BNIP3 and NIX Mediate Mieap-Induced Accumulation of Lysosomal Proteins within Mitochondria

Nakamura, Yasuyuki; Kitamura, Noriaki; Shinogi, Daisuke; Yoshida, Masaki; Goda, Olga; Murai, Ryuya; Kamino, Hiroki; Arakawa, Hirofumi

doi:10.1371/journal.pone.0030767

Cited by 45 publications

(71 citation statements)

References 14 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…It is known that a TP53-inducible protein, Mieap (18), controls mitochondrial quality (19). Using TP53-specific siRNA, we confirmed, as published previously (19), that Mieap is TP53 inducible (Fig. 2A).…”

Section: Resultssupporting

confidence: 89%

“…In addition, TP53 has been reported to activate necrosis by opening the mitochondrial permeability transition pore (42). Although our results point to the involvement of TP53-induced Mieap and BNIP3-mediated regulation of the hypoxic processing of VDAC1, we do not conclude, as suggested previously (19,20), that lysosome-like organelles or lysosomal proteins accumulate in mitochondria. However, the latter studies examined exogenous overexpression of adenovirus-infected Mieap in normoxia, which contrasts with the conditions of the present study, which examined endogenous proteins in hypoxic cells.…”

Section: Discussioncontrasting

confidence: 91%

“…3F; Table 1), which further implicates lysosome involvement in resistance to apoptosis in hypoxia. However, Mieap was not pulled down, suggesting that BNIP3 and Mieap did not bind directly, which contrasts with the findings of a previous report (19). Since pulldown experiments showed that clathrin bound BNIP3 in hypoxic cells and that clathrin is involved in vesicle trafficking, the effect of brefeldin A, an inhibitor of transport of secretory proteins from the endoplasmic reticulum to the Golgi apparatus, was examined.…”

Section: Resultscontrasting

confidence: 69%

“…It is known that a TP53-inducible protein, Mieap (also referred to as Spata18) (18), controls mitochondrial quality through interaction with the HIF-1-inducible protein BNIP3 (19). In addition, Mieap has been proposed to induce the accumulation of lysosomal proteins within mitochondria by way of repairing damaged mitochondria (20).…”

mentioning

confidence: 99%

See 3 more Smart Citations

Local Mitochondrial-Endolysosomal Microfusion Cleaves Voltage-Dependent Anion Channel 1 To Promote Survival in Hypoxia

Brahimi-Horn

Lacas‐Gervais

Adaixo

et al. 2015

Molecular and Cellular Biology

View full text Add to dashboard Cite

The oxygen-limiting (hypoxic) microenvironment of tumors induces metabolic reprogramming and cell survival, but the underlying mechanisms involving mitochondria remain poorly understood. We previously demonstrated that hypoxia-inducible factor 1 mediates the hyperfusion of mitochondria by inducing Bcl-2/adenovirus E1B 19-kDa interacting protein 3 and posttranslational truncation of the mitochondrial ATP transporter outer membrane voltage-dependent anion channel 1 in hypoxic cells. In addition, we showed that truncation is associated with increased resistance to drug-induced apoptosis and is indicative of increased patient chemoresistance. We now show that silencing of the tumor suppressor TP53 decreases truncation and increases drug-induced apoptosis. We also show that TP53 regulates truncation through induction of the mitochondrial protein Mieap. While we found that truncation was independent of mitophagy, we observed local microfusion between mitochondria and endolysosomes in hypoxic cells in culture and in patients' tumor tissues. Since we found that the endolysosomal asparagine endopeptidase was responsible for truncation, we propose that it is a readout of mitochondrial-endolysosomal microfusion in hypoxia. These novel findings provide the framework for a better understanding of hypoxic cell metabolism and cell survival through mitochondrial-endolysosomal microfusion regulated by hypoxia-inducible factor 1 and TP53. Hypoxia is a natural occurring stress that results in compensatory changes in metabolism and cell survival during embryonic development and tumor growth. Hypoxia stabilizes and activates the transcription factor hypoxia-inducible factor (HIF) through inhibition of oxygen-dependent hydroxylases that earmark the alpha subunit of HIF for proteasomal degradation (1). HIF induces or represses the expression of genes implicated in a myriad of functions, including those regulating metabolism and resistance to drug-induced cell death. Genes coding for the enzymes of the glycolytic pathway, including hexokinase, are highly induced by HIF-1, and this is in part responsible for the switch in metabolism from mitochondrial respiration to glycolysis in cancer cells. Considerable studies have pointed to the Warburg effect, also termed aerobic glycolysis, as the major adaptive response of cancer cells, but mitochondrial metabolism and mitochondrial dynamics are also starting to be recognized as important adaptive strategies of cancer cells (2). Mitochondria are critical organelles that regulate both metabolism and cell death. They are dynamic organelles that continuously undergo fission and fusion during cell growth (3, 4). Under stress conditions, such as nutrient depletion or hypoxia, mitochondria either fragment or are degraded by HIF-dependent mitophagy (mitochondrial removal by autophagy) (5) or hyperfuse together to form elongated or rounded structures that optimize ATP production and promote cell survival (6-11).We reported previously that certain cell lines exposed to hypoxia contained enlarged mitochon...

