Transaldolase deficiency influences the pentose phosphate pathway, mitochondrial homoeostasis and apoptosis signal processing

Qian, Yueming; Banerjee, Sanjay K.; Grossman, Craig E.; Amidon, Wendy; Nagy, György; Barcza, Maureen; Niland, Brian; Karp, David R.; Middleton, Frank A.; Bánki, Katalin; Perl, András

doi:10.1042/bj20080722

Cited by 45 publications

(45 citation statements)

References 48 publications

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“…The GSH synthetase and transaldolase are enzymes involved in the generation of GSH 32 and NADPH, respectively. 41 The downmodulation of these two proteins in cells expressing the DN-STAT5A mutant could be responsible for their sensitivity to apoptosis via the decrease of their protective effect against oxygen-free radicals. The promoter of the GSH synthetase gene contains multiple binding sites for STAT family members including STAT5, suggesting that STAT5 might regulate the transcriptional activation of this gene.…”

Section: Discussionmentioning

confidence: 99%

Evidence for a protective role of the STAT5 transcription factor against oxidative stress in human leukemic pre-B cells

Cholez

Debuysscher

Bourgeais³

et al. 2012

Leukemia

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,5,6 STAT5 transcription factors are involved in normal B lymphocyte development and in leukemogenesis. We show that the inhibition of STAT5A expression or activity in the NALM6, 697 and Reh leukemic pre-B cell lines, results in a higher spontaneous apoptosis and an increased FAS-induced cell death. However, the molecular mechanisms underlying the altered pre-B cell survival are unclear. We used a proteomic approach to identify proteins that are differentially regulated in cells expressing (NALM6D5A) or not a dominant negative form of STAT5A. Among the 14 proteins identified, six were involved in the control of the oxidative stress like glutathione (GSH) synthetase and DJ-1. Accordingly, we showed increased levels of reactive oxygen species (ROS) in NALM6D5A cells and suppression of the increased sensitivity to Fas-mediated apoptosis by the GSH tripeptide. Similar results were observed when NALM6 cells were treated with TAT-STAT5D5A fusion proteins or STAT5A shRNA. In addition, the 697 and Reh pre-B cells were found to share number of molecular changes observed in NALM6D5A cells including ROS generation, following inhibition of STAT5 expression or function. Our results point out to a hitherto undescribed link between STAT5 and oxidative stress and provide new insights into STAT5 functions and their roles in leukemogenesis.Leukemia ( INTRODUCTIONThe signal transducer and activator of transcription factors STAT5A and STAT5B are two closely related STAT family members that play a major role in cytokine and growth factor signaling. 1 Number of studies have demonstrated that STAT5 plays a crucial role in hematopoiesis. In particular, the knockout mice models (Stat5a/ b DN/DN and Stat5a/b null/null ) have pointed up the important role of STAT5 in hematopoietic cell development. 2,3 These mice have multiple hematopoietic defects, which affect the proliferation and/ or survival of both myeloid and lymphoid lineages, including B-cell development. 4 In the Stat5a/b null/null mice, the precursor B-cell compartment is substantially reduced presumably due to an inability of progenitor B cells to proliferate in response to interleukin-7 (IL-7). However, differentiation towards mature B cells seems to be unaffected. 5,6 STAT5 is also involved in the regulation of IL-7-dependent germline transcription, histone acetylation and DNA recombination of distal VH gene segments, which are the hallmark of B lymphocyte development. 7 Accordingly, a constitutively active form of STAT5B in IL-7R À / À mice, is sufficient to restore B-cell development. 8 However, the instructive role for STAT5 and IL-7-R signaling in early B-cell development has been controversial in a mouse model of conditional mutagenesis of STAT5. 9 This model showed that the main role of IL-7-mediated activation of STAT5 is to promote pro-B-cell survival via Mcl1 and to prevent premature rearrangements of the immunoglobulin-k light-chain locus (Igk) by binding to the

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Section: Discussionmentioning

confidence: 99%

Evidence for a protective role of the STAT5 transcription factor against oxidative stress in human leukemic pre-B cells

Cholez

Debuysscher

Bourgeais³

et al. 2012

Leukemia

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“…Furthermore, Gabpa disruption caused very early embryonic lethality (39), which suggests that embryonic loss was not caused solely by its role in mitochondrial regulation. Gabpa disruption dramatically reduced Tfb1m expression, and the phenotype of reduced mitochondrial biogenesis was similar to that caused by short hairpin RNA knockdown of TFB1M.…”

Section: Discussionmentioning

confidence: 99%

GABP Transcription Factor (Nuclear Respiratory Factor 2) Is Required for Mitochondrial Biogenesis

