PMID-sentid	Pub_year	Sent_text		comp_official_name	comp_offsetprotein_name	organism	prot_offset
24635079-8	2014	ATRA also induced G1 cell-cycle arrest, inhibited the expression of cyclin D1/cyclin-dependent kinase (CDK)4 and cyclinE/CDK2, and increased the expression of the cyclin-dependent kinase inhibitors p21 and p27.	Tretinoin	0-4	interferon alpha inducible protein 27	Homo sapiens	206-209	
24646031-3	2014	In many cases, downregulation of CDK activity by ATRA and vitamin D3 is a result of elevated p21- and p27-bound CDKs.	Tretinoin	49-53	interferon alpha inducible protein 27	Homo sapiens	102-105	
28656276-7	2017	Further investigations indicated that with ATRA-induced expression of RIG-I, levels of phosphorylated (p)AKT-Thr308 and pForkhead Box (FOX) O3A-Thr32 were decreased, the expression levels of cell cycle arrest protein p27 and the apoptotic protein, tumor necrosis factor-related apoptosis-inducing ligand (TRAIL), directly transcribed by FOXO3A were increased.	Tretinoin	43-47	interferon alpha inducible protein 27	Homo sapiens	217-220	
28656276-8	2017	By contrast, following the knockdown of ATRA-induced expression of RIG-I, the levels of pAKT-Thr308 and pFOXO3A-Thr32 were increased, and the protein expression levels of p27 and TRAIL were decreased.	Tretinoin	40-44	interferon alpha inducible protein 27	Homo sapiens	171-174	
24851929-4	2014	The purpose of this study is to examine whether Cdk5 is involved in ATRA-induced growth arrest of the castration-resistant cancer cell line DU145 through up-regulating Cdk inhibitor protein, p27.	Tretinoin	68-72	interferon alpha inducible protein 27	Homo sapiens	191-194	
25520935-5	2014	Also, the common cell cycle inhibiting protein, p27, and the new cell cycle regulator, Cdk5, are involved in retinoic acid"s effects.	Tretinoin	109-122	interferon alpha inducible protein 27	Homo sapiens	48-51	
24851929-7	2014	RESULTS: ATRA treatment inhibited DU145 cell proliferation and significantly increased p27 expression through Cdk5 up-regulation.	Tretinoin	9-13	interferon alpha inducible protein 27	Homo sapiens	87-90	
24851929-8	2014	Immunocytochemical data showed that a Cdk5 inhibitor reduced ATRA-triggered nuclear distribution of p27 in DU145 cells.	Tretinoin	61-65	interferon alpha inducible protein 27	Homo sapiens	100-103	
24851929-10	2014	CONCLUSIONS: Our results demonstrate that ATRA induced growth inhibition in castration-resistant prostate cancer cells through activating Cdk5 and p27.	Tretinoin	42-46	interferon alpha inducible protein 27	Homo sapiens	147-150	
23489885-8	2013	Furthermore, Retinoic acid (RA) treatment confirmed the expression of the multipotent differentiation markers in the SP cells, including TUJ1, pancytokeratin, glial fibrillary acidic protein (GFAP), and p27(Kip1).	Tretinoin	13-26	interferon alpha inducible protein 27	Homo sapiens	203-206	
23489885-8	2013	Furthermore, Retinoic acid (RA) treatment confirmed the expression of the multipotent differentiation markers in the SP cells, including TUJ1, pancytokeratin, glial fibrillary acidic protein (GFAP), and p27(Kip1).	Tretinoin	28-30	interferon alpha inducible protein 27	Homo sapiens	203-206	
15492811-0	2004	Expression of p27 and MAPK proteins involved in all-trans retinoic acid-induced apoptosis and cell cycle arrest in matched primary and metastatic melanoma cells.	Tretinoin	58-71	interferon alpha inducible protein 27	Homo sapiens	14-17	
23518499-6	2013	CDK1 modulates the levels of P27(kip) and AKT phosphorylation in response to ATRA treatment.	Tretinoin	77-81	interferon alpha inducible protein 27	Homo sapiens	29-37	
21383690-4	2011	RA treatment rapidly induced morphology changes, induced growth arrest at G1/G0 to S transition, decreased cyclin D1 expression and increased p27 expression.	Tretinoin	0-2	interferon alpha inducible protein 27	Homo sapiens	142-145	
20170512-6	2010	1) The evidence indicated that 4-hydroxytamoxifen, dexamethasone, and various retinoic acids up-regulated expression of p27 in both estrogen receptor-positive and negative human breast cancer cells in vitro.	Tretinoin	78-92	interferon alpha inducible protein 27	Homo sapiens	120-123	
