Nix and Nip3 Form a Subfamily of Pro-apoptotic Mitochondrial Proteins

Chen, Gao; Cizeau, Jeannick; Velde, Christine Vande; Park, Jae Hoon; Bozek, Gracjan; Bolton, Shay-Lee; Shi, Li; Dubik, Don; Greenberg, Arnold H.

doi:10.1074/jbc.274.1.7

Cited by 272 publications

(229 citation statements)

References 18 publications

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“…The protein contains a BH3 domain that induces apoptosis (Yasuda et al, 1998) and a C-terminal transmembrane domain that is required for both its mitochondrial localisation and its proapoptotic activity (Chen et al, 1997(Chen et al, , 1999Yasuda et al, 1998); it has been suggested that BNIP3 mediates a necrosis-like cell death by causing mitochondrial dysfunction (Harris, 2002). Hypoxia induces expression of a group of genes, among which is the transcriptional regulator HIF-1.…”

Section: Discussionmentioning

confidence: 99%

Aberrant DNA methylation associated with silencing BNIP3 gene expression in haematopoietic tumours

et al. 2005

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Hypoxia is a key factor contributing to the progression of human neoplasias and to the development of resistance to chemotherapy. BNIP3 is a proapoptotic member of the Bcl-2 protein family involved in hypoxia-induced cell death. We evaluated the expression and methylation status of BNIP3 gene to better understand the role of epigenetic alteration of its expression in haematopoietic tumours. Methylation of the region around the BNIP3 transcription start site was detected in four acute lymphocytic leukaemia, one multiple myeloma and one Burkitt lymphoma cell lines, and was closely associated with silencing the gene. That expression of BNIP3 was restored by treatment with 5-aza2 0 -deoxycytidine (5-aza-dC), a methyltransferase inhibitor, which confirmed the gene to be epigenetically inactivated by methylation. Notably, re-expression of BNIP3 using 5-aza2-dC also restored hypoxia-mediated cell death in methylated cell lines. Acetylation of histone H3 in the 5 0 region of the gene, which was assessed using chromatin immunoprecipitation assays, correlated directly with gene expression and inversely with DNA methylation. Among primary tumours, methylation of BNIP3 was detected in five of 34 (15%) acute lymphocytic leukaemias, six of 35 (17%) acute myelogenous leukaemias and three of 14 (21%) multiple myelomas. These results suggest that aberrant DNA methylation of the 5 0 CpG island and histone deacetylation play key roles in silencing BNIP3 expression in haematopoietic tumours.

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Section: Discussionmentioning

confidence: 99%

Aberrant DNA methylation associated with silencing BNIP3 gene expression in haematopoietic tumours

et al. 2005

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“…Both of these BH3-only factors localize to and (by activating BAX and BAK) permeabilize mitochondrial outer membranes, which activates the intrinsic apoptosis signaling pathway (Chen et al, 1999). Preventing mitochondrial localization of either BNIP3 or NIX/BNIP3L by mutational deletion of C-terminal mitochondrial targeting sequences creates dominant inhibitory proteins (Regula et al, 2002;Yussman et al, 2002).…”

Section: Cardiomyocyte Apoptosis and Bcl2 Proteins In Myocardial Diseasementioning

confidence: 99%

“…Preventing mitochondrial localization of either BNIP3 or NIX/BNIP3L by mutational deletion of C-terminal mitochondrial targeting sequences creates dominant inhibitory proteins (Regula et al, 2002;Yussman et al, 2002). Both proteins are also subject to rapid degradation by the ubiquitin-proteosome pathway (Chen et al, 1999;Cizeau et al, 2000), accounting for barely detectable levels observed in the unstressed myocardium. Importantly, there appears to be no essential physiological or developmental function for either NIX/BNIP3L or BNIP3 in the heart, as cardiac structure and function are normal in the respective cardiac-specific and germ-line gene knockout mouse models (Diwan et al, 2007b(Diwan et al, , 2008b.…”

Section: Cardiomyocyte Apoptosis and Bcl2 Proteins In Myocardial Diseasementioning

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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“…Paradoxically, expression of the antiapoptotic regulator, IAP-A (Goyal, 2001), decreased more than 50%, whereas expression of NIX (Chen et al, 1999), a pro-apoptotic Bcl-2 family member, increased approximately twofold in differentiating C2C12 cells (Table 2). These observations suggest that the survival of differentiating C2C12 cells and differentiated myotubes may depend on the balance of pro-and anti-apoptotic activities at the cellular level.…”

Section: Coordinate Regulation Of Cell Cycle Withdrawal and Apoptosismentioning

confidence: 99%

Genome‐wide examination of myoblast cell cycle withdrawal during differentiation

Shen

Collier

Hlaing

et al. 2002

Developmental Dynamics

105

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Skeletal and cardiac myocytes cease division within weeks of birth. Although skeletal muscle retains limited capacity for regeneration through recruitment of satellite cells, resident populations of adult myocardial stem cells have not been identified. Because cell cycle withdrawal accompanies myocyte differentiation, we hypothesized that C2C12 cells, a mouse myoblast cell line previously used to characterize myocyte differentiation, also would provide a model for studying cell cycle withdrawal during differentiation. C2C12 cells were differentiated in culture medium containing horse serum and harvested at various time points to characterize the expression profiles of known cell cycle and myogenic regulatory factors by immunoblot analysis. BrdU incorporation decreased dramatically in confluent cultures 48 hr after addition of horse serum, as cells started to form myotubes. This finding was preceded by up-regulation of MyoD, followed by myogenin, and activation of Bcl-2. Cyclin D1 was expressed in proliferating cultures and became undetectable in cultures containing 40% fused myotubes, as levels of p21 WAF1/Cip1 increased and ␣-actin became detectable. Because C2C12 myoblasts withdraw from the cell cycle during myocyte differentiation following a course that recapitulates this process in vivo, we performed a genome-wide screen to identify other gene products involved in this process. Using microarrays containing ϳ10,000 minimally redundant mouse sequences that map to the UniGene database of the National Center for Biotechnology Information, we compared gene expression profiles between proliferating, differentiating, and differentiated C2C12 cells and verified candidate genes demonstrating differential expression by RT-PCR. Cluster analysis of differentially expressed genes revealed groups of gene products involved in cell cycle withdrawal, muscle differentiation, and apoptosis. In addition, we identified several genes, including DDAH2 and Ly-6A, whose expression specifically was up-regulated during cell cycle withdrawal coincident with early myoblast differentiation. Developmental Dynamics 226:128 -138, 2003.

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Nix and Nip3 Form a Subfamily of Pro-apoptotic Mitochondrial Proteins

Cited by 272 publications

References 18 publications

Aberrant DNA methylation associated with silencing BNIP3 gene expression in haematopoietic tumours

Aberrant DNA methylation associated with silencing BNIP3 gene expression in haematopoietic tumours

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

Genome‐wide examination of myoblast cell cycle withdrawal during differentiation

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