Proteomics

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The proteomic landscape of CTNNB1 mutated low-grade early-stage endometrial carcinomas


ABSTRACT: Endometrial carcinoma is the most frequent gynecologic malignancy in western countries. In recent years, mutations in CTNNB1 have been associated with worse prognosis in low-risk carcinomas. However, there is a lack of understanding of the proteomic implications of CTNNB1 mutations in this type of tumor. In this study, we performed shotgun proteomics using Formalin Fixed Paraffin Embedded (FFPE) tissue samples of CTNNB1 mutated and wild type low-risk endometrial carcinomas. A publicly available proteomic and transcriptomic database was used to validate results. Differential protein expression and Gene Set Enrichment Analysis revealed dysregulation of pathways associated with cell keratinization, immune response modulation, and intracellular calcium regulation. CTNNB1 mutated tumors showed immune dysregulation at multiple levels including cytokine secretion, cell adhesion, and lymphocyte activation. These results were supported by tissue multiplex immunofluorescence analysis, demonstrating reduced CD8 tumor infiltrating lymphocytes and different immune spatial interaction patterns. Intracellular calcium dysfunction was associated with key transcript dysregulation. We found an increased expression of CAMK2A and ROR2, suggesting a potential role for non-canonical Wnt pathway activation in CTNNB1 mutated tumors.

INSTRUMENT(S):

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Uterine Endometrium

DISEASE(S): Endometrial Cancer

SUBMITTER: Alberto Pelaez García  

LAB HEAD: Alberto Pelaez-Garcia

PROVIDER: PXD068004 | Pride | 2025-11-24

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
TMT_1_EP_F_1_5.raw Raw
TMT_1_EP_F_2_6.raw Raw
TMT_1_EP_F_3_7.raw Raw
TMT_1_EP_F_4_8.raw Raw
TMT_2_EP_F_1_5.raw Raw
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Publications


Endometrial carcinoma is the most frequent gynecologic malignancy in western countries. In recent years, mutations in <i>CTNNB1</i> have been associated with worse prognosis in low-risk carcinomas. However, there is a lack of understanding of the proteomic implications of <i>CTNNB1</i> mutations in this type of tumor. In this study, we performed shotgun proteomics using Formalin-Fixed Paraffin-Embedded (FFPE) tissue samples of <i>CTNNB1</i> mutated and wild-type low-risk endometrial carcinomas.  ...[more]

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