Saraco Nora, Berensztein Esperanza, Sciara Mariela, de Davila Maria T G, Ciaccio Marta, Ferrari Patricia, Belgorosky Alicia, Rivarola Marco A
Laboratorio de Investigación, Hospital de Pediatria Garrahan, Buenos Aires, Argentina.
Pediatr Dev Pathol. 2006 May-Jun;9(3):181-9. doi: 10.2350/06-04-0074.1.
Large cell calcifying Sertoli cell tumors (LCCSCT) are associated with Carney complex and Peutz-Jeghers syndrome. The mechanisms linking these 2 genetic defects to the genesis of this tumor are obscure. Studies of CYP19 (aromatase) and transforming growth factor (TGF)-beta1 messenger RNA (mRNA) abundance, estrogen receptor (ER), TGFbeta1, and TGFbeta type II receptor (R) immunochemistry were carried out in the testis of a patient with this tumor to gain information on possible mechanisms of cell tumor development. Testicular tissue of a prepubertal patient, collected at gonadectomy, was separated into 2 macroscopically distinct fractions: tumoral nodules (Tu) and extratumoral, normal-looking testicular tissue (ExTu). The patient was a 9.5-year-old boy with a 5-year history of bilateral gynecomastia (Tanner stage 4), no pubic hair, incipient genital development, and bilateral testicular nodules. Multiple pigmented lesions of the skin were present. Bilateral mammectomy and gonadectomy was performed. RNA was extracted from Tu and ExTu for semiquantitative reverse transcriptase-polymerase chain reaction of CYP19 and TGFbeta1. Protein expression of ER, TGFbeta1, and TGFbeta type II R in Tu and ExTu was detected by immunohistochemistry. Cell proliferation was estimated by Ki-67 antigen immunochemistry and apoptosis using a modified TUNEL assay. Mean expression of aromatase and TGFbeta1 mRNAs in Tu was 6- and 2.3-fold higher than in ExTu, respectively (P<0.05). Tumoral cells exhibited ER staining with a predominant extranuclear localization. Positive staining of Sertoli cells in Tu was higher than in ExTu. TGFbeta1 immunostaining of the interstitial cells in Tu was higher than in ExTu. TGFbeta type II R immunostaining was detected in most Sertoli and interstitial cells, but intensity in ExTu was lower than in Tu. No significant difference was detected in the proliferation index, but in Tu, the percentage of Sertoli cells in apoptosis (1.4%) was significantly lower (P<0.01) than in ExTu (14.0%). The following hypothesis is proposed. The congenital gene defects of Carney complex or of Peutz-Jeghers syndrome might trigger a cascade of intracellular events that leads to overexpression of aromatase in Sertoli cells, favoring the development of a LCCSCT. At some point in the evolution of the disease, a mutational event might induce a higher expression of the ER. Also, TGFbeta1 protein expression is increased in neighboring cells. In this environment, TGFbeta1 might switch from tumor suppressor to oncogenic factor and, along with estrogen-ER complexes, might favor tumor progression by inhibiting apoptosis.
大细胞钙化性支持细胞瘤(LCCSCT)与卡尼综合征和黑斑息肉综合征相关。将这两种基因缺陷与该肿瘤发生联系起来的机制尚不清楚。对一名患有此肿瘤患者的睾丸进行了细胞色素P450 19(芳香化酶)和转化生长因子(TGF)-β1信使核糖核酸(mRNA)丰度、雌激素受体(ER)、TGFβ1及TGFβⅡ型受体(R)免疫化学研究,以获取有关细胞瘤发展可能机制的信息。在青春期前患者性腺切除时收集的睾丸组织,在宏观上被分为两个不同部分:肿瘤结节(Tu)和肿瘤外外观正常的睾丸组织(ExTu)。该患者为一名9.5岁男孩,有5年双侧乳腺增生( Tanner 4期)病史,无阴毛,生殖器刚开始发育,双侧睾丸有结节。皮肤上有多个色素沉着病变。进行了双侧乳房切除术和性腺切除术。从Tu和ExTu中提取RNA,用于CYP19和TGFβ1的半定量逆转录聚合酶链反应。通过免疫组织化学检测Tu和ExTu中ER、TGFβ1及TGFβⅡ型R的蛋白表达。通过Ki-67抗原免疫化学估计细胞增殖,并使用改良的TUNEL法检测细胞凋亡。Tu中芳香化酶和TGFβ1 mRNA的平均表达分别比ExTu高6倍和2.3倍(P<0.05)。肿瘤细胞表现出ER染色,主要为核外定位。Tu中支持细胞的阳性染色高于ExTu。Tu中间质细胞的TGFβ1免疫染色高于ExTu。在大多数支持细胞和间质细胞中检测到TGFβⅡ型R免疫染色,但ExTu中的强度低于Tu。增殖指数未检测到显著差异,但在Tu中,凋亡的支持细胞百分比(1.4%)显著低于ExTu(14.0%)(P<0.01)。提出了以下假设。卡尼综合征或黑斑息肉综合征的先天性基因缺陷可能引发一系列细胞内事件,导致支持细胞中芳香化酶过度表达,有利于LCCSCT的发展。在疾病发展的某个阶段,突变事件可能诱导ER更高的表达。此外,相邻细胞中TGFβ1蛋白表达增加。在这种环境下,TGFβ1可能从肿瘤抑制因子转变为致癌因子,并与雌激素-ER复合物一起,通过抑制细胞凋亡促进肿瘤进展。