show abstract

Section: Resultssupporting

confidence: 89%

Section: Discussioncontrasting

confidence: 91%

Section: Resultscontrasting

confidence: 69%

mentioning

confidence: 99%

See 2 more Smart Citations

Local Mitochondrial-Endolysosomal Microfusion Cleaves Voltage-Dependent Anion Channel 1 To Promote Survival in Hypoxia

Brahimi-Horn

Lacas‐Gervais

Adaixo

et al. 2015

Molecular and Cellular Biology

View full text Add to dashboard Cite

show abstract

“…In response to stress, such as DNA damage, Mieap is induced and translocates to the mitochondrial matrix in a ROS-dependent manner [89], allowing lysosomal enzymes to move into the matrix thereby facilitating degradation of oxidatively damaged mitochondrial proteins (designated MALM for Mieap-induced accumulation of lysosome-like organelles within mitochondria [88]). This occurs only when BNIP3 and NIX coexist at the mitochondrial surface [90]. The interaction between Mieap, BNIP3 and NIX appears to facilitate the formation of a mitochondrial membrane pore involving both mitochondrial membranes, thus causing a drop in membrane potential.…”

Section: P53 and Mitochondrial Quality Controlmentioning

confidence: 99%

p53 and mitochondrial function in neurons

Wang

Kinoshita

et al. 2014

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

149

108

View full text Add to dashboard Cite

The p53 tumor suppressor plays a central role in dictating cell survival and death as a cellular sensor for a myriad of stresses including DNA damage, oxidative and nutritional stress, ischemia and disruption of nucleolar function. Activation of p53-dependent apoptosis leads to mitochondrial apoptotic changes via the intrinsic and extrinsic pathways triggering cell death execution most notably by release of cytochrome c and activation of the caspase cascade. Although it was previously believed that p53 induces apoptotic mitochondrial changes exclusively through transcription-dependent mechanisms, recent studies suggest that p53 also regulates apoptosis via a transcription-independent action at the mitochondria. Recent evidence further suggests that p53 can regulate necrotic cell death and autophagic activity including mitophagy. An increasing number of cytosolic and mitochondrial proteins involved in mitochondrial metabolism and respiration are regulated by p53, which influences mitochondrial ROS production as well. Cellular redox homeostasis is also directly regulated by p53 through modified expression of pro- and anti-oxidant proteins. Proper regulation of mitochondrial size and shape through fission and fusion assures optimal mitochondrial bioenergetic function while enabling adequate mitochondrial transport to accommodate local energy demands unique to neuronal architecture. Abnormal regulation of mitochondrial dynamics has been increasingly implicated in neurodegeneration, where elevated levels of p53 may have a direct contribution as the expression of some fission/fusion proteins are directly regulated by p53. Thus, p53 may have a much wider influence on mitochondrial integrity and function than one would expect from its well-established ability to transcriptionally induce mitochondrial apoptosis. However, much of the evidence demonstrating that p53 can influence mitochondria through nuclear, cytosolic or intra-mitochondrial sites of action has yet to be confirmed in neurons. Nonetheless, as mitochondria are essential for supporting normal neuronal functions and in initiating/propagating cell death signaling, it appears certain that the mitochondria-related functions of p53 will have broader implications than previously thought in acute and progressive neurological conditions, providing new therapeutic targets for treatment.

show abstract

Mitophagy programs: mechanisms and physiological implications of mitochondrial targeting by autophagy

Hamacher-Brady

Brady

2015

Cell. Mol. Life Sci.

339

287

View full text Add to dashboard Cite

Mitochondria are an essential source of ATP for cellular function, but when damaged, mitochondria generate a plethora of stress signals, which lead to cellular dysfunction and eventually programmed cell death. Thus, a major component of maintaining cellular homeostasis is the recognition and removal of dysfunctional mitochondria through autophagy-mediated degradation, i.e., mitophagy. Mitophagy further constitutes a developmental program, and undergoes a high degree of crosstalk with apoptosis. Reduced mitochondrial quality control is linked to disease pathogenesis, suggesting the importance of process elucidation as a clinical target. Recent work has revealed multiple mitophagy programs that operate independently or undergo crosstalk, and require modulated autophagy receptor activities at outer membranes of mitochondria. Here, we review these mitophagy programs, focusing on pathway mechanisms which recognize and target mitochondria for sequestration by autophagosomes, as well as mechanisms controlling pathway activities. Furthermore, we provide an introduction to the currently available methods for detecting mitophagy.

show abstract

BNIP3 and NIX Mediate Mieap-Induced Accumulation of Lysosomal Proteins within Mitochondria

Cited by 45 publications

References 14 publications

Local Mitochondrial-Endolysosomal Microfusion Cleaves Voltage-Dependent Anion Channel 1 To Promote Survival in Hypoxia

Local Mitochondrial-Endolysosomal Microfusion Cleaves Voltage-Dependent Anion Channel 1 To Promote Survival in Hypoxia

p53 and mitochondrial function in neurons

Mitophagy programs: mechanisms and physiological implications of mitochondrial targeting by autophagy

Contact Info

Product

Resources

About