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|
|---|---|---|---|---|---|---|---|
P12821
|
P01019
| 1
|
cleavage
|
up-regulates activity
| 0.782
|
Angiotensin I-converting enzyme is a zinc metallopeptidase that plays an important role in blood pressure regulation by cleaving the inactive decapeptide angiotensin I to angiotensin II, a potent vasopressor octapeptide.
|
SIGNOR-253326
|
P05112
|
P78552
| 1
|
binding
|
up-regulates
| 0.782
|
It is now known that this alternate receptor is a heterodimer, the type ii il-4 receptor or the il-13 receptor, which is comprised of IL-4R And IL-13R1.
|
SIGNOR-100759
|
P01275-PRO_0000011258
|
P43220
| 1
|
binding
|
up-regulates activity
| 0.782
|
GLP-1 and GIP exert their physiological actions via stimulation of the two G protein-coupled receptors (GPCRs): the GLP-1 receptor (GLP-1R) and the GIP receptor (GIPR), respectively.
|
SIGNOR-278133
|
Q07325
|
P49682
| 1
|
binding
|
up-regulates activity
| 0.782
|
The chemokines CXCL9, 10, and 11 exert their action via CXC chemokine receptor-3 (CXCR3), a receptor highly expressed on activated T cells.
|
SIGNOR-260970
|
Q14289
|
P56945
| 1
|
phosphorylation
|
up-regulates activity
| 0.782
|
Pyk2 knockdown also decreased p130Cas.|p130Cas and paxillin can be phosphorylated by Fak or Pyk2, and bind directly to these kinases.
|
SIGNOR-280100
|
P01275
|
P43220
| 1
|
binding
|
up-regulates
| 0.782
|
In the present study we stably expressed the rat b-cell glp-i receptor in cho cells and studied binding characteristics and receptor activation utilizing the naturally occurring receptor agonist glp-i(7-36)-amide (glp-i), the proglucagon-derived glp-i-related peptide oxyntomodulin, the glp-i receptor agonist exendin-4, and the specific antagonist exendin
|
SIGNOR-34855
|
P02647
|
P04180
| 1
|
binding
|
up-regulates activity
| 0.782
|
Activation of LCAT by apolipoprotein (apo) A-I on nascent (discoidal) high density lipoproteins (HDL) is essential for formation of mature (spheroidal) HDL during the antiatherogenic process of reverse cholesterol transport. After attachment of LCAT to discoidal HDL, the helix 5/5 domains in apoA-I form amphipathic presentation tunnels for migration of hydrophobic acyl chains and amphipathic UC from the bilayer to the phospholipase A2-like and esterification active sites of LCAT, respectively.
|
SIGNOR-252103
|
Q9BXW4
|
Q9NT62
| 1
|
binding
|
up-regulates activity
| 0.782
|
Lc3-i is activated by the same atg7 involved in atg12 conjugation, transferred to atg3, a second e2-like enzyme, and finally conjugated to pe
|
SIGNOR-191552
|
Q86Y01
|
P46531
| 1
|
ubiquitination
|
up-regulates activity
| 0.781
|
The human Deltex (DTX1) gene encodes a cytoplasmic protein that functions as a positive regulator of the Notch signaling pathway.
|
SIGNOR-85942
|
P27361
|
P05412
| 1
|
phosphorylation
|
up-regulates
| 0.781
|
Up-regulation of c-jun mrna in cardiac myocytes requires the extracellular signal-regulated kinase cascade, but c-jun n-terminal kinases are required for efficient up-regulation of c-jun protein.
|
SIGNOR-91379
|
P40225
|
P40238
| 1
|
binding
|
up-regulates
| 0.781
|
Thrombopoietin(tpo) controls the formation of megakaryocytes and platelets from hematopoietic stem cells via activation of the c-mplreceptorand multiple downstream signal transduction pathways.
|
SIGNOR-113955
|
Q16690
|
P28482
| 1
|
dephosphorylation
|
down-regulates
| 0.781
|
Here we demonstrate that dusp5, an inducible nuclear phosphatase, interacts specifically with erk2 via a kinase interaction motif (kim) within its amino-terminal noncatalytic domain. This binding determines the substrate specificity of dusp5 in vivo, as it inactivates erk2 but not jun n-terminal protein kinase or p38 map kinase.
|
SIGNOR-134049
|
P51617
|
Q9HAT8
| 2
|
phosphorylation
|
up-regulates activity
| 0.781
|
The phosphorylation of Pellino2 by activated IRAK1 and IRAK4 could trigger and modulate the translocation of IRAKs from complex I to complex II.
