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Cyclophosphamide-Induced Disruptions to Appetitive Qualities and Detection Thresholds of NaCl: Comparison of Single-Dose and Dose Fractionation Effects

机译:环磷酰胺诱导的NaCl对食欲品质和检测阈值的破坏:单剂量和剂量分馏效应的比较

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Chemotherapy is one of the most common treatments for cancer; however, a side effect is often altered taste. This study examined how cyclophosphamide, a chemotherapy drug, affects salt taste in mice. On the basis of previous findings, it was predicted that cyclophosphamide-induced disruptions in salt taste would be observed near days 2-4, 8-12, and 22-24 posttreatment, and that multiple, smaller doses would cause more severe disruptions to taste. To test these predictions, two experiments were performed, one using brief access testing to measure appetitive qualities, and another using operant conditioning to measure detection thresholds. After a single 100 mg/kg cyclophosphamide injection, peak alterations in brief access lick rates were seen near days 5-8 and 15 posttreatment, whereas peak alterations in detection thresholds were seen days 6, 14, and 20 posttreatment. After five 20 mg/kg injections of cyclophosphamide, brief access lick rates revealed disruptions only on postinjection day 8 whereas thresholds appeared to cycle, gradually increased to and decreased from peak elevations on posttreatment days 4, 10, 15, 20, and 23. Although salt taste functions were disrupted by cyclophosphamide, the patterns of these disruptions were less severe and shorter than expected from cell morphology studies, suggesting a functional adjustment to maintain behavioral accuracy. Fractionation of cyclophosphamide dosing had minimum effect on brief access responses but caused longer, cyclic-like disruptions of detection thresholds compared to single-dose administration.
机译:化疗是癌症中最常见的治疗方法之一;然而,副作用往往改变了味道。本研究研究了环磷酰胺,化疗药物如何影响小鼠的盐味。在先前的发现的基础上,预测盐味的环磷酰胺诱导的破坏将在2-4,8-​​12和22-24天后观察,并且多个较小剂量会导致味道更严重的破坏。为了测试这些预测,进行了两个实验,使用简要访问测试来测量满足品质,以及使用操作分发来测量检测阈值的另一个实验。在单一100毫克/千克环磷酰胺注射后,在5-8天和15天后,在第5-8天和15天和15天的峰值改变时,检测阈值的峰值改变是在第6,14天和20天的后处理。经过五次20mg / kg环磷酰胺的注射后,简要访问舔率仅显示出关注的第8天的中断,而阈值似乎循环,则从后处理时期4,10,15,20和23上的峰值高度逐渐增加和减少。盐味函数被环磷酰胺破坏,这些破坏的模式较小,细胞形态学研究的预期较小,表明函数调整以维持行为准确性。与单剂量给药相比,环磷酰胺定量给药的分馏具有最小的效果,但导致较长的检测阈值的循环异常中断。

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