IdA
stringlengths 6
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| IdB
stringlengths 6
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| labels
int64 0
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| mechanism
stringclasses 40
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stringclasses 10
values | score
float64 0.1
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stringlengths 10
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⌀ | signor_id
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14
|
|---|---|---|---|---|---|---|---|
P49023
|
Q99942
| 0
|
ubiquitination
|
down-regulates quantity
| 0.407
|
Here we demonstrate that the human homologue of RNF5 associates with the amino-terminal domain of paxillin, resulting in its ubiquitination. RNF5 requires intact RING and C-terminal domains to mediate paxillin ubiquitination. Concomitantly, RNF5 expression results in inhibition of cell motility. Via targeting of paxillin ubiquitination, which alters its localization, RNF5 emerges as a novel regulator of cell motility.
|
SIGNOR-271479
|
P20042
|
Q14232
| 0
|
guanine nucleotide exchange factor
|
up-regulates activity
| 0.78
|
EIF2B converts the protein synthesis initiation factor 2 (eIF2) from an inactive GDP-bound form to an active eIF2-GTP complex owing to its guanine nucleotide exchange factor (GEF) activity.
|
SIGNOR-269129
|
Q99759
|
O14920
| 1
|
phosphorylation
|
up-regulates activity
| 0.569
|
Genetic analysis showed that MEKK3, which is thought to activate IKK2 through phosphorylation (Yang et al., 2001), is necessary for TNF-alpha-induced NF-kappaB activation.|Our results also suggest that IKK2 is phosphorylated on S177 and S181 on its activation loop by MEKK3.
|
SIGNOR-279468
|
Q12772
|
O43462
| 0
|
cleavage
|
up-regulates activity
| 0.673
|
In order to activate transcription, the NH2-terminal domain of the SREBP must be released from the membrane so that it can enter the nucleus. This release has been studied most extensively for one of the SREBPs, namely, SREBP-2. However, the mechanism appears to be similar for the other SREBPs (SREBP-1a and -1c) (1). Release of the NH2-terminal domain is accomplished by a two-step proteolytic event that is regulated by sterols (3). In sterol-depleted mammalian cells, this proteolysis is initiated by the Site-1 protease (S1P), which cleaves human SREBP-2 between the Leu522-Ser523 bond in the sequence RSVL S (4). This cleavage requires formation of a complex between SREBP and SCAP, a polytopic membrane protein of the ER, and it is prevented when this complex is disrupted
|
SIGNOR-267498
|
P21917
|
P09471
| 2
|
binding
|
up-regulates activity
| 0.46
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-256982
|
Q13188
|
P31751
| 0
|
phosphorylation
|
down-regulates
| 0.261
|
Akt phosphorylates mst2 at thr117 in vitro and in vivo, which leads to mst2 cleavage and kinase activity as well as nuclear translocation.
|
SIGNOR-164302
|
P68400
|
Q9H2G2
| 1
|
phosphorylation
|
down-regulates
| 0.2
|
Slk down-regulation by v-src is indirect and is accompanied by slk hyperphosphorylation on serine residues. Deletion analysis revealed that casein kinase ii (ck2) sites at position 347/348 are critical for v-src-dependent modulation of slk activity.
|
SIGNOR-147879
|
O14757
|
Q7Z6Z7
| 0
|
ubiquitination
|
down-regulates quantity by destabilization
| 0.298
|
Taken together, these results are consistent with our hypothesis that HUWE1 directly poly-ubiquitinates and targets Chk1 to the proteasome.
|
SIGNOR-278568
|
P42658
|
Q9Y6K1
| 0
|
transcriptional regulation
|
down-regulates quantity by repression
| 0.2
|
In the absence of Dnmt3b, Dnmt3a was associated with Dpp6 gene promoter and regulated its expression and methylation in P19 cells.
|
SIGNOR-268962
|
P07900
|
Q15185
| 2
|
binding
|
up-regulates activity
| 0.916
|
The mutant Hsp90 proteins tested are defective in the binding and ATP hydrolysis-dependent cycling of the co-chaperone p23, which is thought to regulate the binding and release of substrate polypeptide from Hsp90.
|
SIGNOR-262831
|
Q9GZQ6
|
P08754
| 2
|
binding
|
up-regulates activity
| 0.25
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-256851
|
O95837
|
P30550
| 2
|
binding
|
up-regulates activity
| 0.435
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-257421
|
P42229
|
P00533
| 2
|
binding
|
up-regulates
| 0.821
|
We identified stat5 as a direct binding partner to egfr and erbb4 and discovered new recognition motifs for shc and stat5.Egf stimulation and subsequent phosphorylation of egfr at tyrosine y978, y998 and y869 would then subsequently lead to recruitment and activation of stat5.
|
SIGNOR-68159
|
P49768
|
P05771
| 0
|
phosphorylation
|
up-regulates activity
| 0.2
|
A phosphorylation site at serine residue 346 was identified that is selectively phosphorylated by PKC but not by PKA. This site is localized within a recognition motif for caspases, and phosphorylation strongly inhibits proteolytic processing of PS1 by caspase activity during apoptosis.
