Tumor-Agnostic Biomarkers: Heed Caution, and Why Cell of Origin Still Matters

Onco Pub Date : 2021-10-27 DOI:10.3390/onco1020008
A. Tan
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Abstract

Since the very beginnings of cancer therapy with chemotherapy, tumors have been treated according to the organ or tissue of origin. The advent of precision medicine however, has recently led to growing promise for tumor-agnostic biomarkers for targeted therapies and immunotherapies, such as NTRK fusions. Despite this, prominent examples such as BRAF V600E mutations in melanoma compared to colorectal cancer, in which the site of tumor origin dramatically influences the efficacy of targeted therapies, heeds caution against disregarding the importance of cell of origin. Indeed, another illustrative example, is the almost complete absence outside of cancers originating from the lung of the classical activating EGFR mutations—exon 19 deletions and exon 21 L858R mutations. Consequently, an understanding of lineage dependency and lineage-survival oncogenes may still offer significant mechanistic insights into the malignant transformation of tumors to ultimately identify further therapeutic vulnerabilities.
肿瘤不可知论的生物标志物:要小心,为什么细胞起源仍然很重要
自从癌症化疗开始以来,肿瘤一直是根据起源的器官或组织来治疗的。然而,精准医学的出现最近带来了肿瘤不可知生物标志物用于靶向治疗和免疫治疗的希望,如NTRK融合。尽管如此,与结直肠癌相比,黑色素瘤中的BRAF V600E突变等突出例子表明,肿瘤起源部位显著影响靶向治疗的疗效,这需要谨慎对待,不要忽视起源细胞的重要性。事实上,另一个说明性的例子是,除了肺癌外,几乎完全没有经典的激活EGFR突变-外显子19缺失和外显子21 L858R突变。因此,对谱系依赖性和谱系存活癌基因的理解可能仍然为肿瘤恶性转化提供重要的机制见解,从而最终确定进一步的治疗脆弱性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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