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一种独特的基因表达特征在黑色素瘤患者的肿瘤阳性或肿瘤阴性前哨淋巴结中存在显著差异表达。

A unique gene expression signature is significantly differentially expressed in tumor-positive or tumor-negative sentinel lymph nodes in patients with melanoma.

作者信息

Tarhini Ahmad A, Floros Theofanis, Lin Hui-Min, Lin Yan, Rahman Zahra, Ashraf Madeeha, Vallabhaneni Priyanka, Sander Cindy, Rao Uma N M, Panelli Monica, LaFramboise William A, Kirkwood John M

机构信息

aDepartment of Medicine, University of Pittsburgh School of Medicine bUniversity of Pittsburgh Cancer Institute cUniversity of Pittsburgh Medical Center, Pittsburgh, Pennsylvania, USA dAthens Naval and Veterans Hospital, Athens, Greece.

出版信息

Melanoma Res. 2017 Oct;27(5):429-438. doi: 10.1097/CMR.0000000000000383.

Abstract

The purpose of this study was to learn whether molecular characterization through gene expression profiling of node-positive and node-negative sentinel lymph nodes (SLNs) in patients with clinical stage I and II melanoma may improve the understanding of mechanisms of metastasis and identify gene signatures for SLNs/SLNs that correlate with diagnosis or clinical outcome. Gene expression profiling was performed on SLN biopsies of 48 (24 SLN and 24 SLN) patients (T3a/b-T4a/b) who underwent staging of SLNs using transcriptome profiling analysis on 5 μm sections of fresh SLNs. U133A 2.0 Affymetrix gene chips were used. Significance analysis of microarrays was used to test the association between gene expression level and SLN status. Genes with fold change more than 1.5 and q value less than 0.05 were considered differentially expressed. Pathway analysis was performed using Ingenuity Pathway Analysis. The Benjamini and Hochberg method was used to adjust for multiple testing in pathway analysis. We identified 89 probe sets that were significantly differentially expressed (1.5-27-fold; q<0.05). Upon performing the pathway analysis, it was found that 25 genes were common among the most significant and biologically relevant canonical pathways. The molecules and pathways that achieved differential expression of highest statistical significance were notably related to melanoma and its microenvironment and to signaling pathways implicated in immunosuppression and development of cancer. A 25-gene signature is significantly differentially expressed between SLN and SLN and is related to melanoma oncogenesis and immunosuppression. The identified expression profile provides a signature of melanoma nodal involvement. These findings warrant further investigation into the mechanisms of metastasis, melanoma metastasis diagnosis, and prediction of outcome.

摘要

本研究的目的是了解通过对临床I期和II期黑色素瘤患者的前哨淋巴结(SLN)进行基因表达谱分析来进行分子特征分析,是否可以增进对转移机制的理解,并识别与诊断或临床结果相关的SLN基因特征。对48例(24例SLN阳性和24例SLN阴性)(T3a/b - T4a/b)患者的SLN活检组织进行基因表达谱分析,这些患者通过对新鲜SLN的5μm切片进行转录组分析来对SLN进行分期。使用U133A 2.0 Affymetrix基因芯片。微阵列显著性分析用于测试基因表达水平与SLN状态之间的关联。将变化倍数大于1.5且q值小于0.05的基因视为差异表达基因。使用Ingenuity Pathway Analysis进行通路分析。在通路分析中采用Benjamini和Hochberg方法对多重检验进行校正。我们鉴定出89个显著差异表达的探针集(1.5 - 27倍;q < 0.05)。在进行通路分析时,发现25个基因在最显著且与生物学相关的经典通路中是共有的。实现最高统计学显著性差异表达的分子和通路与黑色素瘤及其微环境以及与免疫抑制和癌症发展相关的信号通路显著相关。一个25基因特征在SLN阳性和SLN阴性之间显著差异表达,并且与黑色素瘤的发生和免疫抑制相关。所鉴定的表达谱提供了黑色素瘤淋巴结受累的特征。这些发现值得进一步研究转移机制、黑色素瘤转移诊断和结果预测。

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