E3 Ligase RNF126 Directly Ubiquitinates Frataxin, Promoting Its Degradation: Identification of a Potential Therapeutic Target for Friedreich Ataxia

Benini Monica; Fortuni Silvia; Condo Ivano; Alfedi Giulia; Malisan Florence; Toschi Nicola; Serio Dario; Massaro Damiano Sergio; Arcuri Gaetano; Testi Roberto; Rufini Alessandra

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E3 Ligase RNF126 Directly Ubiquitinates Frataxin, Promoting Its Degradation: Identification of a Potential Therapeutic Target for Friedreich Ataxia

机译：E3连接酶RNF126直接泛蛋白毒素，促进其降解：鉴定Friedreich Ataxia的潜在治疗目标

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Friedreich ataxia (FRDA) is a severe genetic neurode-generative disease caused by reduced expression of the mitochondrial protein frataxin. To date, there is no therapy to treat this condition. The amount of residual frataxin critically affects the severity of the disease; thus, attempts to restore physiological frataxin levels are considered therapeutically relevant. Frataxin levels are controlled by the ubiquitin-proteasome system; therefore, inhibition of the frataxin E3 ligase may represent a strategy to achieve an increase in frataxin levels. Here, we report the identification of the RING E3 ligase RNF126 as the enzyme that specifically mediates frataxin ubiquitination and targets it for degradation. RNF126 interacts with frataxin and promotes its ubiquitination in a catalytic activity-dependent manner, both in vivo and in vitro. Most importantly, RNF126 depletion results in frataxin accumulation in cells derived from FRDA patients, highlighting the relevance of RNF126 as a new therapeutic target for Friedreich ataxia.

机译：Friedreich Ataxia（FRDA）是一种严重的遗传神经生成疾病，由线粒体蛋白质脱脂蛋白的表达降低引起。迄今为止，没有治疗这种情况。残留的呋喃啉的量主要影响疾病的严重程度;因此，试图恢复生理稻草素水平被认为是治疗相关的。脱蛋白水平由泛素 - 蛋白酶体系控制;因此，抑制脱脂E3连接酶的抑制可以代表达到脱脂蛋白水平增加的策略。在这里，我们报告了环E3连接酶RNF126作为特异性介导脱脂蛋白染色的酶并靶向降解的酶。 RNF126与Frataxin相互作用，并以催化活性依赖性方式促进其泛素，无论是体内和体外的。最重要的是，RNF126耗竭导致衍生自FRDA患者的细胞中的脱脂蛋白积累，突出了RNF126作为Friedreich Ataxia的新治疗目标的相关性。

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来源
《Journal of Turbulence》 |2017年第8期|共11页
作者
Benini Monica; Fortuni Silvia; Condo Ivano; Alfedi Giulia; Malisan Florence; Toschi Nicola; Serio Dario; Massaro Damiano Sergio; Arcuri Gaetano; Testi Roberto; Rufini Alessandra;
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作者单位

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Med Phys Sect Dept Biomed &

Prevent Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

Univ Roma Tor Vergata Dept Biomed &

Prevent Lab Signal Transduct Via Montpellier 1 I-00133 Rome Italy;

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正文语种 eng
中图分类流体力学;
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入库时间 2022-08-20 10:25:52

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1. E3 Ligase RNF126 Directly Ubiquitinates Frataxin, Promoting Its Degradation: Identification of a Potential Therapeutic Target for Friedreich Ataxia [J] . Monica Benini, Silvia Fortuni, Ivano Condò, Cell Reports . 2017,第8期

机译：E3连接酶RNF126直接泛素Frataxin，促进其降解：弗雷德里希共济失调的潜在治疗靶标的鉴定。
2. E3 ubiquitin ligase RNF126 promotes cancer cell proliferation by targeting the tumor suppressor p21 for ubiquitin-mediated degradation [J] . ZhiX., ZhaoD., WangZ., Cancer research: The official organ of the American Association for Cancer Research, Inc . 2013,第1期

机译：E3泛素连接酶RNF126通过靶向肿瘤抑制因子p21进行泛素介导的降解来促进癌细胞增殖
3. PUB22 and PUS23 U-BOX E3 ligases directly ubiquitinate RPN6, a 26S proteasome lid subunit, for subsequent degradation in Arabidopsis thaliana [J] . Cho Seok Keun, Bae Hansol, Ryu Moon Young, Biochemical and Biophysical Research Communications . 2015,第4期

机译：PUB22和PUS23 U-BOX E3连接酶直接泛素化RPN6（一种26S蛋白酶体盖亚基），用于随后在拟南芥中的降解
4. Identification of target analogues of E3 ubiquitin ligase involved in the incidence of breast cancer: A rational drug designing approach [C] . Shreya Kumari, Priyanka Narad, Abhishek Sengupta International Conference on Bioinformatics and Systems Biology . 2018

机译：鉴定参与乳腺癌发病的E3泛素连接酶的靶类似物：一种合理的药物设计方法
5. Identification and characterization of a SUMO-targeted ubiquitin ligase (E3) complex in Saccharomyces cerevisiae. [D] . Xie, Yang. 2009

机译：酿酒酵母中以SUMO为靶标的泛素连接酶（E3）复合物的鉴定和表征。
6. E3 Ligase RNF126 Directly Ubiquitinates Frataxin Promoting Its Degradation: Identification of a Potential Therapeutic Target for Friedreich Ataxia [O] . Monica Benini, Silvia Fortuni, Ivano Condò, -1

机译：E3连接酶RNF126直接泛素Frataxin促进其降解：弗雷德里希共济失调的潜在治疗靶标的鉴定。
7. E3 Ligase RNF126 Directly Ubiquitinates Frataxin, Promoting Its Degradation: Identification of a Potential Therapeutic Target for Friedreich Ataxia [O] . Benini, M, Fortuni, S, Condò, I, 2017

机译：E3连接酶RNF126直接遍在泛素，促进其降解：弗雷德里希共济失调的潜在治疗靶标的鉴定。
8. Identification of Small Non-Peptidic Ligands that Bind the Scf-beta- TRCP Ubiquitin Ligase to Target to ER for Ubiquitination and Degradation [R] . Sakamoto, K. M. 2005

机译：鉴定小的非肽配体结合scf-β-TRCp泛素连接酶靶向ER以进行泛素化和降解

E3 Ligase RNF126 Directly Ubiquitinates Frataxin, Promoting Its Degradation: Identification of a Potential Therapeutic Target for Friedreich Ataxia

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