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口服短链脂肪酸可减轻食用商业饲料或要素膳的小鼠因阿糖胞苷治疗引起的肠道粘膜炎。

Oral administration of short-chain fatty acids reduces the intestinal mucositis caused by treatment with Ara-C in mice fed commercial or elemental diets.

作者信息

Ramos M G, Bambirra E A, Cara D C, Vieira E C, Alvarez-Leite J I

机构信息

Departamento de Bioquímica e Immunologia, Faculdade de Medicina, Universidade Federal de Minas Gerais, Belo Horizonte, Brazil.

出版信息

Nutr Cancer. 1997;28(2):212-7. doi: 10.1080/01635589709514577.

Abstract

Swiss mice fed commercial or elemental diets and an oral short-chain fatty acid (SCFA) solution or saline were treated with the cytostatic drug Ara-C (cytarabine, 3.6 mg/mouse/day) for two or four days. Histopathological examination revealed less damage (atrophy, inflammation, or necrosis) to the small intestine and colon caused by Ara-C when SCFA was administered. Accordingly, protein and nucleotide concentrations in the intestinal mucosa were higher in the group receiving SCFA than in the group receiving a placebo of the same pH and osmolarity. Improvement by SCFA treatment was correlated with an increase in the height of the intestinal villi, with no alterations of the crypts. Furthermore, the number of intraepithelial lymphocytes was similar to normal values in animals receiving SCFA and Ara-C. When large doses of SCFA were administered, xanthomized enterocytes appeared, suggesting an accumulation of fatty acids in these cells. We conclude that oral administration of SCFA at close to physiological proportions reduces the inflammation and necrosis caused by Ara-C administration, thus representing a potential factor for the improvement of patients with mucositis caused by cancer treatment.

摘要

给喂食商业饲料或元素饮食并口服短链脂肪酸(SCFA)溶液或生理盐水的瑞士小鼠,用细胞抑制药物阿糖胞苷(Ara-C,3.6毫克/小鼠/天)处理两天或四天。组织病理学检查显示,给予SCFA时,Ara-C对小肠和结肠造成的损伤(萎缩、炎症或坏死)较轻。因此,接受SCFA的组中肠黏膜的蛋白质和核苷酸浓度高于接受相同pH和渗透压安慰剂的组。SCFA治疗带来的改善与肠绒毛高度增加相关,隐窝无变化。此外,接受SCFA和Ara-C的动物上皮内淋巴细胞数量与正常值相似。当给予大剂量SCFA时,出现了黄色化的肠上皮细胞,表明这些细胞中脂肪酸积累。我们得出结论,以接近生理比例口服SCFA可减轻Ara-C给药引起的炎症和坏死,因此是改善癌症治疗引起的粘膜炎患者的一个潜在因素。

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