p73 coordinates with Δ133p53 to promote DNA double-strand break repair

Gong, Hongjian; Zhang, Yuxi; Jiang, Kunpeng; Ye, Shengfan; Chen, Shuming; Zhang, Qinghe; Peng, Jinrong; Chen, Jun

doi:10.1038/s41418-018-0085-8

Cited by 59 publications

(66 citation statements)

References 58 publications

(65 reference statements)

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“…In the present study, we report that the AMPK‐Mfn1 pathway is closely regulated by resveratrol . This finding provides an easy and effective approach to activate protective the AMPK‐Mfn1 pathway in the setting of cerebral IR injury …”

Section: Discussionsupporting

confidence: 63%

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Resveratrol attenuates cerebral ischaemia reperfusion injury via modulating mitochondrial dynamics homeostasis and activating AMPK‐Mfn1 pathway

Gao

Wang

et al. 2019

Int J Experimental Path

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Summary The pathogenesis of cerebral ischaemia reperfusion injury (IRI) has not been fully described. Accordingly, there is little effective drug available for the treatment of cerebral IRI. The aim of our study was to explore the exact role played by Mfn1‐mediated mitochondrial protection in cerebral IRI and evaluate the beneficial action of resveratrol on reperfused brain. Our study demonstrated that hypoxia‐reoxygenation (HR) injury caused N2a cell apoptosis and this process was highly affected by mitochondrial dysfunction. Decreased mitochondrial membrane potential, increased mitochondrial oxidative stress, and an activated mitochondrial apoptosis pathway were noted in HR‐treated N2a cells. Interestingly, resveratrol treatment could attenuate N2a cell apoptosis via sustaining mitochondrial homeostasis. Further, we found that resveratrol modulated mitochondrial performance via activating the Mfn1‐related mitochondrial protective system. Knockdown of Mfn1 could abolish the beneficial effects of resveratrol on HR‐treated N2a cells. Besides, we also report that resveratrol regulated Mfn1 expression via the AMPK pathway; inhibition of AMPK pathway also neutralized the anti‐apoptotic effect of resveratrol on N2a cells in the setting of cerebral IRI. Taken together our results show that mitochondrial damage is closely associated with the progression of cerebral IRI. In addition we also demonstrate the protective action played by resveratrol on reperfused brain and show that this effect is achieved via activating the AMPK‐Mfn1 pathway.

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Section: Discussionsupporting

confidence: 63%

“…74,75 This finding provides an easy and effective approach to activate protective the AMPK-Mfn1 pathway in the setting of cerebral IR injury. 76…”

Section: Discussionmentioning

confidence: 99%

Resveratrol attenuates cerebral ischaemia reperfusion injury via modulating mitochondrial dynamics homeostasis and activating AMPK‐Mfn1 pathway

Gao

Wang

et al. 2019

Int J Experimental Path

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“…Δ133p53 works together with the p53 gene family member p73 to join the promoters of all three repair genes Ligase4, Rad51, and Impact of Δ133p53 on the chemosensitivity K. Liu and J. Lin Rad52. Δ133p53, which cooperates with p73, acts synergistically to promote the expression of Rad51, Rad52, and Ligase4 and the repair of damaged DNA in various cancer cells Gong et al, , 2018. In this study, Δ133p53 reduced the sensitivity of H1299 to the chemotherapeutic drugs, due to which DNA of the cell line H1299 was injured.…”

Section: Discussionmentioning

confidence: 57%

“…Δ133p53 works together with the p53 gene family member p73 to join the promoters of all three repair genes Ligase4, Rad51, and Rad52. Δ133p53, which cooperates with p73, acts synergistically to promote the expression of Rad51, Rad52, and Ligase4 and the repair of damaged DNA in various cancer cells (Gong and Chen, ; Gong et al, , ).…”

