Lymphocyte antigen 6G6D-mediated modulation through p38α MAPK and DNA methylation in colorectal cancer.

Anti-tumor immunity Colorectal cancer DNA methylation Lymphocyte antigen 6G6D

Journal

Cancer cell international
ISSN: 1475-2867
Titre abrégé: Cancer Cell Int
Pays: England
ID NLM: 101139795

Informations de publication

Date de publication:
11 Aug 2022
Historique:
received: 19 02 2022
accepted: 27 06 2022
entrez: 11 8 2022
pubmed: 12 8 2022
medline: 12 8 2022
Statut: epublish

Résumé

In addition to being novel biomarkers for poor cancer prognosis, members of Lymphocyte antigen-6 (Ly6) gene family also play a crucial role in avoiding immune responses to tumors. However, it has not been possible to identify the underlying mechanism of how Ly6 gene regulation operates in human cancers. Transcriptome, epigenome and proteomic data from independent cancer databases were analyzed in silico and validated independently in 334 colorectal cancer tissues (CRC). RNA mediated gene silencing of regulatory genes, and treatment with MEK and p38 MAPK inhibitors were also tested in vitro. We report here that the Lymphocyte antigen 6G6D is universally downregulated in mucinous CRC, while its activation progresses through the classical adenoma-carcinoma sequence. The DNA methylation changes in LY6G6D promoter are intimately related to its transcript regulation, epigenomic and histological subtypes. Depletion of DNA methyltransferase 1 (DNMT1), which maintains DNA methylation, results in the derepression of LY6G6D expression. RNA-mediated gene silencing of p38α MAPK or its selective chemical inhibition, however, reduces LY6G6D expression, reducing trametinib's anti-inflammatory effects. Patients treated with FOLFOX-based first-line therapy experienced decreased survival due to hypermethylation of the LY6G6D promoter and decreased p38α MAPK signaling. We found that cancer-specific immunodominant epitopes are controlled by p38α MAPKs signaling and suppressed by DNA methylation in histological variants with Mucinous differentiation. This work provides a promising prospective for clinical application in diagnosis and personalized therapeutic strategies of colorectal cancer.

Identifiants

DOI: 10.1186/s12935-022-02672-1 PMID: 35953834 PMC: PMC9373545
pubmed: 35953834
doi: 10.1186/s12935-022-02672-1
pii: 10.1186/s12935-022-02672-1
pmc: PMC9373545
doi:

Types de publication

Journal Article

Langues

eng

Pagination

253

Subventions

Organisme : MIUR "FFABR"
ID : n.4982

Informations de copyright

© 2022. The Author(s).

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Auteurs

Francesca Pia Caruso (FP)

Bioinformatics Laboratory, BIOGEM scrl, Ariano Irpino, Avellino, Italy.

Mario Rosario D'Andrea (MR)

UOSD Oncologia, Ospedale S. Paolo, 00053, Civitavecchia, Italy.

Luigi Coppola (L)

UOC Anatomia ed Istologia Patologica e Citologia Diagnostica, Dipartimento dei Servizi Diagnostici e della Farmaceutica, Ospedale Sandro Pertini, ASL Roma 2, 00157, Rome, Italy.

Matteo Landriscina (M)

Laboratory of Pre-Clinical and Translational Research, IRCCS, Referral Cancer Center of Basilicata (CROB), Rionero in Vulture, Potenza, Italy.

Valentina Condelli (V)

Laboratory of Pre-Clinical and Translational Research, IRCCS, Referral Cancer Center of Basilicata (CROB), Rionero in Vulture, Potenza, Italy.

Luigi Cerulo (L)

Bioinformatics Laboratory, BIOGEM scrl, Ariano Irpino, Avellino, Italy.

Guido Giordano (G)

Unit of Medical Oncology and Biomolecular Therapy, Department of Medical and Surgical Sciences, University of Foggia, Policlinico Riuniti, 71122, Foggia, Italy. guido.giordano@unifg.it.

Almudena Porras (A)

Department of Biochemistry and Molecular Biology, Faculty of Pharmacy, Complutense University Madrid, 28040, Madrid, Spain. maporras@ucm.es.
Health Research Institute of the Hospital Clínico San Carlos (IdISSC), 28040, Madrid, Spain. maporras@ucm.es.

Massimo Pancione (M)

Department of Sciences and Technologies, University of Sannio, Benevento, Italy. massimo.pancione@unisannio.it.

Classifications MeSH