|
SIGNOR-249237
|
Q13621
|
O95747
| 0
|
phosphorylation
|
up-regulates activity
| 0.502
|
We establish that the SPAK and OSR1 kinases activated by WNK interact with an RFQV motif on NKCC2 and directly phosphorylate Thr95, Thr100, Thr105 and, possibly, Ser91.Using these phosphorylation-specific antibodies we establish that hypotonic low-chloride stimulation induces marked phosphorylation of overexpressed NKCC2 in HEK-293 cells at Ser91, Thr100, Thr105 and Ser130 (Fig. 3A).
|
SIGNOR-276309
|
P05556
|
Q9Y5I4
| 2
|
binding
|
up-regulates activity
| 0.2
|
The clustered protocadherins comprise the largest subfamily of the cadherin superfamily and are predominantly expressed in the nervous system. Pcdh-alpha proteins interact with beta1-integrin to promote cell adhesion.
|
SIGNOR-269033
|
P17612
|
P61586
| 1
|
phosphorylation
|
down-regulates activity
| 0.518
|
PKA phosphorylates RhoA on Ser188. the addition of a negative charge to Ser188 is sufficient to diminish both RhoA activation and activity within the context of a cell.
|
SIGNOR-250047
|
P36544
|
P12931
| 0
|
phosphorylation
|
down-regulates
| 0.2
|
Alpha7 neuronal nicotinic acetylcholine receptors are negatively regulated by tyrosine phosphorylation and src-family kinasesmutant alpha7 nachrs lacking cytoplasmic loop tyrosine residues because of alanine replacement of tyr-386 and tyr-442 were more active than wild-type receptorsexpression of active src reduced _7 nachr activity
|
SIGNOR-141311
|
Q01094
|
P06493
| 0
|
phosphorylation
|
up-regulates
| 0.7
|
Association of e2f with rb inhibits its transactivation potential. phosphorylation of e2f-1 on serine residues 332 and 337 prevented its interaction with rbthese residues were phosphorylated in vivo and by p34cdc2 kinase in vitro.
|
SIGNOR-36026
|
P78563
|
P31749
| 0
|
phosphorylation
|
down-regulates activity
| 0.2
|
AKT-dependent phosphorylation of the adenosine deaminases ADAR-1 and -2 inhibits deaminase activity. Coimmunoprecipitation studies and in vitro kinase assays revealed that AKT-1, -2, and -3 interact with both ADAR1p110 and ADAR2 and phosphorylate these RNA editases. Using site-directed mutagenesis of suspected AKT phosphorylation sites, AKT was found to primarily phosphorylate ADAR1p110 and ADAR2 on T738 and T553, respectively
|
SIGNOR-276194
|
Q96QF0
|
Q15208
| 0
|
phosphorylation
|
up-regulates activity
| 0.366
|
We identified 5 potential NDR1 substrates in the mouse brain and chose two for functional validation. We show that one NDR1 substrate is another kinase, AP-2 associated kinase-1 (AAK1) which regulates dendritic branching as a result of NDR1 phosphorylation. Another substrate is the Rab8 guanine nucleotide exchange factor (GEF) Rabin8 (a Sec2p homolog) which we find is involved in spine synapse formation.
|
SIGNOR-263036
|
P31785
|
P15248
| 2
|
binding
|
up-regulates
| 0.58
|
The common gamma-chain (gamma(c)) is an indispensable subunit of the functional receptor complexes for il-4, il-7, il-9, and il-15 as well as il-2. Here we show that the gamma(c) is also shared with the il-21r complex
|
SIGNOR-108867
|
Q5JVL4
|
Q92949
| 0
|
transcriptional regulation
|
up-regulates quantity by expression
| 0.356
|
FOXJ1 expression in basal cells induced the expression of a panel of cilia-associated genes, including centrin 2 (CETN2); dynein, axonemal, heavy chain 11 (DNAH11); dynein, axonemal, intermediate chain 1 (DNAI1); dynein, axonemal, light intermediate chain 1 (DNALI1); EF-hand domain, C-terminal, containing 1 (EFHC1); sperm associated antigen 6 (SPAG6); tektin 1 (TEKT1), TEKT2 and tubulin, alpha 1a (TUBA1A; Figure 3C and Additional file 2: Table S1).
|
SIGNOR-266934
|
P56524
|
Q16566
| 0
|
phosphorylation
|
down-regulates activity
| 0.62
|
CaMKIV phosphorylates HDAC4 in vitro and promotes its nuclear-cytoplasmic shuttling in vivo. | Thus, CaMKIV can phosphorylate HDAC4 at Ser-467 and/or Ser-632 in vitro. | Collectively, our results suggest that CaMKIV reverses the transcriptional repression activity of HDAC4 by stimulating the mobilization of HDAC4 out of the nucleus.
