نتایج جستجو برای: p63 protein

تعداد نتایج: 1236271  

2016
Pandurangan Harikrishnan Sowmiya Murali

P63 is basically a stem cell marker. It belongs to p53 protein family which comprises of transcription factors p53, p63, p73. P63 also possesses two isoforms which are interestingly with opposing characters. Its complexity remains unrevealed with helps in maintenance of genetic stability of germ cells, mechanisms of p63 behaves both monogenic as well as tumor suppressor of its various isoforms....

2012
Giustina Ferone Helen A Thomason Dario Antonini Laura De Rosa Bing Hu Marica Gemei Huiqing Zhou Raffaele Ambrosio David P Rice Dario Acampora Hans van Bokhoven Luigi Del Vecchio Maranke I Koster Gianluca Tadini Bradley Spencer-Dene Michael Dixon Jill Dixon Caterina Missero

Ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome, which is characterized by cleft palate and severe defects of the skin, is an autosomal dominant disorder caused by mutations in the gene encoding transcription factor p63. Here, we report the generation of a knock-in mouse model for AEC syndrome (p63(+/L514F) ) that recapitulates the human disorder. The AEC mutation exerts a se...

Journal: :The Journal of biological chemistry 2005
Carole Abi Farah Dalinda Liazoghli Sébastien Perreault Mylène Desjardins Alain Guimont Angela Anton Michel Lauzon Gert Kreibich Jacques Paiement Nicole Leclerc

Neurons are polarized cells presenting two distinct compartments, dendrites and an axon. Dendrites can be distinguished from the axon by the presence of rough endoplasmic reticulum (RER). The mechanism by which the structure and distribution of the RER is maintained in these cells is poorly understood. In the present study, we investigated the role of the dendritic microtubule-associated protei...

2010
Annie Yang Zhou Zhu Arminja Kettenbach Philipp Kapranov Frank McKeon Thomas R. Gingeras Kevin Struhl

BACKGROUND The p53 homologs, p63 and p73, share approximately 85% amino acid identity in their DNA-binding domains, but they have distinct biological functions. PRINCIPAL FINDINGS Using chromatin immunoprecipitation and high-resolution tiling arrays covering the human genome, we identify p73 DNA binding sites on a genome-wide level in ME180 human cervical carcinoma cells. Strikingly, the p73 ...

Journal: :Frontiers in oncology 2016
Maria Ferraiuolo Silvia Di Agostino Giovanni Blandino Sabrina Strano

The p53 gene family members p53, p73, and p63 display several isoforms derived from the presence of internal promoters and alternative splicing events. They are structural homologs but hold peculiar functional properties. p53, p73, and p63 are tumor suppressor genes that promote differentiation, senescence, and apoptosis. p53, unlike p73 and p63, is frequently mutated in cancer often displaying...

Journal: :Biomedical papers of the Medical Faculty of the University Palacky, Olomouc, Czechoslovakia 2004
Drahomíra Cernochová Eva Pospísilová Dana Kylarová

We studied p53, p63, p73 protein expression in the orofacial region of five human embryos aged 7-18 weeks of intrauterine development using a three-step immunohistochemical method. Expression of proteins in various locations was evaluated semiquantitatively. A decrease in p53, p63 and p73 proteins occurred in the 13-week-old material with the exception of the tooth germ where a drop in p73 appe...

2006
Elisabetta Sbisà Giuseppe Mastropasqua Kostantinos Lefkimmiatis Mariano Francesco Caratozzolo Anna Maria D'Erchia Apollonia Tullo

An unresolved issue regards the role of p73 and p63, the two homologs of the p53 oncosuppressor gene, in normal cells and in tumor development. Specific target genes for each protein need to be identified and characterized in order to understand the specific role of each protein in tumor initiation and progression as well as in oncosuppression and development. We tested whether p63 is implicate...

2016
Carla Regina Mirco Compagnone Angelo Peschiaroli AnnaMaria Lena Margherita Annicchiarico-Petruzzelli Maria Cristina Piro Gerry Melino Eleonora Candi

ΔNp63 has been recently involved in self-renewal potential of breast cancer stem cells. Although the p63 transcriptional profile has been extensively characterized, our knowledge of the p63-binding partners potentially involved in the regulation of breast tumour progression is limited. Here, we performed the yeast two hybrid approach to identify p63α interactors involved in breast tumorigenesis...

2012
Sumihisa Imakado Ryo Masuda

The authors report a case of mucinous carcinoma of the male breast firstly diagnosed as a mucinous carcinoma of the skin. The immunohistochemical results of this tumor were as follows: cytokeratin7 (-), gross cystic disease fluid protein 15 (-), p63 (-), estrogen receptor (+), and progesterone receptor (+) for the primary nodule; cytokeratin7 (-), thyroid transcription factor-1 (-), gross cysti...

Journal: :Cancer research 2009
Konstantinos Lefkimmiatis Mariano Francesco Caratozzolo Paola Merlo Anna Maria D'Erchia Beatriz Navarro Massimo Levrero Elisabetta Sbisa' Apollonia Tullo

Despite extensive studies on the role of tumor suppressor p53 protein and its homologues, p73 and p63, following their overexpression or cellular stress, very little is known about the regulation of the three proteins in cells during physiologic cell cycle progression. We report a role for p73 and p63 in supporting cellular proliferation through the transcriptional activation of the genes invol...

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