Mitochondrial biogenesis and metabolic hyperactivation limits the application of MTT assay in the estimation of radiation induced growth inhibition

Rai, Yogesh; Pathak, Richa; Kumari, Neeraj; Sah, Dhananjay Kumar; Pandey, Sanjay; Kalra, Namita; Soni, Ravi; Dwarakanath, B. S.; Bhatt, Anant Narayan

doi:10.1038/s41598-018-19930-w

Cited by 215 publications

(160 citation statements)

References 39 publications

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“…Several studies have shown that E2 has the ability to increase mitochondrial function and biogenesis (reviewed in [42]), therefore, we explored whethe Sirt3 plays a role in E2-induced metabolic fitness of MCF-7 cells. As observed in Figure 3A,C, Sirt3 potentiated this inducing effect of E2 leading to increased metabolic activity, primarily as a result of the induced rise in SDH-A expression ( Figure 3B) [26]. This is not surprising, considering that ERα is an essential estrogen receptor for most E2-mediated increases in respiratory chain proteins and antioxidant enzymes [43,44].…”

Section: Discussionsupporting

confidence: 56%

“…First, we tested the effect of E2 and Sirt3 on metabolic activity of MCF-7 cells using MTT assay. The MTT salt is reduced to formazan in the metabolically active cells predominantly by mitochondrial complex-II subunit succinate dehydrogenase A (SDH-A) and is considered to be a marker of metabolic potential of the cell [26]. The Sirt3-overexpressing cells had significantly higher basal metabolic activity (p < 0.001) and Sirt3 further enhanced the inducing effect of E2 ( Figure 3A), while ICI effectively abolished E2-induced metabolic activity to control levels in both cell lines.…”

Section: Sirt3 Amplifies E2-induced Metabolic Activity and Mitochondrmentioning

confidence: 99%

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Sirt3 Exerts Its Tumor-Suppressive Role by Increasing p53 and Attenuating Response to Estrogen in MCF-7 Cells

et al. 2020

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Estrogen (E2) is a major risk factor for the initiation and progression of malignancy in estrogen receptor (ER) positive breast cancers, whereas sirtuin 3 (Sirt3), a major mitochondrial NAD+-dependent deacetylase, has the inhibitory effect on the tumorigenic properties of ER positive MCF-7 breast cancer cells. Since it is unclear if this effect is mediated through the estrogen receptor alpha (ERα) signaling pathway, in this study, we aimed to determine if the tumor-suppressive function of Sirt3 in MCF-7 cells interferes with their response to E2. Although we found that Sirt3 improves the antioxidative response and mitochondrial fitness of the MCF-7 cells, it also increases DNA damage along with p53, AIF, and ERα expression. Moreover, Sirt3 desensitizes cells to the proliferative effect of E2, affects p53 by disruption of the ERα–p53 interaction, and decreases proliferation, colony formation, and migration of the cells. Our observations indicate that these tumor-suppressive effects of Sirt3 could be reversed by E2 treatment only to a limited extent which is not sufficient to recover the tumorigenic properties of the MCF-7 cells. This study provides new and interesting insights with respect to the functional role of Sirt3 in the E2-dependent breast cancers.

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Section: Discussionsupporting

confidence: 56%

Section: Sirt3 Amplifies E2-induced Metabolic Activity and Mitochondrmentioning

confidence: 99%

Sirt3 Exerts Its Tumor-Suppressive Role by Increasing p53 and Attenuating Response to Estrogen in MCF-7 Cells

et al. 2020

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“…The fourth Cell passage were used in this study. During passaging, fibroblasts were transported from flask to another flask with trypsenization process using Trypsin EDTA solution aiming to de-adhering cells from the flask (11,12) .…”

Section: Methodsmentioning

confidence: 99%

“…Once the fibroblast cultures were found at 80-90% confluence, they were separated from the flask with trypsin-EDTA. Then 5×10 4 cells were overlaid in 100 µL of culture medium onto insert culture plates and incubated for 5h period at 99F, 6% CO 2 , and 97% humidity (12) . Initially, the complete media was added without material extract, to allow adaptation of the cells to the plate for 24h.…”