Yang

Drumea

Mott

et al. 2014

Molecular and Cellular Biology

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c Mitochondria are membrane-bound cytoplasmic organelles that serve as the major source of ATP production in eukaryotic cells. GABP (also known as nuclear respiratory factor 2) is a nuclear E26 transformation-specific transcription factor (ETS) that binds and activates mitochondrial genes that are required for electron transport and oxidative phosphorylation. We conditionally deleted Gabpa, the DNA-binding component of this transcription factor complex, from mouse embryonic fibroblasts (MEFs) to examine the role of Gabp in mitochondrial biogenesis, function, and gene expression. Gabp␣ loss modestly reduced mitochondrial mass, ATP production, oxygen consumption, and mitochondrial protein synthesis but did not alter mitochondrial morphology, membrane potential, apoptosis, or the expression of several genes that were previously reported to be GABP targets. However, the expression of Tfb1m, a methyltransferase that modifies ribosomal rRNA and is required for mitochondrial protein translation, was markedly reduced in Gabp␣-null MEFs. We conclude that Gabp regulates Tfb1m expression and plays an essential, nonredundant role in mitochondrial biogenesis. Mitochondria are semiautonomous, membrane-bound cytoplasmic organelles that are the major source of ATP production in the eukaryotic cell. In addition to their roles in generating cellular energy through electron transfer and oxidative phosphorylation, mitochondria are also required for lipid biosynthesis, cell signaling, apoptosis, and other essential cellular functions. Because the 16-kb mitochondrial genome does not encode any transcription factors, it depends on nuclear transcription factors for the expression of mitochondrial DNA (mtDNA) genes. Mitochondrial transcription factor A (TFAM) and TFBM are nuclear transcription factors that exclusively regulate mtDNA genes. Other transcription factors, including NRF1 (nuclear respiratory factor 1) and NRF2, control both mtDNA genes and nuclear genes (1-4).There are two distinct TFBM proteins, TFB1M and TFB2M, both of which have rRNA methyltransferase activity (5, 6). Shadel and colleagues reported that TFB1M and TFB2M play crucial but distinct roles in the control of mitochondrial biogenesis in both human and Drosophila cells (7-9). TFB2M mainly regulates mtDNA replication and mitochondrial gene transcription. Ectopic expression of TFB1M did not significantly affect mitochondrial function, but reduced expression of TFB1M decreased mitochondrial protein translation through impaired methylation of the 12S rRNA, impaired mitochondrial ribosome assembly, and abolished mitochondrial translation. Genetic disruption of Tfb1m caused early (embronic day 8.5 [E8.5]) embryonic lethality but neither activated nor repressed mitochondrial gene transcription (10). Thus, adequate levels of TFB1M are required for normal mitochondrial protein synthesis and biogenesis.Scarpulla and colleagues recognized that the multiprotein NRF2 complex is the human homologue of GABP, or GA-binding protein (11). GABP is the only obligate multimer among th...

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“…1C-1D). DHR123 is used as a fluorescent indicator for reactive oxygen species (ROS) generation measured such that increases in ROS production increase fluorescence (20,33). Cells overexpressing SelM showed significantly reduced ROS production when measured by DHR123 fluorescence in the presence of varying concentrations of hydrogen peroxide (Figs.…”

Section: Resultsmentioning

confidence: 99%

The Neuroprotective Functions of Selenoprotein M and its Role in Cytosolic Calcium Regulation

Reeves

Bellinger

Berry

2010

Antioxidants & Redox Signaling

138

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Selenoproteins contain the trace element selenium incorporated as selenocysteine, the 21 st amino acid. Some members of the selenoprotein family, such as the glutathione peroxidases, have well-characterized antioxidant activity, functioning in enzymatic breakdown of hydroperoxides to protect cells against oxidative stress. However, the functions of many of the 25 human selenoproteins, including the brain-enriched selenoprotein M, are unknown. We investigated selenoprotein M function by manipulating expression in murine hippocampal HT22 cells, cerebellar astrocyte C8-D1A cells, and primary neuronal cultures. Overexpression of the protein resulted in a reduction in reactive oxygen species and apoptotic cell death in response to oxidative challenge with hydrogen peroxide. In contrast, knock-down of selenoprotein M using shRNA in primary neuronal cultures caused apoptotic cell death comparable to levels resulting from addition of hydrogen peroxide. Calcium measurements with the indicator cameleon demonstrated that overexpression of selenoprotein M decreased calcium influx in response to hydrogen peroxide. Additionally, knock-down of selenoprotein M expression in cortical cultures caused higher baseline levels of cytosolic calcium than in control cells. These results suggest that selenoprotein M may have an important role in protecting against oxidative damage in the brain and may potentially function in calcium regulation. Antioxid. Redox Signal. 12, 809-818.

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Transaldolase deficiency influences the pentose phosphate pathway, mitochondrial homoeostasis and apoptosis signal processing

Cited by 45 publications

References 48 publications

Evidence for a protective role of the STAT5 transcription factor against oxidative stress in human leukemic pre-B cells

Evidence for a protective role of the STAT5 transcription factor against oxidative stress in human leukemic pre-B cells

GABP Transcription Factor (Nuclear Respiratory Factor 2) Is Required for Mitochondrial Biogenesis

The Neuroprotective Functions of Selenoprotein M and its Role in Cytosolic Calcium Regulation

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