|
SIGNOR-250712
|
Q9NZC9
|
Q13535
| 0
|
phosphorylation
|
down-regulates activity
| 0.538
|
ATR phosphorylates SMARCAL1 on S652, thereby limiting its fork regression activities and preventing aberrant fork processing. Thus, phosphorylation of SMARCAL1 is one mechanism by which ATR prevents fork collapse, promotes the completion of DNA replication, and maintains genome integrity.
|
SIGNOR-273516
|
P55085
|
P17655
| 0
|
cleavage
|
down-regulates activity
| 0.298
|
PAR1E and PAR2E (10 microM) were incubated in the presence of the different proteases | The enzymes were used at the following concentrations: 0.5 unit/mL thrombin, 2.5 nM trypsin, 20 nM plasmin, 20 nM cathepsin G, 20 nM elastase, 20 nM proteinase 3, and 2 units/mL calpain I and II|Protease-activated receptors (PARs) mediate cell activation after proteolytic cleavage of their extracellular amino terminus.|Mass spectrometry studies of PAR2E predicted activation of PAR2 by trypsin through cleavage at the Arg36-Ser37 site, no effect of thrombin, and inactivation of the receptor by plasmin, calpain and leukocyte elastase, cathepsin G, and proteinase 3
|
SIGNOR-263581
|
O94806
|
Q9UQL6
| 1
|
phosphorylation
|
up-regulates activity
| 0.265
|
Histone deacetylase (HDAC) 5 and 7, two members of the class II of classical HDAC [62], are in vivo substrates of PKD3 and PKD [63]. In response to a variety of signals, including phorbol esters, T cell receptor engagement, vascular endothelial growth factor and angiotensin stimulation, the activity of HDAC5 and 7 are regulated by a mechanism that involves PKD3 and PKD-mediated phosphorylation of the highly conserved Ser259 and Ser498 residues that are located in N-terminus of class II HDACs [63–67].
|
SIGNOR-275926
|
Q9Y5F9
|
Q9Y5I2
| 2
|
binding
|
up-regulates activity
| 0.2
|
The clustered protocadherins comprise the largest subfamily of the cadherin superfamily and are predominantly expressed in the nervous system. Pcdh-alpha proteins interact with beta1-integrin to promote cell adhesion. They also form oligomers with Pcdh-gamma proteins at the same membrane sites.
|
SIGNOR-265706
|
P25101
|
P63092
| 2
|
binding
|
up-regulates activity
| 0.477
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ‚â• -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ‚â• -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ‚â• -1.0.
|
SIGNOR-256780
|
P31749
|
O75925
| 0
|
sumoylation
|
up-regulates activity
| 0.378
|
Although multiple sites on Akt could be SUMOylated, K276 was identified as a major SUMO acceptor site. K276R or E278A mutation reduced SUMOylation of Akt but had little effect on its ubiquitination. Strikingly, these mutations also completely abolished Akt kinase activity. In support of these results, we found that expression of PIAS1 and SUMO1 increased Akt activity, whereas expression of SENP1 reduced Akt1 activity.
|
SIGNOR-252735
|
P51532
|
Q12824
| 2
|
binding
|
up-regulates activity
| 0.943
|
The remodeling activity of brg1 and hbrm is stimulated by baf170/baf155 and is further stimulated when ini1 is added.
|
SIGNOR-65438
|
P09471
|
P08172
| 2
|
binding
|
up-regulates activity
| 0.349
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-256964
|
Q9UM11
|
P23919
| 2
|
binding
|
down-regulates quantity by destabilization
| 0.226
|
We demonstrate that TMPK is recognized and degraded by APC/C-Cdc20/Cdh1-mediated pathways from mitosis to the early G1 phase, whereas TK1 is targeted for degradation by APC/C-Cdh1 after mitotic exit.
|
SIGNOR-272652
|
P01106
|
Q8N1E6
| 0
|
ubiquitination
|
down-regulates quantity by destabilization
| 0.349
|
In this study, we demonstrate that the deubiquitinase USP13 stabilizes c-Myc by antagonizing FBXL14-mediated ubiquitination to maintain GSC self-renewal and tumorigenic potential. USP13 was preferentially expressed in GSCs, and its depletion potently inhibited GSC proliferation and tumor growth by promoting c-Myc ubiquitination and degradation.
|
SIGNOR-274125
|
Q9NRF2
|
Q8WV28
| 1
|
dephosphorylation
|
down-regulates activity
| 0.2
|
SHP-1 is recruited by the phosphorylated ITIM-bearing receptors such as CD22 and it dephosphorylates proximal BCR signaling molecules such as CD79, SYK, BLNK.
|
SIGNOR-268446
|
P62834
|
Q9H4E7
| 2
|
binding
|
up-regulates activity
| 0.257
|
Mechanistic studies revealed that SLAT interacts, through its PH domain, with a key component of inside-out signaling, namely the active form of the small GTPase Rap1 (which has two isoforms, Rap1A and Rap1B). This interaction has been further shown to facilitate the interdependent recruitment of Rap1 and SLAT to the T cell immunological synapse upon TCR engagement. Furthermore, a SLAT mutant lacking its PH domain drastically inhibited LFA-1 activation and CD4(+) T cell adhesion.
