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慢性溴隐亭治疗雌酮诱导的分泌催乳素的大鼠垂体腺瘤的效果。

Effects of chronic bromocriptine treatment of an estrone-induced, prolactin-secreting rat pituitary adenoma.

作者信息

Eljarmak D, Lis M, Cantin M, Carrière P D, Collu R

出版信息

Horm Res. 1985;21(3):160-7. doi: 10.1159/000180041.

Abstract

Bromocriptine (BROM), a dopamine (DA) agonist, is commonly and successfully used for long-term treatment of human prolactinomas. We have studied the effects of chronic BROM administration to female 344 Fisher/Lis rats bearing an estrone-induced, prolactin (PRL)-secreting pituitary tumor recently characterized as a model for human prolactinoma. The animals were injected twice daily with BROM (2.5 mg/kg) or with diluent. After 1 month of treatment, the animals were sacrificed, and plasma collected and stored at -20 degrees C for PRL radioimmunoassay. The pituitary tumors were removed and tumoral mammotrophs dispersed enzymatically for studies of DA receptor binding and PRL release in vitro. BROM treatment significantly reduced tumor weight, cell size, rough endoplasmic reticulum, Golgi complexes and plasma PRL levels. [3H]-spiroperidol binding to tumoral mammotrophs was also evaluated. BROM induced a significant decrease in the number of DA binding sites without any changes in affinity. These results indicate that chronic BROM treatment of an animal model of prolactinoma induces tumor involution, reduction of PRL release and probably synthesis, and down regulation of dopaminergic binding sites.

摘要

溴隐亭(BROM)是一种多巴胺(DA)激动剂,常用于成功治疗人类泌乳素瘤。我们研究了长期给予携带雌酮诱导的泌乳素(PRL)分泌型垂体瘤的雌性344 Fisher/Lis大鼠溴隐亭的效果,该垂体瘤最近被确定为人类泌乳素瘤的模型。这些动物每天注射两次溴隐亭(2.5毫克/千克)或稀释剂。治疗1个月后,处死动物,收集血浆并储存在-20℃用于PRL放射免疫测定。切除垂体瘤,用酶法分散肿瘤性乳腺细胞用于体外DA受体结合和PRL释放的研究。溴隐亭治疗显著降低了肿瘤重量、细胞大小、粗面内质网、高尔基体复合物和血浆PRL水平。还评估了[3H] - 螺哌啶与肿瘤性乳腺细胞的结合。溴隐亭导致DA结合位点数量显著减少,亲和力无任何变化。这些结果表明,对泌乳素瘤动物模型进行长期溴隐亭治疗可诱导肿瘤 involution,减少PRL释放并可能减少其合成,以及下调多巴胺能结合位点。

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