[I 型干扰素在黑色素瘤遗传进展中的潜在作用]。

Magyar onkologia Pub Date : 2023-09-28 Epub Date: 2023-08-18
Laura Vízkeleti, Andrea Ladányi, Orsolya Papp, Viktória Doma, Sarolta Kárpáti, Erzsébet Rásó, Tamás Barbai, József Tímár
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引用次数: 0

摘要

我们通过全基因组拷贝数分析,跟踪了内脏转移的皮肤黑色素瘤的基因组进展。我们发现,由于多个 DNA 修复基因的缺失,染色体不稳定性增加。此外,我们还在转移灶中发现了 HGF 和 MET 基因的共同扩增。最有趣的发现是肺转移瘤中几个主要由 IFN 调控的免疫细胞基因扩增。接下来,我们利用人体细胞系定义了 IFN 抗性基因表达特征(GES),其中几个元素在体外和体内都被证明是稳定的。在 TCGA 和公开的免疫疗法治疗黑色素瘤病例数据集中都检测到了这一 GES 的成分。在曾接受过 IFN 治疗的黑色素瘤病例样本中,我们发现了治疗特异性基因组改变(主要是扩增),这是脑转移瘤的最大特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[Potential role of type I interferon in the genetic progression of melanoma].

We have followed the genomic progression of cutaneous melanoma in visceral metastases using genome-wide copy number analysis. We have detected an increased chromosomal instability due to the loss of several DNA repair genes. Furthermore, we found co-amplifications of HGF and MET genes in metastases. The most interesting finding was gene amplifications of several, mostly IFN-regulated immune cell genes in lung metastases. Next we have defined a type I IFN resistance gene expression signature (GES) using human cell lines, several elements of which were proved to be stable in vitro and in vivo as well. The components of this GES have been detected in TCGA as well as in publicly available datasets of immunotherapy-treated melanoma cases. In case of samples from previously IFN-treated melanoma cases we have identified treatment-specific genomic alterations (predominantly amplifications) which were most characteristic for brain metastases.

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