胰岛素治疗对糖尿病患者肝细胞癌发生发展的促进作用。
Facilitatory effect of insulin treatment on hepatocellular carcinoma development in diabetes.
作者信息
Baba Hayato, Kurano Makoto, Nishida Takeshi, Hatta Hideki, Hokao Ryoji, Tsuneyama Koichi
机构信息
Department of Pathology and Laboratory Medicine, Institute of Biomedical Sciences, Tokushima University Graduate School, 3-18-15 Kuramoto, Tokushima, Tokushima, 770-8503, Japan.
Department of Surgery and Science, Graduate School of Medicine and Pharmaceutical Sciences, University of Toyama, 2630 Sugitani, Toyama, Toyama, 930-0194, Japan.
出版信息
BMC Res Notes. 2017 Sep 13;10(1):478. doi: 10.1186/s13104-017-2783-6.
BACKGROUND
To evaluate the effect of insulin treatment on the incidence and/or severity of hepatocellular carcinoma (HCC) in a mouse model of HCC based on diabetes.
METHODS
We recently reported that neonatal streptozotocin (STZ) treatment causes type 1 diabetes and subsequent HCC in ddY, Institute for Animal Reproduction (DIAR) mice. Newborn male DIAR mice were divided into three groups based on STZ and insulin (INS) treatment. STZ was subcutaneously injected (60 mg/g) into the STZ-treated group (DIAR-nSTZ mice, N = 13) and the STZ/insulin-treated group (DIAR-nSTZ/INS mice, N = 20). A physiologic solution was injected into the control group (DIAR-control mice, N = 8) 1.5 days after birth. Insulin was subcutaneously injected into the DIAR-nSTZ/INS mice according to the following protocol: 2 IU/day at 4-5 weeks of age, 3 IU/day at 5-7 weeks of age, and 4 IU/day at 7-12 weeks of age. All mice were fed a normal diet and were subjected to physiological and histopathological assessments at 12 weeks of age.
RESULTS
DIAR-nSTZ mice had significantly lower body weight and higher blood glucose levels than DIAR-control mice, whereas no significant differences were observed between DIAR-nSTZ/INS mice and control mice. At 12 weeks of age, lower weight of paratesticular fat and higher levels of total cholesterol, triglyceride, and free fatty acids were observed in DIAR-nSTZ mice compared to DIAR-control mice, whereas there were no significant differences between DIAR-nSTZ/INS mice and DIAR-control mice. In the livers of DIAR-nSTZ mice, HCC was observed in 15% of cases, and dysplastic nodules were observed in 77% of cases. In the livers of DIAR-nSTZ/INS mice, HCC was observed in 39% of cases and dysplastic nodules were observed in 61% of cases (p = 0.011). Moreover, the average tumor size was significantly larger in STZ/INS-treated mice than in STZ-treated mice. Immunohistochemical analysis demonstrated that the expression of ERK1/2, downstream substrates of insulin signaling that activate cell proliferation, was significantly higher in STZ/INS-treated mice compared to STZ-treated mice.
CONCLUSIONS
Insulin treatment promoted, rather than inhibited, the progression of liver carcinogenesis in DIAR-nSTZ mice. Hyperinsulinemia rather than hyperglycemia can accelerate the progression of HCC via insulin signaling.
背景
在基于糖尿病的肝细胞癌(HCC)小鼠模型中,评估胰岛素治疗对HCC发病率和/或严重程度的影响。
方法
我们最近报道,新生期链脲佐菌素(STZ)处理可导致实验动物繁殖研究所(DIAR)的ddY小鼠发生1型糖尿病及后续的HCC。新生雄性DIAR小鼠根据STZ和胰岛素(INS)处理分为三组。将STZ皮下注射(60mg/g)到STZ处理组(DIAR-nSTZ小鼠,N = 13)和STZ/胰岛素处理组(DIAR-nSTZ/INS小鼠,N = 20)。出生后1.5天,将生理溶液注射到对照组(DIAR-对照小鼠,N = 8)。根据以下方案将胰岛素皮下注射到DIAR-nSTZ/INS小鼠中:4-5周龄时2IU/天,5-7周龄时3IU/天,7-12周龄时4IU/天。所有小鼠均给予正常饮食,并在12周龄时进行生理和组织病理学评估。
结果
DIAR-nSTZ小鼠的体重明显低于DIAR-对照小鼠,血糖水平更高,而DIAR-nSTZ/INS小鼠与对照小鼠之间未观察到显著差异。在12周龄时,与DIAR-对照小鼠相比,DIAR-nSTZ小鼠的睾丸旁脂肪重量更低,总胆固醇、甘油三酯和游离脂肪酸水平更高,而DIAR-nSTZ/INS小鼠与DIAR-对照小鼠之间无显著差异。在DIAR-nSTZ小鼠的肝脏中,15%的病例观察到HCC,77%的病例观察到发育异常结节。在DIAR-nSTZ/INS小鼠的肝脏中,39%的病例观察到HCC,61%的病例观察到发育异常结节(p = 0.011)。此外,STZ/INS处理的小鼠的平均肿瘤大小明显大于STZ处理的小鼠。免疫组织化学分析表明,与STZ处理的小鼠相比,STZ/INS处理的小鼠中激活细胞增殖的胰岛素信号下游底物ERK1/2的表达明显更高。
结论
胰岛素治疗促进而非抑制DIAR-nSTZ小鼠肝癌的进展。高胰岛素血症而非高血糖症可通过胰岛素信号加速HCC的进展。
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