Gervais Nicole J, Hamel Laurie M, Brake Wayne G, Mumby Dave G
Center for Studies in Behavioral Neurobiology (CSBN), Department of Psychology, Concordia University, 7141 Sherbrooke Street West (SP-244), Montreal, Quebec H4B 1R6, Canada.
Neurobiol Learn Mem. 2016 Sep;133:89-99. doi: 10.1016/j.nlm.2016.06.012. Epub 2016 Jun 15.
Intra-rhinal cortical infusion of 17-β estradiol (E2, 244.8pg/μl) enhances performance on the Novel-Object Preference (NOP) test and impairs accuracy on the delayed nonmatching-to-sample (DNMS) task in the same set of ovariectomized rats (Gervais, Jacob, Brake, & Mumby, 2013). These results appear paradoxical, as normal performance on both tests require intact object-recognition memory (ORM) ability. While demonstrating a preference for the novel object requires recognizing the sample object, rodents can recognize the sample object and still fail to demonstrate a preference. Therefore, enhanced NOP test performance is consistent with both improved ORM and increased novel-object exploration independent of memory processes. There is some evidence suggesting that estrogen receptor (ER) β agonists enhance NOP test performance (Jacome et al., 2010), but no study to date has examined the role of this receptor in DNMS task performance in rodents. The aim of the present study was to determine whether intra-PRh infusion of an ER β agonist, diarylpropionitrile (DPN, 2μg/μl), has divergent effects on novel-object preference (i.e. novelty preference) and accuracy on the DNMS task. Ovariectomized (OVX) rats (n=7) received chronic low E2 (∼22pg/ml serum) replacement, then intra-PRh infusion of DPN (2μg/μl), E2 (244.8pg/μl), or vehicle before each mixed-delay session (0.5-5min) of the DNMS task. A different set of OVX rats (n=10) received the same infusions before each NOP test trial, and were tested either 4 or 72h later. Consistent with Gervais et al. (2013), intra-PRh E2 reduced accuracy on the DNMS task following a 5-min retention delay and enhanced novelty preference on both tests. Intra-PRh DPN was associated with accuracy that was similar to the vehicle-infusion condition, despite enhancing novelty preference on both tests. The accuracy results suggest that while intra-PRh E2 impairs ORM, ERβ does not play a role. However, ERβ in the PRh appears to be important for the expression of novelty preference, in a manner that is unaffected by retention delay. These findings suggest that the modulation of novelty preference by intra-PRh E2/ERβ may be due to factors unrelated to ORM.
在一组卵巢切除的大鼠中,经鼻内皮质注入17-β雌二醇(E2,244.8皮克/微升)可提高新奇物体偏好(NOP)测试的表现,并损害延迟非匹配样本(DNMS)任务的准确性(热尔韦、雅各布、布雷克和蒙比,2013年)。这些结果似乎自相矛盾,因为这两项测试的正常表现都需要完整的物体识别记忆(ORM)能力。虽然表现出对新奇物体的偏好需要识别样本物体,但啮齿动物可以识别样本物体却仍无法表现出偏好。因此,NOP测试表现的提高与ORM的改善以及独立于记忆过程的新奇物体探索增加均相符。有一些证据表明雌激素受体(ER)β激动剂可提高NOP测试的表现(雅科梅等人,2010年),但迄今为止尚无研究考察该受体在啮齿动物DNMS任务表现中的作用。本研究的目的是确定经鼻内梨状皮质注入ERβ激动剂二芳基丙腈(DPN,2微克/微升)对新奇物体偏好(即新奇性偏好)和DNMS任务准确性是否有不同影响。卵巢切除(OVX)大鼠(n = 7)接受慢性低剂量E2(血清约22皮克/毫升)替代,然后在DNMS任务的每个混合延迟时段(0.5 - 5分钟)前经鼻内梨状皮质注入DPN(2微克/微升)、E2(244.8皮克/微升)或赋形剂。另一组不同的OVX大鼠(n = 10)在每次NOP测试试验前接受相同的注入,并在4或72小时后进行测试。与热尔韦等人(2013年)的研究一致,经鼻内梨状皮质注入E2在5分钟的保持延迟后降低了DNMS任务的准确性,并提高了两项测试中的新奇性偏好。经鼻内梨状皮质注入DPN尽管提高了两项测试中的新奇性偏好,但其准确性结果与注入赋形剂的情况相似。准确性结果表明,虽然经鼻内梨状皮质注入E2会损害ORM,但ERβ不起作用。然而,梨状皮质中的ERβ似乎对新奇性偏好的表达很重要,其方式不受保持延迟的影响。这些发现表明,经鼻内梨状皮质注入E2/ERβ对新奇性偏好的调节可能是由于与ORM无关的因素。
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