Transmission of cell stress from endoplasmic reticulum to mitochondria

Hori, Osamu; Ichinoda, Fusae; Tamatani, Takashi; Yamaguchi, Atsushi; Sato, Naoya; Ozawa, Kentaro; Kitao, Yasuko; Miyazaki, Mutsuko; Harding, Heather P.; Ron, David; Tohyama, Masaya; Stern, David M.; Ogawa, Satoshi

doi:10.1083/jcb.200108103

Cited by 193 publications

(183 citation statements)

References 38 publications

(50 reference statements)

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“…2b). Hypoxia and ER stress increase expression of lon protease [10]. Since cholesterol and palmitate triggered ER stress, the influences of this treatment on expression of lon protease were investigated.…”

Section: Resultsmentioning

confidence: 99%

“…Additionally, lon protease exhibits chaperon-like functions that are independent of its proteolytic activity. Lon protease is also necessary for the assembly of mitochondrial electron transport chain complexes, especially COX II [10,11]. Indeed, in the absence of Pim1, yeast becomes respiratorydeficient because it is unable to maintain mDNA, leading to accumulatin of electron-dense inclusion bodies in the mitochondrial matrix [12].…”

Section: Introductionmentioning

confidence: 99%

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Downregulation of mitochondrial lon protease impairs mitochondrial function and causes hepatic insulin resistance in human liver SK-HEP-1 cells

et al. 2011

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Aims/hypothesis Lon protease degrades oxidatively damaged proteins in mitochondrial matrix. To examine the relationships between mitochondrial quality control, mitochondrial functions and diabetes, we investigated whether lon protease deficiency influences insulin resistance by affecting mitochondrial function. Methods Lon protease-specific small interfering RNA (siRNA) was transfected into human liver SK-HEP-1 cells and changes in molecules related to insulin resistance were analysed. Results Reduction in lon protease was achieved using specific siRNA-induced mitochondrial dysfunction in human liver SK-HEP-1 cells. Concurrently, insulin signalling and subsequent insulin action were impaired and levels of gluconeogenic enzymes were increased by lon protein deficiency. Moreover, the activity of mitogen-activated protein kinases and transcription factors related to hepatic gluconeogenesis were elevated in LON (also known as LONP1) siRNA-transfected cells via increased intracellular reactive oxygen species production. Overproduction of lon protease restored mitochondrial function and also diminished the insulin resistance induced by treatment with cholesterol and palmitate. In addition, levels of lon protease decreased dramatically in livers of diabetic db/db mice compared with their lean mice counterparts. Conclusions/interpretationHere we have demonstrated that reduction of lon protease induced hepatic insulin resistance by lowering mitochondrial function. This is the first study to report that defects in mitochondrial protein quality control could cause insulin resistance and diabetes.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Downregulation of mitochondrial lon protease impairs mitochondrial function and causes hepatic insulin resistance in human liver SK-HEP-1 cells

et al. 2011

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“…PRSS15 is a multifunctional protein widely preserved throughout species from yeast to mammals (Lu et al, 2003). Its expression, in a rat model and in the human HeLa cell line, has been found to be induced by hypoxia (Hori et al, 2002). HeLa cells transfected with PRSS15 were relatively more resistant to the decrease in mitochondrial membrane potential induced by hypoxia than the mocktransfected cells (Hori et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

“…Its expression, in a rat model and in the human HeLa cell line, has been found to be induced by hypoxia (Hori et al, 2002). HeLa cells transfected with PRSS15 were relatively more resistant to the decrease in mitochondrial membrane potential induced by hypoxia than the mocktransfected cells (Hori et al, 2002). Human PRSS15 binds to TG-rich elements, where it is presented in the context of a single DNA strand.…”

Section: Discussionmentioning

confidence: 99%

Gene expression signature for angiogenic and nonangiogenic non-small-cell lung cancer

Bianchi

Ferguson

et al. 2004

Oncogene

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Angiogenesis is regarded as essential for tumour growth. However, we have demonstrated that some other aggressive non-small-cell lung carcinomas (n-SCLC) do not have angiogenesis. In this study, using cDNA microarray analysis, we demonstrate that angiogenic and nonangiogenic tumour types can be distinguished by their gene expression profiles. Tissue samples from 42 n-SCLC patients were obtained with consent. In all, 12 tumours were nonangiogenic and 30 angiogenic. The two groups were matched by age, sex, smoking and tumour stage. Total RNAs were extracted followed by microarray hybridization and image scan procedure. Data were analysed using GeneSpring 5.1 software. A total of 62 genes were found to be able to separate angiogenic from nonangiogenic tumours. Nonangiogenic tumours have higher levels of genes concerned with mitochondrial metabolism, mRNA transcription, protein synthesis and the cell cycle. Angiogenic tumours have higher levels of genes coding for membrane vesicles, integrins, remodelling, angiogenesis and apoptosis. These results further support our first finding that nonangiogenic lung tumours are fast-growing tumours filling the alveoli in the absence of vascular remodelling. We raise the hypothesis that in nonangiogenic tumours, hypoxia leads to a higher activation of the mitochondrial respiratory chain, which allows tumour growth without triggering angiogenesis.

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“…In bacteria, in addition to proteolysis of damaged proteins, Lon also plays a key role in turnover of specific unstable proteins involved in a variety of biological processes (3,4). Similarly, the steroidogenic acute regulatory protein StAR, several subunits of cytochrome c oxidase, and oxidized mitochondrial aconitase are known to be Lon substrates in animal mitochondria (10)(11)(12)(13)(14).…”

mentioning

confidence: 99%

Mitochondrial Lon protease regulates mitochondrial DNA copy number and transcription by selective degradation of mitochondrial transcription factor A (TFAM)

Matsushima

Goto

Kaguni

2010

Proc. Natl. Acad. Sci. U.S.A.

243

214

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Lon is the major protease in the mitochondrial matrix in eukaryotes, and is well conserved among species. Although a role for Lon in mitochondrial biogenesis has been proposed, the mechanistic basis is unclear. Here, we demonstrate a role for Lon in mtDNA metabolism. An RNA interference (RNAi) construct was designed that reduces Lon to less than 10% of its normal level in Drosophila Schneider cells. RNAi knockdown of Lon results in increased abundance of mitochondrial transcription factor A (TFAM) and mtDNA copy number. In a corollary manner, overexpression of Lon reduces TFAM levels and mtDNA copy number. Notably, induction of mtDNA depletion in Lon knockdown cells does not result in degradation of TFAM, thereby causing a dramatic increase in the TFAM∶mtDNA ratio. The increased TFAM∶mtDNA ratio in turn causes inhibition of mitochondrial transcription. We conclude that Lon regulates mitochondrial transcription by stabilizing the mitochondrial TFAM∶ mtDNA ratio via selective degradation of TFAM.AAA+ protease | mtDNA maintenance | quality control

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Transmission of cell stress from endoplasmic reticulum to mitochondria

Cited by 193 publications

References 38 publications

Downregulation of mitochondrial lon protease impairs mitochondrial function and causes hepatic insulin resistance in human liver SK-HEP-1 cells

Downregulation of mitochondrial lon protease impairs mitochondrial function and causes hepatic insulin resistance in human liver SK-HEP-1 cells

Gene expression signature for angiogenic and nonangiogenic non-small-cell lung cancer

Mitochondrial Lon protease regulates mitochondrial DNA copy number and transcription by selective degradation of mitochondrial transcription factor A (TFAM)

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