|
SIGNOR-278947
|
O14757
|
P54132
| 1
|
phosphorylation
|
down-regulates quantity by destabilization
| 0.781
|
We now provide evidence that BLM undergoes K48-linked ubiquitylation and subsequent degradation during mitosis due to the E3 ligase, Fbw7α. Fbw7α carries out its function after GSK3β- and CDK2/cyclin A2-dependent phosphorylation events on Thr171 and Ser175 of BLM which lies within a well-defined phosphodegron, a sequence which is conserved in all primates.Phosphorylation on BLM Thr171 and Ser175 depends on prior phosphorylation at Thr182 by Chk1/Chk2. Thr182 phosphorylation not only controls BLM ubiquitylation and degradation during mitosis but is also a determinant for its localization on the ultrafine bridges.
|
SIGNOR-276909
|
P18031
|
P12931
| 1
|
dephosphorylation
|
up-regulates activity
| 0.781
|
Incubation of the inactivated c-Src with PTP1B results in a dose-dependent reactivation of c-Src tyrosine kinase activity. Incubation of c-Src with 2 or 10 g of PTP1B results in partial or full restoration of c-Src kinase activity, respectively. The activation is accompanied by dephosphorylation of c-Src, both of Tyr-419 and of Tyr-530
|
SIGNOR-245299
|
Q15628
|
Q13158
| 1
|
binding
|
up-regulates activity
| 0.781
|
Tradd recruits fadd
|
SIGNOR-177958
|
Q96PU5
|
Q15796
| 1
|
ubiquitination
|
down-regulates activity
| 0.781
|
Through its ww domain, nedd4l specifically recognizes a tgf-beta-induced phosphothr-protyr motif in the linker region, resulting in smad2/3 polyubiquitination and degradation
|
SIGNOR-217622
|
Q9Y275
|
O14836
| 1
|
binding
|
up-regulates
| 0.781
|
Tumor necrosis factor (tnf) receptor superfamily member taci is a high affinity receptor for tnf family members april and blys.
|
SIGNOR-81360
|
Q9HAT8
|
P51617
| 2
|
ubiquitination
|
up-regulates
| 0.781
|
These studies suggest that pellino isoforms may be the e3 ubiquitin ligases that mediate the il-1-stimulated formation of k63-pub-irak1 in cells, which may contribute to the activation of ikkbeta and the transcription factor nf-kappab, as well as other pathways dependent on irak1/4.
|
SIGNOR-159058
|
Q96GD4
|
O95235
| 1
|
phosphorylation
|
down-regulates activity
| 0.781
|
We identify MKlp2 as an essential protein for promoting abscission, which may regulate tethering and stabilizing of the PM to the microtubule cytoskeleton. Aurora B phosphorylation of MKlp2 S878 in the LAM is a key inhibitory signal for abscission. Conversely, B56-PP2A promotes abscission by opposing Aurora B phosphorylation of MKlp2 S878.
|
SIGNOR-262659
|
O14757
|
P04637
| 1
|
phosphorylation
|
up-regulates activity
| 0.78
|
Phosphorylation by chk1 of at least three of these sites, Ser366, Ser378, and Thr387, was induced by DNA damage.
|
SIGNOR-217861
|
P45983
|
P15336
| 1
|
phosphorylation
|
up-regulates
| 0.78
|
Activating transcription factor-2 (atf2) was found to be a target of the jnk signal transduction pathway. Atf2 was phosphorylated by jnk on two closely spaced threonine residues within the nh2-terminal activation domain.
|
SIGNOR-33914
|
P63165
|
P29590
| 1
|
sumoylation
|
up-regulates
| 0.78
|
We have shown previously that wild type PML, but not PML-RARalpha, is covalently modified by the sentrin family of ubiquitin-like proteins|We show that Lys65 in the RING finger domain, Lys160 in the B1 Box, and Lys490 in the nuclear localization signal contributes three major sentrinization sites| Furthermore, the triple substitution mutant is localized predominantly to the nucleoplasm, in contrast to wild type PML, which is localized to the nuclear bodies. Thus, sentrinization of PML, in the context of the RING finger and the B1 box, regulates nuclear body formation.
|
SIGNOR-261786
|
Q8IU57
|
P23458
| 1
|
binding
|
up-regulates
| 0.78
|
Each r1-type chain (il-10r1, il-20r1, il-22r1, ifn-_r1 and ifn-_r1) is associated with jak1 tyrosine kinase and mediates recruitment of a variety of signaling molecules after being phosphorylated on its intracellular domain.
|
SIGNOR-124480
|
P10145
|
P25024
| 1
|
binding
|
up-regulates
| 0.78
|
Il-8 activates both the cxcr1 and the cxcr2 on microvascular endothelial cells, using different signal transduction cascades.
