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首页> 外文期刊>Nutrition and Cancer: An International Journal >Perigestational dietary folic acid deficiency protects against medulloblastoma formation in a mouse model of nevoid basal cell carcinoma syndrome
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Perigestational dietary folic acid deficiency protects against medulloblastoma formation in a mouse model of nevoid basal cell carcinoma syndrome

机译:围产期饮食中的叶酸缺乏可预防空巢性基底细胞癌综合征小鼠模型中的成髓细胞瘤形成

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摘要

Hereditary nevoid basal cell carcinoma syndrome (NBCCS) is caused by PTCH1 gene mutations that result in diverse neoplasms including medulloblastoma (MB). Epidemiological studies report reduced pediatric brain tumor risks associated with maternal intake of prenatal vitamins containing folic acid (FA) and FA supplements specifically. We hypothesized that low maternal FA intake during the perigestational period would increase MB incidence in a transgenic NBCCS mouse model, which carries an autosomal dominant mutation in the Ptch1 gene. Female wild-type C57BL/6 mice (n = 126) were randomized to 1 of 3 diets with differing FA amounts: 0.3 mg/kg (low), 2.0 mg/kg (control), and 8.0 mg/kg (high) 1 mo prior to mating with Ptch1 +/- C57BL/6 males. Females were maintained on the diet until pup weaning; the pups were then aged for tumor development. Compared to the control group, offspring MB incidence was significantly lower in the low FA group (Hazard Ratio = 0.47; 95% confidence interval 0.27-0.80) at 1 yr. No significant difference in incidence was observed between the control and high FA groups. Low maternal perigestational FA levels may decrease MB incidence in mice genetically predisposed to tumor development. Our results could have implications for prenatal FA intake recommendations in the presence of cancer syndromes.
机译:遗传性空洞性基底细胞癌综合征(NBCCS)是由PTCH1基因突变引起的,该突变导致包括髓母细胞瘤(MB)在内的多种肿瘤。流行病学研究报告表明,降低了与孕妇摄入含有叶酸(FA)和FA补充剂的产前维生素相关的小儿脑肿瘤的风险。我们假设在围孕期母体FA摄入量低会增加转基因NBCCS小鼠模型的MB发病率,该模型在Ptch1基因中携带常染色体显性突变。将雌性野生型C57BL / 6小鼠(n = 126)随机分配到FA量不同的3种饮食中的1种:0.3 mg / kg(低),2.0 mg / kg(对照)和8.0 mg / kg(高)1在与Ptch1 +/- C57BL / 6雄性交配之前。雌性保持饮食直到幼仔断奶。然后将幼犬老化以进行肿瘤发展。与对照组相比,低FA组在1年时后代MB发生率显着降低(危险比= 0.47; 95%置信区间0.27-0.80)。在对照组和高FA组之间,未观察到发病率的显着差异。孕妇围产期FA水平低可能会降低遗传上易患肿瘤的小鼠的MB发病率。我们的结果可能对存在癌症综合征的产前FA摄入量建议产生影响。

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