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对连续乳腺癌活检样本中基因表达的数字化定量分析揭示了免疫反应的激活。

Digital quantification of gene expression in sequential breast cancer biopsies reveals activation of an immune response.

机构信息

Center for Functional Cancer Epigenetics, Dana-Farber Cancer Institute, Boston, Massachusetts, United States of America.

出版信息

PLoS One. 2013 May 31;8(5):e64225. doi: 10.1371/journal.pone.0064225. Print 2013.

Abstract

Advancements in molecular biology have unveiled multiple breast cancer promoting pathways and potential therapeutic targets. Large randomized clinical trials remain the ultimate means of validating therapeutic efficacy, but they require large cohorts of patients and are lengthy and costly. A useful approach is to conduct a window of opportunity study in which patients are exposed to a drug pre-surgically during the interval between the core needle biopsy and the definitive surgery. These are non-therapeutic studies and the end point is not clinical or pathological response but rather evaluation of molecular changes in the tumor specimens that can predict response. However, since the end points of the non-therapeutic studies are biologic, it is critical to first define the biologic changes that occur in the absence of treatment. In this study, we compared the molecular profiles of breast cancer tumors at the time of the diagnostic biopsy versus the definitive surgery in the absence of any intervention using the Nanostring nCounter platform. We found that while the majority of the transcripts did not vary between the two biopsies, there was evidence of activation of immune related genes in response to the first biopsy and further investigations of the immune changes after a biopsy in early breast cancer seem warranted.

摘要

分子生物学的进展揭示了多种乳腺癌促进途径和潜在的治疗靶点。大型随机临床试验仍然是验证治疗效果的最终手段,但它们需要大量的患者,并且耗时且昂贵。一种有用的方法是进行机会之窗研究,在这种研究中,患者在核心针活检和确定性手术之间的间隔期间接受术前药物暴露。这些是非治疗性研究,终点不是临床或病理反应,而是评估肿瘤标本中的分子变化,这些变化可以预测反应。然而,由于非治疗性研究的终点是生物学的,因此首先定义在没有治疗的情况下发生的生物学变化至关重要。在这项研究中,我们使用 Nanostring nCounter 平台比较了诊断性活检时和在没有任何干预的情况下确定性手术时乳腺癌肿瘤的分子谱。我们发现,虽然大多数转录物在两次活检之间没有差异,但有证据表明,在第一次活检时免疫相关基因被激活,并且似乎有必要进一步研究早期乳腺癌活检后的免疫变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6e3e/3669373/b0f5255b5352/pone.0064225.g001.jpg

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