20170512-11	2010	Retinoic acids up-regulated expression of p27 without using either 4E-BP1 or RTKs/PI3K/Akt/AMPK/mTOR protein kinase signaling pathways.	Tretinoin	0-14	interferon alpha inducible protein 27	Homo sapiens	42-45	
20170512-13	2010	Retinoic acids also up-regulated translation initiation of p27, but without using any of these pathways.	Tretinoin	0-14	interferon alpha inducible protein 27	Homo sapiens	59-62	
20193324-11	2009	The expression of p27(Kip1) and p21(Waf1) in myeloma cells was up-regulated by RGZ and this change was more apparent when RGZ was used in combination with ATRA.	Tretinoin	155-159	interferon alpha inducible protein 27	Homo sapiens	18-21	
19035179-6	2008	Western blot displayed that ATRA could decrease the expression of cyclin A, up-regulate the expression of p21 and p27, and down-regulate the expression of p27 related proteins Skp2.	Tretinoin	28-32	interferon alpha inducible protein 27	Homo sapiens	114-117	
19035179-6	2008	Western blot displayed that ATRA could decrease the expression of cyclin A, up-regulate the expression of p21 and p27, and down-regulate the expression of p27 related proteins Skp2.	Tretinoin	28-32	interferon alpha inducible protein 27	Homo sapiens	155-158	
16752155-3	2007	RA treatment resulted in an increase of p21, p27 and p53 protein levels and G1 arrest in UM cells, which correlated with significant down-modulation of surface Her2/neu proto-oncogene expression.	Tretinoin	0-2	interferon alpha inducible protein 27	Homo sapiens	45-48	
15695403-3	2005	RA induces cell accumulation in G(0)-G(1) together with a marked up-regulation of p27(Kip1) by inhibiting ubiquitination and proteasome-dependent degradation of the protein.	Tretinoin	0-2	interferon alpha inducible protein 27	Homo sapiens	82-85	
15695403-5	2005	Most of RA-induced p27(Kip1) was bound to cyclin D1/cyclin-dependent kinase 4 complexes, probably contributing to the decreased cyclin-dependent kinase 4 kinase activity and pRb hypophosphorylation observed in RA-treated cells.	Tretinoin	8-10	interferon alpha inducible protein 27	Homo sapiens	19-22	
15695403-5	2005	Most of RA-induced p27(Kip1) was bound to cyclin D1/cyclin-dependent kinase 4 complexes, probably contributing to the decreased cyclin-dependent kinase 4 kinase activity and pRb hypophosphorylation observed in RA-treated cells.	Tretinoin	210-212	interferon alpha inducible protein 27	Homo sapiens	19-22	
15492811-1	2004	We investigated whether p27 and mitogen-activated protein kinase (MAPK) proteins were involved in all-trans retinoic acid (atRA)-induced apoptosis and cell cycle arrest.	Tretinoin	108-121	interferon alpha inducible protein 27	Homo sapiens	24-27	
15492811-1	2004	We investigated whether p27 and mitogen-activated protein kinase (MAPK) proteins were involved in all-trans retinoic acid (atRA)-induced apoptosis and cell cycle arrest.	Tretinoin	123-127	interferon alpha inducible protein 27	Homo sapiens	24-27	
15492811-9	2004	These data indicate that up-regulation of p27 and down-regulation of MAPK proteins were involved in atRA-induced apoptosis and cell cycle arrest in melanoma.	Tretinoin	100-104	interferon alpha inducible protein 27	Homo sapiens	42-45	
12955881-4	2003	We demonstrate that RA induces growth arrest and differentiation in HepG2 cells by influencing the activities of cyclin-cdk complexes involved in the regulation of G1/S transition and S-phase progression, in particular by modifying the binding of these complexes to p21 and p27 inhibitors.	Tretinoin	20-22	interferon alpha inducible protein 27	Homo sapiens	274-277	
15256728-3	2004	The expression of p21 and p27 among the CDK inhibitors we examined increased during the differentiation induced with ATRA.	Tretinoin	117-121	interferon alpha inducible protein 27	Homo sapiens	26-29	
