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溴隐亭抵抗性泌乳素瘤中两种D2多巴胺受体亚型的表达降低。

Decreased expression of the two D2 dopamine receptor isoforms in bromocriptine-resistant prolactinomas.

作者信息

Caccavelli L, Feron F, Morange I, Rouer E, Benarous R, Dewailly D, Jaquet P, Kordon C, Enjalbert A

机构信息

ICNE, UMR9941 CNRS, Université Aix-Marseille II, Faculté de Médecine Nord, Marseille, France.

出版信息

Neuroendocrinology. 1994 Sep;60(3):314-22. doi: 10.1159/000126764.

DOI:10.1159/000126764
PMID:7969790
Abstract

Bromocriptine or other dopamine agonists are usually effective for the treatment of prolactin-secreting adenomas. Five to 18% of prolactinomas, however, do not respond to such therapy. We have shown previously that such resistance to bromocriptine correlates with reduced binding to the D2 receptor subtype of dopamine, the major PRL inhibiting factor. In the present work, we demonstrated that reduced binding actually corresponds to decreased expression of the gene coding for the D2 receptor in the pituitary from bromocriptine-resistant patients, as shown by 4-fold lower levels of the corresponding mRNAs compared to those coding for actin. The existence of two D2 receptor isoforms, D2S and D2L generated by alternative splicing, has been described in several tissues, including the pituitary. Both are negatively coupled to adenylyl cyclase and inhibit prolactin secretion, but, in addition, the shortest one (D2S) is more efficiently coupled to phospholipase C. Consequently, we also investigated whether expression of a particular D2 receptor isoform was preferentially affected in resistant adenomas. The proportion of messengers corresponding to the short receptor isoform (D2S) was lower in resistant compared to responsive adenomas: D2S/D2L = 0.74 +/- 0.08 and 1.00 +/- 0.07, respectively. In parallel, much lower levels of D2 receptor mRNAs were found in growth hormone-secreting adenomas, with a D2S/D2L ratio comparable to those of both normal human pituitary and bromocriptine-sensitive prolactinomas (1.05 +/- 0.11). Thus, resistance to bromocriptine therapy seems to involve defects in D2 dopamine receptor expression and possibly in posttranscriptional splicing.

摘要

溴隐亭或其他多巴胺激动剂通常对治疗分泌催乳素的腺瘤有效。然而,5%至18%的催乳素瘤对这种治疗无反应。我们之前已经表明,对溴隐亭的这种耐药性与多巴胺D2受体亚型(主要的催乳素抑制因子)的结合减少有关。在目前的研究中,我们证明,结合减少实际上对应于溴隐亭耐药患者垂体中编码D2受体的基因表达降低,与编码肌动蛋白的mRNA水平相比,相应mRNA水平低4倍。通过选择性剪接产生的两种D2受体亚型D2S和D2L已在包括垂体在内的多个组织中被描述。两者均与腺苷酸环化酶负偶联并抑制催乳素分泌,但此外,最短的一种(D2S)与磷脂酶C的偶联更有效。因此,我们还研究了在耐药腺瘤中,特定D2受体亚型的表达是否受到优先影响。与反应性腺瘤相比,耐药腺瘤中对应短受体亚型(D2S)的信使比例较低:D2S/D2L分别为0.74±0.08和1.00±0.07。同时,在分泌生长激素的腺瘤中发现D2受体mRNA水平低得多,其D2S/D2L比值与正常人类垂体和溴隐亭敏感的催乳素瘤相当(1.05±0.11)。因此,对溴隐亭治疗的耐药性似乎涉及D2多巴胺受体表达缺陷以及可能的转录后剪接缺陷。

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