|
SIGNOR-107920
|
Q96GD4
|
Q9H0H5
| 1
|
phosphorylation
|
up-regulates activity
| 0.78
|
It was found that the 5A fragment in which five Ser/Thr residues were substituted with Ala (S144A/T145A/S185A/T186A/S187A) fully prevented phosphorylation (Fig. 5B), confirming that Aurora B primarily phosphorylates five Ser/Thr residues in the basic region of MgcRacGAP. | the strong phosphorylation of the basic region of MgcRacGAP by Aurora B kinase was demonstrated, and this phosphorylation prevents the inhibition of MgcRacGAP GAP activity by PRC1
|
SIGNOR-250590
|
Q07889
|
P01111
| 1
|
guanine nucleotide exchange factor
|
up-regulates activity
| 0.78
|
Sos and Ras-GRF are two families of guanine nucleotide exchange factors that activate Ras proteins in cells. Sos proteins are ubiquitously expressed and are activated in response to cell-surface tyrosine kinase stimulation Sos1 and Ras-GRF1 activate the Ras proteins Ha-Ras, N-Ras, and Ki-Ras
|
SIGNOR-110566
|
Q14527
|
P12004
| 1
|
ubiquitination
|
up-regulates activity
| 0.78
|
HLTF promotes the Lys-63-linked polyubiquitination of proliferating cell nuclear antigen (PCNA) that is required for maintaining genomic stability.
|
SIGNOR-278608
|
P12644
|
Q13873
| 1
|
binding
|
up-regulates
| 0.78
|
Bmp-4 bound to alk-3 and alk-6 efficiently
|
SIGNOR-35763
|
Q14232
|
P20042
| 1
|
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
|
Q8WU20
|
Q06124
| 1
|
phosphorylation
|
up-regulates
| 0.78
|
In addition to the direct interactions with grb2, tyrosine-phosphorylated frs2 forms a complex with the sh2 domain-containing protein tyrosine phosphatase shp2. This interaction results in tyrosine phosphorylation of shp2 and complex formation between shp2 and grb2. the catalytic activity of shp2 is essential for a sustained map kinase response and for potentiation of fgf-induced neurite outgrowth in pc12 cells
|
SIGNOR-58196
|
O95476
|
Q14693
| 1
|
dephosphorylation
|
up-regulates activity
| 0.78
|
Dullard significantly dephosphorylates mouse lipin 1b only in BHK cells (Fig. 5A). This is most clearly seen by using the antibody prepared against the phosphorylation site Ser-106.|Dephosphorylation of lipin results in its translocation to the nuclear envelope and endoplasmic reticulum membranes from the cytosol and generation of diacylglycerol
|
SIGNOR-248346
|
P16333
|
O00401
| 1
|
binding
|
up-regulates
| 0.78
|
Nck and cdc42 activate n-wasp by redundant mechanisms.
|
SIGNOR-107634
|
Q14674
|
O60216
| 1
|
cleavage
|
down-regulates quantity by destabilization
| 0.78
|
In order to segregate sister chromatids to opposite poles in anaphase, cohesin has to be removed from chromosomes. In budding yeast, the prevalent mode of cohesin removal is by proteolytic cleavage of the Scc1 subunit at the onset of anaphase by the endopeptidase separase
|
SIGNOR-275537
|
O00206
|
P58753
| 1
|
binding
|
up-regulates activity
| 0.78
|
Here we describe a protein, Mal (MyD88-adapter-like), which joins MyD88 as a cytoplasmic TlR-domain-containing protein in the human genome. Mal activates NF-_B, Jun amino-terminal kinase and extracellular signal-regulated kinase-1 and -2.
|
SIGNOR-252064
|
Q7Z412
|
Q13608
| 1
|
binding
|
up-regulates activity
| 0.78
|
Pex26 recruits Pex6–Pex1 complexes to peroxisomes. Pex26 anchors Pex6 and Pex1 through Pex26–Pex6 and Pex6–Pex1 interactions.
|
SIGNOR-253614
|
Q9BUB5
|
P06730
| 1
|
phosphorylation
|
up-regulates
| 0.779
|
Mnk1 and mnk2 regulate protein synthesis by phosphorylating the initiation factor eif4e.
|
SIGNOR-166646
|
P01106
|
P38936
| 1
|
transcriptional regulation
|
down-regulates quantity by repression
| 0.779
|
C-myc also directly represses transcription of cdk kinase inhibitors including p27kip1, p21cip1, p15ink4b and p16ink4a
|
SIGNOR-102740
|
P03952
|
P01042
| 1
|
cleavage
|
up-regulates activity
| 0.779
|
Bradykinin is a nonapeptide composed of the sequence Arg-Pro-Pro-Gly-Phe-Ser-Pro-Phe-Arg and functions as an inflammatory mediator. BK is the product of the kallikrein–kinin system following activation of FXII. FXIIa leads to proteolysis of PK, and the resulting PKa cleaves HK to generate BK (Figure 1).
|
SIGNOR-263548
|
P18031
|
P35568
| 1
|
dephosphorylation
|
down-regulates
| 0.779
|
Tyrosine dephosphorylation and deactivation of insulin receptor substrate-1 by protein-tyrosine phosphatase 1B. Possible facilitation by the formation of a ternary complex with the Grb2 adaptor protein.
