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CDH1 — PIK3R1

Pathways - manually collected, often from reviews:

• NCI Pathway Database E-cadherin signaling in keratinocytes: E-cadherin/Ca2+/beta catenin-gamma catenin/alpha catenin/p120 catenin complex (CDH1-CTNNB1_JUP-CTNNA1-CTNND1) → PI3K complex (PIK3CA-PIK3R1) (modification, activates)
  Xie et al., Mol Biol Cell 2005, Xie et al., J Biol Chem 2007
  Evidence: assay, physical interaction
• NCI Pathway Database a6b1 and a6b4 Integrin signaling: PI3K complex (PIK3CA-PIK3R1) → E-cadherin (CDH1) (modification, collaborate) Chartier et al., J Cell Sci 2006
  Evidence: mutant phenotype, assay

Text-mined interactions from Literome

De Santis et al., Oncogene 2009 (Ovarian Neoplasms) : E-cadherin directly contributes to PI3K/AKT activation by engaging the PI3K-p85 regulatory subunit to adherens junctions of ovarian carcinoma cells
Georgopoulos et al., PloS one 2010 : Functional inactivation of E-cadherin interferes with the capacity of NHU cells to form stable calcium mediated contacts, attenuates E-cadherin mediated PI3-K/AKT induction and enhances NHU cell proliferation by allowing de-repression of the EGFR/ERK pathway and constitutive activation of ß-catenin-TCF signalling
Lau et al., Oncogene 2011 (Ovarian Neoplasms) : E-cadherin inhibits tumor cell growth by suppressing PI3K/Akt signaling via ß-catenin-Egr1 mediated PTEN expression ... Thus, the loss of E-cadherin itself may contribute to dysregulated PI3K/Akt signaling through its effects on PTEN, or it may exacerbate the frequent activation of PI3K/Akt signaling that occurs as a result of overexpression, mutation and/or amplification
Lau et al., PloS one 2013 (Neoplasm Invasiveness...) : The pharmacological inhibition of phosphatidylinositol-3-kinase (PI3K), mammalian target of rapamycin (mTOR), and MEK suggests that both PI3K/Akt/mTOR and MAPK/ERK signaling are required for FGF2 induced E-cadherin down-regulation