|
SIGNOR-253365
|
Q13627
|
Q9NYY3
| 1
|
phosphorylation
|
up-regulates quantity by stabilization
| 0.313
|
In the present study, it was demonstrated that dual specificity tyrosine-phosphorylation-regulated kinase 1A (DYRK1A) interacts with and phosphorylates PLK2 at Ser358. DYRK1A-mediated phosphorylation of PLK2 increases its protein stability.
|
SIGNOR-277805
|
Q96PU4
|
P24385
| 1
|
ubiquitination
|
down-regulates quantity by destabilization
| 0.294
|
We found that NIRF directly ubiquitinated cyclins D1 and E1, as evidenced by the appearance of the tail (Fig. 4B). In summary, the above findings suggest that NIRF tightly cooperates with the core cell cycle machinery and induces G1 arrest, which is accompanied by ubiquitination of cyclins D1 and E1.
|
SIGNOR-271885
|
Q7Z6G8
|
Q9UQM7
| 0
|
phosphorylation
|
down-regulates activity
| 0.257
|
CaMKII-mediated displacement of AIDA-1 out of the postsynaptic density core. The present study indicates that CaMKII activation is necessary for the NMDA-induced movement of AIDA-1 out of the PSD core.
|
SIGNOR-264231
|
Q16611
|
P04637
| 2
|
binding
|
up-regulates
| 0.691
|
P53 interacts with the pro-apoptotic mitochondrial membrane protein bak
|
SIGNOR-124122
|
O95750
|
P18848
| 0
|
transcriptional regulation
|
up-regulates quantity by expression
| 0.2
|
Reporter gene analyses using the 5'-promoter region of FGF19 revealed that a functional AARE (amino-acid-response element) was localized in this region, and this site was responsible for inducing its transcription through ATF4 (activating transcription factor 4), which is activated in response to ER stress
|
SIGNOR-253727
|
P14618
|
Q99708
| 1
|
phosphorylation
|
up-regulates activity
| 0.2
|
Here, we uncover an unexpected mechanism through which pyruvate kinase M2 (PKM2), the highly expressed PK isoform in cancer cells and a master regulator of cancer metabolic reprogramming, integrates with the DDR to directly promote DNA double-strand break (DSB) repair. In response to ionizing radiation and oxidative stress, ATM phosphorylates PKM2 at T328 resulting in its nuclear accumulation.
|
SIGNOR-277413
|
P17706
|
P00533
| 1
|
dephosphorylation
|
down-regulates
| 0.635
|
Here, we report that the 45-kda variant of the protein tyrosine phosphatase tcptp (tc45) can recognize delta egfr as a cellular substrate
|
SIGNOR-132316
|
Q9P2D8
|
Q8N2C7
| 2
|
binding
|
up-regulates activity
| 0.803
|
The NALCN complex in the brain consists of NALCN, UNC80 and UNC79. UNC80 directly associates with NALCN and UNC79 forms part of the complex by its interaction with UNC80.
|
SIGNOR-265183
|
Q13501
|
Q12981
| 2
|
binding
|
up-regulates activity
| 0.334
|
RNF185 functions as a ubiquitin E3 ligase, enabling BNIP1-p62 interaction. BNIP1 is polyubiquitinated by RNF185 and associates with autophagy receptor p62. In addition, we checked the endogenous localization of BNIP1 and p62 in HeLa cells (Fig. 7F). Alexa Fluor 488 conjugated endogenous BNIP1 and TRITIC conjugated endogenous p62 overlapped well in the cytoplasm, further providing the locational evidence for the recruitment of p62 by BNIP1.
|
SIGNOR-271932
|
P55211
|
P42574
| 2
|
cleavage
|
up-regulates activity
| 0.639
|
Following autoprocessing in the apoptosome, caspase-9 cleaves and activates caspase-3.
|
SIGNOR-133267
|
Q9HAV7
|
P11142
| 2
|
binding
|
down-regulates activity
| 0.62
|
As we had observed earlier,HMGE bound avidly to DnaK (Fig. 5A). In addition, bothMt-Hsp70 and Hsc70 bound to GST-HMGE, but Hsc70 appeared to bind with lower affinity. HMGE inhibitedthe co-chaperone enhancement of Hsc70 ATPase activity byapproximately 50% (Table 1).
|
SIGNOR-261241
|
Q04759
|
P32942
| 1
|
phosphorylation
|
up-regulates activity
| 0.334
|
Ser489 was a phosphorylation site in vitro for recombinant protein kinase Ctheta. Finally, treatment of Jurkat cells with chelerythrine chloride, a protein kinase C inhibitor, prevented ICAM-3-triggered spreading.
