PMID-sentid	Pub_year	Sent_text		comp_official_name	comp_offsetprotein_name	organism	prot_offset
22246639-0	2012	Caspase-3 feeds back on caspase-8, Bid and XIAP in type I Fas signaling in primary mouse hepatocytes.	ammonium ferrous sulfate	58-61	caspase 3	Mus musculus	0-9	
25015658-10	2014	Overall, the results indicate that Fas-initiated, caspase-3-dependent HPC apoptosis increases TF procoagulant activity through a mechanism involving PS externalization.	ammonium ferrous sulfate	35-38	caspase 3	Mus musculus	50-59	
24928990-7	2014	The rate of caspase 3/7 biosensor activation was unexpectedly rapid following granzyme B- compared with Fas-mediated signal induction in murine CTLs; the latter appeared gradually after a 90-min delay in perforin- or granzyme B-deficient CTLs.	ammonium ferrous sulfate	104-107	caspase 3	Mus musculus	12-21	
21470397-9	2011	Smaller increases of several apoptosis markers, such as caspase-3 and -8, were demonstrated in Fas-deficient mice, even though the bacterial burdens in Fas-deficient and wild type mice were similar.	ammonium ferrous sulfate	95-98	caspase 3	Mus musculus	56-72	
16420519-12	2006	CONCLUSION: Fas may rely on both caspase-8 activation (extrinsic pathway) and mitochondria (intrinsic pathway) to activate caspase-3.	ammonium ferrous sulfate	12-15	caspase 3	Mus musculus	123-132	
17182568-8	2007	In the absence of PKC-theta, Fas-induced activation of apoptotic molecules such as caspase-8, caspase-3, and Bid was not efficient.	ammonium ferrous sulfate	29-32	caspase 3	Mus musculus	94-103	
16621521-12	2006	However, estradiol enhanced caspase-3 activity in Fas-induced apoptosis on mature osteoclasts, suggesting that this might interact with the Fas-signaling pathway.	ammonium ferrous sulfate	50-53	caspase 3	Mus musculus	28-37	
19120440-7	2009	The neutralization of Fas ligand (FasL) protected against traumatically induced or Fas-mediated caspase-3 activation and the loss of mitochondrial membrane potential and tBid expression in wild-type spinal cord cultures.	ammonium ferrous sulfate	22-25	caspase 3	Mus musculus	96-105	
15300908-8	2004	Fas expression in hepatocytes transfected with anti-Fas ribozyme was decreased remarkably and correlated with the resistance to Fas-mediated apoptosis as determined by flow cytometry and caspase-3 proteolytic activity.	ammonium ferrous sulfate	0-3	caspase 3	Mus musculus	187-196	
15300908-8	2004	Fas expression in hepatocytes transfected with anti-Fas ribozyme was decreased remarkably and correlated with the resistance to Fas-mediated apoptosis as determined by flow cytometry and caspase-3 proteolytic activity.	ammonium ferrous sulfate	52-55	caspase 3	Mus musculus	187-196	
15202504-6	2004	Fas expression in Yac-1 cells transfected with anti-Fas ribozyme was decreased remarkably and correlated with resistance to Fas-mediated apoptosis as determined by flow cytometry and caspase-3 proteolytic activity.	ammonium ferrous sulfate	0-3	caspase 3	Mus musculus	183-192	
12802593-16	2003	Caspase-3 was also observed in numerous Fas-positive cells in heavily infiltrated islets.	ammonium ferrous sulfate	40-43	caspase 3	Mus musculus	0-9	
11559023-9	2001	We conclude that Fas may rely exclusively on caspase-8 activation and mitochondria to activate caspase-3, which can process more procaspase-8 and thus propagate the amplification of the apoptotic signal.	ammonium ferrous sulfate	17-20	caspase 3	Mus musculus	95-104	
12657159-0	2003	Prostaglandin F2alpha- and FAS-activating antibody-induced regression of the corpus luteum involves caspase-8 and is defective in caspase-3 deficient mice.	ammonium ferrous sulfate	27-30	caspase 3	Mus musculus	130-139	
11821950-6	2002	Furthermore, cytochrome c release from mitochondria and caspase 3 activation were restored to normal levels in HBx/Bcl-2 mice during transduction of the Fas signal.	ammonium ferrous sulfate	153-156	caspase 3	Mus musculus	56-65	
11749068-3	2002	Here we show that LEC treated with Fas agonist (Jo2 mAb at 0.1 microg/ml) and TNF had a greater caspase-3 activity (twofold increase) than cells treated with each factor alone.	ammonium ferrous sulfate	35-38	caspase 3	Mus musculus	96-105	
11276016-6	2001	In conclusion, the typical apoptotic ultrastructure and DNA fragmentation occur simultaneously in association with caspase-3 activation in Fas-stimulated cultured cardiomyocytes.	ammonium ferrous sulfate	139-142	caspase 3	Mus musculus	115-124	
