Bid-induced release of AIF from mitochondria causes immediate neuronal cell death

Landshamer, Stefan; Hoehn, Miriam; Barth, Nicole; Duvezin-Caubet, Stéphane; Schwake, Gerlinde; Tobaben, S; Kazhdan, Irene; Becattini, Barbara; Zahler, Stefan; Vollmar, Angelika M.; Pellecchia, Maurizio; Reichert, A; Plesnila, Nikolaus; Wagner, Ernst; Culmsee, Carsten

doi:10.1038/cdd.2008.78

Cited by 134 publications

(184 citation statements)

References 30 publications

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“…Further, depolarization of the MOM and mitochondrial fragmentation are both important key events of apoptosis induced by oxidative stress, and both events were apparently Bid dependent ( Supplementary Figures 8a-d). 5,19 The pivotal role for Bid upstream of such mitochondrial dysfunction is substantiated by experiments demonstrating pronounced neuroprotective effects of the Bid inhibitor BI-6c9 in models of glutamate-induced excitotoxicity and OGD in primary cultured neurons, and similar studies in HT-22 neurons using Bid siRNA. 19,20,30,31 Further, reduced Bid expression attenuated neuronal death in a model of OGD in vitro and reduced brain damage in models of cerebral ischemia and brain trauma in vivo.…”

Section: Discussionmentioning

confidence: 86%

“…5,19 The pivotal role for Bid upstream of such mitochondrial dysfunction is substantiated by experiments demonstrating pronounced neuroprotective effects of the Bid inhibitor BI-6c9 in models of glutamate-induced excitotoxicity and OGD in primary cultured neurons, and similar studies in HT-22 neurons using Bid siRNA. 19,20,30,31 Further, reduced Bid expression attenuated neuronal death in a model of OGD in vitro and reduced brain damage in models of cerebral ischemia and brain trauma in vivo. 21 Recent studies showed that tBid and full-length Bid exert similar effects on mitochondria and AIF-dependent cell death in neurons.…”

Section: Discussionmentioning

confidence: 86%

“…21 Recent studies showed that tBid and full-length Bid exert similar effects on mitochondria and AIF-dependent cell death in neurons. 19,32 Mitochondrial translocation of full-length Bid was sufficient to induce Bax oligomerization and integration into the outer mitochondrial membrane in Hela cells 33 and to induce mitochondrial dysfunction in neurons. 32 Activated tBid induces rapid mitochondrial demise in caspase-dependent death receptor mediated pathways, while full-length Bidmediated caspase-independent cell death pathways, however with slower kinetics compared with tBid.…”

Section: Discussionmentioning

confidence: 99%

“…Our recent data demonstrated a role for the proapoptotic BH3-only protein Bid for enhanced mitochondrial fragmentation in the present model systems of HT-22 cell oxytosis and primary neuron cell death induced by glutamate or OGD. 5,19 We documented that Bid is involved in the loss of MMP and release of mitochondrial AIF, which mediates delayed neuronal death after cerebral ischemia. [19][20][21] Here, we examined the role of Drp1 in Bid-mediated neuronal cell death and observed that treatment of cells with mdiviA or mdiviB also prevented tBid-induced mitochondrial fission and preserved cell viability ( Figure 5).…”

mentioning

confidence: 99%

“…5,19 We documented that Bid is involved in the loss of MMP and release of mitochondrial AIF, which mediates delayed neuronal death after cerebral ischemia. [19][20][21] Here, we examined the role of Drp1 in Bid-mediated neuronal cell death and observed that treatment of cells with mdiviA or mdiviB also prevented tBid-induced mitochondrial fission and preserved cell viability ( Figure 5). Vector-induced expression of tBid reduced cell viability to 30% of control levels, whereas cell viability was restored to control levels when the Drp1 inhibitors were applied to tBid expressing cells ( Figure 5c).…”

