Pack S D, Kirschner L S, Pak E, Zhuang Z, Carney J A, Stratakis C A
Unit on Genetics and Endocrinology, Developmental Endocrinology Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892-1862, USA.
J Clin Endocrinol Metab. 2000 Oct;85(10):3860-5. doi: 10.1210/jcem.85.10.6875.
Carney complex (CNC) is a familial multiple neoplasia and lentiginosis syndrome with features overlapping those of McCune-Albright syndrome (MAS) and other multiple endocrine neoplasia (MEN) syndromes, MEN type 1 (MEN 1), in particular. GH-producing pituitary tumors have been described in individual reports and in at least two large CNC patient series. It has been suggested that the evolution of acromegaly in CNC resembles that of the other endocrine manifestations of CNC in its chronic, often indolent, progressive nature. However, histologic and molecular evidence has not been presented in support of this hypothesis. In this investigation, the pituitary glands of eight patients with CNC and acromegaly [age, 22.9+/-11.6 yr (mean +/- SD)] were studied histologically. Tumor DNA was used for comparative genomic hybridization (CGH) (four tumors). All tumors stained for both GH and prolactin PRL (eight of eight), and some for other hormones, including alpha-subunit. Evidence for somatomammotroph hyperplasia was present in five of the eight patients in proximity to adenoma tissue; in the remaining three only adenoma tissue was available for study. CGH showed multiple changes involving losses of chromosomal regions 6q, 7q, 11p, and 11q, and gains of 1pter-p32, 2q35-qter, 9q33-qter, 12q24-qter, 16, 17, 19p, 20p, 20q, 22p and 22q in the most aggressive tumor, an invasive macroadenoma; no chromosomal changes were seen in the microadenomas diagnosed prospectively (3 tumors). We conclude that, in at least some patients with CNC, the pituitary gland is characterized by somatotroph hyperplasia, which precedes GH-producing tumor formation, in a pathway similar to that suggested for MAS-related pituitary tumors. Three GH-producing microadenomas showed no genetic changes by CGH, whereas a macroadenoma in a patient, whose advanced acromegaly was not cured by surgery, showed extensive CGH changes. We speculate that these changes represent secondary and tertiary genetic "hits" involved in pituitary oncogenesis. The data (1) underline the need for early investigation for acromegaly in patients with CNC; (2) provide a molecular hypothesis for its clinical progression; and (3) suggest a model for MAS- and, perhaps, MEN 1-related GH-producing tumor formation.
卡尼综合征(CNC)是一种家族性多发性肿瘤和雀斑综合征,其特征与麦库恩-奥尔布赖特综合征(MAS)及其他多发性内分泌肿瘤(MEN)综合征,尤其是MEN 1型综合征(MEN 1)有重叠。个别报告及至少两个大型CNC患者系列中均描述过生长激素(GH)分泌性垂体肿瘤。有人提出,CNC中肢端肥大症的发展过程在其慢性、通常隐匿且渐进的性质方面类似于CNC的其他内分泌表现。然而,尚未有组织学和分子学证据支持这一假说。在本研究中,对8例患有CNC和肢端肥大症的患者[年龄,22.9±11.6岁(均值±标准差)]的垂体进行了组织学研究。肿瘤DNA用于比较基因组杂交(CGH)分析(4个肿瘤)。所有肿瘤均同时表达GH和催乳素(PRL)(8/8),部分肿瘤还表达其他激素,包括α亚基。8例患者中有5例在腺瘤组织附近存在生长激素泌乳素细胞增生的证据;其余3例仅获得腺瘤组织用于研究。CGH显示,在侵袭性大腺瘤这一最具侵袭性的肿瘤中存在多个变化,包括6号染色体长臂、7号染色体长臂、11号染色体短臂和11号染色体长臂区域缺失,以及1号染色体短臂末端至32区、2号染色体长臂35区至末端、9号染色体长臂33区至末端、12号染色体长臂24区至末端、16号、17号、19号染色体短臂、20号染色体短臂、20号染色体长臂、22号染色体短臂和22号染色体长臂区域增加;前瞻性诊断的微腺瘤(3个肿瘤)未见染色体变化。我们得出结论,至少在部分CNC患者中,垂体的特征是生长激素细胞增生,这在产生GH的肿瘤形成之前发生,其途径类似于MAS相关垂体肿瘤所提示的途径。3个产生GH的微腺瘤通过CGH未显示基因变化,而1例患者的大腺瘤,其晚期肢端肥大症手术未能治愈,显示出广泛的CGH变化。我们推测这些变化代表垂体肿瘤发生过程中涉及的继发性和三级基因“打击”。这些数据(1)强调了对CNC患者进行肢端肥大症早期检查的必要性;(2)为其临床进展提供了分子学假说;(3)提出了一个关于MAS以及可能的MEN 1相关GH分泌性肿瘤形成的模型。
