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内源性与肿瘤特异性宿主对乳腺癌的反应:同步原发性乳腺癌和活检部位变化中基质反应的研究。

Endogenous versus tumor-specific host response to breast carcinoma: a study of stromal response in synchronous breast primaries and biopsy site changes.

机构信息

Department of Pathology, Stanford University Medical Center, Stanford, California 94305, USA.

出版信息

Clin Cancer Res. 2011 Feb 1;17(3):437-46. doi: 10.1158/1078-0432.CCR-10-1709. Epub 2010 Nov 22.

Abstract

PURPOSE

We recently described two types of stromal response in breast cancer derived from gene expression studies of tenosynovial giant cell tumors and fibromatosis. The purpose of this study is to elucidate the basis of this stromal response--whether they are elicited by individual tumors or whether they represent an endogenous host reaction produced by the patient.

EXPERIMENTAL DESIGN

Stromal signatures from patients with synchronous dual primaries were analyzed by immunohistochemistry on a tissue microarray (n = 26 pairs) to evaluate the similarity of stromal responses in different tumors within the same patient. We also characterized the extent to which the stromal signatures were conserved between stromal response to injury compared to the stromal response to carcinoma using gene expression profiling and tissue microarray immunohistochemistry.

RESULTS

The two stromal response signatures showed divergent associations in synchronous primaries: the DTF fibroblast response is more likely to be similar in a patient with multiple breast primaries (permutation analysis P = 0.0027), whereas CSF1 macrophage response shows no significant concordance in separate tumors within a given patient. The DTF fibroblast signature showed more concordance across normal, cancer, and biopsy site samples from within a patient, than across normal, cancer, and biopsy site samples from a random group of patients, whereas the CSF1 macrophage response did not.

CONCLUSIONS

The results suggest that the DTF fibroblast response is host-specific, whereas the CSF1 response may be tumor-elicited. Our findings provide further insight into stromal response and may facilitate the development of therapeutic strategies to target particular stromal subtypes.

摘要

目的

我们最近根据腱膜组织巨细胞瘤和纤维瘤病的基因表达研究,描述了两种乳腺癌基质反应类型。本研究旨在阐明这种基质反应的基础——它们是由单个肿瘤引起的,还是代表患者产生的内源性宿主反应。

实验设计

通过免疫组织化学在组织微阵列上分析来自同步双原发患者的基质特征(n = 26 对),以评估同一患者不同肿瘤中基质反应的相似性。我们还通过基因表达谱和组织微阵列免疫组织化学分析,表征了基质损伤反应与癌相关的基质反应之间基质特征的保守程度。

结果

两种基质反应特征在同步原发性肿瘤中表现出不同的相关性:在多个乳腺癌原发性患者中,DTF 成纤维细胞反应更可能相似(置换分析 P = 0.0027),而 CSF1 巨噬细胞反应在同一患者的不同肿瘤中没有明显的一致性。与从随机患者组的正常、癌症和活检部位样本相比,DTF 成纤维细胞特征在患者内的正常、癌症和活检部位样本之间具有更高的一致性,而 CSF1 巨噬细胞反应则没有。

结论

结果表明,DTF 成纤维细胞反应是宿主特异性的,而 CSF1 反应可能是肿瘤诱导的。我们的发现为基质反应提供了进一步的见解,并可能有助于开发针对特定基质亚型的治疗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/80e2/3033467/ed92cb2a10b7/nihms-249213-f0001.jpg

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