Alexandroff A B, Jackson A M, Chisholm G D, James K
Medical School, University of Edinburgh, UK.
Eur J Cancer. 1995 Nov;31A(12):2059-66. doi: 10.1016/0959-8049(95)00210-3.
Epidermal growth factor is a potential mitogen for many different human tumours. Its effect is mediated via a bispecific receptor (EGFR), the expression of which correlates well with invasive disease. We investigated the modulation of EGFR by cytokines produced following bacillus Calmette Guerin (BCG)-immunotherapy. Our data demonstrate the IFN gamma, TNF alpha and IL-1 alpha can decrease the expression of EGFR on some bladder tumour cell lines. IFN gamma reduced EGFR expression on two of eight cell lines (RT4, SD). However, IL-1 and TNF did not share this activity. When cells were treated with a combination of all three cytokines, EGFR was decreased on three cell lines (RT4, RT112, SD) and furthermore, the change in the receptor expression was even more marked. Treatment with phorbol ester (thereby activating protein kinase C) resulted in rapid disappearance of the receptor from the cell surface. Interestingly, the decrease of EGFR expression did not require protein synthesis. Although the cytokines studied could down modulate EGFR, this only occurred on three out of eight cell lines; therefore, it is unlikely that the suppression of proliferative activity caused by cytokine-induced decrease of EGFR expression is central to the antitumour action of BCG therapy, but in a proportion of tumours this mechanism may be involved.
表皮生长因子是许多不同人类肿瘤的潜在促分裂原。其作用通过一种双特异性受体(表皮生长因子受体,EGFR)介导,该受体的表达与侵袭性疾病密切相关。我们研究了卡介苗(BCG)免疫治疗后产生的细胞因子对EGFR的调节作用。我们的数据表明,γ干扰素、肿瘤坏死因子α和白细胞介素-1α可降低某些膀胱肿瘤细胞系上EGFR的表达。γ干扰素降低了8个细胞系中2个(RT4、SD)的EGFR表达。然而,白细胞介素-1和肿瘤坏死因子并不具有这种活性。当细胞用这三种细胞因子联合处理时,3个细胞系(RT4、RT112、SD)上的EGFR降低,而且,受体表达的变化更为明显。用佛波酯处理(从而激活蛋白激酶C)导致受体从细胞表面迅速消失。有趣的是,EGFR表达的降低并不需要蛋白质合成。虽然所研究的细胞因子可下调EGFR,但这仅发生在8个细胞系中的3个;因此,细胞因子诱导的EGFR表达降低所导致的增殖活性抑制不太可能是BCG治疗抗肿瘤作用的核心,但在一部分肿瘤中可能涉及这一机制。
