Crosstalk from Estrogen signaling pathway to Notch signaling pathway

List of curated literature with evidence for crosstalk from Estrogen signaling pathway to Notch signaling pathway

  • Cross-talk between notch and the estrogen receptor in breast cancer suggests novel therapeutic approaches.

    • PubMed ID : 18593923
    • Molecule in Estrogen signaling pathway: estrogen
    • Species : Homo sapiens
    • Transcription : no

    • Molecule in Notch signaling pathway: unknown
    • Tissue breast
    • Regulation type : Inhibiting
    • Sentence from paper : Our data suggest that estrogen inhibits Notch signaling through an ERa-dependent effect

  • Targeting Notch signaling cross-talk with estrogen receptor and ErbB-2 in breast cancer.

    • PubMed ID : 19344631
    • Molecule in Estrogen signaling pathway: 17beta-estradiol
    • Species : Homo sapiens
    • Transcription : no

    • Molecule in Notch signaling pathway: NOTCH1
    • Tissue breast
    • Regulation type : Inhibiting
    • Sentence from paper : We determined that in 17β-estradiol-treated cells, Notch-1 is primarily distributed to the cell membrane but it is not efficiently activated by Notch ligands

  • Role of Notch and its oncogenic signaling crosstalk in breast cancer.

    • PubMed ID : 21193018
    • Molecule in Estrogen signaling pathway: ESR1
    • Species : Homo sapiens
    • Transcription : yes

    • Molecule in Notch signaling pathway: NOTCH1
    • Tissue MCF-7 cell
    • Regulation type : Activating
    • Sentence from paper : E2 promoted 8-fold and 6-fold increase in Notch1 and JAG1 expression, respectively, in breast cancer MCF-7 cells

  • Role of Notch and its oncogenic signaling crosstalk in breast cancer.

    • PubMed ID : 21193018
    • Molecule in Estrogen signaling pathway: ESR1
    • Species : Homo sapiens
    • Transcription : yes

    • Molecule in Notch signaling pathway: JAG1
    • Tissue MCF-7 cell
    • Regulation type : Activating
    • Sentence from paper : E2 promoted 8-fold and 6-fold increase in Notch1 and JAG1 expression, respectively, in breast cancer MCF-7 cells

  • GPER activates Notch signaling in breast cancer cells and cancer-associated fibroblasts (CAFs).

    • PubMed ID : 24275097
    • Molecule in Estrogen signaling pathway: GPER1
    • Species : Homo sapiens
    • Transcription : yes

    • Molecule in Notch signaling pathway: NOTCH1
    • Tissue breast
    • Regulation type : Activating
    • Sentence from paper : The mechanism through which GPER leads to Notch-1 activation seems to be transcriptional, as an increase of Notch-1 mRNA levels was found in response to E2 and G-1

  • GPER activates Notch signaling in breast cancer cells and cancer-associated fibroblasts (CAFs).

    • PubMed ID : 24275097
    • Molecule in Estrogen signaling pathway: GPER1
    • Species : Homo sapiens
    • Transcription : yes

    • Molecule in Notch signaling pathway: HES1
    • Tissue SK-BR-3 cell
    • Regulation type : Activating
    • Sentence from paper : We show that estradiol and the GPER selective ligand G-1 induce both the y-secretase-dependent activation of Notch1 and the expression of the Notch target gene Hes-1.

Molecules mediating the crosstalk
Molecule in Estrogen signaling pathwayMolecule in Notch signaling pathwayTissueSpeciesPubMed Identifier
estrogenunknownbreastHomo sapiens18593923
17beta-estradiolNOTCH1breastHomo sapiens19344631
ESR1NOTCH1MCF-7 cellHomo sapiens21193018
ESR1JAG1MCF-7 cellHomo sapiens21193018
GPER1NOTCH1breastHomo sapiens24275097
GPER1HES1SK-BR-3 cellHomo sapiens24275097

Note: We direct each interaction from the molecule in the first pathway to the molecule in the second pathway. The direction of the interaction does not imply that the first molecule regulates the second molecule or that they directly interact. Hence, the interactions in this network may be indirect and may not indicate any mechanism.

Attribute NameDescription
Pathway A

The name of the upstream (first) pathway in a pair of crosstalking pathways.

Pathway B

The name of the downstream (second) pathway in a pair of crosstalking pathways.

Pubmed Query

The string used as a structured query in PubMed that returned the recorded PMID as a result.

PMID

The PubMed identifier for the reported publication.
We recorded "NO_RESULTS_FOR_PUBMED_QUERY" as a dummy PMID when the PubMed query returned no results.

Crosstalk

yes, if Pathway A elicits a downstream transcriptional response in Pathway B.
no, otherwise.

Transcriptional

yes, if the crosstalk is transcriptional.
no, otherwise.

Regulation type

The downstream effect on Pathway B. This attribute can take one of the following two values:

  • Activating: Stimulation of Pathway A up-regulates a gene or activates a protein that is representative of Pathway B.
  • Inhibiting: Stimulation of Pathway A down-regulates a gene or inhibits a protein that is representative of Pathway B.
Molecule A*

The molecule in Pathway A responsible for mediating crosstalk to Pathway B.

Molecule A Identifier

Unique identifier for Molecule A in the namespace recorded in "Molecule A Source", e.g., the UniProt ID of a protein.

Molecule A Source

The name of database that the value in "Molecule A Identifier" comes from, e.g., "UniProt" if the molecule is a protein.

Molecule B*

The molecule in Pathway B responsible for mediating crosstalk from Pathway A.

Molecule B Identifier

Unique identifier for Molecule B in the namespace recorded in "Molecule B Source", e.g., the UniProt ID of a protein.

Molecule B Source

The name of database that the value in "Molecule B Identifier" comes from, e.g., "UniProt" if the molecule is a protein.

Species

The name of the species in which the crosstalk was observed.

Tissue

The name of the tissue or cell line in which the crosstalk was observed.

BTO ID

The BRENDA Tissue Ontology (BTO) Identifier of the tissue or cell line in which the crosstalk was observed.

Condition

Notes on the experimental condition in the publication.

Sentence from paper

The sentence in the publication supporting the crosstalk. We record a sentence only if it states that Pathway A increases or decreases Pathway B signaling. The sentence may also include information about the proteins or genes responsible for mediating the crosstalk.

Misleading evidence for crosstalk

A sentence in the paper that appears to support evidence for crosstalk when the study does not conclude there is crosstalk.

Additional notes

A curator's notes that may provide rationale for the values recorded for the attributes.

*This attribute may represent either an individual molecule or several molecules. We use the following syntax for this attribute.

  • colon (:): The molecules participate in the complex, e.g., SMAD3:SMAD4 in the case of crosstalk from the TGF-beta signaling pathway to the Hippo signaling pathway (the complex consisting of SMAD3 and SMAD4 mediates this crosstalk).
  • slash (/): Either of the molecules can mediate the crosstalk, e.g., YAP1/WWTR1 for the same pair of pathways (YAP1 or WWTR1 can mediate the crosstalk).
  • comma (,): All the molecules are required for the crosstalk but they do not form a complex, e.g., TSC2,RPTOR for the crosstalk from the MAPK signaling pathway to the mTOR signaling pathway (both TSC2 and RPTOR act as mediators).
  • brackets ([]): If we cannot identify the specific molecule, we record all molecules in the family, e.g., [TEAD1/TEAD2/TEAD3/TEAD4]. In this case, the publication only listed the protein TEAD as mediating the crosstalk (from the Hippo signaling pathway to the Wnt signaling pathway).