FUS Interacts with HSP60 to Promote Mitochondrial Damage

Deng, Jianwen; Yang, Mengxue; Chen, Yanbo; Chen, Xiaoping; Liu, Jianghong; Sun, Shuhong; Cheng, Haipeng; Li, Yang; Bigio, Eileen H.; Mesulam, Marsel; Xu, Qi; Du, Sidan; Fushimi, Kazuo; Zhu, Li; Wu, Jane Y.

doi:10.1371/journal.pgen.1005357

Cited by 148 publications

(178 citation statements)

References 100 publications

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“…Our recent work has shown that fused in sarcoma/translocated in liposarcoma (FUS/TLS or FUS), a nuclear RNA binding protein, interacts with and targets mitochondria (Deng et al, 2015). This prompted us to carefully examine effects of wild-type and ALS-mutant FUS on axonal mitochondrial transport.…”

Section: Resultsmentioning

confidence: 99%

“…To further examine FUS activity in vivo , we used our previously established fly model for FUS proteinopathy (Chen et al, 2011; Deng et al, 2015). We crossed mitoGFP into the transgenic flies expressing human Wt- or P525L-mutant FUS to track mitochondrial movement in motor neuron axons of these transgenic flies.…”

Section: Resultsmentioning

confidence: 99%

“…These data are consistent with that obtained from cultured mammalian neurons, both supporting that increased FUS expression reduces axonal mitochondrial transport. Previous studies have shown increased FUS expression in patients affected by frontotemporal lobar degeneration associated with FUS (FTLD-FUS) (Mackenzie et al, 2011; Sabatelli et al, 2013; Deng et al, 2015). Consistently, transgenic animals overexpressing the human FUS protein recapitulate critical pathological and clinical features of FUS proteinopathy (e.g, Huang et al, 2011; Chen et al, 2011; Lanson et al, 2011).…”

Section: Resultsmentioning

confidence: 99%

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A new method for quantifying mitochondrial axonal transport

Chen

Yang

et al. 2016

Protein Cell

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Axonal transport of mitochondria is critical for neuronal survival and function. Automatically quantifying and analyzing mitochondrial movement in a large quantity remain challenging. Here, we report an efficient method for imaging and quantifying axonal mitochondrial transport using microfluidic-chamber-cultured neurons together with a newly developed analysis package named “MitoQuant”. This tool-kit consists of an automated program for tracking mitochondrial movement inside live neuronal axons and a transient-velocity analysis program for analyzing dynamic movement patterns of mitochondria. Using this method, we examined axonal mitochondrial movement both in cultured mammalian neurons and in motor neuron axons of Drosophila in vivo. In 3 different paradigms (temperature changes, drug treatment and genetic manipulation) that affect mitochondria, we have shown that this new method is highly efficient and sensitive for detecting changes in mitochondrial movement. The method significantly enhanced our ability to quantitatively analyze axonal mitochondrial movement and allowed us to detect dynamic changes in axonal mitochondrial transport that were not detected by traditional kymographic analyses.Electronic supplementary materialThe online version of this article (doi:10.1007/s13238-016-0268-3) contains supplementary material, which is available to authorized users.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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A new method for quantifying mitochondrial axonal transport

Chen

Yang

et al. 2016

Protein Cell

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“…On the contrary, other chaperones such as HSP70/Hsc70, cyclophilin-A, aB-crystallin and glutathione peroxidase have no effect in blocking SOD1 misplacing onto the mitochondrial outer membrane which consequently, leads to damaged mitochondrial integrity [176]. Recently, reduced expression of HSP60 has exhibited the protective role against mitochondrial damage in ALS because interaction between mitochondrial chaperonin, HSP60 and FUS protein causes its translocation to mitochondria and leads to cell damage [177]. Further, it has been reported that small HSPs, including the HSP27, HSP25 and α-crystallin family also impart neuroprotective and cardioprotective effect against secondary complications of T2D [178].…”

Section: Chaperones Mediated Therapy For Altered Mitochondrial Dynamicsmentioning

confidence: 99%

Linking mitochondrial dysfunction, metabolic syndrome and stress signaling in Neurodegeneration

