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组织切片移植:一种人前列腺雄激素信号的活体模型。

Tissue slice grafts: an in vivo model of human prostate androgen signaling.

机构信息

Department of Urology, Stanford University School of Medicine, Stanford, CA 94305-5118, USA.

出版信息

Am J Pathol. 2010 Jul;177(1):229-39. doi: 10.2353/ajpath.2010.090821. Epub 2010 May 14.

Abstract

We developed a tissue slice graft (TSG) model by implanting thin, precision-cut tissue slices derived from fresh primary prostatic adenocarcinomas under the renal capsule of immunodeficient mice. This new in vivo model not only allows analysis of approximately all of the cell types present in prostate cancer within an intact tissue microenvironment, but also provides a more accurate assessment of the effects of interventions when tissues from the same specimen with similar cell composition and histology are used as control and experimental samples. The thinness of the slices ensures that sufficient samples can be obtained for large experiments as well as permits optimal exchange of nutrients, oxygen, and drugs between the grafted tissue and the host. Both benign and cancer tissues displayed characteristic histology and expression of cell-type specific markers for up to 3 months. Moreover, androgen-regulated protein expression diminished in TSGs after androgen ablation of the host and was restored after androgen repletion. Finally, many normal secretory epithelial cells and cancer cells in TSGs remained viable 2 months after androgen ablation, consistent with similar observations in postprostatectomy specimens following neoadjuvant androgen ablation. Among these were putative Nkx3.1(+) stem cells. Our novel TSG model has the appropriate characteristics to serve as a useful tool to model all stages of disease, including normal tissue, premalignant lesions, well-differentiated cancer, and poorly differentiated cancer.

摘要

我们通过在免疫缺陷小鼠的肾包膜下植入来自新鲜原发性前列腺腺癌的薄型、精密切割组织切片,开发了一种组织切片移植(TSG)模型。这种新的体内模型不仅允许在完整的组织微环境中分析前列腺癌中存在的几乎所有细胞类型,而且还能更准确地评估干预措施的效果,因为使用具有相似细胞组成和组织学的同一标本的组织作为对照和实验样本。切片的薄度确保了可以获得足够的样本用于大型实验,并且还允许移植组织和宿主之间最佳的营养、氧气和药物交换。良性和癌症组织在长达 3 个月的时间内均表现出特征性的组织学和细胞类型特异性标志物的表达。此外,在宿主去雄激素处理后,TSG 中的雄激素调节蛋白表达减少,在雄激素补充后恢复。最后,在去雄激素处理后 2 个月,TSG 中的许多正常分泌上皮细胞和癌细胞仍然存活,这与新辅助雄激素剥夺后前列腺切除术标本中的类似观察结果一致。其中包括假定的 Nkx3.1(+)干细胞。我们的新型 TSG 模型具有适当的特征,可以作为一种有用的工具来模拟疾病的所有阶段,包括正常组织、癌前病变、高分化癌症和低分化癌症。

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