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Interaction ID

Mol A

Type

Species

Verb

Nature

Mol B

Type

Species

14835

IL1R1

Protein

Homo sapiens

Bind

direct

RAC1

Protein

Homo sapiens

Glutathione S-transferase (GST) fusion proteins, containing either the full-length IL-1R cytosolic domain (GST-IL-1Rcd) or the terminal 68 amino acids of IL-1R required for IL-1-dependent signal transduction, specifically coprecipitated both RhoA and Rac-1, but not p21(ras), from Triton-soluble HeLa cell extracts.

Structure

Disease

Interaction id

14835

MOLECULE A

3554

Type

Protein

Species

Homo sapiens

Attribute

Structure Details

Disease Details

MOLECULE B

5879

Type

Protein

Species

Homo sapiens

Attribute

Structure Details

Disease Details

Kinetics

General Information

Interaction term

Bind ( direct )

Pathway

Cytokine And Chemokine Mediated Signaling Pathway:IL1 Signaling Pathway

Disease Details

disease: :Inflammation

Experimental location and method

Experimental method::Immunoprecipitation
species::Human
cell::HeLa cells

Comments

Domain_motif_site_residue

(PF01582)[RES:Terminal 68 amino acids](IL1R1)

References

PubMed Id

10359565

Author

Singh R, Wang B, Shirvaikar A, Khan S, Kamat S, Schelling JR, Konieczkowski M, Sedor JR

Title

The IL-1 receptor and Rho directly associate to drive cell activation in inflammation.

129994

RAC1

Protein

Homo sapiens-e

Increases activity

indirect

p38 MAPK

Family

Homo sapiens-e

Constitutively activated forms of Rac and Cdc42Hs are efficient activators of a cascade leading to JNK and p38/Mpk2 activation.

Interaction id

129994

MOLECULE A

5879

Type

Protein

Species

Homo sapiens-e

Attribute

Structure Details

Disease Details

MOLECULE B

EZHsF00051

Type

Family

Species

Homo sapiens-e

Attribute

Structure Details

Disease Details

Kinetics

General Information

Interaction term

Increases activity ( indirect )

Pathway

Small GTPase Mediated Signal Transduction:RAC Protein Signal Transduction

References

PubMed Id

7600582

Author

Minden A, Lin A, Claret FX, Abo A, Karin M

Title

Selective activation of the JNK signaling cascade and c-Jun transcriptional activity by the small GTPases Rac and Cdc42Hs.

172637

Rac1

Protein

Mus musculus

Increases activity

direct

Map3k1

Protein

Mus musculus

We investigate here the transcriptional activation of the murine PGS2 gene in NIH 3T3 cells, in response to the mitogens platelet-derived growth factor (PDGF) or serum. / Cotransfection of plasmids expressing dominant-negative Ras, Rac1, MEKK-1, or JNK along with the [PGS2][luciferase] reporter prevents induction by PDGF or serum, demonstrating that serum and PDGF induction of the PGS2 gene in NIH 3T3 cells requires activation of a Ras/Rac1/MEKK-1/JNK kinase/JNK signal transduction leading to phosphorylation of c-Jun.

Interaction id

172637

MOLECULE A

19353

Type

Protein

Species

Mus musculus

Attribute

Structure Details

Disease Details

MOLECULE B

26401

Type

Protein

Species

Mus musculus

Attribute

Structure Details

Disease Details

Kinetics

General Information

Interaction term

Increases activity ( direct )

Pathway

Transmembrane Receptor Protein Tyrosine Kinase Signaling Pathway:Platelet-Derived Growth Factor Receptor Signaling PathwaySmall GTPase Mediated Signal Transduction:RAC Protein Signal Transduction

Interaction result

Other Resultant

Leads to activation of Jnkk and increased activation of Ptgs2 gene

Experimental location and method

Experimental method::Dominant negative analysis
species::Mouse
condition::Platelet-derived growth factor treated cells
cell::NIH3T3 cells

Comments

Property

Dominant negative molecule:Rac1

References

PubMed Id

8940199

Author

Xie W, Herschman HR

Title

Transcriptional regulation of prostaglandin synthase 2 gene expression by platelet-derived growth factor and serum.