15256728-6	2004	These results suggest that increased expression of CDK inhibitors, p21 and p27, is necessary for the differentiation of HL-60 cells induced with ATRA.	Tretinoin	145-149	interferon alpha inducible protein 27	Homo sapiens	75-78	
14980522-0	2004	Retinoic acid causes cell growth arrest and an increase in p27 in F9 wild type but not in F9 retinoic acid receptor beta2 knockout cells.	Tretinoin	0-13	interferon alpha inducible protein 27	Homo sapiens	59-62	
14980522-5	2004	In F9 Wt cells, cyclin D1, D3, and cyclin E protein levels decreased, while cyclin D2 and p27 levels increased after RA treatment.	Tretinoin	117-119	interferon alpha inducible protein 27	Homo sapiens	90-93	
14980522-9	2004	Moreover, RA increased the half-life of p27 protein in F9 Wt cells.	Tretinoin	10-12	interferon alpha inducible protein 27	Homo sapiens	40-43	
14980522-11	2004	Using both genetic and molecular approaches, we have identified some of the molecular mechanisms, such as the large elevation of p27, through which RARbeta(2) mediates these growth inhibitory effects of RA in F9 cells.	Tretinoin	148-150	interferon alpha inducible protein 27	Homo sapiens	129-132	
11877298-0	2002	Retinoic acid-induced cell cycle arrest of human myeloid cell lines is associated with sequential down-regulation of c-Myc and cyclin E and posttranscriptional up-regulation of p27(Kip1).	Tretinoin	0-13	interferon alpha inducible protein 27	Homo sapiens	177-180	
12421932-5	2002	The presence of atRA led to elevated levels of cyclin D3, -E, and -A, decreased levels of p27(Kip1), increased activity of cyclin-dependent kinase 2, and enhanced phosphorylation of the retinoblastoma protein (pRB).	Tretinoin	16-20	interferon alpha inducible protein 27	Homo sapiens	90-93	
12186376-4	2002	The cell lines (MCF-7, T-47D, ZR-75-1), which expressed both BRCA1 and p27, were extremely sensitive to the inhibitory effect of the combination of TGZ and either ATRA or 9-cis-RA (ED90, 2-5 x 10(-11) M).	Tretinoin	163-167	interferon alpha inducible protein 27	Homo sapiens	71-74	
12186376-4	2002	The cell lines (MCF-7, T-47D, ZR-75-1), which expressed both BRCA1 and p27, were extremely sensitive to the inhibitory effect of the combination of TGZ and either ATRA or 9-cis-RA (ED90, 2-5 x 10(-11) M).	Tretinoin	171-179	interferon alpha inducible protein 27	Homo sapiens	71-74	
12012012-7	2002	Our results indicate that ATRA-pretreatment modified the CDDP-induced regulation of CDK2 activity by the CDK inhibitors p21 and p27.	Tretinoin	26-30	interferon alpha inducible protein 27	Homo sapiens	128-131	
11877298-8	2002	These results thus identify a decrease in c-Myc and cyclin E levels and a posttranscriptional up-regulation of p27(Kip1) as important early changes, and position them in the complex chain of events regulating ATRA-induced cell cycle arrest of myeloid cells.	Tretinoin	209-213	interferon alpha inducible protein 27	Homo sapiens	111-114	
11595732-4	2001	We found a striking difference between these cells in that while ATRA induces an elevation in the cdk inhibitor p27 in T-47D cells, this is not observed in the ATRA-resistant MCF-7 cells.	Tretinoin	65-69	interferon alpha inducible protein 27	Homo sapiens	112-115	
11595732-5	2001	Furthermore, we demonstrate that ATRA promotes the ubiquitylation of Skp2, an F-box protein that targets p27 for degradation.	Tretinoin	33-37	interferon alpha inducible protein 27	Homo sapiens	105-108	
11464914-5	2001	Within 24 hr of RA treatment, there was a 4-fold increase in the expression of p27Kip1, although p27 mRNA levels were unchanged.	Tretinoin	16-18	interferon alpha inducible protein 27	Homo sapiens	79-82	
11478839-0	2001	Retinoic acid- and bone morphogenetic protein 4-induced apoptosis in P19 embryonal carcinoma cells requires p27.	Tretinoin	0-13	interferon alpha inducible protein 27	Homo sapiens	108-111	
11478839-8	2001	In contrast, RA and BMP4 induce the Cdk inhibitor p27.	Tretinoin	13-15	interferon alpha inducible protein 27	Homo sapiens	50-53	
11478839-13	2001	These data support the hypothesis that RA and BMP4 together induce the p27 protein leading to Rb activation and ultimately apoptosis.	Tretinoin	39-41	interferon alpha inducible protein 27	Homo sapiens	71-74	
