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时钟样突变特征可能比皮肤黑色素瘤中紫外线损伤特征对更差的生存率具有预后意义。

Clock-like Mutation Signature May Be Prognostic for Worse Survival Than Signatures of UV Damage in Cutaneous Melanoma.

作者信息

Fröhlich Fabienne, Ramelyte Egle, Turko Patrick, Dzung Andreas, Freiberger Sandra N, Mangana Joanna, Levesque Mitchell P, Dummer Reinhard

机构信息

Department of Dermatology, University Hospital of Zurich, 8091 Zurich, Switzerland.

Faculty of Medicine, University of Zurich, 8091 Zurich, Switzerland.

出版信息

Cancers (Basel). 2023 Jul 27;15(15):3818. doi: 10.3390/cancers15153818.

Abstract

Novel treatment modalities comprising immune checkpoint inhibitors and targeted therapies have revolutionized treatment of metastatic melanoma. Still, some patients suffer from rapid progression and decease within months after a diagnosis of stage IV melanoma. We aimed to assess whether genomic alterations may predict survival after the development of stage IV disease, irrespective of received therapy. We analyzed tumor samples of 79 patients with stage IV melanoma using a custom next-generation gene-sequencing panel, MelArray, designed to detect alterations in 190 melanoma-relevant genes. We classified the patients: first, as short survivors (survival ≤6 months after stage IV disease, n = 22) and long survivors (survival >6 months, n = 57); second, by using a cut-off of one year; and third, by comparing the longest surviving 20 patients to the shortest surviving 20. Among analyzed genes, no individual gene alterations, or combinations of alterations, could be dichotomously associated with survival. However, the cohort's mutational profiles closely matched three known mutational signatures curated by the Catalog of Somatic Mutations in Cancer (COSMIC): UV signature COSMIC_7 (cosine-similarity 0.932), clock-like signature COSMIC_5 (cosine-similarity 0.829), and COSMIC_30 (cosine-similarity 0.726). Patients with UV signature had longer survival compared to patients with clock-like and COSMIC 30 ( < 0.0001). Subgroup dichotomization at 6 months showed that 75% of patients with UV signature survived longer than 6 months, and about 75% of patients with clock-like signature survived less than 6 months after development of stage IV disease. In our cohort, clock-like COSMIC_5 mutational signature predicted poor survival while a UV signature COSMIC_7 predicted longer survival. The prognostic value of mutational signatures should be evaluated in prospective studies.

摘要

包括免疫检查点抑制剂和靶向疗法在内的新型治疗方式彻底改变了转移性黑色素瘤的治疗方法。然而,一些患者在被诊断为IV期黑色素瘤后的数月内病情迅速进展并死亡。我们旨在评估基因组改变是否可以预测IV期疾病发生后的生存期,而不考虑所接受的治疗。我们使用定制的新一代基因测序平台MelArray分析了79例IV期黑色素瘤患者的肿瘤样本,该平台旨在检测190个与黑色素瘤相关基因的改变。我们对患者进行了分类:首先,分为短期存活者(IV期疾病后生存期≤6个月,n = 22)和长期存活者(生存期>6个月,n = 57);其次,以一年为分界点;第三,将存活时间最长的20名患者与存活时间最短的20名患者进行比较。在所分析的基因中,没有单个基因改变或改变的组合与生存期存在二分法关联。然而,该队列的突变谱与癌症体细胞突变目录(COSMIC)策划的三个已知突变特征密切匹配:紫外线特征COSMIC_7(余弦相似度0.932)、时钟样特征COSMIC_5(余弦相似度0.829)和COSMIC_30(余弦相似度0.726)。与具有时钟样特征和COSMIC 30的患者相比,具有紫外线特征的患者生存期更长(<0.0001)。6个月时的亚组二分法显示,75%具有紫外线特征的患者在IV期疾病发生后生存期超过6个月,而约75%具有时钟样特征的患者生存期少于6个月。在我们的队列中,时钟样COSMIC_5突变特征预示着生存期较差,而紫外线特征COSMIC_7预示着生存期更长。突变特征的预后价值应在前瞻性研究中进行评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/34df/10418148/a615c4921801/cancers-15-03818-g001.jpg

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