversely, knockdown of PTEN reduced centrosomal levels of pericentrin in an Akt-independent manner. Inhibition of Akt activation with MK2206 reduced the whole-cell and centrosome levels of PLK-1 and γ-tubulin and also prevented the recruitment of PTEN to mitotic centrosomes. This reduction in centrosome-associated proteins upon inhibition of Akt activity may contribute to the increase in defects in centrosome number and separation observed in metaphase cells. Concomitant PTEN knockdown and Akt inhibition reduced the frequency of metaphase cells with centrosome defects when compared with MK2206 treatment alone, indicating that both PTEN and pAkt are required to properly regulate centrosome composition during mitosis. The findings presented in this study demonstrate a novel role for PTEN and Akt in controlling centrosome composition and integrity during mitosis and provide insight into how PTEN functions as a multifaceted tumor suppressor.

show abstract

Section: Methodsmentioning

confidence: 99%

“…Cells were transfected with non-silencing control or PTEN specific siRNA using a previously described protocol, excepting the use of Lipofectamine RNAiMax instead of Oligofectamine (Life Technologies). 21 The two Akt inhibitors, MK2206 and Perifosine, were purchased from SelleckChem.…”

Section: Methodsmentioning

confidence: 99%

The PTEN-Akt pathway impacts the integrity and composition of mitotic centrosomes

Leonard

Hill²,

Bubulya³

et al. 2013

Cell Cycle

View full text Add to dashboard Cite

show abstract

“…[121][122][123][124][125][126] While the DBD domain is highly conserved among vertebrates and invertebrates, the C terminus varies, resulting in a change from dimeric structure to a tetramer in the vertebrates. [127][128][129] The more ancient members of the family include p73, involved in cancer, 130 neurodevelopment, 131,132 and aging, 133 and p63, involved in epidermal development, 119,[134][135][136] cancer, [137][138][139][140][141] reproduction, 142 and heart development. 143 Understanding the structural restrain of its structure is pivotal to understand the function of p53 [144][145][146] as well as its potential therapeutic exploitation.…”

Section: Discussionmentioning

confidence: 99%

Molecular dynamics of the full-length p53 monomer

Chillemi¹,

Davidovich

D’Abramo³

et al. 2013

Cell Cycle

View full text Add to dashboard Cite

The p53 protein is frequently mutated in a very large proportion of human tumors, where it seems to acquire gain-of-function activity that facilitates tumor onset and progression. A possible mechanism is the ability of mutant p53 proteins to physically interact with other proteins, including members of the same family, namely p63 and p73, inactivating their function. Assuming that this interaction might occurs at the level of the monomer, to investigate the molecular basis for this interaction, here, we sample the structural flexibility of the wild-type p53 monomeric protein. The results show a strong stability up to 850 ns in the DNA binding domain, with major flexibility in the N-terminal transactivations domains (TAD1 and TAD2) as well as in the C-terminal region (tetramerization domain). Several stable hydrogen bonds have been detected between N-terminal or C-terminal and DNA binding domain, and also between N-terminal and C-terminal. Essential dynamics analysis highlights strongly correlated movements involving TAD1 and the proline-rich region in the N-terminal domain, the tetramerization region in the C-terminal domain; Lys120 in the DNA binding region. The herein presented model is a starting point for further investigation of the whole protein tetramer as well as of its mutants

show abstract

“…As a transcriptional repressor, p63 maintains proliferation of basal epidermal keratinocytes by directly repressing expression of antiproliferative target genes, including 14-3-3s, p16/Ink4a, p19/Arf, p21, and PTEN (Westfall et al 2003;Watt et al 2008;Su et al 2009a;Leonard et al 2011;Ferone et al 2012). In addition to cellcycle-associated genes, p63 inhibits the expression of nonkeratinocyte genes (i.e., mesodermal genes), as well as a number of other genes such as distinct components of the Notch (Notch1, Hes1) and bone morphogenetic protein (BMP) signaling pathways (Smad7) in epidermal keratinocytes (Nguyen et al 2006;De Rosa et al 2009;Shalom-Feuerstein et al 2011).…”

Section: Va Botchkarev and Er Floresmentioning

confidence: 99%

p53/p63/p73 in the Epidermis in Health and Disease

Botchkarev

Flores

2014

Cold Spring Harbor Perspectives in Medicine

100

View full text Add to dashboard Cite

Although p53 has long been known as the "guardian of the genome" with a role in tumor suppression in many tissues, the discovery of two p53 ancestral genes, p63 and p73, more than a decade ago has triggered a considerable amount of research into the role of these genes in skin development and diseases. In this review, we primarily focus on mechanisms of action of p53 and p63, which are the best-studied p53 family members in the skin. The existence of multiple isoforms and their roles as transcriptional activators and repressors are key to their function in multiple biological processes including the control of skin morphogenesis, regeneration, tumorigenesis, and response to chemotherapy. Last, we provide directions for further research on this family of genes in skin biology and pathology.

show abstract

ΔNp63α regulates keratinocyte proliferation by controlling PTEN expression and localization

Cited by 54 publications

References 36 publications

The PTEN-Akt pathway impacts the integrity and composition of mitotic centrosomes

The PTEN-Akt pathway impacts the integrity and composition of mitotic centrosomes

Molecular dynamics of the full-length p53 monomer

p53/p63/p73 in the Epidermis in Health and Disease

Contact Info

Product

Resources

About