|
SIGNOR-248979
|
Q12802
|
P61586
| 1
|
guanine nucleotide exchange factor
|
up-regulates activity
| 0.744
|
We therefore developed a screening-compatible live-cell imaging assay, using FRET-based biosensors for the prototype GTPases RHOA, RAC1 and CDC4215,19,20 (Extended Data Fig. 2 and Supplementary Note 1)|We found catalytic activities for 45/75 RhoGEFs and 48/63 RhoGAPs| Our data thus not only reveal extensive promiscuity among regulators, but also that the inactivating RhoGAPs are less selective than the activating RhoGEFs (p-value=0.02)(Supplementary Table 2).
|
SIGNOR-260527
|
P51692
|
Q15788
| 2
|
binding
|
up-regulates
| 0.323
|
Ncoa-1/src-1 is an essential coactivator of stat5 that binds to the fdl motif in the alpha-helical region of the stat5 transactivation domain.
|
SIGNOR-100261
|
Q53EL6
|
P23443
| 0
|
phosphorylation
|
down-regulates
| 0.614
|
Both akt and p70(s6k) phosphorylate pdcd4, allowing for binding of the e3-ubiquitin ligase beta-trcp and consequently ubiquitylation.
|
SIGNOR-150144
|
Q92974
|
Q96SB3
| 2
|
binding
|
up-regulates activity
| 0.396
|
The Rho Family GEF Lfc Interacts with Neurabin and Spinophilin. Neurabin and spinophilin are homologous protein phosphatase 1 and actin binding proteins that regulate dendritic spine function. The results obtained in the present study suggest a mechanism by which neurabin or spinophilin contributes to the organization of the F-actin cytoskeleton in dendritic spines, and in turn to the regulation of spine morphology, via the activity-dependent recruitment of the Rho-specific GEF Lfc
|
SIGNOR-269176
|
P38117
|
Q8IXQ9
| 0
|
methylation
|
down-regulates activity
| 0.2
|
Accordingly, we found that METTL20-mediated methylation of ETFβ in vitro reduced its ability to receive electrons from the medium chain acyl-CoA dehydrogenase and the glutaryl-CoA dehydrogenase. In conclusion, the present study establishes METTL20 as the first human KMT localized to mitochondria and suggests that it may regulate cellular metabolism through modulating the interaction between its substrate ETFβ and dehydrogenases.
|
SIGNOR-269450
|
Q16819
|
Q99626
| 0
|
transcriptional regulation
|
up-regulates quantity by expression
| 0.471
|
TNF-α-induced down-regulation of CDX2 suppresses MEP1A expression in colitis|
|
SIGNOR-253965
|
P55196
|
Q92963
| 2
|
binding
|
up-regulates activity
| 0.2
|
Rit and Rin were found to interact with the known Ras binding proteins RalGDS, Rlf, and AF-6/Canoe. These interactions were GTP and effector domain dependent and suggest that RalGDS, Rlf, and AF-6 are Rit and Rin effectors.
|
SIGNOR-220917
|
Q13882
|
P51692
| 1
|
phosphorylation
|
up-regulates
| 0.429
|
Phosphospecific antibodies, mutational analysis, and in vitro kinase assays demonstrated that brk specifically mediated stat5b phosphorylation at the activating tyrosine, y699.
|
SIGNOR-159066
|
Q15797
|
Q9GZU7
| 0
|
dephosphorylation
|
down-regulates
| 0.498
|
In human cells, rnai-mediated depletion of scp1 and scp2 increases the extent and duration of smad1 phosphorylation in response to bmp, the transcriptional action of smad1, and the strength of endogenous bmp gene responses. The present identification of the scp family as smad c-terminal phosphatases sheds light on the events that attenuate smad signaling and reveals unexpected links to the essential phosphatases that control rna polymerase ii in eukaryotes.
|
SIGNOR-148396
|
P20339
|
Q9GZQ3
| 2
|
binding
|
up-regulates activity
| 0.2
|
The N terminus of COMMD5 binds to the endosomal Rab5, and its C terminus, including the COMMD domain, binds to the cytoskeletal scaffolding.
|
SIGNOR-261691
|
P37231
|
Q00535
| 0
|
phosphorylation
|
down-regulates activity
| 0.574
|
CDK5 in turn phosphorylates PPARgamma at Ser273 and prevents the transcription of specific PPARgamma target genes that have anti-diabetic effects .
|
SIGNOR-278189
|
Q92538
|
Q13131
| 0
|
phosphorylation
|
down-regulates
| 0.2
|
These results indicate that gbf1 is a novel ampk substrate and that the ampk-mediated phosphorylation of gbf1 at thr(1337) has a critical role, presumably by attenuating the function of gbf1, in the disassembly of the golgi apparatus induced under stress conditions that lower the intracellular atp concentration.
|
SIGNOR-159639
|
P19525
|
Q9UQ80
| 1
|
phosphorylation
|
up-regulates activity
| 0.243
|
Ebp1 itself is phosphorylated by the PKR protein kinase, suggesting that the effects of Ebp1 overexpression evidenced in vivo on eIF2alpha phosphorylation could be achieved by competition between Ebp1 and eIF2alpha for PKR kinase activity.
