Colao A, Merola B, Sarnacchiaro F, Di Sarno A, Landi M L, Marzullo P, Cerbone G, Ferone D, Lombardi G
Department of Molecular and Clinical Endocrinology and Oncology, Federico II University, Naples, Italy.
Horm Res. 1995;44(5):222-8. doi: 10.1159/000184630.
In the last decade, the treatment of macroprolactinomas has been significantly improved by the introduction in the clinical practice of new drugs with dopamine-agonist properties. In particular, the availability of different forms of bromocriptine (BRC) with long duration of action and slow absorption, suitable for injectable (BRC-LAR) or oral (BRC-SRO) administration, has allowed one to obtain a more constant bromocriptinemia than with standard BRC, thus reducing adverse reactions. Moreover, a selective action on dopamine D2 receptors has been achieved using a new non-ergot derivative: the quinagolide (CV 205-502). The aim of this study was to evaluate the effects of BRC-LAR, BRC-SRO and CV 205-502 in 34 patients with macroprolactinoma. PROTOCOL OF THE STUDY: BRC-LAR was given at the monthly dose of 50-100 mg for 6-24 months to 8 patients whose PRL levels were 150-700 micrograms/l. BRC-SRO was given at the daily dose of 5-20 mg for 1-24 months to 10 patients whose PRL levels were 120-900 micrograms/l. CV 205-502 was given at the daily dose of 0.075-0.6 mg for 6-12 months to 16 patients whose PRL levels were 250-2,050 micrograms/l. CT and/or MRI scans were performed before and during treatment to evaluate tumor shrinkage. Data are presented as Mean +/- SD.
Serum PRL levels normalized in 8/8 with BRC-LAR, 7/10 with BRC-SRO and 12/16 patients with CV 205-502. A significant shrinkage of tumor mass was obtained in 7/8 with BRC-LAR, 9/10 with BRC-SRO and 16/16 patients with CV 205-502, with consequent improvement of visual-field defects. Overall, the drugs were rather well tolerated: no patient stopped BRC-LAR or BRC-SRO and only 2 stopped CV 205-502. In particular, nausea, vomiting, headache, hypotension that disappeared spontaneously were observed in 5/8 with BRC-LAR, 4/10 with BRC-SRO and 4/16 with CV 205-502.
The medical approach with long-acting BRC preparations and CV 205-502 which selectively binds D2 receptors allows one to obtain rapid normalization of PRL levels and shrinkage of macroprolactinomas in a large series of patients. These drugs are rather well tolerated also by patients proven to be untolerant to standard BRC.
在过去十年中,具有多巴胺激动剂特性的新药引入临床实践,显著改善了大泌乳素瘤的治疗。特别是,不同形式的溴隐亭(BRC)具有长效作用和缓慢吸收特性,适用于注射(BRC-LAR)或口服(BRC-SRO)给药,与标准BRC相比,能使溴隐亭血症更稳定,从而减少不良反应。此外,使用一种新的非麦角衍生物喹高利特(CV 205-502)实现了对多巴胺D2受体的选择性作用。本研究的目的是评估BRC-LAR、BRC-SRO和CV 205-502对34例大泌乳素瘤患者的疗效。
8例泌乳素(PRL)水平为150 - 700微克/升的患者接受BRC-LAR治疗,每月剂量为50 - 100毫克,持续6 - 24个月。10例PRL水平为120 - 900微克/升的患者接受BRC-SRO治疗,每日剂量为5 - 20毫克,持续1 - 24个月。16例PRL水平为250 - 2050微克/升的患者接受CV 205-502治疗,每日剂量为0.075 - 0.6毫克,持续6 - 12个月。在治疗前和治疗期间进行CT和/或MRI扫描以评估肿瘤缩小情况。数据以平均值±标准差表示。
接受BRC-LAR治疗的8例患者中有8例血清PRL水平恢复正常,接受BRC-SRO治疗的10例患者中有7例,接受CV 205-502治疗的16例患者中有12例。接受BRC-LAR治疗的8例患者中有7例、接受BRC-SRO治疗的10例患者中有9例以及接受CV 205-502治疗的16例患者中的16例肿瘤体积显著缩小,视野缺损随之改善。总体而言,这些药物耐受性良好:没有患者停用BRC-LAR或BRC-SRO,只有2例停用CV 205-502。具体而言,接受BRC-LAR治疗的8例患者中有5例、接受BRC-SRO治疗的10例患者中有4例以及接受CV 205-502治疗的16例患者中有4例出现了自发消失的恶心、呕吐、头痛、低血压症状。
使用长效BRC制剂和选择性结合D2受体的CV 205-502进行药物治疗,可使大量患者的PRL水平迅速恢复正常,大泌乳素瘤缩小。这些药物对被证明不耐受标准BRC的患者也具有较好的耐受性。
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