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多巴胺激动剂药物对分泌催乳素的垂体腺瘤的影响。一项包括免疫细胞化学、电子显微镜检查和原位杂交的形态学研究。

Effect of dopamine agonist medication on prolactin producing pituitary adenomas. A morphological study including immunocytochemistry, electron microscopy and in situ hybridization.

作者信息

Kovacs K, Stefaneanu L, Horvath E, Lloyd R V, Lancranjan I, Buchfelder M, Fahlbusch R

机构信息

Department of Pathology, St. Michael's Hospital, University of Toronto, Ontario, Canada.

出版信息

Virchows Arch A Pathol Anat Histopathol. 1991;418(5):439-46. doi: 10.1007/BF01605931.

Abstract

Conventional light microscopy, immunocytochemistry, electron microscopy and in situ hybridization were used to evaluate the effect of dopamine agonists (bromocriptine-LAR and bromocriptine) on the morphology of surgically removed prolactin (PRL)-producing pituitary adenomas. Dopamine agonist therapy resulted in decrease of serum PRL, clinical improvement and tumour shrinkage. Using light and electron microscopy cellular atrophy, interstitial and perivascular fibrosis were noted; in several tumours connective tissue accumulation was pronounced. The cellular response was not uniform. In some adenomas populations of large cells and small cells were distinguished. The large cells contained immunoreactive PRL and expressed the PRL gene indicating resistance to dopamine agonists. It appears that these cells retained the potential to secrete PRL and proliferate despite exposure to dopamine agonists. In the small cells, PRL immunoreactivity and PRL gene expression decreased providing evidence that both PRL release and synthesis were blocked. Small cells can persist in tumours after discontinuation of dopamine agonist medication suggesting these small cells are irreversibly suppressed and are not capable of regaining their endocrine function and proliferative capability. The formation of irreversibly suppressed PRL cells may explain why some PRL-producing adenomas do not recur after withdrawal of dopamine agonists.

摘要

采用传统光学显微镜、免疫细胞化学、电子显微镜及原位杂交技术,评估多巴胺激动剂(长效溴隐亭和溴隐亭)对手术切除的泌乳素(PRL)分泌型垂体腺瘤形态学的影响。多巴胺激动剂治疗导致血清PRL水平降低、临床症状改善及肿瘤缩小。通过光学显微镜和电子显微镜观察发现细胞萎缩、间质及血管周围纤维化;在一些肿瘤中,结缔组织积聚明显。细胞反应并不一致。在一些腺瘤中,可区分出大细胞群体和小细胞群体。大细胞含有免疫反应性PRL并表达PRL基因,表明对多巴胺激动剂具有抗性。似乎这些细胞尽管暴露于多巴胺激动剂,仍保留分泌PRL和增殖的潜能。在小细胞中,PRL免疫反应性和PRL基因表达降低,这表明PRL的释放和合成均被阻断。停用多巴胺激动剂药物后,小细胞仍可在肿瘤中持续存在,提示这些小细胞被不可逆地抑制,且无法恢复其内分泌功能和增殖能力。不可逆抑制的PRL细胞的形成可能解释了为什么一些PRL分泌型腺瘤在停用多巴胺激动剂后不会复发。

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