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首页> 外文期刊>British Journal of Cancer >Pretreatment with transforming growth factor beta-3 protects small intestinal stem cells against radiation damage in vivo
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Pretreatment with transforming growth factor beta-3 protects small intestinal stem cells against radiation damage in vivo

机译:用转化生长因子β-3进行预处理可保护小肠干细胞免受体内辐射损伤

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The gastrointestinal tract, with its rapid cell replacement, is sensitive to cytotoxic damage and can be a site of dose-limiting toxicity in cancer therapy. Here, we have investigated the use of one growth modulator to manipulate the cell cycle status of gastrointestinal stem cells before cytotoxic exposure to minimize damage to this normal tissue. Transforming growth factor beta-3 (TGF-beta3), a known inhibitor of cell cycle progression through G1, was used to alter intestinal crypt stem cell sensitivity before 12-16 Gy of gamma irradiation, which was used as a model cytotoxic agent. Using a crypt microcolony assay as a measure of functional competence of gastrointestinal stem cells, it was shown that the administration of TGF-beta3 over a 24-h period before irradiation increased the number of surviving crypts by four- to six-fold. To test whether changes in crypt survival are reflected in the well-being of the animal, survival time analyses were performed. After 14.5 Gy of radiation, only 35% of the animals survived within a period of about 12 days, while prior treatment with TGF-beta3 provided significant protection against this early gastrointestinal animal death, with 95% of the treated animals surviving for greater than 30 days.
机译:胃肠道及其快速的细胞置换功能,对细胞毒性损伤敏感,在癌症治疗中可能是剂量限制性毒性的部位。在这里,我们已经研究了使用一种生长调节剂在暴露于细胞毒素之前操纵胃肠干细胞的细胞周期状态,以最大程度地减少对该正常组织的损害。转化生长因子β-3(TGF-β3)是通过G1引起的细胞周期进展的已知抑制剂,被用来在12-16 Gy的γ射线照射之前改变肠隐窝干细胞的敏感性,用作模型细胞毒剂。使用隐窝微菌落测定法作为胃肠干细胞功能能力的量度,结果表明,在照射前24小时内施用TGF-β3使存活的隐窝数目增加了四到六倍。为了测试隐窝存活率的变化是否反映在动物的福祉中,进行了存活时间分析。在14.5 Gy辐射后,仅35%的动物在约12天的时间内存活,而先前用TGF-β3的治疗为这种早期胃肠道动物的死亡提供了显着的保护,其中95%的被治疗动物的存活率超过30天。

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