The Protooncogene <i>bcl‐2</i> Inhibits Apoptosis in PC12 Cells

Mah, Steven; Zhong, Li-tao; Liu, Yahui; Roghani, Ali; Edwards, Robert H.; Bredesen, Dale E.

doi:10.1111/j.1471-4159.1993.tb03275.x

Cited by 224 publications

(117 citation statements)

References 16 publications

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“…In vitro evidence that this gene could be involved in neuronal apoptosis comes from overexpression of this gene in neurons deprived of trophic factors (Garcia et al, 1992;Allsopp et al, 1993;Mah et al, 1993).…”

Section: Discussionmentioning

confidence: 99%

Apoptotic cell death induced by optic nerve lesion in the neonatal rat

et al. 1994

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Cell death can be ascribed to one of two distinct modes of degeneration: apoptosis (programmed or active cell death) or necrosis (passive degeneration). While apoptosis is generally assumed to occur in physiological conditions such as normal development or tissue turnover, necrotic cell degeneration is induced in pathological situations. Here we report that also in a pathological situation, such as after axotomy in the CNS, apoptotic type of cell death comes into play: following intracranial transection of the optic nerve in the neonatal rat in vivo, retinal ganglion cells undergo an active, apoptotic cell death. In fact, the administration of protein synthesis inhibitors (actinomycin D and cycloheximide) prevents the appearance of pyknotic nuclei as well as of fragmented DNA of ganglion cells at 24 hr postlesion. Correspondingly, the number of surviving cells after actinomycin D and cycloheximide treatment is comparable to normal, unlesioned retinas. In addition, cycloheximide decreases the number of pyknotic ganglion cells during spontaneous cell death.

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Section: Discussionmentioning

confidence: 99%

Apoptotic cell death induced by optic nerve lesion in the neonatal rat

et al. 1994

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“…Culture of GT1-7 cells (puro and bcl-2 transfected) GT1-7 cells, a hypothalamic neuron cell-derived line (GT1-7puro cells) 28 and bcl-2 transfected cells (GT1-7bcl-2 cells), as previously verified by Mah et al 17 or Kane et al, 29 were maintained in DMEM containing 25 mM D-glucose, supplemented with 10% heat-inactivated fetal bovine serum, 100 U/ml penicillin and 100 mg/ml streptomycin on poly-L-lysine coated plates, in an atmosphere of 5% CO 2 /95% air, at 378C. The medium was changed every 3 days.…”

Section: Methodsmentioning

confidence: 99%

“…9 ± 11 The cell death repressor protein Bcl-2 inhibits cellular free radical formation 12 ± 14 and cyt c release, 15 blocks the activation of caspases 16 and inhibits apoptosis. 17 Bcl-2 increases the capacity of mitochondria to accumulate Ca 2+ 18 and shifts the redox potential of cells towards reduction. 19 Vander Heiden et al 6 have reported that Bclx(L)-expressing cells adapt to STS treatment by maintaining a decreased DC M , while Shimizu et al 20 have suggested that Bcl-2 over-expression decreases the effectiveness of protonophores in depolarizing the mitochondria by enhancing ion flux.…”

Section: Introductionmentioning

confidence: 99%

The mechanism of mitochondrial membrane potential retention following release of cytochrome c in apoptotic GT1-7 neural cells

