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LNCaP 肿瘤异种移植的转录组学分析,旨在阐明肿瘤微环境对前列腺癌的作用机制,并为饮食预防前列腺癌的研究提供靶点。

Transcriptomic Analysis of LNCaP Tumor Xenograft to Elucidate the Components and Mechanisms Contributed by Tumor Environment as Targets for Dietary Prostate Cancer Prevention Studies.

机构信息

Department of Nutrition and Food Science, University of Maryland, College Park, MD 20742, USA.

Animal Parasitic Diseases Laboratory, Beltsville Area Research Center, ARS, USDA, Beltsville, MD 20705, USA.

出版信息

Nutrients. 2021 Mar 19;13(3):1000. doi: 10.3390/nu13031000.

Abstract

LNCaP athymic xenograft model has been widely used to allow researchers to examine the effects and mechanisms of experimental treatments such as diet and diet-derived cancer preventive and therapeutic compounds on prostate cancer. However, the biological characteristics of human LNCaP cells before/after implanting in athymic mouse and its relevance to clinical human prostate outcomes remain unclear and may dictate interpretation of biological efficacies/mechanisms of diet/diet-derived experimental treatments. In this study, transcriptome profiles and pathways of human prostate LNCaP cells before (in vitro) and after (in vivo) implanting into xenograft mouse were compared using RNA-sequencing technology (RNA-seq) followed by bioinformatic analysis. A shift from androgen-responsive to androgen nonresponsive status was observed when comparing LNCaP xenograft tumor to culture cells. Androgen receptor and aryl-hydrocarbon pathway were found to be inhibited and interleukin-1 (IL-1) mediated pathways contributed to these changes. Coupled with in vitro experiments modeling for androgen exposure, cell-matrix interaction, inflammation, and hypoxia, we identified specific mechanisms that may contribute to the observed changes in genes and pathways. Our results provide critical baseline transcriptomic information for a tumor xenograft model and the tumor environments that might be associated with regulating the progression of the xenograft tumor, which may influence interpretation of diet/diet-derived experimental treatments.

摘要

LNCaP 无胸腺异种移植模型已被广泛用于研究饮食和饮食衍生的癌症预防和治疗化合物等实验性治疗对前列腺癌的影响和机制。然而,在将人 LNCaP 细胞植入无胸腺小鼠前后的生物学特征及其与临床人类前列腺结果的相关性尚不清楚,这可能会影响对饮食/饮食衍生的实验性治疗的生物学功效/机制的解释。在这项研究中,使用 RNA 测序技术(RNA-seq)和生物信息学分析比较了人前列腺 LNCaP 细胞在植入异种移植小鼠前后(体外和体内)的转录组图谱和途径。与培养细胞相比,当比较 LNCaP 异种移植肿瘤时,观察到从雄激素反应状态向雄激素非反应状态的转变。发现雄激素受体和芳香烃途径受到抑制,白细胞介素 1(IL-1)介导的途径促成了这些变化。结合体外实验模拟雄激素暴露、细胞-基质相互作用、炎症和缺氧,我们确定了可能导致观察到的基因和途径变化的特定机制。我们的结果为肿瘤异种移植模型及其肿瘤环境提供了关键的基础转录组信息,这些信息可能与调节异种移植肿瘤的进展有关,这可能会影响对饮食/饮食衍生的实验性治疗的解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0bc2/8003580/b7a344ee26a7/nutrients-13-01000-g001.jpg

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