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Inhibition of Drp1 provides neuroprotection in vitro and in vivo

et al. 2012

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Impaired regulation of mitochondrial dynamics, which shifts the balance towards fission, is associated with neuronal death in age-related neurodegenerative diseases, such as Alzheimer's disease or Parkinson's disease. A role for mitochondrial dynamics in acute brain injury, however, has not been elucidated to date. Here, we investigated the role of dynamin-related protein 1 (Drp1), one of the key regulators of mitochondrial fission, in neuronal cell death induced by glutamate toxicity or oxygen-glucose deprivation (OGD) in vitro, and after ischemic brain damage in vivo. Drp1 siRNA and small molecule inhibitors of Drp1 prevented mitochondrial fission, loss of mitochondrial membrane potential (MMP), and cell death induced by glutamate or tBid overexpression in immortalized hippocampal HT-22 neuronal cells. Further, Drp1 inhibitors protected primary neurons against glutamate excitotoxicity and OGD, and reduced the infarct volume in a mouse model of transient focal ischemia. Our data indicate that Drp1 translocation and associated mitochondrial fission are key features preceding the loss of MMP and neuronal cell death. Thus, inhibition of Drp1 is proposed as an efficient strategy of neuroprotection against glutamate toxicity and OGD in vitro and ischemic brain damage in vivo. Mitochondria play crucial roles in energy metabolism, regulation of free radical formation and calcium storage, thereby determining essential metabolic functions and cell survival. 1 Further, mitochondria are highly dynamic organelles that undergo constant fission and fusion and these morphological changes are required for efficient ATP production, calcium buffering, regulation of signal transduction and apoptosis. 2 In neurons, mitochondrial fission is also essential for axonal transport of the organelles into areas of high metabolic demand, 3 whereas mitochondrial fusion supports substitution and regeneration of mitochondrial proteins, mtDNA repair and functional recovery. 2,4 Consistent with the critical roles of mitochondrial dynamics in neurons, defects in mitochondrial fission and fusion proteins are associated with a wide array of inherited or acquired neurodegenerative diseases such as Charcot-Marie-Tooth disease or Alzheimer's disease, respectively. 2 Fission and fusion defects may limit mitochondrial motility, decrease energy production, promote oxidative stress and lead to accumulating of mtDNA defects, thereby promoting neuronal dysfunction and cell death. 1 Recently, enhanced mitochondrial fragmentation was associated with induction of neuronal death triggered by oxidative stress. 5 These data imply that during neuronal cell death, the tubular mitochondrial network is fragmented into smaller and functionally impaired organelles. 5 It is, however, a matter of ongoing controversy, whether mitochondrial fragmentation is cause or consequence in programmed cell death.Current knowledge of the mechanisms regulating mitochondrial dynamics indicates that fission and fusion of mitochondria are under control of highly conserved dynamin-relate...

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Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Inhibition of Drp1 provides neuroprotection in vitro and in vivo

et al. 2012

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Molecular Mechanisms Underlying Oxytosis

Dolga

Oppermann

Richter

et al. 2018

Apoptosis and Beyond

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Fluorescence‐Guided Spatial Drug Screening in 3D Colorectal Cancer Spheroids

Yau,

Yempala,

Muthuramalingam

et al. 2024

Adv Healthcare Materials

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The limited recapitulation of critical cancer features in two‐dimensional (2D) cultures causes poor translatability of preclinical results from in vitro assays to in vivo tumor models. This contributes to slow drug development with a low success rate. Three‐dimensional (3D) cultures better recapitulate the tumor microenvironment, enabling more accurate predictions when screening drug candidates and improving the development of chemotherapeutics. Platinum (Pt) (IV) compounds are promising prodrugs designed to reduce the severe systemic toxicity of widely‐used Food and Drug Administration (FDA)‐approved Pt(II) drugs such as cisplatin. Here, we present spatiotemporal evaluations in 3D colorectal cancer (CRC) spheroids of mitochondria‐targeting Pt(IV) complexes. CRC spheroids provide a greater pathophysiological recapitulation of in vivo tumors than 2D cultures by a marked upregulation of the ABCG2 chemoresistance marker expression. Furthermore, we introduce new 3D‐staining protocols to evaluate the real‐time decrease in mitochondria membrane potential (ΔΨ) in CRC spheroids, and a Pt‐sensing dye to quantify the Pt mitochondrial accumulation. Finally, we demonstrate a correlation between in vitro results and the efficacy of the compounds in vivo. Overall, the CRC spheroids represent a fast and cost‐effective model to assess the behavior of Pt compounds in vitro and predict their translational potential in CRC treatment.This article is protected by copyright. All rights reserved

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Bid-induced release of AIF from mitochondria causes immediate neuronal cell death

Cited by 134 publications

References 30 publications

Inhibition of Drp1 provides neuroprotection in vitro and in vivo

Inhibition of Drp1 provides neuroprotection in vitro and in vivo

Molecular Mechanisms Underlying Oxytosis

Fluorescence‐Guided Spatial Drug Screening in 3D Colorectal Cancer Spheroids

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