PMID-sentid	Pub_year	Sent_text		comp_official_name	comp_offsetprotein_name	organism	prot_offset
17222797-0	2007	Small heat shock protein alphaB-crystallin binds to p53 to sequester its translocation to mitochondria during hydrogen peroxide-induced apoptosis.	Hydrogen Peroxide	110-127	transformation related protein 53, pseudogene	Mus musculus	52-55	
17205518-7	2007	Other stressors like H2O2 also mediated a decrease in P53 concentration in p53 defective cells.	Hydrogen Peroxide	21-25	transformation related protein 53, pseudogene	Mus musculus	54-57	
17205518-7	2007	Other stressors like H2O2 also mediated a decrease in P53 concentration in p53 defective cells.	Hydrogen Peroxide	21-25	transformation related protein 53, pseudogene	Mus musculus	75-78	
10660095-3	1999	After exposure to gamma-ionizing radiation or hydrogen peroxide, DNA ladders and labeling of nucelosomal fragments were detected in cells with wild-type p53 gene, but not in p53 null cells or NLS-I deleted cells, suggesting that the NLS-I of p53 protein is necessary for apoptosis.	Hydrogen Peroxide	46-63	transformation related protein 53, pseudogene	Mus musculus	153-156	
10748185-5	2000	Expression of N-JNK in cells that were treated with H(2)O(2) impaired transcriptional output as reflected in a delayed and lower level of c-Jun-, limited ATF2-, and reduced p53-transcriptional activities.	Hydrogen Peroxide	52-60	transformation related protein 53, pseudogene	Mus musculus	173-176	
10748185-6	2000	N-JNK elicited an increase in H(2)O(2)-induced cell death, which is p53-dependent, because it was not seen in p53 null cells yet could be observed upon coexpression of p53 and N-JNK.	Hydrogen Peroxide	30-38	transformation related protein 53, pseudogene	Mus musculus	68-71	
34285767-9	2021	Moreover, under H2O2 and juglone treatment, a large amount of ROS was produced, and phosphorylation of p53 was induced.	Hydrogen Peroxide	16-20	transformation related protein 53, pseudogene	Mus musculus	103-106	
34223980-7	2021	Usp10 inhibition attenuated H2O2-induced senescence in MLO-Y4 cells, as indicated by p53/p21 quantification, a senescence-associated beta-galactosidase (SA-beta-gal) assay, and p53 localization visualization with a confocal microscope.	Hydrogen Peroxide	28-32	transformation related protein 53, pseudogene	Mus musculus	85-88	
34223980-7	2021	Usp10 inhibition attenuated H2O2-induced senescence in MLO-Y4 cells, as indicated by p53/p21 quantification, a senescence-associated beta-galactosidase (SA-beta-gal) assay, and p53 localization visualization with a confocal microscope.	Hydrogen Peroxide	28-32	transformation related protein 53, pseudogene	Mus musculus	177-180	
34679653-6	2021	Sesamol suppressed H2O2-induced expression of phospho-IKKalpha, p53, and caspase-3.	Hydrogen Peroxide	19-23	transformation related protein 53, pseudogene	Mus musculus	64-67	
32943614-6	2020	Furthermore, 4-OI inhibited H2O2-induced programmed necrosis by suppressing mitochondrial depolarization, mitochondrial cyclophilin D-ANT1 (adenine nucleotide translocase 1)-p53 association, and cytosol lactate dehydrogenase release in osteoblasts.	Hydrogen Peroxide	28-32	transformation related protein 53, pseudogene	Mus musculus	174-177	
35123567-15	2022	The HIF1alpha-p53 relationship was negative in YBMSCs and NAC-treated ABMSCs, but positive in ABMSCs and H2O2-treated YBMSCs.	Hydrogen Peroxide	105-109	transformation related protein 53, pseudogene	Mus musculus	14-17	
34026845-10	2021	We found decreased intracellular p53 protein levels under glutamate and hydrogen peroxide treatment in KO cortical cells.	Hydrogen Peroxide	72-89	transformation related protein 53, pseudogene	Mus musculus	33-36	