11063125-0	2000	Retinoic acid induces neuronal differentiation of embryonal carcinoma cells by reducing proteasome-dependent proteolysis of the cyclin-dependent inhibitor p27.	Tretinoin	0-13	interferon alpha inducible protein 27	Homo sapiens	155-158	
11063125-2	2000	In the present study, we provide a functional link between RA and p27 function in the control of neuronal differentiation in NT2/D1 cells.	Tretinoin	59-61	interferon alpha inducible protein 27	Homo sapiens	66-69	
11063125-3	2000	We report that RA enhances p27 expression, which results in increased association with cyclin E/cyclin-dependent kinase 2 complexes and suppression of their activity; however, antisense clones, which have greatly reduced RA-dependent p27 inducibility (NT2-p27AS), continue to synthesize DNA and are unable to differentiate properly in response to RA as determined by lack of neurite outgrowth and by the failure to modify surface antigens.	Tretinoin	15-17	interferon alpha inducible protein 27	Homo sapiens	27-30	
11063125-4	2000	As to the mechanism involved in RA-dependent p27 upregulation, our data support the concept that RA reduces p27 protein degradation through the ubiquitin/proteasome-dependent pathway.	Tretinoin	32-34	interferon alpha inducible protein 27	Homo sapiens	45-48	
11063125-4	2000	As to the mechanism involved in RA-dependent p27 upregulation, our data support the concept that RA reduces p27 protein degradation through the ubiquitin/proteasome-dependent pathway.	Tretinoin	32-34	interferon alpha inducible protein 27	Homo sapiens	108-111	
11063125-4	2000	As to the mechanism involved in RA-dependent p27 upregulation, our data support the concept that RA reduces p27 protein degradation through the ubiquitin/proteasome-dependent pathway.	Tretinoin	97-99	interferon alpha inducible protein 27	Homo sapiens	45-48	
11063125-4	2000	As to the mechanism involved in RA-dependent p27 upregulation, our data support the concept that RA reduces p27 protein degradation through the ubiquitin/proteasome-dependent pathway.	Tretinoin	97-99	interferon alpha inducible protein 27	Homo sapiens	108-111	
10090931-0	1999	1,25-Dihydroxyvitamin D3 induces differentiation of a retinoic acid-resistant acute promyelocytic leukemia cell line (UF-1) associated with expression of p21(WAF1/CIP1) and p27(KIP1).	Tretinoin	54-67	interferon alpha inducible protein 27	Homo sapiens	173-176	
10896783-6	2000	Evaluation of the kinase activity of cyclin-Cdk complexes showed that RA increases p27(Kip1) expression in CH27 cells leading to markedly reduced cyclin A/Cdk2 kinase activity and slightly reduced cyclin E/Cdk2 kinase activity, with no effect on cyclin D/Cdk4 and cyclin D/Cdk6 activities.	Tretinoin	70-72	interferon alpha inducible protein 27	Homo sapiens	83-86	
10896783-0	2000	Retinoic acid-mediated G1 arrest is associated with induction of p27(Kip1) and inhibition of cyclin-dependent kinase 3 in human lung squamous carcinoma CH27 cells.	Tretinoin	0-13	interferon alpha inducible protein 27	Homo sapiens	65-68	
10896783-3	2000	Here we report that RA mediated the dose- and time-dependent growth arrest in G1 phase, accompanied by the up-regulation of p27(Kip1) and the down-regulation of the cyclin-dependent kinase 3 (Cdk3) and p21(CIP1/Waf1) proteins.	Tretinoin	20-22	interferon alpha inducible protein 27	Homo sapiens	124-127	
10090931-14	1999	Interestingly, the combination of 1, 25(OH)2D3 and RA markedly enhanced the levels of p27(KIP1) transcript and protein as compared with levels induced by 1, 25(OH)2D3 alone.	Tretinoin	51-53	interferon alpha inducible protein 27	Homo sapiens	86-89	
9366521-8	1997	Interestingly, when U343 cells are growth arrested by p16, p21 or p27 induction and treated simultaneously with RA, a dramatic morphological change occurs, cells acquiring multiple long, tapering processes reminiscent of primary astrocytes.	Tretinoin	112-114	interferon alpha inducible protein 27	Homo sapiens	66-69