|
SIGNOR-74852
|
Q13418
|
P31749
| 1
|
phosphorylation
|
up-regulates
| 0.779
|
Ilk can phosphorylate pkb-akt on serine-473, whereas kinase-deficient ilk severely inhibits endogenous phosphorylation of pkb-akt on serine-473, demonstrating that ilk is involved in agonist stimulated, pi(3)k-dependent, pkb-akt activation.
|
SIGNOR-252597
|
P04629
|
Q8WU20
| 1
|
binding
|
up-regulates
| 0.779
|
The signaling adapter frs-2 competes with shc for binding to the nerve growth factor receptor trka:a model for discriminating proliferation and differentiation
|
SIGNOR-65955
|
P04629
|
Q92529-2
| 1
|
phosphorylation
|
up-regulates activity
| 0.778
|
We also obtained tryptic phosphopeptide maps of N-Shc protein phosphorylated in vitro by other tyrosine kinases, TrkB, v-Src and EGFR. The overall patterns of the phosphopeptide maps generated by these tyrosine kinases were similar, although there were some differences among these maps (Figure 4a–d).We performed phosphopeptide mapping analysis using GST-fused N-Shc protein, and found that N-Shc phosphorylated by TrkA in vitro was resolved into at least seven phosphopeptides (Y1 through Y7, Figure 4a). Phosphopeptide mapping revealed that N-Shc has novel tyrosine-phosphorylation sites at Y259/Y260 and Y286; in vivo-phosphorylation of these tyrosines was demonstrated by site-specific anti-pTyr antibodies. Phosphorylated Y286 bound to several proteins, of which one was Crk. The pY221/pY222 site, corresponding to one of the Grb2-binding sites of Shc, also preferentially bound to Crk. The phosphorylation-dependent interaction between N-Shc and Crk was demonstrated in vitro and in vivo.
|
SIGNOR-273915
|
Q06187
|
P16885
| 1
|
phosphorylation
|
up-regulates
| 0.778
|
By measuring the ability of human plcgamma2 to restore calcium responses to the b-cell receptor stimulation or oxidative stress in a b-cell line (dt40) deficient in plcgamma2, we have demonstrated that two tyrosine residues, tyr(753) and tyr(759), were important for the plcgamma2 signaling function.Of the two kinases that previously have been proposed to phosphorylate plcgamma2, btk, and syk, purified btk had much greater ability to phosphorylate recombinant plcgamma2 in vitro, whereas syk efficiently phosphorylated adapter protein blnk.
|
SIGNOR-111069
|
Q15796
|
Q9HAU4
| 2
|
binding
|
up-regulates activity
| 0.778
|
We show that in the presence of TGF-beta signalling, Smad2 interacts through its proline-rich PPXY motif with the tryptophan-rich WW domains of Smurf2, a recently identified E3 ubiquitin ligases.Thus, stimulation by TGF-beta can induce the assembly of a Smad2-Smurf2 ubiquitin ligase complex that functions to target substrates for degradation.
|
SIGNOR-108490
|
P01116
|
P48736
| 1
|
binding
|
up-regulates
| 0.778
|
Grb2 binds and activates sos, which then activates ras, and this activates p110 independently of p85./it was also described that ras interacts with pi3k in a direct manner.
|
SIGNOR-59819
|
O75593
|
Q15796
| 1
|
binding
|
up-regulates activity
| 0.778
|
FAST-2 also interacts directly with Smad2, a cytoplasmic protein which is translocated to the nucleus in response to TGF-beta, and forms a multimeric complex with Smad2 and Smad4 on the activin response element, a high-affinity binding site for FAST-1.
|
SIGNOR-108333
|
Q92918
|
Q13094
| 1
|
phosphorylation
|
up-regulates
| 0.778
|
The serine/threonine kinase hpk-1 phosphorylates serine 376 of slp-76 and induces the interaction with 14-3-3 proteins
|
SIGNOR-153613
|
O14965
|
P04637
| 1
|
phosphorylation
|
up-regulates activity
| 0.778
|
The N-terminus of E2F1 can interact directly with a region towards the C-terminus of p53, resulting in increased nuclear retention of p53 and p53-mediated transcription and apoptosis. This is inhibited by competition between p53 and cyclin A at the binding site within E2F19,10. The interaction between p53 and E2F1 is enhanced by phosphorylation of p53 on Ser315, a residue within the E2F1 binding region that is phosphorylated by cell cycle kinases such as cdk1, cdk2, cdk9 and Aurora kinase A
|
SIGNOR-120836
|
P15153
|
Q13153
| 1
|
binding
|
up-regulates
| 0.778
|
This report shows that rac1 binds to and stimulates the kinase activity of pak1 approximately 2- and 4-5-fold, respectively, better than rac2.
|
SIGNOR-59546
|
P28482
|
P04637
| 1
|
phosphorylation
|
up-regulates activity
| 0.778
|
In summary, our results suggest that phosphorylation of p53Thr55 by ERK2 is important for doxorubicin-induced p53 activation and cell death.