33475982-0	2021	MicroRNA-125b alleviates hydrogen-peroxide-induced abnormal mitochondrial dynamics in HT22 cells by inhibiting p53.	Hydrogen Peroxide	25-42	transformation related protein 53, pseudogene	Mus musculus	111-114	
33475982-3	2021	Following stimulation with H2O2, we observed downregulation of miR-125b expression, upregulation of p53 expression, mitochondria were damaged and increased cell death.	Hydrogen Peroxide	27-31	transformation related protein 53, pseudogene	Mus musculus	100-103	
33475982-6	2021	Thus, miR-125b alleviates abnormal mitochondrial homeostasis in H2O2-treated HT22 cells by suppressing p53 expression.	Hydrogen Peroxide	64-68	transformation related protein 53, pseudogene	Mus musculus	103-106	
33569547-6	2021	Our findings suggest that H2O2 downregulates P53 by enhancing the P53 suppressor mouse double minute 2 homolog (MDM2), as well as by increasing the apyrimidinic endonuclease 1/redox factor 1 (APE1/Ref1).	Hydrogen Peroxide	26-30	transformation related protein 53, pseudogene	Mus musculus	45-48	
33569547-6	2021	Our findings suggest that H2O2 downregulates P53 by enhancing the P53 suppressor mouse double minute 2 homolog (MDM2), as well as by increasing the apyrimidinic endonuclease 1/redox factor 1 (APE1/Ref1).	Hydrogen Peroxide	26-30	transformation related protein 53, pseudogene	Mus musculus	66-69	
35101250-11	2022	The results demonstrated that EGb protection can effectively diminish H2O2-induced apoptosis by inhibiting p53 acetylation, reducing the ratio of Bax/Bcl-2 and suppressing the expression of specific cleavage of Caspase-9 and Caspase-3.	Hydrogen Peroxide	70-74	transformation related protein 53, pseudogene	Mus musculus	107-110	
28127704-0	2017	Effect of potential role of p53 on embryo development arrest induced by H2O2 in mouse.	Hydrogen Peroxide	72-76	transformation related protein 53, pseudogene	Mus musculus	28-31	
31144365-8	2019	In addition, the phosphorylation of p53, cathepsin B, and Bax/Bcl-2 protein levels, and the translocation of Bax from the cytosol to mitochondria induced by H2 O2 in C2C12 cells was significantly reduced by PTL.	Hydrogen Peroxide	157-162	transformation related protein 53, pseudogene	Mus musculus	36-39	
30693443-4	2019	Our results revealed that sublethal concentrations of hydrogen peroxide (H2O2) exposure initiated a DNA damage response illustrated by increased gammaH2AX and 53BP1 expression and foci formation mainly in sensory hair cells, together with increased levels of p-Chk2 and p53.	Hydrogen Peroxide	54-71	transformation related protein 53, pseudogene	Mus musculus	270-273	
30693443-4	2019	Our results revealed that sublethal concentrations of hydrogen peroxide (H2O2) exposure initiated a DNA damage response illustrated by increased gammaH2AX and 53BP1 expression and foci formation mainly in sensory hair cells, together with increased levels of p-Chk2 and p53.	Hydrogen Peroxide	73-77	transformation related protein 53, pseudogene	Mus musculus	270-273	
28989026-8	2017	Under diabetic oxidative stress or H2O2 stimulation, nuclear beta-catenin accumulation upregulated downstream c-Myc and further facilitated DNA damage and p53-mediated apoptosis as well as cell viability reduction, followed by phenotypic changes of cardiac dysfunction, interstitial fibrosis deposition and myocardial atrophy.	Hydrogen Peroxide	35-39	transformation related protein 53, pseudogene	Mus musculus	155-158	
