Cell Death by Necrosis, a Regulated Way to Go

Henríquez, Mauricio; Armisén, Ricardo; Stutzin, Andrés; Quest, Andrew F. G.

doi:10.2174/156652408784221289

Cited by 78 publications

(60 citation statements)

References 245 publications

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“…Treatment of isolated macrophages activated in vivo in mice with apoptosis-inducing agents lead to a dramatic increase in Caveolin-1 levels while Caveolin-2 is not affected. Phosphatidylserine (PS) externalization is considered a defining feature associated with apoptosis [111]. Interestingly, Caveolin-1 is present in lipid rafts and colocalizes with PS at the cell surface of apoptotic macrophages, where it is suggested to be involved in the efficient externalization of PS [112].…”

Section: Caveolin-1 and Apoptosismentioning

confidence: 99%

The Caveolin-1 Connection to Cell Death and Survival

Quest

Lobos-González²,

Núñez³

et al. 2013

Current Molecular Medicine

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Abstract:Caveolins are a family of membrane proteins required for the formation of small plasma membrane invaginations called caveolae that are implicated in cellular trafficking processes. In addition to this structural role, these scaffolding proteins modulate numerous intracellular signaling pathways; often via direct interaction with specific binding partners. Caveolin-1 is particularly well-studied in this respect and has been attributed a large variety of functions. Thus, Caveolin-1 also represents the best-characterized isoform of this family with respect to its participation in cancer. Rather strikingly, available evidence indicates that Caveolin-1 belongs to a select group of proteins that function, depending on the cellular settings, both as tumor suppressor and promoter of cellular traits commonly associated with enhanced malignant behavior, such as metastasis and multi-drug resistance. The mechanisms underlying such ambiguity in Caveolin-1 function constitute an area of great interest. Here, we will focus on discussing how Caveolin-1 modulates cell death and survival pathways and how this may contribute to a better understanding of the ambiguous role this protein plays in cancer.

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Section: Caveolin-1 and Apoptosismentioning

confidence: 99%

The Caveolin-1 Connection to Cell Death and Survival

Quest

Lobos-González²,

Núñez³

et al. 2013

Current Molecular Medicine

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“…These organelles are the predominant sites for intracellular calcium stores, and the highly organized subcellular architecture of adult cardiac myocytes enforces close proximity between SR and mitochondria, making it possible for calcium to transfer from SR to mitochondria through junctional microdomains referred to as 'calcium hot-spots' (Rizzuto and Pozzan, 2006). Calcium delivery to mitochondria and uptake by the calcium uniporter are a potent stimulus for mitochondrial permeability transition (MPT) in the heart and elsewhere, and the resulting inner and outer membrane rupture leads to cell death from ATP depletion, called 'programmed necrosis' (Nakayama et al, 2007;Henriquez et al, 2008). The Dorn group found that there is a direct relationship between NIX/BNIP3L level in NIX/BNIP3L-overexpressing and -knockout mice and SR calcium content, suggesting that ER/SRlocalized NIX/BNIP3L can affect intracellular calcium stores in a similar manner as previously reported for BCL2 and BAX (Foyouzi-Youssefi et al, 2000;Nutt et al, 2002;Scorrano et al, 2003).…”

Section: Transgenic Cardiac Overexpression Studies Of Bnip3 and Nix/bmentioning

confidence: 99%

Cardiac reanimation: targeting cardiomyocyte death by BNIP3 and NIX/BNIP3L

Dorn

Kirshenbaum

2008

Oncogene

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Programmed cardiac myocyte death contributes to pathological ventricular remodeling and the progression of myocardial infarction or pressure overload hypertrophy to dilated cardiomyopathy. Recent work has identified importance of stress-mediated transcriptional induction of BNIP3 (BCL2 and 19-kDa interacting protein-3) and NIX/BNIP3L in cardiac remodeling. Here, the regulatory mechanisms for these two factors in the heart and their effects on programmed cardiomyocyte death are reviewed, with a focus on information derived from studies using mouse models of cardiac BNIP3 and NIX/BNIP3L overexpression and gene ablation.

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“…Prominent features of necrosis are ATP depletion, loss of ion homeostasis and membrane polarity leading to rapid swelling of the cell, membrane rupture, and subsequent release of cellular contents. Necrosis is neither organized nor executed in a similar manner to apoptosis, and cell death is a consequence of irreparable damage (Henriquez et al ., 2008). Necrosis therefore frequently occurs during pathological conditions including stroke, ischemia, and neurodegenerative disorders (Syntichaki et al ., 2002; Malhi et al ., 2006; Henriquez et al ., 2008).…”

Section: Introductionmentioning

confidence: 99%

“…Necrosis is neither organized nor executed in a similar manner to apoptosis, and cell death is a consequence of irreparable damage (Henriquez et al ., 2008). Necrosis therefore frequently occurs during pathological conditions including stroke, ischemia, and neurodegenerative disorders (Syntichaki et al ., 2002; Malhi et al ., 2006; Henriquez et al ., 2008). Inflammation is associated with necrosis and not with apoptotic cell death (Scaffidi et al ., 2002).…”

Section: Introductionmentioning

confidence: 99%

Apoptosis and necrosis mediate skeletal muscle fiber loss in age‐induced mitochondrial enzymatic abnormalities

et al. 2015

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SummarySarcopenia, the age‐induced loss of skeletal muscle mass and function, results from the contributions of both fiber atrophy and loss of myofibers. We have previously characterized sarcopenia in FBN rats, documenting age‐dependent declines in muscle mass and fiber number along with increased fiber atrophy and fibrosis in vastus lateralis and rectus femoris muscles. Concomitant with these sarcopenic changes is an increased abundance of mitochondrial DNA deletion mutations and electron transport chain (ETC) abnormalities. In this study, we used immunohistological and histochemical approaches to define cell death pathways involved in sarcopenia. Activation of muscle cell death pathways was age‐dependent with most apoptotic and necrotic muscle fibers exhibiting ETC abnormalities. Although activation of apoptosis was a prominent feature of electron transport abnormal muscle fibers, necrosis was predominant in atrophic and broken ETC‐abnormal fibers. These data suggest that mitochondrial dysfunction is a major contributor to the activation of cell death processes in aged muscle fibers. The link between ETC abnormalities, apoptosis, fiber atrophy, and necrosis supports the hypothesis that mitochondrial DNA deletion mutations are causal in myofiber loss. These studies suggest a progression of events beginning with the generation and accumulation of a mtDNA deletion mutation, the concomitant development of ETC abnormalities, a subsequent triggering of apoptotic and, ultimately, necrotic events resulting in muscle fiber atrophy, breakage, and fiber loss.

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Cell Death by Necrosis, a Regulated Way to Go

Cited by 78 publications

References 245 publications

The Caveolin-1 Connection to Cell Death and Survival

The Caveolin-1 Connection to Cell Death and Survival

Cardiac reanimation: targeting cardiomyocyte death by BNIP3 and NIX/BNIP3L

Apoptosis and necrosis mediate skeletal muscle fiber loss in age‐induced mitochondrial enzymatic abnormalities

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