|
SIGNOR-279068
|
P01189
|
P32245
| 1
|
binding
|
up-regulates activity
| 0.778
|
The melanocortin (MC) receptor family consists of five Gs-coupled receptors that control various physiological functions in response to four distinct agonists, adrenocorticotropic hormone (ACTH, also known as corticotrophin) and alpha, beta, and gamma melanocyte-stimulating hormone (MSH), which are derived from the proopiomelanocortin precursor protein, and two inverse agonists, agouti and agouti-related proteins
|
SIGNOR-268710
|
Q9HAU4
|
Q15796
| 2
|
ubiquitination
|
down-regulates activity
| 0.778
|
The ability of smurf2 to promote smad2 destruction required the hect catalytic activity of smurf2 and depended on the proteasome-dependent pathway.
|
SIGNOR-236133
|
P12931
|
P03372
| 1
|
phosphorylation
|
up-regulates
| 0.778
|
Although the molecular mechanisms underlying ligand-independent activation of era are not completely understood, phosphorylation of a serine residue in af1 has been implicated in the response to epidermal growth factor. Era is also a target for tyrosine phosphorylation, anda single tyrosine residue located immediately adjacent to af2 has been identified as a substrate for src-family tyrosine kinases.
|
SIGNOR-55857
|
P50750
|
P24928
| 1
|
phosphorylation
|
up-regulates
| 0.777
|
Cyclin-dependent kinase 9 (cdk9) promotes elongation by rna polymerase ii (rnapii), mrna processing, and co-transcriptional histone modification. Cdk9 phosphorylates multiple targets, including the conserved rnapii elongation factor spt5 and rnapii itself
|
SIGNOR-203528
|
P01275
|
P47871
| 1
|
binding
|
up-regulates
| 0.777
|
In contrast, stimulation of gs-coupled receptors by glucagon or epinephrine activates lats1/2 kinase activity, thereby inhibiting yap function.
|
SIGNOR-198504
|
P10911
|
P60953
| 1
|
guanine nucleotide exchange factor
|
up-regulates activity
| 0.777
|
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-260558
|
Q8NFA2
|
Q86UR1
| 1
|
relocalization
|
up-regulates activity
| 0.777
|
Tks4 and Tks5 bind NoxA1 through their SH3 domains in a Rac-independent manner|NoxO1 is required for full Nox1 and Nox3 oxidase activity at least partially because of its role in the plasma membrane recruitment of the NoxA1 activator protein|Tks4 and Tks5 support Nox1- and Nox3-dependent ROS generation
|
SIGNOR-264709
|
Q00535
|
Q9UD71
| 1
|
phosphorylation
|
up-regulates activity
| 0.777
|
We find that DARPP-32 is converted into an inhibitor of PKA when phosphorylated at threonine 75 by cyclin-dependent kinase 5 (Cdk5). Cdk5 phosphorylates DARPP-32 in vitro and in intact brain cells. Phospho-Thr 75 DARPP-32 inhibits PKA in vitro by a competitive mechanism.
|
SIGNOR-250671
|
P21802
|
Q8WU20
| 1
|
phosphorylation
|
up-regulates activity
| 0.777
|
In this report, we demonstrate that FGF stimulation induces tyrosine phosphorylation of a novel lipid anchored docking protein, termed FRS2, that forms a complex with Grb2/Sos, thus linking FGF-receptor activation to the Ras/MAPK signaling pathway.
|
SIGNOR-236950
|
P42345
|
Q8IYT8
| 1
|
phosphorylation
|
down-regulates
| 0.777
|
Mtor phosphorylates a mammalian homologue of atg13 and the mammalian atg1 homologues ulk1 and ulk2
|
SIGNOR-183961
|
Q9NR81
|
P61586
| 1
|
guanine nucleotide exchange factor
|
up-regulates activity
| 0.777
|
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-260530
|
P09341
|
P25025
| 1
|
binding
|
up-regulates activity
| 0.777
|
CXCL1 produces cellular chemotactic activity by binding to the CXC chemokine receptor 2 (CXCR2). In PC, this chemokine has been associated with a variety of carcinogenic mechanisms, including oncogene-induced senescence (OIS), angiogenesis, cancer metastasis, and immunosuppressive microenvironments
|
SIGNOR-277717
|
P06493
|
O60566
| 1
|
phosphorylation
|
up-regulates
| 0.777
|
Here, we demonstrate that bubr1 is phosphorylated on the cdk1 site t620, which triggers the recruitment of plk1 and phosphorylation of bubr1 by plk1 both in vitro and in vivo. Phosphorylation does not appear to be required for spindle checkpoint function but instead is important for the stability of kinetochore-microtubule (kt-mt) interactions
|
SIGNOR-157642
|
P61278
|
P31391
| 1
|
binding
|
up-regulates
| 0.777
|
The five receptor subtypes bind the natural SST peptides, SST-14 and SST-28, with low nanomolar affinity.