28237267-8	2017	Expressions of endothelial nitric oxide synthase and silent information regulator protein 1 (SIRT1) were significantly up-regulated but those of P53 and P21 were markedly down-regulated both in aged mice and in hydrogen peroxide-treated MAECs in the absence of the TRPC5 gene.	Hydrogen Peroxide	211-228	transformation related protein 53, pseudogene	Mus musculus	145-148	
26703444-3	2016	In the present study we observed that H2O2 induces the mitochondrial permeability transition pore (mPTP) opening and exerts p53 activation in a time-dependent way, with a maximum response after 1-2h of treatment.	Hydrogen Peroxide	38-42	transformation related protein 53, pseudogene	Mus musculus	124-127	
27249370-4	2017	We report that E2 protects skeletal myoblasts against apoptosis induced by H2 O2 modulating p53 and FoxO transcription factors and then their target genes Bcl-2, Bim, Puma, PERP, and MDM2, without affecting Noxa gene.	Hydrogen Peroxide	75-80	transformation related protein 53, pseudogene	Mus musculus	92-95	
22348305-3	2012	We found that the Bach1-p53 interaction was inhibited by oncogenic Ras, bleomycin, and hydrogen peroxide.	Hydrogen Peroxide	87-104	transformation related protein 53, pseudogene	Mus musculus	24-27	
26406155-7	2015	And the chemical activation of Sirt 1 inhibited the H2O2-induced apoptosis via the downregulation of p53 acetylation.	Hydrogen Peroxide	52-56	transformation related protein 53, pseudogene	Mus musculus	101-104	
25242411-7	2014	Moreover, the proanthocyanidins inhibit H2O2-induced apoptosis signaling which is mediated by p53.	Hydrogen Peroxide	40-44	transformation related protein 53, pseudogene	Mus musculus	94-97	
24067374-5	2013	Furthermore, p53-dependent induction of Tpt1 was able to reduce oxidative stress, minimize apoptosis, and promote cell survival in response to H 2O2 challenge.	Hydrogen Peroxide	143-148	transformation related protein 53, pseudogene	Mus musculus	13-16	
23533505-8	2013	These observations imply that gallic acid-mediated hydrogen peroxide formation acts as an initiator of JNK signaling pathways, leading to p53 activation and apoptosis in mouse lung fibroblasts.	Hydrogen Peroxide	51-68	transformation related protein 53, pseudogene	Mus musculus	138-141	
25535325-5	2015	For this effect, H2O2 upregulated levels of p14, increased ubiquitin-dependent degradation of mouse double minute 2 (MDM2), and reduced the interaction between MDM2 and p53 to prevent p53 degradation, resulting in accumulation of p53 and subsequent activation of p53-dependent apoptotic pathways.	Hydrogen Peroxide	17-21	transformation related protein 53, pseudogene	Mus musculus	169-172	
25535325-5	2015	For this effect, H2O2 upregulated levels of p14, increased ubiquitin-dependent degradation of mouse double minute 2 (MDM2), and reduced the interaction between MDM2 and p53 to prevent p53 degradation, resulting in accumulation of p53 and subsequent activation of p53-dependent apoptotic pathways.	Hydrogen Peroxide	17-21	transformation related protein 53, pseudogene	Mus musculus	184-187	
25535325-5	2015	For this effect, H2O2 upregulated levels of p14, increased ubiquitin-dependent degradation of mouse double minute 2 (MDM2), and reduced the interaction between MDM2 and p53 to prevent p53 degradation, resulting in accumulation of p53 and subsequent activation of p53-dependent apoptotic pathways.	Hydrogen Peroxide	17-21	transformation related protein 53, pseudogene	Mus musculus	184-187	
25535325-5	2015	For this effect, H2O2 upregulated levels of p14, increased ubiquitin-dependent degradation of mouse double minute 2 (MDM2), and reduced the interaction between MDM2 and p53 to prevent p53 degradation, resulting in accumulation of p53 and subsequent activation of p53-dependent apoptotic pathways.	Hydrogen Peroxide	17-21	transformation related protein 53, pseudogene	Mus musculus	184-187	
