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首页> 外文期刊>Journal of Ovarian Research >Use of a Small Animal Radiation Research Platform (SARRP) facilitates analysis of systemic versus targeted radiation effects in the mouse ovary
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Use of a Small Animal Radiation Research Platform (SARRP) facilitates analysis of systemic versus targeted radiation effects in the mouse ovary

机译:使用小动物辐射研究平台(SARRP)促进了小鼠卵巢中系统性与靶向辐射效应的分析

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Radiation exposure is known to cause accelerated aging and damage to the ovary, but the contribution of indirect versus direct effects is not well understood. We used the Small Animal Radiation Research Platform (SARRP) (Xstrahl) to deliver radiation to precise fields equivalent to clinical practice, allowing us to investigate systemic versus targeted damage in a structure as small as the mouse ovary. The X-ray dose was kept constant at 1?Gy, but the field varied. Mice either received total body irradiation (TBI), radiation targeted to both ovaries (T2), or radiation targeted to one ovary (left) while the contralateral ovary (right) was spared (T1). Sham mice, handled similarly to the other cohorts but not exposed to radiation, served as controls. Two weeks post-exposure, ovaries were harvested and analyzed histologically to identify and count follicles within each ovary. Radiation significantly reduced primordial follicles in the TBI and T2 cohorts compared to the Sham cohort. There were no significant differences between these two irradiated groups. These findings suggest that at 1?Gy, the extent of damage to the ovary caused by radiation is similar despite the different delivery methods. When investigating the T1 cohort, targeted ovaries showed a significant decrease in primordial and growing follicles compared to non-targeted contralateral ovaries. These findings demonstrate that the SARRP is an effective strategy for delivering precise ionizing radiation to small organs such as mouse ovaries. Such tools will facilitate identifying the relative risks to ovarian function associated with different radiation fields as well as screening the efficacy of emerging fertoprotective agents.
机译:众所周知,辐射暴露会导致加速老化和对卵巢的损伤,但间接与直接效应的贡献尚不清楚。我们使用小型动物辐射研究平台(SARRP)(XSTRAHL)(XSTRAHL)向辐射提供相当于临床实践的精确领域,允许我们在小鼠卵巢的结构中调查全身与靶向损伤。 X射线剂量保持恒定在1?GY,但场变化。小鼠接受总体照射(TBI),靶向卵巢(T2)的辐射,或靶向一个卵巢(左)的辐射,而对侧卵巢(右)被施加(t1)。假小鼠,与其他队列类似但没有暴露在辐射,作为对照。暴露后两周,收获卵巢并在组织学上分析,以鉴定每个卵巢内的卵泡。与假群相比,辐射显着减少了TBI和T2群中的原始卵泡。这两个辐照群体之间没有显着差异。这些研究结果表明,尽管不同的递送方法,由辐射引起的卵巢损坏程度相似。当研究T1队列时,与非靶向对侧卵巢相比,靶卵巢显示出原始和生长卵泡的显着降低。这些发现表明,SARRP是一种有效的策略,用于将精确电离辐射递送到小器官,例如小鼠卵巢。这些工具将有助于识别与不同辐射场相关的卵巢功能的相对风险以及筛选出现的培发剂药物的功效。

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