|
SIGNOR-82496
|
Q8WXE9
|
P21579
| 1
|
binding
|
up-regulates quantity
| 0.777
|
the monomeric adaptor proteins AP180/CALM and stonin-2 are required for the efficient retrieval of synaptobrevin II (sybII) and synaptotagmin-1 respectively .Stonin-2 and AP-2 are also Required for Efficient Synaptotagmin-1 Retrieval. the monomeric adaptor proteins AP180/CALM and stonin-2 are required for the efficient retrieval of synaptobrevin II (sybII) and synaptotagmin-1 respectively.
|
SIGNOR-264115
|
P01241
|
P16471
| 1
|
binding
|
up-regulates
| 0.777
|
Hprl does not bind to the hgh receptor, but hgh binds to both the hghr and hprlr, and mutagenesis studies have shown that the receptor-binding sites on hgh overlap.
|
SIGNOR-35575
|
O14625
|
P49682
| 1
|
binding
|
up-regulates activity
| 0.777
|
The chemokines CXCL9, 10, and 11 exert their action via CXC chemokine receptor-3 (CXCR3), a receptor highly expressed on activated T cells.
|
SIGNOR-260971
|
O43612
|
O43614
| 1
|
binding
|
up-regulates
| 0.776
|
Identification and initial biological characterization of two orexins as well as their two receptors
|
SIGNOR-55848
|
P50750
|
O00267
| 1
|
phosphorylation
|
up-regulates
| 0.776
|
We describe an evolutionarily conserved repetitive heptapeptide motif (consensus = g-s-r/q-t-p) in the c-terminal region (ctr) of hspt5, which, like the c-terminal domain (ctd) of rna pol ii, is highly phosphorylated by p-tefb. Thr-4 residues of the ctr repeats are functionally important phosphorylation sites. In vitro, thr-4 phosphorylation is critical for the elongation activation activity of dsif
|
SIGNOR-143939
|
Q13705
|
Q15796
| 1
|
phosphorylation
|
up-regulates activity
| 0.776
|
It has been suggested that binding of myostatin to the ActRIIB results in the phosphorylation of two serine residues of Smad2 or Smad3 at COOH domains
|
SIGNOR-254984
|
Q5JTC6
|
P35222
| 1
|
binding
|
down-regulates activity
| 0.776
|
We show that Amer1 binds directly to beta-catenin via a novel interaction motif, the REA repeats. This amino acid motif, including the core sequence arginine, glutamic acid and alanine, and this REA repeats mediate binding of Amer1 to the armadillo repeats of beta-catenin. The data suggest that Amer1 exerts its negative regulatory role in Wnt signaling by acting as a scaffold protein for the beta-catenin destruction complex and promoting stabilization of Axin at the plasma membrane.
|
SIGNOR-217950
|
O60716
|
P33151
| 1
|
binding
|
up-regulates quantity by stabilization
| 0.776
|
To clarify the role of p120 in mammalian cells, we have knocked down p120 with siRNA in cells expressing epithelial (E-), placental (P-), neuronal (N-), and vascular endothelial (VE-) cadherins. We report that each of these cadherins, as well as α- and β-catenins, were rapidly degraded in the absence of p120, resulting in loss of cell–cell adhesion. The effect was clearly dose dependent, indicating that p120 expression levels may directly determine cadherin levels. Degradation of p120-uncoupled cadherin occurred after its arrival at the surface, indicating that p120 regulates cadherin turnover at the level of internalization or recycling. p120 homologues ARVCF and δ-catenin could substitute for p120, so at least one family member is likely required to maintain adhesion. Thus, cadherin complexes are rapidly turned over and degraded in mammalian cells in the absence of direct interaction with p120 or a p120 family member.
|
SIGNOR-252126
|
Q8N2Q7
|
P78352
| 1
|
relocalization
|
up-regulates activity
| 0.776
|
Like NRXNs, NLGNs bind to intracellular PDZ-domain proteins, but in contrast to NRXNs, NLGNs bind to class I PDZ domains such as those contained in PSD95, a postsynaptic MAGUK protein65. PSD95 and its homologues are centrally involved in recruiting glutamate receptors at postsynaptic sites66. Similarly to CASK, PSD95 binds to intracellular adaptor proteins, and especially to GKAP (a protein that binds to the guanylate-kinase domain of PSD95), which, in turn, binds to SHANK proteins (Fig. 1b). A possible role of these interactions is to recruit postsynaptic adaptor proteins to the site of synaptic junctions.
|
SIGNOR-264191
|
Q92837
|
P49841
| 2
|
binding
|
up-regulates
| 0.776
|
The frat family consists of three members: frat-1, -2, and -3. It has been shown that different sites of frat-1 interact with gsk-3 and dvl-1 and that wnt-1 disintegrates the complex formation of frat-1, dvl-1, and axin, resulting in the activation of the wnt signaling pathway
|
SIGNOR-58219
|
O95150
|
Q93038
| 1
|
binding
|
up-regulates
| 0.776
|
The ligand of dr3 is tl1a
|
SIGNOR-103078
|
P51532
|
O14746
| 1
|
binding
|
up-regulates
| 0.776
|
Tert activates wnt reporter plasmids in a brg1-dependent manner.
