Proteomics

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SOX4 AND SMARCA4 COOPERATIVELY REGULATE PI3K SIGNALING THROUGH TRANSCRIPTIONAL ACTIVATION OF TGFBR2 IN TRIPLE NEGATIVE BREAST CANCER


ABSTRACT: Dysregulation of PI3K/Akt signaling is a dominant feature in basal-like or triple-negative breast cancers (TNBC). However, the mechanisms regulating this pathway are largely unknown in this subset of aggressive tumors. Here we demonstrate that the transcription factor SOX4 is a key regulator of PI3K signaling in TNBC. Genomic and proteomic analyses coupled with mechanistic studies identified TGFBR2 as a direct transcriptional target of SOX4 and demonstrated that TGFBR2 is required to mediate SOX4-dependent PI3K signaling. We further report that SOX4 and the SWI/SNF ATPase SMARCA4, which are uniformly overexpressed in basal-like tumors, form a previously unreported complex that is required to maintain an open chromatin conformation at the TGFBR2 regulatory regions in order to mediate TGFBR2 expression and PI3K signaling. Collectively, our findings delineate the mechanism by which SOX4 and SMARCA4 cooperatively regulate PI3K/Akt signaling and suggest that this complex may play an essential role in TNBC genesis and/or progression. Kinase enrichment proteomic analysis was performed using HCC1143 breast cancer cells treated with a control siRNA pool or a pool targeting SOX4 in biological triplicate to evaluate the effects on the functional kinome.

INSTRUMENT(S): Q Exactive

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Epithelial Cell, Breast

DISEASE(S): Breast Cancer

SUBMITTER: Steven Angus  

LAB HEAD: Michael L. Gatza, PhD

PROVIDER: PXD022596 | Pride | 2021-03-03

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
2020_11_177_QEPlus_Angus_SOX4_1.raw Raw
2020_11_177_QEPlus_Angus_SOX4_2.raw Raw
2020_11_177_QEPlus_Angus_SOX4_3.raw Raw
2020_11_177_QEPlus_Angus_ctrl1.raw Raw
2020_11_177_QEPlus_Angus_ctrl2.raw Raw
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