Jha

Kumar

et al. 2017

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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Mounting evidence suggests a link between metabolic syndrome (MetS) such as diabetes, obesity, non-alcoholic fatty liver disease in the progression of Alzheimer's disease (AD), Parkinson's disease (PD) and other neurodegenerative diseases (NDDs). For instance, accumulated Aβ oligomer is enhancing neuronal Ca release and neural NO where increased NO level in the brain through post translational modification is modulating the level of insulin production. It has been further confirmed that irrespective of origin; brain insulin resistance triggers a cascade of the neurodegeneration phenomenon which can be aggravated by free reactive oxygen species burden, ER stress, metabolic dysfunction, neuorinflammation, reduced cell survival and altered lipid metabolism. Moreover, several studies confirmed that MetS and diabetic sharing common mechanisms in the progression of AD and NDDs where mitochondrial dynamics playing a critical role. Any mutation in mitochondrial DNA, exposure of environmental toxin, high-calorie intake, homeostasis imbalance, glucolipotoxicity is causative factors for mitochondrial dysfunction. These cumulative pleiotropic burdens in mitochondria leads to insulin resistance, increased ROS production; enhanced stress-related enzymes that is directly linked MetS and diabetes in neurodegeneration. Since, the linkup mechanism between mitochondrial dysfunction and disease phenomenon of both MetS and NDDs is quite intriguing, therefore, it is pertinent for the researchers to identify and implement the therapeutic interventions for targeting MetS and NDDs. Herein, we elucidated the pertinent role of MetS induced mitochondrial dysfunction in neurons and their consequences in NDDs. Further, therapeutic potential of well-known biomolecules and chaperones to target altered mitochondria has been comprehensively documented. This article is part of a Special Issue entitled: Oxidative Stress and Mitochondrial Quality in Diabetes/Obesity and Critical Illness Spectrum of Diseases - edited by P. Hemachandra Reddy.

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“…And RNA binding proteins could be potential targets in prostate cancer [13]. RNA binding protein FUS has been shown to interact with HSP60 (Heat Shock Protein Family 60) to promote mitochondrial damage [14]. FUS-CHOP promotes invasion in myxoid liposarcoma through a SRC (SRC Proto-Oncogene, Non-Receptor Tyrosine Kinase)/FAK (Focal Adhesion Kinase)/RHO (Rhodopsin)/ROCK (Rho Associated Coiled-Coil Containing Protein Kinase)-dependent pathway [15].…”

Section: Introductionmentioning

confidence: 99%

A FUS-LATS1/2 Axis Inhibits Hepatocellular Carcinoma Progression via Activating Hippo Pathway

Bao

Yuan

et al. 2018

Cell Physiol Biochem

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Background/Aims: The roles and related mechanisms of RNA binding protein FUS (fused in sarcoma/translocated in liposarcoma) are unclear in numerous cancers, including hepatocellular carcinoma (HCC). Methods: Quantitative reverse transcription PCR (qRT-PCR), western blot, cell viability, transwell migration and invasion, tumor spheres formation and in vivo tumor formation assays were used to examine the effects of FUS on HCC progression in HuH7 and MHCC97 cells. Additionally, transcriptome analysis based on RNA-sequencing data, qRT-PCR, western blots, luciferase reporter and RNA binding protein immunoprecipitation (RIP) assays were used to explore the LATS1/2 (large tumor suppressor kinases 1/2)-related mechanisms contributing to FUS functions. Finally, qRT-PCR and western blot analysis were used to detect the levels of FUS and LATS1/2 in HCC and adjacent normal tissues, and the correlation between them in HCC tissues. Results: Overexpression of FUS decreased cell viability, migration, invasion and stemness. Moreover, FUS interacted and stabilized LATS1/2 stability, and thus promoted LATS1/2 expression and activated Hippo pathway. Finally, FUS and LAST1/2 levels were positively correlated and significantly down-regulated in HCC tissues. Conclusion: We demonstrate that FUS/LATS1/2 axis inhibits HCC progression via activating Hippo pathway.

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FUS Interacts with HSP60 to Promote Mitochondrial Damage

Cited by 148 publications

References 100 publications

A new method for quantifying mitochondrial axonal transport

A new method for quantifying mitochondrial axonal transport

Linking mitochondrial dysfunction, metabolic syndrome and stress signaling in Neurodegeneration

A FUS-LATS1/2 Axis Inhibits Hepatocellular Carcinoma Progression via Activating Hippo Pathway

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