نتایج جستجو برای: p62

تعداد نتایج: 2412  

Journal: :The Journal of neuroscience : the official journal of the Society for Neuroscience 2013
Harumi Harada Eiji Warabi Taizo Matsuki Toru Yanagawa Kosuke Okada Junya Uwayama Akira Ikeda Kazuhiro Nakaso Kyoko Kirii Noriko Noguchi Hiroki Bukawa Richard C M Siow Giovanni E Mann Junichi Shoda Tetsuro Ishii Takeshi Sakurai

The cytoplasmic regulatory protein p62 (Sequestosome 1/A170) is known to modulate various receptor-mediated intracellular signaling pathways. p62 deficiency was shown to result in mature-onset obesity in mice, but the mechanisms underlying this abnormality remained unclear. Here we report that hyperphagia due to central leptin resistance is the cause of obesity in p62(-/-) mice. We found that t...

2017
Shun Nakayama Hideaki Karasawa Takashi Suzuki Shinichi Yabuuchi Kiyoshi Takagi Takashi Aizawa Yoshiaki Onodera Yasuhiro Nakamura Mika Watanabe Fumiyoshi Fujishima Hiroshi Yoshida Takanori Morikawa Tomohiko Sase Takeshi Naitoh Michiaki Unno Hironobu Sasano

p62/sequestosome 1 (p62) is a multi-domain protein that functions as a receptor for ubiquitinated targets in the selective autophagy and serves as a scaffold in various signaling cascades. p62 have been reported to be up-regulated in several human malignancies, but the biological roles and significance of p62 are still poorly understood in colorectal carcinoma. We immunohistochemically evaluate...

Journal: :Arteriosclerosis, thrombosis, and vascular biology 2012
Geun-Young Kim Patrizia Nigro Keigi Fujiwara Jun-ichi Abe Bradford C Berk

OBJECTIVE Protein kinase C (PKC) ζ is a key pathological mediator of endothelial cell apoptosis. p62 is a scaffold protein that regulates several cell signaling pathways by binding to target proteins. Because PKCζ and p62 contain Phox/Bem1p (PB1) modules that mediate protein-protein interactions, we hypothesized that an interaction between p62 and PKCζ is required for tumor necrosis factor α-in...

Journal: :Neuromuscular disorders : NMD 2017
Satoshi Nakano Mitsuaki Oki Hirofumi Kusaka

We examined selective autophagy against ubiquitinated protein aggregates in sporadic inclusion body myositis (s-IBM) patients. The form of autophagy requires phosphorylation of serine 403 in p62/SQSTM1 to bind to Lys63-linked ubiquitin and the binding of the p62-ubiquitinated protein conjugates to LC3. In muscle biopsy specimens from 16 s-IBM patients, we compared the distribution of p62 (aa120...

Journal: :The FEBS journal 2014
Seung-Hyun Ro Ian A Semple Haewon Park Haeli Park Hwan-Woo Park Myungjin Kim Jeong Sig Kim Jun Hee Lee

Autophagy is a homeostatic process that is important for degrading protein aggregates, nutrient deposits, dysfunctional organelles and several signaling molecules. p62/sequestosome-1 is a protein that binds to several autophagy substrates, such as ubiquitinated proteins, damaged mitochondria and signaling molecules such as an Nrf2 inhibitor Keap1, promoting their autophagic degradation. Sestrin...

Journal: :The Journal of biological chemistry 2013
Shengbing Huang Koichi Okamoto Chunrong Yu Frank A Sinicrope

Autophagy and apoptosis regulate cancer cell viability in response to cytotoxic stress; however, their functional relationship remains unclear. p62/sequestosome 1 is a multifunctional protein and a signaling hub that shuttles ubiquitinated proteins to the lysosome during autophagy. Autophagy inhibition up-regulates p62, and prior data suggest that p62 may mediate apoptosis. Here, we demonstrate...

2013
Franco Venanzi Victor Shifrin Michael Y. Sherman Vladimir Gabai Oleg Kiselev Andrey Komissarov Mikhail Grudinin Maria Shartukova Ekaterina A. Romanovskaya-Romanko Yuri Kudryavets Natalya Bezdenezhnykh Oleksandra Lykhova Nadiia Semesyuk Antonio Concetti Anatoly Tsyb Marina Filimonova Victoria Makarchuk Raisa Yakubovsky Andrey Chursov Vita Shcherbinina Alexander Shneider

Autophagy plays an important role in neoplastic transformation of cells and in resistance of cancer cells to radio- and chemotherapy. p62 (SQSTM1) is a key component of autophagic machinery which is also involved in signal transduction. Although recent empirical observations demonstrated that p62 is overexpressed in variety of human tumors, a mechanism of p62 overexpression is not known. Here w...

2016
Tetsuya Saito Yoshinobu Ichimura Keiko Taguchi Takafumi Suzuki Tsunehiro Mizushima Kenji Takagi Yuki Hirose Masayuki Nagahashi Tetsuro Iso Toshiaki Fukutomi Maki Ohishi Keiko Endo Takefumi Uemura Yasumasa Nishito Shujiro Okuda Miki Obata Tsuguka Kouno Riyo Imamura Yukio Tada Rika Obata Daisuke Yasuda Kyoko Takahashi Tsutomu Fujimura Jingbo Pi Myung-Shik Lee Takashi Ueno Tomoyuki Ohe Tadahiko Mashino Toshifumi Wakai Hirotatsu Kojima Takayoshi Okabe Tetsuo Nagano Hozumi Motohashi Satoshi Waguri Tomoyoshi Soga Masayuki Yamamoto Keiji Tanaka Masaaki Komatsu

p62/Sqstm1 is a multifunctional protein involved in cell survival, growth and death, that is degraded by autophagy. Amplification of the p62/Sqstm1 gene, and aberrant accumulation and phosphorylation of p62/Sqstm1, have been implicated in tumour development. Herein, we reveal the molecular mechanism of p62/Sqstm1-dependent malignant progression, and suggest that molecular targeting of p62/Sqstm...

2013
Wentao Gao Zhixia Chen Wei Wang Michael T. Stang

p62 is constitutively degraded by autophagy via its interaction with LC3. However, the interaction of p62 with LC3 species in the context of the LC3 lipidation process is not specified. Further, the p62-mediated protein aggregation's effect on autophagy is unclear. We systemically analyzed the interactions of p62 with all known Atg proteins involved in LC3 lipidation. We find that p62 does not ...

Journal: :The Journal of biological chemistry 2008
Yoshinobu Ichimura Taichi Kumanomidou Yu-shin Sou Tsunehiro Mizushima Junji Ezaki Takashi Ueno Eiki Kominami Takashi Yamane Keiji Tanaka Masaaki Komatsu

Impairment of autophagic degradation of the ubiquitin- and LC3-binding protein "p62" leads to the formation of cytoplasmic inclusion bodies. However, little is known about the sorting mechanism of p62 to autophagic degradation. Here we identified a motif of murine p62 consisting of 11 amino acids (Ser334-Ser344) containing conserved acidic and hydrophobic residues across species, as an LC3 reco...

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