4.6 Article

Immunological and classical subtypes of oral premalignant lesions

期刊

ONCOIMMUNOLOGY
卷 7, 期 12, 页码 -

出版社

TAYLOR & FRANCIS INC
DOI: 10.1080/2162402X.2018.1496880

关键词

Oral leukoplakia; immune infiltrate; premalignant; molecular subtypes; prevention; biomarker; oral cancer

资金

  1. Canceropole Lyon Auvergne Rhone-Alpes (CLARA) 2014-2016 Structured Program [CVPPRCAN000153]
  2. LYric Grant [INCa-DGOS-4664]
  3. Projets libres de recherche Biologie et Sciences du Cancer [INCa-PLBIO17-338]
  4. Annee recherche-Assistance Publique des Hopitaux de Paris
  5. Soutien pour la formation a la recherche translationnelle en cancerologie from INCa
  6. AVIESAN
  7. Fondation Synergie Lyon-Cancer
  8. NCI [CVPPRCAN000153, P30-CA023100-29, HHSN2612012000311, R01DE026644-01, NCI HHSN2612012000311, NCI P30-CA023100-29]
  9. Targeting Signaling Vulnerabilities for Oral Cancer Prevention [R01DE026644-01]

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Oral squamous cell carcinoma (OSCC) is a major cause of cancer-associated morbidity and mortality and may develop from oral premalignant lesions (OPL). An improved molecular classification of OPL may help refining prevention strategies. We identified two main OPL gene-expression subtypes, named immunological and classical, in 86 OPL (discovery dataset). A gene expression-based score was then developed to classify OPL samples from three independent datasets, including 17 (GSE30784),13 (GSE10174) and 15 (GSE85195) OPLs, into either one of the two gene-expression subtypes. Using the single sample gene set enrichment analysis, enrichment scores for immune-related pathways were different between the two OPL subtypes. In OPL from the discovery set, loss of heterozygosities (LOH) at 3p14, 17p13, TP53, 9p21 and 8p22 and miRNA gene expression profiles were analyzed. Deconvolution of the immune infiltrate was performed using the Microenvironment Cell Populations-counter tool. A multivariate analysis revealed that decreased miRNA-142-5p expression (P = 0.0484) and lower T-cell, monocytic and myeloid dendritic cells (MDC) immune infiltration (T-cells, P = 0.0196; CD8 T cells, P = 0.0129; MDC, P = 0.0481; and monocytes, P = 0.0212) were associated with oral cancer development in the immunological subtype only. In contrast, LOH at 3p14 (P = 0.0241), 17p13 (P = 0.0348) and TP53 (P = 0.004) were associated with oral cancer development in the classical subtype only. In conclusion, we identified 2 subtypes of OPLs, namely immune and classical, which may benefit from different and specific personalized prevention interventions.

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