Sanfilippo J S, Rao C V, Guarnaschelli J J, Woost P G, Byrd V M, Jones E, Schultz G S
Department of Obstetrics and Gynecology, University of Louisville School of Medicine, Kentucky.
Surg Gynecol Obstet. 1993 Nov;177(5):488-96.
Epidermal growth factor (EGF) and transforming growth factor alpha (TGF alpha) are potent mitogens for normal cells of ectodermal and mesodermal origin. Evidence is accumulating that suggests that EGF, TGF alpha and their common receptor (EGF/TGF alpha-R) influence development and functioning of tissues of the central nervous system (CNS). To further investigate the possible roles of EGF, TGF alpha and their receptor in autocrine/paracrine regulation of tumor growth in the CNS, a series of tumors of the CNS were analyzed for the presence of specific, high affinity EGF/TGF alpha receptors and for the presence of immunoreactive TGF alpha protein. Binding of 125I-EGF to crude membranes from a pool of meningiomas was competed for equally well by low concentrations of unlabeled EGF or TGF alpha, but not by high concentrations of other protein hormones, demonstrating the high degree of specificity of the EGF/TGF alpha receptor. Specific binding of 125I-EGF was dependent upon time and temperature, with maximum specific binding achieved after two hours at 22 degrees C. Scatchard analysis of six tumors of the CNS large enough to permit titration analysis generated linear plots with an average kilodalton of 1.1 +/- 0.1 nanometer (+/- standard error of the mean), suggesting the presence of a single class of EGF/TGF alpha-R with high affinity. EGF also stimulated phosphorylation of a 170 kilodalton protein in membrane fraction of a meningioma, demonstrating that the EGF/TGF alpha-R in this tumor retained EGF-stimulated kinase autophosphorylating activity. Membranes for 17 additional smaller tumors of the CNS were analyzed for specific binding of 125I-EGF by single, high concentration method, and all 17 tumors were found to contain specific binding of 125I-EGF. The average level of 125I-EGF for all 23 tumors of the CNS was 46 +/- 27 femtomoles per milligram protein with a range of 1 femtomoles per milligram for both a pituitary adenoma and meningioma to 638 femtomoles per milligram for a glioblastoma. A series of 13 tumors of the CNS were analyzed for EGF alpha with use of a specific radioimmunoassay. TGF alpha immunoreactive protein was detected in all four malignant tumors of the CNS assayed at an average level of 2.6 +/- 1.1 nanograms per milligram soluble protein, whereas TGF alpha immunoreactive protein was detected in only two of nine benign tumors of the CNS. These results add support to the hypothesis that TGF alpha and its receptor may act by autocrine/paracrine mechanisms to influence growth of tumors of the CNS in vivo.
表皮生长因子(EGF)和转化生长因子α(TGFα)是外胚层和中胚层来源正常细胞的强效有丝分裂原。越来越多的证据表明,EGF、TGFα及其共同受体(EGF/TGFα-R)会影响中枢神经系统(CNS)组织的发育和功能。为了进一步研究EGF、TGFα及其受体在CNS肿瘤生长的自分泌/旁分泌调节中的可能作用,对一系列CNS肿瘤进行了分析,以检测特异性高亲和力EGF/TGFα受体的存在以及免疫反应性TGFα蛋白的存在。低浓度的未标记EGF或TGFα能同样有效地竞争125I-EGF与脑膜瘤池粗膜的结合,但高浓度的其他蛋白质激素则不能,这证明了EGF/TGFα受体的高度特异性。125I-EGF的特异性结合依赖于时间和温度,在22℃下两小时后达到最大特异性结合。对六个足够大以进行滴定分析的CNS肿瘤进行Scatchard分析,生成了线性图,平均千道尔顿为1.1±0.1纳米(±平均标准误差),表明存在一类具有高亲和力的EGF/TGFα-R。EGF还刺激了脑膜瘤膜部分中一种170千道尔顿蛋白质的磷酸化,表明该肿瘤中的EGF/TGFα-R保留了EGF刺激的激酶自磷酸化活性。通过单一高浓度方法分析了另外17个较小的CNS肿瘤的膜,以检测它们对125I-EGF的特异性结合,发现所有17个肿瘤都含有125I-EGF的特异性结合。所有23个CNS肿瘤的125I-EGF平均水平为每毫克蛋白质46±27飞摩尔,范围从垂体腺瘤和脑膜瘤的每毫克1飞摩尔到胶质母细胞瘤的每毫克638飞摩尔。使用特异性放射免疫测定法对一系列13个CNS肿瘤进行了EGFα分析。在所检测的所有四个CNS恶性肿瘤中均检测到TGFα免疫反应性蛋白,平均水平为每毫克可溶性蛋白2.6±1.1纳克,而在九个CNS良性肿瘤中仅在两个肿瘤中检测到TGFα免疫反应性蛋白。这些结果支持了以下假设,即TGFα及其受体可能通过自分泌/旁分泌机制在体内影响CNS肿瘤的生长。