|
SIGNOR-279170
|
P38405
|
P32238
| 2
|
binding
|
up-regulates activity
| 0.264
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-256906
|
P16112
|
O60882
| 0
|
cleavage
|
down-regulates quantity by destabilization
| 0.477
|
Matrix metalloproteinases 19 and 20 cleave aggrecan and cartilage oligomeric matrix protein (COMP)|It has been suggested that MMPs play a role in the hydrolysis of COMP and, therefore, compromise the integrity of the cartilage ECM structure leading to the ultimate loss of joint function
|
SIGNOR-266981
|
P27361
|
Q12772
| 1
|
phosphorylation
|
up-regulates
| 0.392
|
Insulin-activated erk-mitogen-activated protein kinases phosphorylate sterol regulatory element-binding protein-2 at serine residues 432 and 455 in vivo.Further characterization by electrophoretic mobility shift assay and promoter reporter gene analyses revealed that phosphorylation does not influence protein/dna interaction, but enhances trans-activity.
|
SIGNOR-123053
|
Q8IWV7
|
O94761
| 2
|
binding
|
up-regulates
| 0.492
|
The isolated recql4, assayed as a complex with ubr1 and ubr2, exhibited dna-stimulated atpase activity but was inactive as either dna helicase or dna translocase / the discovery, in the present work, that these ub ligases, ubr1 and ubr2, interact with the putative helicase recql4 (fig. 2), and that recql4 is a long-lived, non-ubiquitylated protein in hela cells
|
SIGNOR-128169
|
P13639
|
P67775
| 0
|
dephosphorylation
|
up-regulates
| 0.404
|
Protein phosphatases-2a and -2c (pp-2a and pp-2c) can each efficiently dephosphorylate phosphorylated eef-2
|
SIGNOR-38566
|
P54753
|
P54753
| 2
|
phosphorylation
|
up-regulates activity
| 0.2
|
Tyrosine-614, the major autophosphorylation site of the receptor tyrosine kinase HEK2, functions as multi-docking site for SH2-domain mediated interactions. a single amino acid substitution (Y614F) clearly reduces the phosphotyrosine content of HEK2 and abrogates its ability to bind rasGAP, Crk and Fyn indicating that this residue functions as major phosphorylation and multi-docking site.
|
SIGNOR-251126
|
P11171
|
Q14980
| 1
|
relocalization
|
up-regulates activity
| 0.533
|
These results indicate that 4.1 proteins recruit NuMA and dynein to the anaphase cell cortex through their conserved CTD (Figure 2I).
|
SIGNOR-266012
|
Q8WVI7
|
P62136
| 2
|
binding
|
down-regulates activity
| 0.389
|
IPP5, a novel inhibitor of protein phosphatase 1, suppresses tumor growth and progression of cervical carcinoma cells by inducing G2/M arrest
|
SIGNOR-275726
|
P45983
|
P37231
| 1
|
phosphorylation
|
down-regulates activity
| 0.527
|
The a/b domain of human ppargamma1 was phosphorylated in vivo, and this was abolished either by mutation of serine 84 to alanine (s84a) or coexpression of a phosphoprotein phosphatase. In vitro, this domain was phosphorylated by erk2 and jnk, and this was markedly reduced in the s84a mutant. Thus, phosphorylation of a mitogen-activated protein kinase site in the a/b region of ppargamma inhibits both ligand-independent and ligand-dependent transactivation functions.
|
SIGNOR-46518
|
Q05086
|
P17612
| 0
|
phosphorylation
|
down-regulates activity
| 0.328
|
These data suggest that PKA phosphorylation at T485 inhibits UBE3A ubiquitin ligase activity in cells.
|
SIGNOR-236899
|
Q8NB16
|
Q9Y572
| 0
|
phosphorylation
|
up-regulates activity
| 0.753
|
MLKL comprises a four-helical bundle tethered to the pseudokinase domain, which contains an unusual pseudoactive site. Although the pseudokinase domain binds ATP, it is catalytically inactive and its essential nonenzymatic role in necroptotic signaling is induced by receptor-interacting serine-threonine kinase 3 (RIPK3)-mediated phosphorylation.[...]S345, S347, and T349 in the MLKL activation loop were phosphorylated by RIPK3 in in vitro kinase assays
|
SIGNOR-266427
|
P05091
|
O15379
| 2
|
binding
|
up-regulates activity
| 0.2
|
Consistent with previous data, HDAC3 only bound to the ATP6V0E2 promoter in the presence of ALDH2.|Taken together, our data demonstrate that in the macrophages of LDLR-KO or ALDH2 rs671 mutant, AMPK phosphorylates ALDH2 at T356, which enables its nuclear translocation. Once in the nucleus, ALDH2 binds to HDAC3 and suppresses the transcription and protein expression of ATP6V0E2.
|
SIGNOR-271867
|
P30679
|
P32238
| 2
|
binding
|
up-regulates activity
| 0.485
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-257410
|
P55211
|
P06454
| 2
|
binding
|
down-regulates
| 0.364
|
PHAP proteins promoted caspase-9 activation after apoptosome formation, whereas ProT negatively regulated caspase-9 activation by inhibiting apoptosome formation.