2001

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The relationship is investigated between mitochondrial membrane potential (DC M ), respiration and cytochrome c (cyt c) release in single neural bcl-2 transfected cells (GT1-7bcl-2) or GT1-7puro cells during apoptosis induced by staurosporine (STS). Bcl-2 inhibited the mitochondrial release of cyt c and apoptosis. Three different cell responses to STS were identified in GT1-7puro cells: (i) neither DC M nor cyt c were significantly affected; (ii) a decrease in DC M was accompanied by a complete release of cyt c; or (iii) cyt c release occurred independently of a loss of DC M . The endogenous inner membrane proton leak of the in situ mitochondria, monitored by respiration in the presence of oligomycin, was increased by STS by 92% in puro cells, but by only 23% in bcl-2 cells. STS decreased respiratory capacity, in the presence of protonophore, by 31% in puro cells and by 20% in bcl-2 cells. In the absence of STS, oligomycin hyperpolarized mitochondria within both puro and bcl-2-transfected cells, indicating that the organelles were net generators of ATP. However after 15 h exposure to STS oligomycin rapidly collapsed residual mitochondrial polarization in the puro cells, indicating that DC M had been maintained by ATP synthase reversal. bcl-2 cells in contrast, maintained DC M until protonophore was added. These results indicate that the maintenance of DC M following release of cyt c may be a consequence of ATP synthase reversal and cytoplasmic ATP hydrolysis in STS-treated GT1-7 cells. Cell Death and Differentiation (2001) 8, 995 ± 1003.

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“…1) was used in conjunction with immunocytochemical methods. Since PC12 cells are a neuroendocrine linederived originally from a rat adrenal phaeochromocytoma-which do not basally express Bcl-2 [10,15,16], they represent an ideal model in which to examine the putative effects of exogenously expressed Bcl-2 on neuroendocrine peptide expression. Moreover, the use of immunohistochemical methods in the present study facilitated the semi-quantitative determination of marker expression, some of which would have proven difficult to detect by immunoblotting due to their low molecular weight.…”

Section: Resultsmentioning

confidence: 99%

“…In view of these findings it would appear that the reported expression of Bcl-2 in neuroendocrine cells [5][6][7][8] relates either to the well-documented anti-apoptotic actions of this oncoprotein or to additional, as yet undiscovered, functions. Previous studies have shown that forced Bcl-2 expression suppresses apoptosis of PC12 cells [15,16] and it has been speculated that the observed expression of Bcl-2 in oxyntic endocrine cells may promote cytosurvival during their maturation and downward migration from isthmal/neck-localised stem cells [8]. Numerous studies have documented Bcl-2 expression in neuroendocrine tumours such as phaeochromocytomas [18], thymic neuroendocrine tumours [19], and gastroenteropancreatic neuroendocrine tumours [20].…”

Section: Resultsmentioning

confidence: 99%

An investigation into the role of Bcl-2 in neuroendocrine differentiation

Cadden

Johnston

Connolly

et al. 2005

Biochemical and Biophysical Research Communications

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Introduction: In addition to its role in apoptosis suppression, Bcl-2 has been reported to be co-expressed with neuroendocrine markers in several tissues, leading to speculation that this oncoprotein may promote neuroendocrine differentiation.Aim: This study investigated whether Bcl-2 modulated neuroendocrine biopeptide expression. Methods: Levels of chromogranin A, neurone specific enolase, protein gene peptide 9.5, pancreatic polypeptide, and the chromogranin-derived peptides, intervening peptide and vasostatin-1 were examined by immunocytochemistry in rat phaeochromocytoma (PC12) cell lines genetically engineered to over-express Bcl-2 and their mock-transfected controls. Intensity of fluorescence was graded using a semi-quantitative scale from (À) indicating negative expression to (+++) indicating intense positivity.Results: Mann-Whitney U analysis indicated that no significant differences in expression existed between control and Bcl2 overexpressing cell lines for any of the six peptides examined.Conclusions: The results of this study do not support the hypothesis that Bcl-2 promotes the acquisition of a neuroendocrine phenotype.

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The Protooncogene bcl‐2 Inhibits Apoptosis in PC12 Cells

Cited by 224 publications

References 16 publications

Apoptotic cell death induced by optic nerve lesion in the neonatal rat

Apoptotic cell death induced by optic nerve lesion in the neonatal rat

The mechanism of mitochondrial membrane potential retention following release of cytochrome c in apoptotic GT1-7 neural cells

An investigation into the role of Bcl-2 in neuroendocrine differentiation

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