25535325-6	2015	Interestingly, HCV core repressed p14 expression via promoter hypermethylation to abolish the potential of H2O2 to activate the p14-MDM2-p53 pathway.	Hydrogen Peroxide	107-111	transformation related protein 53, pseudogene	Mus musculus	137-140	
25535325-7	2015	As a consequence, HCV core-expressing cells could overcome p53-mediated apoptosis provoked by H2O2.	Hydrogen Peroxide	94-98	transformation related protein 53, pseudogene	Mus musculus	59-62	
26406155-4	2015	Results demonstrated that Sirt 1 and Bcl-2 were inhibited, whereas p53 acetylation, Bax, and caspase 9 were promoted by H2O2, as was aggravated by the Sirt 1 inhibitor, EX-527.	Hydrogen Peroxide	120-124	transformation related protein 53, pseudogene	Mus musculus	67-70	
26406155-5	2015	Instead, RSV inhibited the H2O2-induced both p53 acetylation and the caspase 9 activation, whereas ameliorated the H2O2-induced Bcl-2 inhibition and apoptosis.	Hydrogen Peroxide	27-31	transformation related protein 53, pseudogene	Mus musculus	45-48	
22922974-11	2012	Phosphorylated p53 protein was increased in MGFs subsequent to treatment with 20 microM H2O2, along with an upregulated transcription of p21 and Mdm2 mRNAs.	Hydrogen Peroxide	88-92	transformation related protein 53, pseudogene	Mus musculus	15-18	
20136445-0	2010	Effects of various polyphenolics on hydrogen peroxide-induced p53 activity in NIH3T3 cells.	Hydrogen Peroxide	36-53	transformation related protein 53, pseudogene	Mus musculus	62-65	
21527937-8	2011	The mechanism of H(2)O(2)-mediated miR-200c upregulation involves p53 and retinoblastoma proteins.	Hydrogen Peroxide	17-25	transformation related protein 53, pseudogene	Mus musculus	66-69	
21654327-2	2011	In cultured endothelial cells, 2 atherogenic stimuli, hydrogen peroxide and tumor necrosis factor-alpha, increased the acetylation of p53 lysine-382, and caspase-3 cleavage, an indicator of apoptotic signaling.	Hydrogen Peroxide	54-71	transformation related protein 53, pseudogene	Mus musculus	134-137	
21211512-6	2011	In addition, we show that ovarian carcinoma A2780 cells with Nrf2 shRNA expression displayed higher levels of p53 activation in response to hydrogen peroxide treatment, leading to increased cell death.	Hydrogen Peroxide	140-157	transformation related protein 53, pseudogene	Mus musculus	110-113	
21799252-2	2011	We found that APO treatment ameliorated oxidative stress in an AD mouse model and specifically attenuated the hydrogen peroxide-induced p53-related apoptosis in the SH-SY5Y neuroblastoma cell line.	Hydrogen Peroxide	110-127	transformation related protein 53, pseudogene	Mus musculus	136-139	
20136445-1	2010	A cell-based assay system was developed to evaluate the potential antioxidant and pro-oxidant effects of various dietary polyphenolic compounds based on the induction of p53 activity by hydrogen peroxide.	Hydrogen Peroxide	186-203	transformation related protein 53, pseudogene	Mus musculus	170-173	
19887573-0	2010	Cadmium induces intracellular Ca2+- and H2O2-dependent apoptosis through JNK- and p53-mediated pathways in skin epidermal cell line.	Hydrogen Peroxide	40-44	transformation related protein 53, pseudogene	Mus musculus	82-85	
18753379-10	2008	In organotypic forebrain slice cultures treated with hydrogen peroxide, p53 is accumulated and colocalized with necdin and Sirt1 in cortical neurons.	Hydrogen Peroxide	53-70	transformation related protein 53, pseudogene	Mus musculus	72-75