10811232-7	2000	Inhibition of de novo Fas expression in betaTC-3 cells expressing the anti-Fas ribozyme correlated with resistance to Fas-mediated apoptosis as determined by the number of cells exhibiting caspase 3 proteolytic activity.	ammonium ferrous sulfate	22-25	caspase 3	Mus musculus	189-198	
11174076-0	2001	Effects of a novel hepatoprotective drug, ZNC-2381, on fas-induced hepatocellular caspase-3 activity and apoptosis in mice.	ammonium ferrous sulfate	55-58	caspase 3	Mus musculus	82-91	
9521092-0	1998	The dominant role of CPP32 subfamily in fas-mediated hepatitis.	ammonium ferrous sulfate	40-43	caspase 3	Mus musculus	21-26	
10078546-5	1999	The cross-linking of Fas by anti-Fas resulted in the elevation of caspase-3-like, but not caspase-1-like, protease activity 2-12 h after the addition of the anti-Fas.	ammonium ferrous sulfate	21-24	caspase 3	Mus musculus	66-75	
10078546-5	1999	The cross-linking of Fas by anti-Fas resulted in the elevation of caspase-3-like, but not caspase-1-like, protease activity 2-12 h after the addition of the anti-Fas.	ammonium ferrous sulfate	33-36	caspase 3	Mus musculus	66-75	
10078546-6	1999	A caspase-3 inhibitor, Z-Asp-Glu-Val-Asp-fluoromethyl ketone, attenuated the Fas-mediated beta-cell apoptosis, while a caspase-1 inhibitor, acetyl-Tyr-Val-Ala-Asp-chloromethylketone, failed to suppress the apoptosis.	ammonium ferrous sulfate	77-80	caspase 3	Mus musculus	2-11	
10078546-9	1999	These observations suggest the essential role of caspase-3 in Fas-mediated apoptosis of the beta-cell line.	ammonium ferrous sulfate	62-65	caspase 3	Mus musculus	49-58	
10528193-0	1999	In vivo evidence that caspase-3 is required for Fas-mediated apoptosis of hepatocytes.	ammonium ferrous sulfate	48-51	caspase 3	Mus musculus	22-31	
10528193-1	1999	Caspase-3 is essential for Fas-mediated apoptosis in vitro.	ammonium ferrous sulfate	27-30	caspase 3	Mus musculus	0-9	
10464143-9	1999	CONCLUSIONS: These results suggest that IL-1beta suppresses Fas-mediated hepatocyte apoptosis by inducing molecule(s) that suppress the apoptosis control machinery upstream of caspase 3.	ammonium ferrous sulfate	60-63	caspase 3	Mus musculus	176-185	
10551900-7	1999	Both compounds inhibited caspases 1, 2, 3, 6, 8, and 9, and both afforded comparable reduction in Fas- and LPS-induced caspase 3-like activity and apoptosis.	ammonium ferrous sulfate	98-101	caspase 3	Mus musculus	119-128	
9811849-0	1998	Caspase-3 controls both cytoplasmic and nuclear events associated with Fas-mediated apoptosis in vivo.	ammonium ferrous sulfate	71-74	caspase 3	Mus musculus	0-9	
9811849-2	1998	However, the role of caspase-1 and caspase-3 in mediating Fas-induced cell death is not clear.	ammonium ferrous sulfate	58-61	caspase 3	Mus musculus	35-44	
9556551-0	1998	Different subcellular distribution of caspase-3 and caspase-7 following Fas-induced apoptosis in mouse liver.	ammonium ferrous sulfate	72-75	caspase 3	Mus musculus	38-47	
9521092-9	1998	We propose here that the CPP32 subfamily plays the dominant role in Fas-mediated hepatitis, and DEVD-CHO would be an effective cure for hepatitis.	ammonium ferrous sulfate	68-71	caspase 3	Mus musculus	25-30	
9036942-9	1997	These results suggest that granzyme B- and Fas-based cytotoxicity exerted by CTL clones converge at the level of CPP32-like protease activation, while granzyme A acts via a different, still undefined, pathway.	ammonium ferrous sulfate	43-46	caspase 3	Mus musculus	113-118	
8920897-0	1996	Systemic injection of a tripeptide inhibits the intracellular activation of CPP32-like proteases in vivo and fully protects mice against Fas-mediated fulminant liver destruction and death.	ammonium ferrous sulfate	137-140	caspase 3	Mus musculus	76-81	
31010354-9	2019	Upon Fas-SiRNA injection, almost all measured parameters of NASH such as overexpression of Fas receptor, caspase3, NF-kB genes and marked increase of hepatic TNF-alpha were significantly restored and were remained nearly unchanged following recovery liking as scrambled groups.	ammonium ferrous sulfate	5-8	caspase 3	Mus musculus	105-113	
8614469-4	1996	We show here that specific inhibitors of ICE- or CPP32-like proteases can inhibit Fas-mediated apoptosis.	ammonium ferrous sulfate	82-85	caspase 3	Mus musculus	49-54	
8614469-9	1996	These results indicate that Fas sequentially activates ICE- and CPP32-like proteases, and that downstream CPP32, together with a component(s) in the cytoplasm, causes apoptosis of nuclei.	ammonium ferrous sulfate	28-31	caspase 3	Mus musculus	64-69