Ovarian Hormones Regulate Nicotine Consumption and Accumbens Glutamatergic Plasticity in Female Rats

尼古丁 伏隔核 谷氨酸的 内科学 内分泌学 去卵巢大鼠 卵巢 雌激素 中棘神经元 激素 医学 受体 谷氨酸受体 多巴胺 纹状体
作者
Erin E. Maher,Zachary A. Kipp,Jonna M. Leyrer‐Jackson,Shailesh Khatri,Emma O. Bondy,Genesee J. Martinez,Joshua S. Beckmann,Terry D. Hinds,Heather A. Bimonte‐Nelson,Cassandra D. Gipson
出处
期刊:ENeuro [Society for Neuroscience]
卷期号:9 (3): ENEURO.0286-21.2022 被引量:12
标识
DOI:10.1523/eneuro.0286-21.2022
摘要

Abstract Women report greater cigarette cravings during the menstrual cycle phase with higher circulating levels of 17β-estradiol (E2), which is metabolized to estrone (E1). Both E2 and E1 bind to estrogen receptors (ERs), which have been highly studied in the breast, uterus, and ovary. Recent studies have found that ERs are also located on GABAergic medium spiny neurons (MSNs) within the nucleus accumbens core (NAcore). Glutamatergic plasticity in NAcore MSNs is altered following nicotine use; however, it is unknown whether estrogens impact this neurobiological consequence. To test the effect of estrogen on nicotine use, we ovariectomized (OVX) female rats that then underwent nicotine self-administration acquisition and compared them to ovary-intact (sham) rats. The OVX animals then received either sesame oil (vehicle), E2, or E1+E2 supplementation for 4 or 20 d before nicotine sessions. While both ovary-intact and OVX females readily discriminated levers, OVX females consumed less nicotine than sham females. Further, neither E2 nor E1+E2 increased nicotine consumption back to sham levels following OVX, regardless of the duration of the treatment. OVX also rendered NAcore MSNs in a potentiated state following nicotine self-administration, which was reversed by 4 d of systemic E2 treatment. Finally, we found that E2 and E1+E2 increased ERα mRNA in the NAcore, but nicotine suppressed this regardless of hormone treatment. Together, these results show that estrogens regulate nicotine neurobiology, but additional factors may be required to restore nicotine consumption to ovary-intact levels.
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