|
SIGNOR-259079
|
P30542
|
P08754
| 2
|
binding
|
up-regulates activity
| 0.461
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-256840
|
Q6U7Q0
|
P48730
| 0
|
phosphorylation
|
down-regulates quantity by destabilization
| 0.2
|
CK1delta and GSK3beta kinases sequentially phosphorylate ZNF322A at serine-396 and then serine-391. Moreover, the doubly phosphorylated ZNF322A protein creates a destruction motif for the ubiquitin ligase FBXW7alpha leading to ZNF322A protein destruction.
|
SIGNOR-264892
|
P07550
|
P63092
| 2
|
binding
|
up-regulates activity
| 0.66
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ‚â• -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ‚â• -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ‚â• -1.0.
|
SIGNOR-256809
|
P26678
|
P16615
| 2
|
binding
|
down-regulates activity
| 0.751
|
Heart failure can be traced, in part, to alterations in the activity of the sarcoplasmic reticulum Ca2+ pump that are induced by its interactions with phospholamban, a reversible inhibitor.
|
SIGNOR-252031
|
Q9UHD2
|
P08631
| 0
|
phosphorylation
|
down-regulates activity
| 0.2
|
The Src family kinases (SFKs) Lck, Hck, and Fgr directly phosphorylate TBK1 at Tyr354/394, to prevent TBK1 dimerization and activation.
|
SIGNOR-276727
|
P51608
|
P18031
| 1
|
transcriptional regulation
|
down-regulates quantity by repression
| 0.2
|
In this study, we have demonstrated that the PTPN1 gene, which encodes PTP1B, was a direct target of MECP2 and that PTP1B protein levels were dramatically increased in Mecp2-mutant mice and in fibroblasts derived from patients with RTT.
|
SIGNOR-264546
|
P24941
|
Q01196
| 1
|
phosphorylation
|
up-regulates activity
| 0.2
|
We have identified four phosphorylation sites on aml1c that are necessary for transcriptional activity of aml1c in k562 and 293t cells (27).4 mutation of these four sites (serine 276, serine 293, serine 303, and threonine 300) to alanine abolishes transcriptional activation, whereas mutation of these sites to aspartic acid (which mimics phosphorylation) results in a hyperactive protein.
|
SIGNOR-138932
|
P84243
|
Q15652
| 0
|
demethylation
|
down-regulates activity
| 0.2
|
We now determine that JMJD1C is recruited by USF-1 to various lipogenic genes for H3K9 demethylation to enhance chromatin accessibility in the fed state.
|
SIGNOR-265169
|
Q15910
|
Q9C0B5
| 0
|
palmitoylation
|
down-regulates activity
| 0.2
|
Mechanistic investigations revealed that mutant p53 transcriptionally upregulated ZDHHC5 along with the nuclear transcription factor NF-Y. These events contributed to the development of glioma by promoting the self-renewal capacity and tumorigenicity of glioma stem-like cells, by altering the palmitoylation and phosphorylation status of the tumor suppressor EZH2.
|
SIGNOR-261144
|
Q9UMS4
|
P27694
| 1
|
polyubiquitination
|
up-regulates activity
| 0.509
|
PRP19 is a ubiquitin ligase involved in pre-mRNA splicing and the DNA damage response (DDR). PRP19 ubiquitylates RPA and promotes ATRIP recruitment.
|
SIGNOR-272076
|
P18084
|
O14713
| 2
|
binding
|
down-regulates activity
| 0.318
|
Integrins also bind to many PTBdomain-containing proteins (Calderwood et al., 2003) – including Dok1 and integrincytoplasmic-domain-associated protein 1 (ICAP1) – and these can compete with talin for binding to integrin and so can impair activation
|
SIGNOR-257660
|
P48729
|
Q00535
| 1
|
phosphorylation
|
up-regulates activity
| 0.297
|
We also show that casein kinase I, but not casein kinase II, can phosphorylate and activate cdk5 in vitro. Ser(159) in cdk5 is homologous to the regulatory Thr(160) in cdk2.
|
SIGNOR-275966
|
Q6ZN28
|
P08581
| 1
|
transcriptional regulation
|
up-regulates quantity by expression
| 0.394
|
Human colon carcinoma SW480 cells express virtually no MACC1. MACC1 cDNA transfection led not only to strong increases in MACC1 mRNA expression (Fig. 3a), but also to a 40-fold upregulation of the HGF receptor MET mRNA expression (Fig. 3b). This was confirmed on the protein level
|
SIGNOR-266058
|
Q16695
|
Q92830
| 0
|
acetylation
|
down-regulates activity
| 0.2
|
The HAT module within the SAGA and ADA complexes acetylates histone H3, mainly on residues K9 and K14.
