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转基因大鼠中血管加压素合成神经元的条件性缺失

Conditional ablation of vasopressin-synthesizing neurons in transgenic rats.

机构信息

Department of Physiology, Jichi Medical University, Shimotsuke, Tochigi, Japan.

Institute for Research Initiatives, Nara Institute of Science and Technology, Ikoma, Nara, Japan.

出版信息

J Neuroendocrinol. 2021 Dec;33(12):e13057. doi: 10.1111/jne.13057. Epub 2021 Nov 8.

Abstract

Vasopressin-synthesizing neurons are located in several brain regions, including the hypothalamic paraventricular nucleus (PVN), supraoptic nucleus (SON) and suprachiasmatic nucleus (SCN). Vasopressin has been shown to have various functions in the brain, including social recognition memory, stress responses, emotional behaviors and circadian rhythms. The precise physiological functions of vasopressin-synthesizing neurons in specific brain regions remain to be clarified. Conditional ablation of local vasopressin-synthesizing neurons may be a useful tool for investigation of the functions of vasopressin neurons in the regions. In the present study, we characterized a transgenic rat line that expresses a mutated human diphtheria toxin receptor under control of the vasopressin gene promoter. Under a condition of salt loading, which activates the vasopressin gene in the hypothalamic PVN and SON, transgenic rats were i.c.v. injected with diphtheria toxin. Intracerebroventricular administration of diphtheria toxin after salt loading depleted vasopressin-immunoreactive cells in the hypothalamic PVN and SON, but not in the SCN. The number of oxytocin-immunoreactive cells in the hypothalamus was not significantly changed. The rats that received i.c.v. diphtheria toxin after salt loading showed polydipsia and polyuria, which were rescued by peripheral administration of 1-deamino-8-d-arginine vasopressin via an osmotic mini-pump. Intrahypothalamic administration of diphtheria toxin in transgenic rats under a normal hydration condition reduced the number of vasopressin-immunoreactive neurons, but not the number of oxytocin-immunoreactive neurons. The transgenic rat model can be used for selective ablation of vasopressin-synthesizing neurons and may be useful for clarifying roles of vasopressin neurons at least in the hypothalamic PVN and SON in the rat.

摘要

加压素合成神经元位于多个脑区,包括下丘脑室旁核(PVN)、视上核(SON)和视交叉上核(SCN)。加压素在大脑中具有多种功能,包括社交识别记忆、应激反应、情绪行为和昼夜节律。特定脑区加压素合成神经元的确切生理功能仍有待阐明。局部加压素合成神经元的条件性缺失可能是研究这些区域加压素神经元功能的有用工具。在本研究中,我们构建了一个表达在加压素基因启动子控制下的突变型人白喉毒素受体的转基因大鼠品系。在盐负荷条件下,激活下丘脑 PVN 和 SON 中的加压素基因,将转基因大鼠脑室内注射白喉毒素。盐负荷后,脑室内给予白喉毒素可耗竭下丘脑 PVN 和 SON 中的加压素免疫反应性细胞,但不影响 SCN。下丘脑内催产素免疫反应性细胞的数量没有明显变化。接受盐负荷后脑室内白喉毒素注射的大鼠表现出多饮多尿,这可通过渗透压微型泵外周给予 1-脱氨-8-D-精氨酸加压素得到挽救。在正常水合条件下,将白喉毒素给予转基因大鼠下丘脑内可减少加压素免疫反应性神经元的数量,但不减少催产素免疫反应性神经元的数量。该转基因大鼠模型可用于选择性耗竭加压素合成神经元,对于阐明至少在大鼠下丘脑 PVN 和 SON 中加压素神经元的作用可能是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/31eb/9285515/2d88fb37e911/JNE-33-0-g007.jpg

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