نتایج جستجو برای: ret ptc rearrangements

تعداد نتایج: 22926  

Journal: :Cancer research 2005
Norisato Mitsutake Jeffrey A Knauf Shin Mitsutake Cleo Mesa Lei Zhang James A Fagin

The activating mutation BRAF(T1796A) is the most prevalent genetic alteration in papillary thyroid carcinomas (PTC). It is associated with advanced PTCs, suggesting that this oncoprotein confers thyroid cancers with more aggressive properties. BRAF(T1796A) is also observed in thyroid micropapillary carcinomas and may thus be an early event in tumor development. To explore its biological consequ...

2014
Emanuela Minna Paola Romeo Loris De Cecco Matteo Dugo Giuliana Cassinelli Silvana Pilotti Debora Degl'Innocenti Cinzia Lanzi Patrizia Casalini Marco A. Pierotti Angela Greco Maria Grazia Borrello

Thyroid cancer incidence is rapidly increasing. Papillary Thyroid Carcinoma (PTC), the most frequent hystotype, usually displays good prognosis, but no effective therapeutic options are available for the fraction of progressive PTC patients. BRAF and RET/PTC are the most frequent driving genetic lesions identified in PTC. We developed two complementary in vitro models based on RET/PTC1 oncogene...

2011
Paula Soares Jorge Lima Ana Preto Patricia Castro João Vinagre Ricardo Celestino Joana P Couto Hugo Prazeres Catarina Eloy Valdemar Máximo M Sobrinho-Simões

Thyroid gland presents a wide spectrum of tumours derived from follicular cells that range from well differentiated, papillary and follicular carcinoma (PTC and FTC, respectively), usually carrying a good prognosis, to the clinically aggressive, poorly differentiated (PDTC) and undifferentiated thyroid carcinoma (UTC).It is usually accepted that PDTC and UTC occur either de novo or progress fro...

Journal: :American journal of cancer research 2011
Carmen J Tartari Carla Donadoni Elisa Manieri Luca Mologni Pamela Della Mina Antonello Villa Carlo Gambacorti-Passerini

The RET receptor tyrosine kinase is a member of the cadherin superfamily and plays a pivotal role in cell survival, differentiation and proliferation. Currently, 12 ret/ptc chimeric oncogenes, characterized by the fusion between the intracellular domain of RET and different activating genes, which can cause ligand-independent dimerization and constitutive activation, have been described. β-cate...

Journal: :The Medical journal of Malaysia 2003
E Omar N H Othman

We found a high prevalence of RET expression among our papillary carcinoma at 77% 08 of 53); p< 0.001. Interestingly, the follicular adenomas and nodular hyperplasia cases exhibited a low expression of RET of 18% (9 of 50 cases) and 22.7% 05 of 66) respectively. RET/PTC re-arrangement has been demonstrated in these lesions before 7,8. It has been postulated that these positive follicular cell r...

Journal: :Endocrinologia japonica 1991
H Namba S Yamashita H C Pei N Ishikawa M C Villadolid T Tominaga H Kimura M Tsuruta N Yokoyama M Izumi

PTC gene, which is derived from the rearranged form of the ret proto-oncogene, was originally discovered in human thyroid papillary carcinomas. This gene has been thought to act as a tumorigenetic factor in thyroid carcinoma, although the action of PTC oncogene products is still unknown. To study the frequency of the PTC gene present in human thyroid carcinomas, we investigated four cell lines ...

Journal: :The open cell signaling journal 2010
Benjamin O'Brien Gregg H Jossart Yuko Ito Karin M Greulich-Bode Jingly F Weier Santiago Munne Orlo H Clark Heinz-Ulrich G Weier

Altered signal transduction can be considered a hallmark of many solid tumors. In thyroid cancers the receptor tyrosine kinase (rtk) genes NTRK1 (Online Mendelian Inheritance in Man = OMIM *191315, also known as 'TRKA'), RET ('Rearranged during Transfection protooncogene', OMIM *164761) and MET (OMIM *164860) have been reported as activated, rearranged or overexpressed. In many cases, a combina...

Journal: :Cancer research 1994
I Bongarzone M G Butti S Coronelli M G Borrello M Santoro P Mondellini S Pilotti A Fusco G Della Porta M A Pierotti

Tumor specific rearrangements of ret gene are frequently detected in papillary thyroid carcinomas. These rearrangements result in the formation of chimeric genes showing the tyrosine kinase domain of ret fused with the 5' end sequences of different genes. We examined a series of 52 patients and identified 10 cases of ret fusion with D10S170 locus resulting in the generation of ret/PTC1 oncogene...

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