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静脉注射地托咪啶和丁丙诺啡后对母马的促甲状腺激素释放激素的催乳素、促甲状腺激素、促黑素细胞激素和促肾上腺皮质激素的反应。

Plasma prolactin, thyroid-stimulating hormone, melanocyte-stimulating hormone, and adrenocorticotropin responses to thyrotropin-releasing hormone in mares treated with detomidine and butorphanol.

机构信息

School of Animal Sciences, Louisiana Agricultural Experiment Station, Louisiana State University Agricultural Center, Baton Rouge, LA, USA.

School of Animal Sciences, Louisiana Agricultural Experiment Station, Louisiana State University Agricultural Center, Baton Rouge, LA, USA.

出版信息

Domest Anim Endocrinol. 2021 Jan;74:106536. doi: 10.1016/j.domaniend.2020.106536. Epub 2020 Aug 7.

Abstract

Stress or excitement is a concern when performing endocrine tests on fractious horses. Sedation may be a solution; however, perturbation of test results may preclude useful information. Thyrotropin-releasing hormone (TRH) is a known stimulator of prolactin, thyroid-stimulating hormone (TSH), melanocyte-stimulating hormone (MSH), and ACTH. Thyrotropin-releasing hormone-induced ACTH is a diagnostic tool for the assessment of endocrinopathies such as pituitary pars intermedia dysfunction. It is unknown if drugs commonly used for sedation alter endocrine responses. The objective of this study was to assess the effects of detomidine (DET) and butorphanol on endocrine responses to TRH. Nine light horse mares were used in a replicated 3 × 3 Latin square with the following treatments: saline, DET, and detomidine + butorphanol (DET/BUT), all administered intravenously at 0.01 mg/kg BW. A 1-wk washout period was allowed between phases, all of which were performed in December. Blood samples were collected at -10 and 0 min before treatment and 5 and 10 min post-treatment. Administration of 1 mg TRH occurred 10 min post-treatment, and blood sampling continued 5, 10, 20, and 30 min post-TRH. Data were analyzed by ANOVA as a replicated Latin square with repeated sampling. Plasma prolactin increased (P < 0.0001) after TRH in all groups, rapidly peaking at 5 min in drug-treated mares and 40 min in saline-treated mares. The peak prolactin response to TRH was 2-fold higher (P < 0.0001) in saline-treated mares compared with those drug-treated. A peak rise in plasma TSH was observed in DET/BUT-treated mares 10 min after TSH and was greater (P ≤ 0.007) compared with DET- and saline-treated mares. Plasma MSH was stimulated (P = 0.001) by DET and DET/BUT before TRH, and the peak MSH response to TRH was greater (P < 0.0001) in drug-treated mares, although not hastened as observed with prolactin and TSH. A peak rise in ACTH was observed in drug-treated mares 5 min after administration of TRH, whereas a peak rise was observed in control mares 10 min post-TRH and was almost 2-fold lower (P = 0.05) than the peak observed in DET and DET/BUT-treated mares. Basal ACTH concentrations were not affected by DET or DET/BUT, indicating that sedation with these compounds may be achieved when needing to measure basal plasma ACTH. Treatment with DET and DET/BUT did alter the prolactin, TSH, MSH, and ACTH responses to TRH; therefore, the use of these drugs may not be advisable when assessing endocrine responses to TRH stimulation.

摘要

在对易怒的马匹进行内分泌测试时,应激或兴奋是一个关注点。镇静可能是一种解决方案;然而,测试结果的干扰可能会排除有用的信息。促甲状腺素释放激素(TRH)是已知的催乳素、促甲状腺激素(TSH)、促黑素细胞激素(MSH)和促肾上腺皮质激素(ACTH)的刺激物。TRH 诱导的 ACTH 是评估垂体中间叶功能障碍等内分泌疾病的诊断工具。目前尚不清楚常用的镇静药物是否会改变内分泌反应。本研究的目的是评估地托咪定(DET)和布托啡诺对 TRH 诱导的内分泌反应的影响。9 匹轻型马在重复 3 × 3 拉丁方设计中进行了研究,以下处理:生理盐水、DET 和地托咪定+布托啡诺(DET/BUT),均以 0.01mg/kgBW 静脉内给药。每个阶段之间允许 1 周的洗脱期,所有阶段均在 12 月进行。在治疗前-10 分钟和 0 分钟以及治疗后 5 分钟和 10 分钟采集血样。在治疗后 10 分钟给予 1mgTRH,在 TRH 后继续采集 5、10、20 和 30 分钟的血样。数据通过重复拉丁方设计的方差分析进行分析,并进行重复采样。所有组在 TRH 后催乳素均增加(P<0.0001),在药物治疗的母马中 5 分钟时迅速达到峰值,在生理盐水治疗的母马中 40 分钟时达到峰值。与药物治疗的母马相比,生理盐水治疗的母马对 TRH 的催乳素反应峰值高 2 倍(P<0.0001)。在 DET/BUT 治疗的母马中,在 TRH 后 10 分钟观察到 TSH 血浆浓度的峰值升高,并且与 DET 和生理盐水治疗的母马相比,升高幅度更大(P≤0.007)。在 TRH 之前,DET 和 DET/BUT 刺激 MSH 升高(P=0.001),并且药物治疗的母马对 TRH 的 MSH 反应峰值更高(P<0.0001),尽管与催乳素和 TSH 相比,观察到的峰值升高没有加快。在 TRH 给药后 5 分钟,药物治疗的母马中观察到 ACTH 的峰值升高,而在对照母马中,在 TRH 后 10 分钟观察到 ACTH 的峰值升高,并且几乎低 2 倍(P=0.05)与 DET 和 DET/BUT 治疗的母马中的峰值相比。DET 或 DET/BUT 对基础 ACTH 浓度没有影响,这表明当需要测量基础血浆 ACTH 时,这些化合物的镇静作用可能会实现。DET 和 DET/BUT 的治疗确实改变了对 TRH 的催乳素、TSH、MSH 和 ACTH 反应;因此,在评估 TRH 刺激的内分泌反应时,不建议使用这些药物。

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