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首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Heat shock protein 70 (HSP70) after laser thermotherapy of an adenocarcinoma transplanted into rat liver.
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Heat shock protein 70 (HSP70) after laser thermotherapy of an adenocarcinoma transplanted into rat liver.

机译:激光热疗法移植到大鼠肝脏中的腺癌后的热休克蛋白70(HSP70)。

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摘要

The heat shock proteins (HSPs) HSP70 and gp96 from necrotic tumour cells are considered to function as chaperones in presenting tumour antigens. We therefore studied HSP70 and immune cells in a transplantable carcinoma in the liver of rats after interstitial laser thermotherapy (ILT). Experiments were performed in Wistar FU rats using a dimethyl-hydrazine-induced adenocarcinoma implanted into the left lateral lobe of the liver. Rats were randomized to one of the following groups: a) ILT of tumour, b) sham ILT, or c) control. ILT was suboptimal and was performed at a steady-state temperature of 43 degrees C at the tumour margin for 30 minutes. Rats were killed 15 minutes, 5 hours, 10 hours, 15 hours or 12 days after treatment. Double immunohistochemistry was performed for HSP70 and ED1 macrophages or CD8 lymphocytes, and ELISA for serum concentrations of HSP70. After ILT, there was an increase of HSP70 immunoreactivity in tumours as compared to sham ILT. At the same time, tumour cells affected by ILT showed a shift of HSP70 from the cytoplasm to the nucleus with a peak at 10 hours. Few CD8-positive cells were found. There was an increase of tumour-infiltrating ED1 macrophages after ILT as compared to sham ILT at 10-15 hours after treatment. HSP70 was present in ED1 macrophages significantly more frequently after ILT than after sham ILT, and this was true both for HSP70 localized to the surface and the cytoplasm of the macrophage. There was a significant increase in serum HSP70 during the first 15 hours after ILT. In conclusion, laser thermotherapy resulted in increased HSP70 immunoreactivity within tumours and HSP70 shifts from cytoplasm to nucleus. Furthermore, it resulted in increased numbers of tumour-infiltrating macrophages and an increased presence of HSP70 in the membrane and cytoplasm of these macrophages.
机译:来自坏死性肿瘤细胞的热休克蛋白(HSPs)HSP70和gp96被认为在呈递肿瘤抗原时起分子伴侣的作用。因此,我们研究了间质激光热疗(ILT)后大鼠肝脏中可移植癌的HSP70和免疫细胞。在Wistar FU大鼠中进行了实验,使用了二甲基肼诱导的腺癌植入肝左叶。将大鼠随机分为以下一组:a)肿瘤的ILT,b)假ILT,或c)对照。 ILT次优,在肿瘤边缘处在43摄氏度的稳态温度下进行30分钟。治疗后15分钟,5小时,10小时,15小时或12天处死大鼠。对HSP70和ED1巨噬细胞或CD8淋巴细胞进行了双重免疫组化,对HSP70的血清浓度进行了ELISA。与假ILT相比,ILT后肿瘤中的HSP70免疫反应性增加。同时,受到ILT影响的肿瘤细胞显示HSP70从细胞质向细胞核转移,在10小时时达到峰值。几乎没有发现CD8阳性细胞。与治疗后10-15小时的假ILT相比,ILT后肿瘤浸润的ED1巨噬细胞增加。在ILT后,HSP70在ED1巨噬细胞中的出现频率要比假ILT后高得多,这对于位于巨噬细胞表面和细胞质的HSP70而言都是如此。在ILT后的最初15小时内,血清HSP70显着增加。总之,激光热疗导致肿瘤内HSP70的免疫反应性增加,并且HSP70从细胞质转移到细胞核。此外,其导致肿瘤浸润巨噬细胞数量增加,并且在这些巨噬细胞的膜和细胞质中HSP70的存在增加。

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