|
SIGNOR-186607
|
P23443
|
P23588
| 1
|
phosphorylation
|
up-regulates
| 0.776
|
S6k1/s6k2 specifically phosphorylate ser422 in vitro. Substitution of ser422 with ala results in a loss of activity in an in vivo translation assay, indicating that phosphorylation of this site plays an important role in eif4b function.
|
SIGNOR-123997
|
P49841
|
Q92837
| 2
|
phosphorylation
|
down-regulates activity
| 0.776
|
Protein kinase A (PKA) was found to phosphorylate Ser188 in vitro as well as in intact cells. Importantly, activation of endogenous cAMP-coupled beta-adrenergic receptors with norepinephrine stimulated the phosphorylation of FRAT1 at Ser188. GSK-3 was also able to phosphorylate FRAT1 at Ser188 and other residues in vitro or when overexpressed in intact cells. Phosphorylation of Ser188 by PKA inhibited the ability of FRAT1 to activate beta-catenin-dependent transcription.
|
SIGNOR-276057
|
Q16539
|
P42574
| 1
|
phosphorylation
|
down-regulates
| 0.775
|
Consequently, p38-mapk can directly phosphorylate and inhibit the activities of caspase-8 and caspase-3 and thereby hinder neutrophil apoptosis, and, in so doing, regulate the inflammatory response.
|
SIGNOR-122099
|
Q9BXM7
|
Q8IXI2
| 1
|
phosphorylation
|
down-regulates quantity by destabilization
| 0.775
|
PINK1 phosphorylates Miro, a component of the primary motor/adaptor complex that anchors kinesin to the mitochondrial surface. The phosphorylation of Miro activates proteasomal degradation of Miro in a Parkin-dependent manner. in Miro1, Ser156 (homologous to Ser182 in Drosophila) and Thr298, 299 (homologous to Ser324, 325 in Drosophila, Figure 6C).
|
SIGNOR-272728
|
Q96PU5
|
P37088
| 1
|
ubiquitination
|
down-regulates quantity by destabilization
| 0.775
|
The serum and glucocorticoid inducible kinase 1 (SGK1) is induced in the aldosterone sensitive distal nephron (ASDN) where it may stimulate Na reabsorption, partly by inhibiting ubiquitin ligase Nedd4-2-mediated retrieval of epithelial Na+ channel ENaC from the luminal membrane.
|
SIGNOR-251948
|
P31749
|
P55211
| 1
|
phosphorylation
|
down-regulates activity
| 0.775
|
Akt phosphorylated recombinant casp9 in vitro on serine-196 and inhibited its protease activity
|
SIGNOR-252581
|
Q04759
|
Q9BXL7
| 1
|
phosphorylation
|
up-regulates activity
| 0.775
|
NF-kappaB activation is triggered by PKCteta-dependent phosphorylation of Carma1 after TCR/CD28 co-stimulation. PKCteta-phosphorylated Carma1 was suggested to function as a molecular scaffold that recruits preassembled Bcl10-Malt1 complexes to the membrane|we demonstrate that PP2A removes PKCteta-dependent phosphorylation of Ser645 in Carma1, and show that maintenance of this phosphorylation is correlated with increased T-cell activation.
|
SIGNOR-249193
|
P78352
|
Q9P244
| 1
|
binding
|
up-regulates activity
| 0.775
|
SALMs 1-3 contain a C-terminal PDZ-binding motif, which interacts with PSD-95, an abundant postsynaptic scaffolding protein, whereas SALM4 and SALM5 lack PDZ binding. Interactions between SALMs 1–3 and PSD-95 family proteinscould serve a number of functions. SALM1 and SALM2, which lack the ability to interact with a presynaptic ligand and thus cannot be directly targeted to sites of early synaptic adhesion, may require PSD-95 binding for their localization to early synapses.
|
SIGNOR-264095
|
P29597
|
P42224
| 1
|
phosphorylation
|
up-regulates activity
| 0.775
|
Co-expression of Stat1 with Tyk2, Jak1, or Jak2 resulted in the specific tyrosine phosphorylation of Stat1 at Tyr701Phosphorylation of purified Stat1 was necessary and sufficient for the acquisition of DNA binding activity.
