核因子红系2相关因子2敲除抑制偶氮甲烷/葡聚糖硫酸钠治疗诱导的雌性小鼠侵袭性结直肠癌的形成

IF 2.5 Q3 ONCOLOGY
Chin-Hee Song, Nayoung Kim, Ryoung Hee Nam, Soo In Choi, Changhee Kang, Jae Young Jang, Heewon Nho, Eun Shin, Ha-Na Lee
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引用次数: 5

摘要

结肠肿瘤在男性中比在女性中更容易发生。核因子红系2相关因子2 (Nrf2)在肿瘤发生分期中起差异作用。本研究的目的是利用Nrf2敲除(KO)雌性小鼠研究Nrf2在结肠炎相关肿瘤发生中的作用。注射偶氮氧甲烷(AOM)和硫酸葡聚糖钠(DSS)处理的野生型(WT)和Nrf2 KO雌性小鼠在注射AOM后第2周和第16周处死。在AOM/ dss治疗的WT和Nrf2 KO小鼠中评估结肠炎的严重程度、肿瘤发生率和炎症介质的水平。对结肠组织进行qRT-PCR、Western blot异常分析和ELISA检测。在第2周,AOM/ dss诱导的Nrf2小鼠结肠组织损伤明显大于WT小鼠。在第16周,与WT相比,Nrf2 KO在近端和远端结肠中的肿瘤数量(> 2mm大小)均显著降低。Nrf2 KO降低了近端结肠腺瘤/癌和远端结肠粘膜下浸润性癌的总体发病率。Nrf2 KO中NF-κ b相关介质(即iNOS和COX-2)和Nrf2相关抗氧化剂(即血红素加氧酶-1和谷氨酸-半胱氨酸连接酶催化亚基)的mRNA和蛋白表达水平显著低于WT小鼠。有趣的是,AOM/ dss处理的Nrf2 KO中15-羟基前列腺素脱氢酶(15-PGDH)的蛋白水平高于WT小鼠。我们的研究结果支持Nrf2在癌变后期的致癌作用,并且上调肿瘤抑制因子15-PGDH可能有助于抑制Nrf2 KO雌性小鼠结肠炎相关肿瘤的发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Nuclear Factor Erythroid 2-related Factor 2 Knockout Suppresses the Development of Aggressive Colorectal Cancer Formation Induced by Azoxymethane/Dextran Sulfate Sodium-Treatment in Female Mice.

Nuclear Factor Erythroid 2-related Factor 2 Knockout Suppresses the Development of Aggressive Colorectal Cancer Formation Induced by Azoxymethane/Dextran Sulfate Sodium-Treatment in Female Mice.

Nuclear Factor Erythroid 2-related Factor 2 Knockout Suppresses the Development of Aggressive Colorectal Cancer Formation Induced by Azoxymethane/Dextran Sulfate Sodium-Treatment in Female Mice.

Nuclear Factor Erythroid 2-related Factor 2 Knockout Suppresses the Development of Aggressive Colorectal Cancer Formation Induced by Azoxymethane/Dextran Sulfate Sodium-Treatment in Female Mice.

Colon tumors develop more frequently in male than in female. Nuclear factor erythroid 2-related factor 2 (Nrf2) plays differential roles in the stage of tumorigenesis. The purpose of this study was to investigate the role of Nrf2 on colitis-associated tumorigenesis using Nrf2 knockout (KO) female mice. Azoxymethane (AOM) and dextran sulfate sodium (DSS)-treated wild-type (WT) and Nrf2 KO female mice were sacrificed at week 2 and 16 after AOM injection. Severity of colitis, tumor incidence, and levels of inflammatory mediators were evaluated in AOM/DSS-treated WT and Nrf2 KO mice. Furthermore, qRT-PCR, Western blot abnalysis, and ELISA were performed in colon tissues. At week 2, AOM/DSS-induced colon tissue damages were significantly greater in Nrf2 KO than in WT mice. At week 16, tumor numbers (> 2 mm size) were significantly lower in both the proximal and distal colon in Nrf2 KO compared to WT. The overall incidences of adenoma/cancer of the proximal colon and submucosal invasive cancer of the distal colon were reduced by Nrf2 KO. The mRNA and protein expression levels of NF-κB-related mediators (i.e., iNOS and COX-2) and Nrf2-related antioxidants (i.e., heme oxygenase-1 and glutamate-cysteine ligase catalytic subunit) were significantly lower in the Nrf2 KO than in WT mice. Interestingly, the protein level of 15-hydroxyprostaglandin dehydrogenase (15-PGDH) was higher in AOM/DSS-treated Nrf2 KO than in WT mice. Our results support the oncogenic effect of Nrf2 in the later stage of carcinogenesis and upregulation of tumor suppressor 15-PGDH might contribute to the repression of colitis-associated tumorigenesis in Nrf2 KO female mice.

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