Overlap in oncogenic and pro-inflammatory pathways associated with areca nut and nicotine exposure

Krati Garg , Anuj Kumar , Vidisha Kizhakkethil , Pramod Kumar , Shalini Singh
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引用次数: 0

Abstract

Background

Betel nut/areca nut/Areca catechu is one of the most commonly used psychoactive substance, and is also a major preventable cause of cancer. Unlike other psychoactive substances, such as nicotine, the mechanisms underlying addiction to areca nuts and related oncogenesis remain elusive. Recent reports suggest a possible overlap in the mechanisms of action of nicotine and areca nuts in the human body. Thus, this study aimed to investigate the interactome of human proteins associated with areca nut exposure and the intricate similarities and differences in the effects of the two psychoactive substances on humans.

Methods

A list of proteins associated with areca nut use was obtained from the available literature using terms from Medical Subject Headings (MeSH). Protein-protein interaction (PPI) networks and functional enrichment were analyzed. The results obtained for both psychoactive substances were compared.

Results

Given the limited number of common proteins (36/226, 16%) in the two sets, a substantial overlap (612/1176 nodes, 52%) was observed in the PPI networks, as well as in Gene Ontology. Areca nuts mainly affect signaling pathways through three hub proteins (alpha serine/threonine-protein kinase, tumor protein 53, and interleukin-6), which are common to both psychoactive substances, as well as two unique hub proteins (epidermal growth factor receptor and master regulator of cell cycle entry and proliferative metabolism). Areca nut-related proteins are associated with unique pathways, such as extracellular matrix organization, lipid storage, and metabolism, which are not found in nicotine-associated proteins.

Conclusions

Areca nuts affect regulatory mechanisms, leading to systemic toxicity and oncogenesis. Areca nuts also affect unique pathways that can be studied as potential markers of exposure, as well as targets for anticancer therapeutic agents.

Abstract Image

与亚麻仁和尼古丁接触相关的致癌和促炎途径的重叠
背景甜菜/夏威夷果/儿茶是最常用的精神活性物质之一,也是可预防癌症的主要原因。与尼古丁等其他精神活性物质不同的是,人们对甜叶菊果实上瘾及相关致癌机制仍难以捉摸。最近的报告表明,尼古丁和亚麻仁在人体内的作用机制可能存在重叠。因此,本研究旨在调查与接触亚麻仁相关的人体蛋白质相互作用组,以及这两种精神活性物质对人体影响的复杂异同。对蛋白质-蛋白质相互作用(PPI)网络和功能富集进行了分析。结果鉴于两组共同蛋白质的数量有限(36/226,16%),在 PPI 网络和基因本体论中观察到大量重叠(612/1176 个节点,52%)。阿雷卡坚果主要通过三种枢纽蛋白(α 丝氨酸/苏氨酸蛋白激酶、肿瘤蛋白 53 和白细胞介素-6)影响信号传导通路,这三种枢纽蛋白是两种精神活性物质所共有的,另外还有两种独特的枢纽蛋白(表皮生长因子受体和细胞周期进入及增殖代谢主调节因子)。阿雷卡坚果相关蛋白与细胞外基质组织、脂质储存和新陈代谢等独特途径有关,而尼古丁相关蛋白中没有这些途径。阿月浑子果还会影响一些独特的途径,这些途径可作为潜在的暴露标记以及抗癌治疗药物的靶点进行研究。
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来源期刊
Cancer pathogenesis and therapy
Cancer pathogenesis and therapy Surgery, Radiology and Imaging, Cancer Research, Oncology
CiteScore
0.80
自引率
0.00%
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审稿时长
54 days
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