نتایج جستجو برای: fadd

تعداد نتایج: 1166  

پایان نامه :وزارت علوم، تحقیقات و فناوری - دانشگاه سیستان و بلوچستان - دانشکده علوم پایه 1391

سرطان سلول های مخاطی دهان (oscc) در سراسر جهان شیوع قابل توجهی دارد . تشخیص نسبتا دشوار آن باعث می شود تا به تحقیق بیشتر بر روی عوامل ایجاد کننده بیماری بپردازیم . امروزه ثابت شده فاکتورهای اپی ژنتیکی می توانند بدون تغییر در توالی dna بیان ژن را تغییر دهند که متیلاسیون dna در جزایر cpg یکی از این عوامل است . اعتقاد بر این است که متیلاسیون چندین ژن ممکن است در oscc دخیل باشد . اپوپتوزیس نقش مهمی...

Journal: :BMB reports 2012
Eun-Woo Lee Jinho Seo Manhyung Jeong Sangsik Lee Jaewhan Song

Fas-associated protein with death domain (FADD), an adaptor that bridges death receptor signaling to the caspase cascade, is indispensible for the induction of extrinsic apoptotic cell death. Interest in the non-apoptotic function of FADD has greatly increased due to evidence that FADD-deficient mice or dominant-negative FADD transgenic mice result in embryonic lethality and an immune defect wi...

Journal: :American journal of physiology. Endocrinology and metabolism 2015
Fang Wang Hongbo Weng Michael J Quon Jingwen Yu Jian-Ying Wang Anne-Odile Hueber Peixin Yang

Endoplasmic reticulum (ER) stress and caspase 8-dependent apoptosis are two interlinked causal events in maternal diabetes-induced neural tube defects (NTDs). The inositol-requiring enzyme 1α (IRE1α) signalosome mediates the proapoptotic effect of ER stress. Diabetes increases tumor necrosis factor receptor type 1R-associated death domain (TRADD) expression. Here, we revealed two new unfolded p...

Journal: :Molecular cancer therapeutics 2011
Katrina A Schinske Shyam Nyati Amjad P Khan Terence M Williams Timothy D Johnson Brian D Ross Ricardo Pérez Tomás Alnawaz Rehemtulla

Fas-associated protein with death domain (FADD) is a cytosolic adapter protein essential for mediating death receptor-induced apoptosis. It has also been implicated in a number of nonapoptotic activities including embryogenesis, cell-cycle progression, cell proliferation, and tumorigenesis. Our recent studies have shown that high levels of phosphorylated FADD (p-FADD) in tumor cells correlate w...

2004
Léa Tourneur Stéphanie Delluc Vincent Lévy Françoise Valensi Isabelle Radford-Weiss Ollivier Legrand Jacques Vargaftig Charlotte Boix Elizabeth A. Macintyre Bruno Varet Gilles Chiocchia Agnès Buzyn

In acute myeloid leukemia (AML), coexpression of death receptors and ligands of the tumor necrosis factor (TNF) receptor/TNFsuperfamily on leukemic cells after chemotherapy is not always accompanied by apoptosis, suggesting that the apoptotic death receptor signaling pathway is disrupted. Because Fas-associated protein with death domain (FADD) is the main adaptor for transmitting the Fas, TNF-r...

Journal: :Urology 2013
Tomohiro Ikeda Nobumichi Tanaka Keiji Shimada Yoshiaki Matsumura Makito Miyake Satoshi Anai Atsushi Tomioka Eijiro Okajima Akihide Hirayama Kiyohide Fujimoto Noboru Konishi Yoshihiko Hirao

OBJECTIVE To assess whether the phosphorylated Fas-associated death domain protein (FADD) at 194 serine (p-FADD) is valuable as a marker of biochemical recurrence in hormone-naive patients who had undergone radical prostatectomy. MATERIALS AND METHODS We used radical prostatectomy specimens from 106 patients. None of the patients had received neoadjuvant or adjuvant therapy. The percentage of...

Journal: :The EMBO journal 1998
K Newton A W Harris M L Bath K G Smith A Strasser

Members of the tumour necrosis factor receptor family that contain a death domain have pleiotropic activities. They induce apoptosis via interaction with intracellular FADD/MORT1 and trigger cell growth or differentiation via TRADD and TRAF molecules. The impact of FADD/MORT1-transduced signals on T lymphocyte development was investigated in transgenic mice expressing a dominant negative mutant...

Journal: :Medical Immunology 2005
Léa Tourneur Agnès Buzyn Gilles Chiocchia

FADD (Fas Associated protein with Death Domain) is a key adaptor molecule transmitting the death signal mediated by death receptors. In addition, this multiple functional protein is implicated in survival/proliferation and cell cycle progression. FADD functions are regulated via cellular sublocalization, protein phosphorylation, and inhibitory molecules. In the present review, we focus on the r...

Journal: :Proceedings of the National Academy of Sciences of the United States of America 2001
N H Kabra C Kang L C Hsing J Zhang A Winoto

FADD/Mort1, initially identified as a Fas-associated death-domain containing protein, functions as an adapter molecule in apoptosis initiated by Fas, tumor necrosis factor receptor-I, DR3, and TRAIL-receptors. However, FADD likely participates in additional signaling cascades. FADD-null mutations in mice are embryonic-lethal, and analysis of FADD(-)/- T cells from RAG-1(-)/- reconstituted chime...

Journal: :Journal of immunology 2006
Hongxia Z Imtiyaz Stephen Rosenberg Yuhang Zhang Ziaur S M Rahman Ying-Ju Hou Tim Manser Jianke Zhang

The Fas-associated death domain protein (FADD)/Mort1 is a signaling adaptor protein which mediates the activation of caspase 8 during death receptor-induced apoptosis. Disruption of FADD in germ cells results in death receptor-independent embryonic lethality in mice. Previous studies indicated that in addition to its function in apoptosis, FADD is also required in peripheral T cell homeostasis ...

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