首页> 美国卫生研究院文献>The Journal of Neuroscience >Administration of testosterone attenuates neuronal loss following axotomy in the brain-stem motor nuclei of female rats
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Administration of testosterone attenuates neuronal loss following axotomy in the brain-stem motor nuclei of female rats

机译:睾丸激素的给药减轻了雌性大鼠脑干运动核在轴突切开后的神经元损失。

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摘要

This study was undertaken to elucidate whether (1) administration of testosterone to female rats attenuates axotomy-induced neuronal loss; (2) the efficacy of testosterone treatment is related to the age of animals, the dosage given, and the time and duration of the treatment; (3) neurons which project or terminate aberrantly can survive; and (4) the trophic actions of testosterone on neuronal survival and axonal outgrowth are operated under the same mechanisms. The hypoglossal and facial nerves were transected unilaterally at 3 and 6 weeks of age. In order to establish the dose-response curve, testosterone propionate (TP) at doses of 0.5, 1.0, 2.0, or 5.0 mg was injected subcutaneously twice weekly during the first 4 postaxotomy weeks, and once weekly thereafter for an additional 6 weeks. Neuronal numbers in the hypoglossal and facial motor nuclei were counted 10–12 weeks after axotomy in serial paraffin sections stained with cresyl violet. To determine the time course of TP effect, neuronal numbers were counted at 1, 4, 12, and 20 weeks after axotomy. In addition, neuronal loss 12 weeks after axotomy in rats treated with TP for the first 3 postaxotomy weeks only was compared with that in rats withheld TP treatment until the 5th postaxotomy week. To determine axonal projections and terminations of the surviving neurons, HRP retrograde tracing technique was used. Results indicated that TP treatment significantly attenuated neuronal loss in prepubertal and young adult female rats in a dose- and time-dependent manner. Only doses which elevated serum testosterone to levels comparable to or surpassing normal male levels were effective.(ABSTRACT TRUNCATED AT 250 WORDS)
机译:进行这项研究以阐明(1)给雌性大鼠施用睾丸激素是否能减轻轴切术引起的神经元丢失; (2)睾丸激素治疗的功效与动物的年龄,给定的剂量以及治疗的时间和持续时间有关; (3)异常突出或终止的神经元可以存活; (4)睾丸激素对神经元存活和轴突生长的营养作用是在相同的机制下进行的。在3周和6周龄时单侧切断舌下神经和面神经。为了建立剂量反应曲线,在断头后的前4周每周两次皮下注射丙酸睾丸酮(TP),剂量分别为0.5、1.0、2.0或5.0 mg,此后每周一次皮下注射,持续6周。轴突切开后10至12周,在连续的石蜡切片中用甲酚紫染色计数舌下和面部运动核的神经元数量。为了确定TP效果的时程,在切开后的第1、4、12和20周对神经元数量进行计数。另外,将仅在TP后3周内接受TP治疗的大鼠的轴突切开后12周的神经元损失与未接受TP治疗的大鼠进行了比较。为了确定存活神经元的轴突投射和终止,使用了HRP逆行追踪技术。结果表明,TP治疗以剂量和时间依赖性方式显着减轻青春期前和成年雌性成年大鼠的神经元损失。只有将血清睾丸激素水平提高到与男性正常水平相当或超过正常水平的剂量才有效。(摘要截断为250个字)

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