Dahia P L, Aguiar R C, Honegger J, Fahlbush R, Jordan S, Lowe D G, Lu X, Clayton R N, Besser G M, Grossman A B
Dept of Endocrinology, St. Bartholomew's Hospital, London, UK.
Oncogene. 1998 Jan 8;16(1):69-76. doi: 10.1038/sj.onc.1201516.
The molecular mechanisms leading to Cushing's disease are unclear. Inhibitors of cyclin-cyclin dependent kinase (CDK) complexes are regulators of the cell cycle and may function as tumour suppressor genes, many of which have been involved in the pathogenesis of several human malignancies. A member of this family, the p27/kip1 gene, maps to chromosome 12p13 and encodes an inhibitor of several cyclin-CDK complexes; these control the progression of the cell cycle from G1 to S-phase. Complete lack of p27/kip1 function, as occurs in the p27/kip1 'knockout' mouse, produces a complex phenotype associated with the development of pituitary tumours, specifically those of the intermediate lobe corticotrophs. We therefore investigated whether structural and functional abnormalities of the p27/kip1 gene and loss at the chromosome 12p13 region were present in human corticotrophin (ACTH)-secreting pituitary tumours. We studied 21 pituitary tumours, of which 20 were ACTH-secreting (two of these had biochemical and histological features of 'intermediate-lobe' tumours and one was malignant) while the remaining tumour was a prolactinoma; three ectopic secretors of ACTH (two bronchial and one thymic carcinoid); and a non-secretory thymic carcinoid. The whole coding region of the p27/ kip1 gene was screened for mutations by PCR-SSCP analysis and/or direct sequencing, while tumour mRNA expression was analysed by means of a semi-quantitative duplex PCR. Three polymorphic microsatellite markers of the 12p13 region were used to assess loss of heterozygosity (LOH) in 12 samples. Finally, tumour p27/kip1 protein expression was assessed by immunohistochemistry using a monoclonal antibody in 12 samples suitable for analysis. No sequence abnormalities were found in any of the samples other than a previously-described polymorphism. No LOH was observed in the tumours analysed. p27/kip1 mRNA expression was similar in tumour samples in comparison with normal pituitaries. Seven of the eight corticotroph tumours analysed by immunohistochemistry stained positive for p27/kip1, including the intermediate lobe. The only malignant pituitary tumour in the original series showed an absence of staining for p27/kip1. In addition, the three carcinoid tumours studied were negative on immunohistochemistry. Of a further three malignant pituitary tumours assessed, two (including a prolactinoma) were essentially negative, while the third was moderately positive. We conclude that mutations of the p27/kip1 gene, deletions of the 12p13 area or changes in expression, are not a general feature of corticotroph tumours, even those with intermediate lobe characteristics. However, other mechanisms of p27/kip1 inactivation, such as an abnormality at the post-translational level, may be related to more aggressive histological subtypes of ACTH-secreting and possibly other pituitary tumours.
导致库欣病的分子机制尚不清楚。细胞周期蛋白 - 细胞周期蛋白依赖性激酶(CDK)复合物抑制剂是细胞周期的调节因子,可能起到肿瘤抑制基因的作用,其中许多已参与多种人类恶性肿瘤的发病机制。该家族的一个成员,p27/kip1基因,定位于染色体12p13,编码几种细胞周期蛋白 - CDK复合物的抑制剂;这些复合物控制细胞周期从G1期到S期的进程。完全缺乏p27/kip1功能,如在p27/kip1“敲除”小鼠中发生的那样,会产生与垂体肿瘤发展相关的复杂表型,特别是中间叶促肾上腺皮质激素细胞的肿瘤。因此,我们研究了人类促肾上腺皮质激素(ACTH)分泌性垂体肿瘤中p27/kip1基因的结构和功能异常以及染色体12p13区域的缺失情况。我们研究了21例垂体肿瘤,其中20例分泌ACTH(其中2例具有“中间叶”肿瘤的生化和组织学特征,1例为恶性),其余1例为催乳素瘤;3例ACTH异位分泌者(2例支气管类癌和1例胸腺类癌);以及1例非分泌性胸腺类癌。通过PCR - SSCP分析和/或直接测序筛选p27/kip1基因的整个编码区的突变,同时通过半定量双链PCR分析肿瘤mRNA表达。使用12p13区域的三个多态性微卫星标记评估12个样本中的杂合性缺失(LOH)。最后,在12个适合分析的样本中,使用单克隆抗体通过免疫组织化学评估肿瘤p27/kip1蛋白表达。除了先前描述的多态性外,在任何样本中均未发现序列异常。在所分析的肿瘤中未观察到LOH。与正常垂体相比,肿瘤样本中p27/kip1 mRNA表达相似。通过免疫组织化学分析的8例促肾上腺皮质激素肿瘤中有7例p27/kip1染色呈阳性,包括中间叶肿瘤。原始系列中唯一的恶性垂体肿瘤p27/kip1染色阴性。此外,所研究的3例类癌肿瘤免疫组织化学染色均为阴性。在另外评估的3例恶性垂体肿瘤中,2例(包括1例催乳素瘤)基本为阴性,而第3例为中度阳性。我们得出结论,p27/kip1基因的突变、12p13区域的缺失或表达变化,并非促肾上腺皮质激素肿瘤的普遍特征,即使是那些具有中间叶特征的肿瘤。然而,p27/kip1失活的其他机制,如翻译后水平的异常,可能与ACTH分泌性以及可能的其他垂体肿瘤的更具侵袭性的组织学亚型有关。