Section: Classification Of the Samplementioning

confidence: 99%

“…Then, the plates were incubated inside the biological incubator for 2h at 99F at 97% humidity and 5% CO 2 . During this period, the metabolically active cells bio-reduced MTT salt to formazan (12) . After this period MTT solution was removed from the cells and 100ul of dimethyl sulfoxide solution was added to each group to dissolve the insoluble formazan crystal formed inside the cells.…”

Section: Classification Of the Samplementioning

confidence: 99%

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Cytotoxicity Evaluation of Three Biocompatible and Bioactive Retrofilling Materials Using Periodontal Ligament Stem Cells: An In-Vitro Study

2019

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Purpose: this study aimed to evaluate the biocompatibility of Mineral Trioxide Aggregate (MTA) versus Biodentine and Retro MTA extracts at three observation periods (24h, 48h, and 72h) using MTT-Assay. Materials and Methods: 72 wells in three culture insert plates were used in this study. MTA, Biodentine and Retro MTA cements were evaluated in a fresh state. Passage four of human PDL cells were included in this study. After cells preparation and culturing, an extract of the three tested materials was prepared and cultured with the complete media in addition to 5×10 4 cells were implanted into each well 24h earlier and incubated in a stem cell incubator. MTT Assay was used to evaluate in vitro cytotoxicity, calculated the viable cells by hundred percent using ELISA system and the inverted light microscope used to reassure their confluence. After three different observation periods (24h, 48h, and 72h), evaluation of cell viability was done after exposure to the material extracts. Results: MTA and Biodentine cements showed no statistically significant differences at all the observation periods. However, Retro MTA cement resulted in a statistically significant difference at all the observation periods but none of them below the cut level. Meanwhile, all the materials extracts resulted in a statistically significant increase in cytotoxicity at 24h and then decrease at 48h and finally a little increase in cytotoxicity at 72h. Conclusions: All the tested materials showed low cytotoxicity and are comparable to the old standard MTA.

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Impact of Chemotherapeutic Stress Depends on The Nature of Breast Cancer Spheroid and Induce Behavioral Plasticity to Resistant Population

Gayan,

Teli,

Sonawane

et al. 2023

Advanced Biology

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Cellular or tumor dormancy, identified recently as one of the main reasons behind post‐therapy recurrence, can be caused by diverse reasons. Chemotherapy has recently been recognized as one of such reasons. However, in‐depth studies of chemotherapy‐induced dormancy are lacking due to the absence of an in vitro human‐relevant model tailor‐made for such a scenario. This report utilized multicellular breast cancer spheroid to create a primary platform for establishing a chemotherapy‐induced dormancy model. It is observed that extreme chemotherapeutic stress affects invasive and non‐invasive spheroids differently. Non‐invasive spheroids exhibit more resilience and maintain viability and migrational ability, while invasive spheroids display heightened susceptibility and improved tumorigenic capacity. Heterogenous spheroids exhibit increased tumorigenic capacity while show minimal survival ability. Further probing of chemotherapeutically dormant spheroids is needed to understand the molecular mechanism and identify dormancy‐related markers to achieve therapeutic success in the future.

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Mitochondrial biogenesis and metabolic hyperactivation limits the application of MTT assay in the estimation of radiation induced growth inhibition

Cited by 215 publications

References 39 publications

Sirt3 Exerts Its Tumor-Suppressive Role by Increasing p53 and Attenuating Response to Estrogen in MCF-7 Cells

Sirt3 Exerts Its Tumor-Suppressive Role by Increasing p53 and Attenuating Response to Estrogen in MCF-7 Cells

Cytotoxicity Evaluation of Three Biocompatible and Bioactive Retrofilling Materials Using Periodontal Ligament Stem Cells: An In-Vitro Study

Impact of Chemotherapeutic Stress Depends on The Nature of Breast Cancer Spheroid and Induce Behavioral Plasticity to Resistant Population

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