Up-regulation of Bcl-2 expression in cultured human lymphocytes after exposure to low doses of gamma radiation

Azimian, Hosein; Bahreyni–Toossi, Mohammad Taghi; Rezaei, Abdul Rahim; Rafatpanah, Houshang; Hamzehloei, Tayebeh; Fardid, Reza

doi:10.4103/0971-6203.152249

Cited by 36 publications

(20 citation statements)

References 36 publications

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“…Microarray analysis of these cells has identified low-dose inducible genes with known roles in apoptosis regulation and cell cycle regulation. Thus low-dose γ-radiation modifies apoptotic-related gene expression in freshly isolated blood lymphocytes, inducing upregulation of Bcl -2, an anti-apoptotic molecule and down-regulation of Bax, a proapoptotic gene [103].…”

Section: Cell Cycle Regulation and Apoptosismentioning

confidence: 99%

Adaptive responses to low doses of radiation or chemicals: their cellular and molecular mechanisms

Guéguen

Bontemps

Ebrahimian

2018

Cell. Mol. Life Sci.

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This article reviews the current knowledge on the mechanisms of adaptive response to low doses of ionizing radiation or chemical exposure. A better knowledge of these mechanisms is needed to improve our understanding of health risks at low level s of environmental or occupational exposure and their involvement in cancer or non-cancer diseases. This response is orchestrated through a multifaceted cellular program involving the concerted action of diverse stress response pathways. These evolutionary highly conserved defense mechanisms determine the cellular response to chemical and physical aggression. They include DNA damage repair (p53, ATM, PARP pathways), antioxidant response (Nrf2 pathway), immune/inflammatory response (NK-B pathway), cell survival/death pathway (apoptosis), endoplasmic response to stress (UPR response), and other cytoprotective processes including autophagy, cell cycle regulation, and the unfolded protein response. The coordinated action of these processes induced by low-dose radiation or chemicals produces biological effects that are currently estimated with the linear non-threshold model. These effects are controversial. They are difficult to detect because of their low magnitude, the scarcity of events in humans, and the difficulty of corroborating associations over the long term. Improving our understanding of these biological consequences should help humans and their environment by enabling better risk estimates , the revision of radiation protection standards, and possible therapeutic advances .

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Section: Cell Cycle Regulation and Apoptosismentioning

confidence: 99%

Adaptive responses to low doses of radiation or chemicals: their cellular and molecular mechanisms

Guéguen

Bontemps

Ebrahimian

2018

Cell. Mol. Life Sci.

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“…Human PBMCs transcriptional response to LDIR as related to apoptosis was elucidated in detail [ 15 ]. The cells were exposed to various LDIR doses ranging from 2 to 10 cGy.…”

Section: Gene Expression Changes In Human Cells Following Low Dosementioning

confidence: 99%

“…Samples for gene expression analysis were taken at 4, 24, 48, 72 h, and up to a week post-LDIR. LDIR was found to induce early repression of the BAX gene in human PBMCs but these changes were restored to near control levels after 168 h [ 15 ]. Generally, the expression of the BCL2 anti-apoptotic gene was elevated, and LDIR-induced changes were transient and disappeared within a week.…”

Section: Gene Expression Changes In Human Cells Following Low Dosementioning

confidence: 99%

Global Gene Expression Alterations as a Crucial Constituent of Human Cell Response to Low Doses of Ionizing Radiation Exposure

Sokolov

Neumann

2015

IJMS

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Exposure to ionizing radiation (IR) is inevitable to humans in real-life scenarios; the hazards of IR primarily stem from its mutagenic, carcinogenic, and cell killing ability. For many decades, extensive research has been conducted on the human cell responses to IR delivered at a low dose/low dose (LD) rate. These studies have shown that the molecular-, cellular-, and tissue-level responses are different after low doses of IR (LDIR) compared to those observed after a short-term high-dose IR exposure (HDIR). With the advent of high-throughput technologies in the late 1990s, such as DNA microarrays, changes in gene expression have also been found to be ubiquitous after LDIR. Very limited subset of genes has been shown to be consistently up-regulated by LDIR, including CDKN1A. Further research on the biological effects and mechanisms induced by IR in human cells demonstrated that the molecular and cellular processes, including transcriptional alterations, activated by LDIR are often related to protective responses and, sometimes, hormesis. Following LDIR, some distinct responses were observed, these included bystander effects, and adaptive responses. Changes in gene expression, not only at the level of mRNA, but also miRNA, have been found to crucially underlie these effects having implications for radiation protection purposes.

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“…Since BTB pretreatment had a marked response on X-ray irradiation-induced apoptosis, the possible molecular mechanisms were further explored. X-ray-radiation-induced apoptosis involves the Bcl-2 family and is mediated by extrinsic and intrinsic pathways [ 26 ]. Bax is a pro-apoptotic member in the Bcl-2-family with the ability of mitochondrial outer membrane permeabilization and consequently promoting the release of cytochrome c, whereas anti-apoptotic members such as Bcl-2 work as protectors of the outer membrane and preserve its integrity by opposing Bax function [ 27 ].…”

Section: Resultsmentioning

confidence: 99%

Selective ATP hydrolysis inhibition in F1Fo ATP synthase enhances radiosensitivity in non-small-cell lung cancer cells (A549)

et al. 2017

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BackgroundF1Fo-ATP synthase (F1Fo-ATPase) is a reversibly rotary molecular machine whose dual functions of synthesizing or hydrolyzing ATP switch upon the condition of cell physiology. The robust ATP-hydrolyzing activity occurs in ischemia for maintaining the transmembrane proton motive force of mitochondria inner membrane, but the effect of F1Fo-ATPase on X-ray response of non-small-cell lung cancer (NSCLC) cells is unknown.Methods and FindingsWe studied whether ATP hydrolysis affected X-ray radiation induced cell death. NSCLC cells (A549) were pretreated with BTB06584 (BTB), an elective ATP hydrolysis inhibitor, followed by X-ray radiation. Cell viability and clonogenic survival were markedly decreased, clear indications of enhanced radiosensitivity through BTB incubation. Additionally, ATP5α1 was upregulated in parallel with elevated ATP hydrolytic activity after X-ray radiation, showing an increased mitochondrial membrane potential (ΔΨm). ATP hydrolysis inhibition led to collapse of ΔΨm suggesting ATP hydrolytic activity could enhance ΔΨm after X-ray radiation. Furthermore, we also demonstrated that apoptosis was pronounced with the prolonged collapse of ΔΨm due to hydrolysis inhibition by BTB incubation.ConclusionOverall, these findings supported that ATP hydrolysis inhibition could enhance the radiosensitivity in NSCLC cells (A549) after X-ray radiation, which was due to the collapse of ΔΨm.

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Up-regulation of Bcl-2 expression in cultured human lymphocytes after exposure to low doses of gamma radiation

Cited by 36 publications

References 36 publications

Adaptive responses to low doses of radiation or chemicals: their cellular and molecular mechanisms

Adaptive responses to low doses of radiation or chemicals: their cellular and molecular mechanisms

Global Gene Expression Alterations as a Crucial Constituent of Human Cell Response to Low Doses of Ionizing Radiation Exposure

Selective ATP hydrolysis inhibition in F1Fo ATP synthase enhances radiosensitivity in non-small-cell lung cancer cells (A549)

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