|
SIGNOR-269604
|
P06241
|
Q96PD2
| 1
|
phosphorylation
|
up-regulates activity
| 0.35
|
Mutagenesis analysis of ESDN's seven intracellular tyrosines in YxxP motifs found several contribute to the binding of ESDN to the SH2 domains of both CrkCT10 regulator of kinase Crk-Like (CrkL) and a representative SFK Fyn. Quantitative mass spectrometry showed that at least three of these (Y565, Y621 and Y750), as well as non-YxxP Y715, are reversibly phosphorylated. SFK activity was shown to be sufficient, but not required for the interaction between ESDN and the CrkL-SH2 domain. Finally, antibody-mediated ESDN clustering induces ESDN tyrosine phosphorylation and CrkL-SH2 binding.
|
SIGNOR-273946
|
P22681
|
O15519
| 1
|
ubiquitination
|
down-regulates quantity by destabilization
| 0.2
|
We therefore conclude that c-cbl is a e3 ubiquitin ligase for flips and that the interaction of flips with c-cbl requires phosphorylation of both ser4 and tyr211 of flips.This interaction triggered proteasomal degradation of FLIP(S), which promoted activation of caspase-8 and apoptosis.
|
SIGNOR-186998
|
Q16539
|
P24385
| 1
|
phosphorylation
|
up-regulates
| 0.426
|
A large number of cytosolic proteins can be phosphorylated by p38 mapks, including phospholipase a2, the microtubule-associated protein tau, nhe-1, cyclin d1, cdk inhibitors, bcl2 family proteins, growth factor receptors or keratins
|
SIGNOR-166594
|
P32243
|
P48742
| 2
|
binding
|
up-regulates activity
| 0.435
|
Here we show that OTX2 directly associates with LIM1 and HNF-3beta. The luciferase assay with the P3C sequence, a specific DNA binding sequence for paired-class homeobox genes, has demonstrated that LIM1 enhances, but HNF-3beta represses, OTX2-directed gene expression.
|
SIGNOR-221161
|
O60674
|
Q12913
| 0
|
dephosphorylation
|
down-regulates activity
| 0.323
|
These results support PTPRJ preferentially dephosphorylating Y813 and Y868 in JAK2.|We revealed that PTPRJ negatively regulates leptin signaling by dephosphorylating specific tyrosine residues (Y813 and Y868) in JAK2, the simultaneous phosphorylation of which plays a pivotal role in JAK2 activation.
|
SIGNOR-277094
|
O15516
|
P49841
| 0
|
phosphorylation
|
down-regulates quantity by destabilization
| 0.341
|
We have identified a conserved cluster of serines that include, Ser431, which is a prerequisite phosphorylation site for the generation of BMAL dependent phospho-primed CLOCK and for the potential GSK-3 phosphorylation at Ser427.
|
SIGNOR-276270
|
P17947
|
Q99684
| 2
|
binding
|
down-regulates activity
| 0.594
|
Our data demonstrate that GFI-1 physically interacts with PU.1, repressing PU.1-dependent transcription. This repression is functionally significant, as GFI-1 blocked PU.1-induced macrophage differentiation of a multipotential hematopoietic progenitor cell line.
|
SIGNOR-256043
|
O15550
|
P68431
| 1
|
demethylation
|
down-regulates activity
| 0.2
|
Ubiquitously Transcribed Tetratricopeptide Repeat on chromosome X (UTX) and Jumonji D3 (JMJD3) as novel histone demethylases that catalyze the removal of di- and trimethyl groups on histone H3 lysine 27, thereby promoting target gene activation.
|
SIGNOR-260017
|
O95292
|
Q14721
| 0
|
relocalization
|
up-regulates quantity
| 0.2
|
Confirmation that Kv2.1 and -2.2 bind VAPA and VAPB employed colocalization/redistribution, siRNA knockdown, and Förster resonance energy transfer (FRET)-based assays.|As Kv2.1 accumulates on the surface it begins to bind ER VAPs and form the large and stable membrane junctions.
|
SIGNOR-262121
|
Q5NUL3
|
P19086
| 2
|
binding
|
up-regulates activity
| 0.25
|
Here we systematically quantified ligand-induced interactions between 148 GPCRs and all 11 unique G alpha subunit C-termini. For each receptor, we probed chimeric G alpha subunit activation via a transforming growth factor-alpha (TGF alpha) shedding response in HEK293 cells lacking endogenous Gq/11- and G12/13- signaling. | We defined positive coupling if any member of the subfamily scored LogRAi ≥ -1 and negative coupling if all of the members scored LogRAi < -1 (Figure 3A-B). ROC analysis gives AUC = 0.78 (Figure S4A) when considering high-confidence known coupling data and suggested a threshold of LogRAi ≥ -1.0 for defining true couplings. | The score associated to this interaction has a LogRAi ≥ -1.0.
|
SIGNOR-257313
|
O75150
|
Q13315
| 0
|
phosphorylation
|
up-regulates
| 0.443
|
E3 ubiquitin ligase, a heterodimeric complex of the ringfinger rfn20/rfn40 is phosphorylated by atm.
|
SIGNOR-175003
|
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