Department of Pharmacology and Experimental Therapeutics, Thomas Jefferson University, Philadelphia, PA 19107, USA.
Int J Cancer. 2011 Jul 15;129(2):331-45. doi: 10.1002/ijc.25688. Epub 2010 Nov 9.
Zinc (Zn)-deficiency (ZD) is implicated in the pathogenesis of human oral-esophageal cancers. Previously, we showed that in ZD mice genetic deletion of cyclooxygenase-2 (Cox-2) enhances N-nitrosomethylbenzylamine-induced forestomach carcinogenesis. By contrast, Cox-2 deletion offers protection in Zn-sufficient (ZS) mice. We hypothesize that ZD activates pathways insensitive to COX-2 inhibition, thereby promoting carcinogenesis. This hypothesis is tested in a Cox-2(-/-) mouse tongue cancer model that mimics pharmacologic blockade of COX-2 by firstly examining transcriptome profiles of forestomach mucosa from Cox-2(-/-) and wild-type mice on a ZD vs. ZS diet, and secondly investigating the roles of identified markers in mouse forestomach/tongue preneoplasia and carcinomas. In Cox-2(-/-) mice exposed to the tongue carcinogen 4-nitroquinoline 1-oxide, dietary ZD elicited tongue/esophagus/forestomach carcinomas that were prevented by ZS. The precancerous ZD:Cox-2(-/-) vs. ZS:Cox-2(-/-) forestomach had an inflammatory signature with upregulation of the proinflammation genes S100a8 and S100a9. Bioinformatics analysis revealed overrepresentation of inflammation processes comprising S100a8/a9 and an nuclear factor (NF)-κB network with connectivity to S100A8. Immunohistochemistry revealed co-overexpression of S100A8, its heterodimeric partner S100A9, the receptor for advanced glycation end-products (RAGE), NF-κB p65, and cyclin D1, in ZD:Cox-2(-/-) forestomach/tongue preneoplasia and carcinomas, evidence for the activation of a RAGE-S100A8/A9 inflammatory pathway. Accumulation of p53 in these carcinomas indicated activation of additional inflammatory pathways. Zn-replenishment in ZD:Cox-2(-/-) mice reversed the inflammation and inhibited carcinogenesis. Thus, ZD activates alternative inflammation-associated cancer pathways that fuel tumor progression and bypass the antitumor effect of Cox-2 ablation. These findings have important clinical implications, as combination cancer therapy that includes Zn may improve efficacy.
锌缺乏(ZD)与人类口腔食管癌的发病机制有关。此前,我们发现 ZD 小鼠中环氧合酶-2(Cox-2)的基因缺失会增强 N-亚硝基甲基苄胺诱导的前胃癌发生。相比之下,Cox-2 缺失在锌充足(ZS)小鼠中提供保护。我们假设 ZD 会激活对 Cox-2 抑制不敏感的途径,从而促进肿瘤发生。该假设通过 Cox-2(-/-)小鼠舌癌模型进行了检验,该模型模拟了 Cox-2 的药理学阻断,首先在前胃粘膜的 Cox-2(-/-)和野生型小鼠的转录组图谱上研究了 ZD 与 ZS 饮食之间的差异,其次研究了鉴定出的标志物在小鼠前胃/舌癌前病变和癌中的作用。在暴露于舌致癌物 4-硝基喹啉 1-氧化物的 Cox-2(-/-)小鼠中,ZD 饮食会引发舌/食管/前胃癌,而 ZS 饮食可预防这些癌症。癌前的 ZD:Cox-2(-/-)与 ZS:Cox-2(-/-)前胃具有炎症特征,促炎基因 S100a8 和 S100a9 上调。生物信息学分析显示,炎症过程的代表性过高,包括 S100a8/a9 和核因子(NF)-κB 网络,与 S100A8 有连接。免疫组织化学显示 S100A8、其异二聚体伴侣 S100A9、晚期糖基化终产物(RAGE)受体、NF-κB p65 和细胞周期蛋白 D1 在 ZD:Cox-2(-/-)前胃/舌癌前病变和癌中的共过表达,表明 RAGE-S100A8/A9 炎症途径的激活。这些癌中的 p53 积累表明激活了其他炎症途径。在 ZD:Cox-2(-/-)小鼠中补充锌可逆转炎症并抑制肿瘤发生。因此,ZD 激活了替代的与炎症相关的癌症途径,这些途径推动了肿瘤的进展,并绕过了 Cox-2 缺失的抗肿瘤作用。这些发现具有重要的临床意义,因为包括锌在内的联合癌症疗法可能会提高疗效。
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