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抗坏血酸-2-葡萄糖苷减轻大鼠膀胱肿瘤模型盆腔放疗期间的肠道损伤。

Ascorbic acid-2 glucoside mitigates intestinal damage during pelvic radiotherapy in a rat bladder tumor model.

作者信息

Ito Yasutoshi, Yamamoto Tetsuo, Miyai Kosuke, Take Junya, Scherthan Harry, Rommel Anna, Eder Stefan, Steinestel Konrad, Rump Alexis, Port Matthias, Shinomiya Nariyoshi, Kinoshita Manabu

机构信息

Military Medicine Research Unit, Test and Evaluation Command, Ground Self-Defense Force, Setagaya, Japan.

NBC Counter Medical Unit, Ground Self-Defense Force, Setagaya, Japan.

出版信息

Int J Radiat Biol. 2022;98(5):942-957. doi: 10.1080/09553002.2021.2009145. Epub 2021 Dec 6.

Abstract

PURPOSE

Ascorbic acid is a strong antioxidant and has potent radioprotective effects on radiation injuries. Ascorbic acid 2-glucoside (AA2G) is a stabilized derivative of ascorbic acid and rapidly hydrolyzed into ascorbic acid and glucose. Since there is the possibility that AA2G treatment interferes with the antitumor activity of radiotherapy, we investigated the effect of AA2G treatment during radiotherapy on acute radiation enteritis and antitumor activity of radiotherapy in rats.

MATERIALS AND METHODS

AY-27 rat bladder tumor cells were used to induce bladder tumors in rats. Two weeks after inoculation rats received fractionated pelvic radiotherapy in eight fractions for 4 weeks totaling 40 Gy. During radiotherapy, one group of rats received per os AA2G (ascorbic acid: 250 mg/kg/day) and its bolus engulfment (ascorbic acid: 250 mg/kg) 8 h before each X-irradiation fraction. Seven days after the last X-irradiation, we studied histology, DNA double strand break (DSB) damage (by 53BP1 foci staining), and the M1/M2 macrophage response by immunohistochemistry of paraffin-fixed bladder and intestinal tissues.

RESULTS

AA2G treatment reduced the intestinal damage (shortening of villi) but did not reduce antitumor effectiveness of radiotherapy against bladder tumors. Like the controls, AA2G-treated rats showed no residual tumor lesions in the bladder after X-irradiation. Both AA2G-treated and control groups showed similar persistent DSB damage (53BP1 foci) both in bladders and ilea seven days after radiotherapy. Radiotherapy tended to reduce CD163 M2 macrophages, which are considered as an anti-inflammatory subtype favoring tissue repair, in the bladders. X-irradiation also reduced the occurrence of M2 macrophages in the ilea. AA2G treatment significantly increased CD163/CD68 macrophage ratio in the ilea of rats after pelvic irradiation in comparison to the sham irradiated control rats. AA2G treatment increased, albeit not significantly, the CD163/CD68 macrophage ratio in the irradiated bladders relative to the control irradiated rats. On the other hand, bladders and ilea of the irradiated rats with and without AA2G treatment showed similar frequencies of CD68 macrophages.

CONCLUSIONS

AA2G treatment mitigated radiation-induced intestinal damage without reducing antitumor activity after fractionated pelvic radiotherapy against bladder tumors in rats. The beneficial effect of AA2G treatment seems to promote a restoration of the M2 answer as well as tissue remodeling and wound healing. Similar residual DNA damage in bladders and ilea seven days post-irradiation is consistent with tumor control in both groups.

摘要

目的

抗坏血酸是一种强抗氧化剂,对辐射损伤具有强大的辐射防护作用。抗坏血酸2 - 葡萄糖苷(AA2G)是抗坏血酸的一种稳定衍生物,可迅速水解为抗坏血酸和葡萄糖。由于AA2G治疗有可能干扰放射治疗的抗肿瘤活性,我们研究了在放射治疗期间给予AA2G治疗对大鼠急性放射性肠炎以及放射治疗抗肿瘤活性的影响。

材料与方法

采用AY - 27大鼠膀胱肿瘤细胞诱导大鼠膀胱肿瘤。接种后两周,大鼠接受盆腔分次放疗,共8次,为期4周,总剂量40 Gy。在放疗期间,一组大鼠口服AA2G(抗坏血酸:250 mg/kg/天),并在每次X线照射前8小时给予大剂量吞服(抗坏血酸:250 mg/kg)。最后一次X线照射7天后,我们通过石蜡包埋的膀胱和肠道组织的免疫组织化学研究组织学、DNA双链断裂(DSB)损伤(通过53BP1灶染色)以及M1/M2巨噬细胞反应。

结果

AA2G治疗减轻了肠道损伤(绒毛缩短),但未降低放射治疗对膀胱肿瘤的抗肿瘤效果。与对照组一样,接受AA2G治疗的大鼠在X线照射后膀胱中未显示残留肿瘤病变。在放疗7天后,接受AA2G治疗的组和对照组在膀胱和回肠中均显示出相似的持续性DSB损伤(53BP1灶)。放射治疗倾向于减少膀胱中被认为是有利于组织修复的抗炎亚型的CD163 M2巨噬细胞。X线照射也减少了回肠中M2巨噬细胞的出现。与假照射对照组大鼠相比,AA2G治疗显著增加了盆腔照射后大鼠回肠中CD163/CD68巨噬细胞比率。相对于对照照射大鼠,AA2G治疗使照射膀胱中的CD163/CD68巨噬细胞比率虽未显著增加,但有所升高。另一方面,接受和未接受AA2G治疗的照射大鼠的膀胱和回肠显示出相似频率的CD68巨噬细胞。

结论

在大鼠盆腔分次放疗治疗膀胱肿瘤后,AA2G治疗减轻了辐射诱导的肠道损伤,而未降低抗肿瘤活性。AA2G治疗的有益作用似乎促进了M2反应的恢复以及组织重塑和伤口愈合。放疗后7天膀胱和回肠中相似的残留DNA损伤与两组的肿瘤控制情况一致。

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