An interaction is inferred when a bait protein is affinity captured from cell extracts by either polyclonal antibody or epitope tag and the associated interaction partner is identified by mass spectrometric methods.

Publication

Combinatorial targeting of a chromatin complex comprising Dot1L, menin and the tyrosine kinase BAZ1B reveals a new therapeutic vulnerability of endocrine therapy-resistant breast cancer.

Salvati A, Melone V, Sellitto A, Rizzo F, Tarallo R, Nyman TA, Giurato G, Nassa G, Weisz A

Targeting vulnerabilities of cancer cells by inhibiting key regulators of cell proliferation or survival represents a promising way to overcome resistance to current therapies. In breast cancer (BC), resistance to endocrine therapy results from constitutively active or aberrant estrogen receptor alpha (ER?) signaling to the genome. Targeting components of the ER? pathway in these tumors represents, therefore, a rational way ... [more]

Breast Cancer Res Dec. 18, 2021; 24(1);52 [Pubmed: 35850772]

Throughput

Low Throughput

Curated By

BioGRID

Interaction Summary

DOT1L

Gene Ontology Biological Process

Gene Ontology Molecular Function

histone-lysine N-methyltransferase activity [IDA]protein binding [IPI]transcription factor binding [IPI]

ARPC3

Gene Ontology Biological Process

Gene Ontology Molecular Function

actin filament binding [IDA]protein binding [IPI]structural constituent of cytoskeleton [IDA]

Gene Ontology Cellular Component

Affinity Capture-MS

Publication

Combinatorial targeting of a chromatin complex comprising Dot1L, menin and the tyrosine kinase BAZ1B reveals a new therapeutic vulnerability of endocrine therapy-resistant breast cancer.

Throughput

Curated By

histone-lysine N-methyltransferase activity [IDA]
protein binding [IPI]
transcription factor binding [IPI]

actin filament binding [IDA]
protein binding [IPI]
structural constituent of cytoskeleton [IDA]