Appearance of sex-determining region Y-box 9 (SOX9)- and glutathione S-transferase placental form (GST-P)-positive hepatocytes as possible carcinogenic events in the early stage of furan-induced hepatocarcinogenesis

IF 2.7 4区 医学 Q3 TOXICOLOGY Journal of Applied Toxicology Pub Date : 2024-08-22 DOI:10.1002/jat.4691
Daisuke Hibi, Meili Soma, Yuta Suzuki, Shinji Takasu, Yuji Ishii, Takashi Umemura
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Abstract

Furan, the basic skeleton of various flavoring agents, induces cholangiocellular tumors with higher incidences in the caudate lobe and hepatocellular tumors without the lobe specificity in rats, but the mechanism is unclear. We investigated the lobe distribution of possible carcinogenic events. Furan caused proliferation/infiltration of oval and inflammatory cells prominently in the caudate lobe as early as 4 weeks and cholangiofibrosis in this lobe at 8 weeks. In vivo mutagenicity assays using DNA extracted from the caudate or left lateral lobe of male gpt delta rats, the reporter gene-transgenic rats, treated with 8 mg/kg furan for 4 or 8 weeks showed negative outcomes. The distribution of glutathione S-transferase placental form (GST-P)-positive or sex-determining region Y-box 9 (SOX9)-positive hepatocytes was examined. Significant increases in the number of GST-P-positive hepatocytes were observed in all lobes of furan-treated rats at 8 weeks. By contrast, SOX9-positive hepatocytes, liver injury-inducible progenitor cells, were also found in all lobes of treated rats, the incidences of which were by far the highest in the caudate lobe. In addition, some of these hepatocytes also co-expressed delta like 1 homolog (DLK1), a hepatoblast marker, particularly in areas with a predominant presence of inflammatory cells. Overall, furan induced liver injury, leading to the appearance of SOX9-positive hepatocytes, some of which were subjected to dedifferentiation in the inflammatory microenvironment of a cholangiocarcinoma-prone lobe. Thus, the appearance of SOX9-positive hepatocytes together with GST-P-positive hepatocytes could be initial events in furan-induced hepatocarcinogenesis via non-genotoxic mechanisms.

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性别决定区 Y-box 9 (SOX9) 和谷胱甘肽 S 转移酶胎盘形式 (GST-P) 阳性肝细胞的出现可能是呋喃诱导肝癌发生早期阶段的致癌事件。
呋喃是各种调味剂的基本骨架,可诱导大鼠尾状叶胆管细胞瘤和肝细胞瘤,尾状叶胆管细胞瘤发病率较高,而肝细胞瘤则无叶特异性,但其机制尚不清楚。我们研究了可能致癌事件的肝叶分布。呋喃会导致尾状叶卵圆形细胞和炎症细胞增殖/浸润,4 周时尾状叶卵圆形细胞和炎症细胞显著增殖/浸润,8 周时尾状叶卵圆形细胞和炎症细胞显著增殖/浸润,8 周时尾状叶卵圆形细胞和炎症细胞显著增殖/浸润,胆管纤维化。使用从雄性 gpt delta 大鼠(报告基因转基因大鼠)尾状叶或左外侧叶提取的 DNA 进行体内诱变性检测,结果显示呋喃的诱变性为阴性。研究人员检测了谷胱甘肽 S 转移酶胎盘形式(GST-P)阳性或性决定区 Y-box 9(SOX9)阳性肝细胞的分布情况。经呋喃处理的大鼠在 8 周时,所有肝叶中 GST-P 阳性肝细胞的数量都显著增加。相比之下,SOX9 阳性肝细胞(肝损伤诱导的祖细胞)也出现在受试大鼠的所有肝叶中,其中尾状叶的发生率最高。此外,其中一些肝细胞还同时表达肝母细胞标记物 delta like 1 homolog (DLK1),尤其是在炎症细胞占主导地位的区域。总之,呋喃会诱导肝损伤,导致出现 SOX9 阳性肝细胞,其中一些会在胆管癌易发叶的炎性微环境中发生去分化。因此,SOX9 阳性肝细胞和 GST-P 阳性肝细胞的出现可能是呋喃通过非遗传毒性机制诱导肝癌发生的初始事件。
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来源期刊
CiteScore
7.00
自引率
6.10%
发文量
145
审稿时长
1 months
期刊介绍: Journal of Applied Toxicology publishes peer-reviewed original reviews and hypothesis-driven research articles on mechanistic, fundamental and applied research relating to the toxicity of drugs and chemicals at the molecular, cellular, tissue, target organ and whole body level in vivo (by all relevant routes of exposure) and in vitro / ex vivo. All aspects of toxicology are covered (including but not limited to nanotoxicology, genomics and proteomics, teratogenesis, carcinogenesis, mutagenesis, reproductive and endocrine toxicology, toxicopathology, target organ toxicity, systems toxicity (eg immunotoxicity), neurobehavioral toxicology, mechanistic studies, biochemical and molecular toxicology, novel biomarkers, pharmacokinetics/PBPK, risk assessment and environmental health studies) and emphasis is given to papers of clear application to human health, and/or advance mechanistic understanding and/or provide significant contributions and impact to their field.
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