|
SIGNOR-246943
|
P12931
|
P01112
| 1
|
phosphorylation
|
down-regulates activity
| 0.775
|
Src binds to and phosphorylates GTP-, but not GDP-, loaded Ras on a conserved Y32 residue within the switch I region in vitro and that in vivo, Ras-Y32 phosphorylation markedly reduces the binding to effector Raf and concomitantly increases binding to GTPase-activating proteins and the rate of GTP hydrolysis
|
SIGNOR-252093
|
P42574
|
P09874
| 1
|
cleavage
|
down-regulates activity
| 0.775
|
Caspase-3 cleaves parp-1. During cd95-mediated apoptosis proteolytic inactivation of parp-1 by caspases prevents atp depletion and thereby ensures the execution of the apoptotic process
|
SIGNOR-116178
|
Q13315
|
P54132
| 1
|
phosphorylation
|
up-regulates
| 0.775
|
Mitotic phosphorylation of blm was partially dependent on atm, and phosphorylation sites on blm were identified. A phosphospecific antibody against one of these sites (thr-99) revealed radiation-induced phosphorylation, which was defective in ataxia-telangiectasia cells. These data suggest that atm and blm function together in recognizing abnormal dna structures by direct interaction and that these phosphorylation sites in blm are important for radiosensitivity status but not for sce frequency.
|
SIGNOR-88010
|
P43405
|
P19174
| 1
|
phosphorylation
|
up-regulates activity
| 0.775
|
Syk isolated from antigen receptor-activated B cells phosphorylated PLC-gamma1 on Tyr-771 and the key regulatory residue Tyr-783 in vitro, whereas Lyn from the same B cells phosphorylated PLC-gamma1 only on Tyr-771.
|
SIGNOR-246576
|
P41221
|
Q01974
| 1
|
binding
|
up-regulates
| 0.775
|
Wnt5a induces ROR1/ROR2 heterooligomerization to enhance leukemia chemotaxis and proliferation|Evolutionarily conserved receptor tyrosine kinase–like orphan receptor-1 and -2 (ROR1/2) are considered distinct receptors for Wnt5a and are implicated in noncanonical Wnt signaling in organogenesis and cancer metastasis.
|
SIGNOR-199647
|
P45983
|
Q07817
| 1
|
phosphorylation
|
down-regulates
| 0.775
|
By site-directed mutagenesis studies, we have identified that serine 62 is the necessary site for taxol- or 2-me-induced bcl-xl phosphorylation in prostate cancer cells. Further studies with the inhibitor of jun kinase (jnk) and phosphorylation mutant of bcl-xl reveal the augmentative role of jnk-mediated bcl-xl phosphorylation in apoptosis of prostate cancer cells. In summary, our studies suggest that the phosphorylation of bcl-xl by stress response kinase signaling might oppose the anti-apoptotic function of bcl-xl to permit prostate cancer cells to die by apoptosis
|
SIGNOR-99219
|
P35222
|
P46531
| 1
|
binding
|
up-regulates
| 0.775
|
Beta-catenin can regulate the level and transcriptional activity of the notch1 and notch1 intracellular domain (nicd). The in vivo and in vitro results demonstrate that beta-catenin binds with notch1 and nicd, for which its armadillo repeat domain is essential.
|
SIGNOR-236858
|
Q96G74
|
Q13114
| 1
|
deubiquitination
|
down-regulates activity
| 0.775
|
TRAF3 is an E3 ubiquitin ligase that preferentially assembled lysine-63-linked polyubiquitin chains. DUBA selectively cleaved the lysine-63-linked polyubiquitin chains on TRAF3, resulting in its dissociation from the downstream signaling complex containing TANK-binding kinase 1.
|
SIGNOR-265873
|
Q13459
|
P61586
| 1
|
gtpase-activating protein
|
down-regulates activity
| 0.774
|
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-260509
|
O00253
|
P32245
| 1
|
binding
|
down-regulates
| 0.774
|
Recombinant agouti-related protein was a potent, selective antagonist of mc3r and mc4r,.
|
SIGNOR-51104
|
Q9NZD4
|
P69905
| 1
|
binding
|
up-regulates quantity by stabilization
| 0.774
|
α-Hemoglobin stabilizing protein (AHSP) binds α-hemoglobin (Hb), avoiding its precipitation and its pro-oxidant activity.
|
SIGNOR-251770
|
O60674
|
P48357
| 2
|
phosphorylation
|
up-regulates activity
| 0.774
|
LRb signaling is initiated by leptin binding to the extracellular domain of the LRb dimer, leading to Jak2 transphosphorylation and activation. Activated Jak2 mediates the tyrosine phosphorylation of Tyr985 and Tyr1138of LRb. These phosphotyrosine residues immediately function as binding sites (double-ended lines) for SHP-2 and STAT3, both of which quickly become tyrosine-phosphorylated by Jak2.
|
SIGNOR-263494
|
P00738
|
P68871
| 1
|
binding
|
down-regulates quantity
| 0.774
|
Haptoglobin forms a complex of extremely high affinity with Hb via a well-characterized globin site. Our results show that upon Hb-haptoglobin binding, the globin radical, loses its ability to be terminated by forming globin dimers.
|
SIGNOR-251815
|
P48357
|
O60674
| 2
|
binding
|
up-regulates activity
| 0.774
|
Janus kinase 2 (JAK2) is associated with LEPRb and autophosphorylates in response to leptin. JAK2 also phosphorylates LEPRb, STAT3, and multiple other downstream molecules.
|
SIGNOR-263491
|
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