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从小鼠到人类:通过比较基因表达序列分析(SAGE)研究鉴定乳腺癌中常见的失调基因

From mice to humans: identification of commonly deregulated genes in mammary cancer via comparative SAGE studies.

作者信息

Hu Yuhui, Sun Hongxia, Drake Jeffrey, Kittrell Frances, Abba Martin C, Deng Li, Gaddis Sally, Sahin Aysegul, Baggerly Keith, Medina Daniel, Aldaz C Marcelo

机构信息

Department of Carcinogenesis, The University of Texas M.D. Anderson Cancer Center, Science Park-Research Division, Smithville 78957, USA.

出版信息

Cancer Res. 2004 Nov 1;64(21):7748-55. doi: 10.1158/0008-5472.CAN-04-1827.

Abstract

Genetically engineered mouse mammary cancer models have been used over the years as systems to study human breast cancer. However, much controversy exists on the utility of such models as valid equivalents to the human cancer condition. To perform an interspecies gene expression comparative study in breast cancer we used a mouse model that most closely resembles human breast carcinogenesis. This system relies on the transplant of p53 null mouse mammary epithelial cells into the cleared mammary fat pads of syngeneic hosts. Serial analysis of gene expression (SAGE) was used to obtain gene expression profiles of normal and tumor samples from this mouse mammary cancer model (>300,000 mouse mammary-specific tags). The resulting mouse data were compared with 25 of our human breast cancer SAGE libraries (>2.5 million human breast-specific tags). We observed significant similarities in the deregulation of specific genes and gene families when comparing mouse with human breast cancer SAGE data. A total of 72 transcripts were identified as commonly deregulated in both species. We observed a systematic and significant down-regulation in all of the tumors from both species of various cytokines, including CXCL1 (GRO1), LIF, interleukin 6, and CCL2. All of the mouse and most human mammary tumors also displayed decreased expression of genes known to inhibit cell proliferation, including NFKBIA (IKBalpha), GADD45B, and CDKN1A (p21); transcription-related genes such as CEBP, JUN, JUNB, and ELF1; and apoptosis-related transcripts such as IER3 and GADD34/PPP1R15A. Examples of overexpressed transcripts in tumors from both species include proliferation-related genes such as CCND1, CKS1B, and STMN1 (oncoprotein 18); and genes related to other functions such as SEPW1, SDFR1, DNCI2, and SP110. Importantly, abnormal expression of several of these genes has not been associated previously with breast cancer. The consistency of these observations was validated in independent mouse and human mammary cancer sets. This is the first interspecies comparison of mammary cancer gene expression profiles. The comparative analysis of mouse and human SAGE mammary cancer data validates this p53 null mouse tumor model as a useful system closely resembling human breast cancer development and progression. More importantly, these studies are allowing us to identify relevant biomarkers of potential use in human studies while leading to a better understanding of specific mechanisms of human breast carcinogenesis.

摘要

多年来,基因工程小鼠乳腺癌模型一直被用作研究人类乳腺癌的系统。然而,对于此类模型作为人类癌症情况的有效等效模型的实用性存在诸多争议。为了在乳腺癌中进行种间基因表达比较研究,我们使用了一种与人类乳腺癌发生最为相似的小鼠模型。该系统依赖于将p53基因敲除的小鼠乳腺上皮细胞移植到同基因宿主的清除后的乳腺脂肪垫中。基因表达系列分析(SAGE)被用于获取来自该小鼠乳腺癌模型的正常和肿瘤样本的基因表达谱(超过30万个小鼠乳腺特异性标签)。将所得的小鼠数据与我们的25个人类乳腺癌SAGE文库(超过250万个人类乳腺特异性标签)进行比较。在比较小鼠和人类乳腺癌SAGE数据时,我们观察到特定基因和基因家族的失调存在显著相似性。总共鉴定出72个转录本在两个物种中均被共同失调。我们观察到在两个物种的所有肿瘤中,包括CXCL1(GRO1)、白血病抑制因子(LIF)、白细胞介素6和CCL2在内的各种细胞因子均出现系统性且显著的下调。所有小鼠和大多数人类乳腺肿瘤还显示出已知抑制细胞增殖的基因表达降低,包括NFKBIA(IκBα)、GADD45B和CDKN1A(p21);与转录相关的基因,如CEBP、JUN、JUNB和ELF1;以及与凋亡相关的转录本,如IER3和GADD34/PPP1R15A。两个物种肿瘤中过表达转录本的例子包括与增殖相关的基因,如CCND1、CKS1B和STMN1(癌蛋白18);以及与其他功能相关的基因,如SEPW1、SDFR1、DNCI2和SP110。重要的是,这些基因中有几个的异常表达以前尚未与乳腺癌相关联。这些观察结果的一致性在独立的小鼠和人类乳腺癌组中得到了验证。这是首次对乳腺癌基因表达谱进行种间比较。对小鼠和人类SAGE乳腺癌数据的比较分析验证了这个p53基因敲除小鼠肿瘤模型是一个类似于人类乳腺癌发生和发展的有用系统。更重要的是,这些研究使我们能够识别在人类研究中可能有用的相关生物标志物,同时有助于更好地理解人类乳腺癌发生的具体机制。

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