Galeotti Nicoletta, Quattrone Alessandro, Vivoli Elisa, Norcini Monica, Bartolini Alessandro, Ghelardini Carla
Department of Preclinical and Clinical Pharmacology, University of Florence, I-50139 Florence, Italy.
Learn Mem. 2008 Apr 25;15(5):315-23. doi: 10.1101/lm.929008. Print 2008 May.
The administration of the ryanodine receptor (RyR) agonist 4-Cmc (0.003-9 nmol per mouse intracerebroventricularly [i.c.v.]) ameliorated memory functions, whereas the RyR antagonist ryanodine (0.0001-1 nmol per mouse i.c.v.) induced amnesia in the mouse passive avoidance test. The role of the type 1, 2, and 3 RyR isoforms in memory processes was then evaluated by inhibiting the expression of the three RyR proteins in the mouse brain. A selective knockdown of the RyR isoforms was obtained by the i.c.v. administration of antisense oligonucleotides (aODNs) complementary to the sequence of RyR1, RyR2 and RyR3 proteins, as demonstrated by immunoblotting experiments. RyR1 (5-9 nmol per mouse i.c.v.) knockdown mice did not show any memory dysfunction. Conversely, RyR2 (1-7 nmol per mouse i.c.v.) and RyR3 (1-7 nmol per mouse i.c.v.) knockdown animals showed an impairment of memory processes. This detrimental effect was temporary and reversible, disappearing 7 d after the end of the aODN treatment. At the highest effective doses, none of the compounds used impaired motor coordination, as revealed by the rota rod test, nor modified spontaneous mobility and inspection activity, as revealed by the hole-board test. In conclusion, the lack of any involvement of cerebral RyR1 was demonstrated. These findings also showed the involvement of type 2 and type 3 RyR in the modulation of memory functions identifying these cerebral RyR isoforms as critical targets underlying memory processes.
给小鼠脑室内注射(i.c.v.)ryanodine受体(RyR)激动剂4-Cmc(每只小鼠0.003 - 9 nmol)可改善记忆功能,而RyR拮抗剂ryanodine(每只小鼠i.c.v. 0.0001 - 1 nmol)在小鼠被动回避试验中诱导失忆。然后通过抑制小鼠脑中三种RyR蛋白的表达来评估1型、2型和3型RyR亚型在记忆过程中的作用。如免疫印迹实验所示,通过脑室内注射与RyR1、RyR2和RyR3蛋白序列互补的反义寡核苷酸(aODNs)实现了RyR亚型的选择性敲低。RyR1敲低小鼠(每只小鼠i.c.v. 5 - 9 nmol)未表现出任何记忆功能障碍。相反,RyR2敲低动物(每只小鼠i.c.v. 1 - 7 nmol)和RyR3敲低动物(每只小鼠i.c.v. 1 - 7 nmol)表现出记忆过程受损。这种有害作用是暂时且可逆的,在aODN治疗结束后7天消失。在最高有效剂量下,旋转棒试验表明所使用的化合物均未损害运动协调性,孔板试验表明也未改变自发活动和探究活动。总之,证明了脑内RyR1没有任何参与。这些发现还表明2型和3型RyR参与了记忆功能的调节,确定这些脑内RyR亚型是记忆过程的关键靶点。