Section: Discussionmentioning

confidence: 99%

Δ133p53 decreases the chemosensitivity of carcinoma cell line H1299

Liu

Lin

2019

Cell Biology International

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The research evaluated the effect of Δ133p53 on the chemosensitivity of lung adenocarcinoma cell line H1299. By this study, the drug‐resistant molecular marker and a new target for cancer therapy could be provided. Δ133p53 or negative control plasmid were transferred into H1299 cells by lentivirus vector. The expression of Δ133p53 in transfected cells was examined using immunofluorescence. The 3‐(4,5‐dimethylthiazol‐2‐yl)‐2,5‐diphenyl tetrazolium bromide (MTT) method and colony formation test were applied to detect drug sensitivity after cisplatin or 5‐fluorouracil (5‐FU) treatment. After cisplatin (CDDP)/FU treatment, MTT assay demonstrated that the inhibition rate of H1299/Δ133p53 cell was reduced compared with that of the H1299 and H1299/NEG cells at the same concentration of drug. The 50% inhibitory concentrations (IC 50) of CDDP and 5‐FU rose by 36.1 and 30.2%, respectively (P < 0.05). The colony formation assay suggested that the cell proliferation ability of H1299/Δ133p53 cell was prominently increased when compared with that of control group H1299 and H1299 /NEG cells (P < 0.05). The present study demonstrated that the transfection of the Δ133p53 gene in H1299 cells led to the reduction of chemosensitivity.

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“…Gong et al (74) found that D133p53 binds to DNp63 and utilizes its TA domain to promote glycolytic metabolism, leading to cancer cell proliferation. Additionally, p73 and D133p53 act synergistically to promote the expression of RAD51, LIG4, and RAD52 by binding to a region containing a D133p53-responsive element and a p73-responsive element in the promoters of all 3 DNA double-strand break repair genes (75). Figure 9.…”

Section: Discussionmentioning

confidence: 99%

Conformational stability and dynamics of the cancer‐associated isoform Δ133p53β are modulated by p53 peptides and p53‐specific DNA

Lei

Tang

et al. 2018

FASEB j.

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p53 is a tumor suppressor protein that maintains genome stability, but its Δ133p53β and Δ160p53β isoforms promote breast cancer cell invasion. The sequence truncations in the p53 core domain raise key questions related to their physicochemical properties, including structural stabilities, interaction mechanisms, and DNA‐binding abilities. Herein, we investigated the conformational dynamics of Δ133p53β and Δ160p53β with and without binding to p53‐specific DNA by using molecular dynamics simulations. We observed that the core domains of the 2 truncated isoforms are much less stable than wild‐type (wt) p53β, and the increased solvent exposure of their aggregation‐triggering segment indicates their higher aggregation propensities than wt p53. We also found that Δ133p53β stability is modulable by peptide or DNA interactions. Adding a p53 peptide (derived from truncated p53 sequence 107–129) may help stabilize Δ133p53. Most importantly, our simulations of p53 isomer‐DNA complexes indicate that Δ133p53β dimer, but not Δ160p53β dimer, could form a stable complex with p53‐specific DNA, which is consistent with recent experiments. This study provides physicochemical insight into Δ133p53β, Δ133p53β‐DNA complexes, Δ133p53β's pathologic mechanism, and peptide‐based inhibitor design against p53‐related cancers.— Lei, J., Qi, R., Tang, Y., Wang, W., Wei, G., Nussinov, R., Ma, B. Conformational stability and dynamics of the cancer‐associated isoform Δ133p53β are modulated by p53 peptides and p53‐specific DNA. FASEB J. 33, 4225–4235 (2019). http://www.fasebj.org

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p73 coordinates with Δ133p53 to promote DNA double-strand break repair

Cited by 59 publications

References 58 publications

Resveratrol attenuates cerebral ischaemia reperfusion injury via modulating mitochondrial dynamics homeostasis and activating AMPK‐Mfn1 pathway

Resveratrol attenuates cerebral ischaemia reperfusion injury via modulating mitochondrial dynamics homeostasis and activating AMPK‐Mfn1 pathway

Δ133p53 decreases the chemosensitivity of carcinoma cell line H1299

Conformational stability and dynamics of the cancer‐associated isoform Δ133p53β are modulated by p53 peptides and p53‐specific DNA

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