Christensen M E
Department of Otolaryngology-Head and Neck Surgery, H:S Rigshospitalet, Copenhagen.
Dan Med Bull. 1998 Apr;45(2):121-34.
The EGF receptor (EGF receptor) and two of the ligands, transforming growth factor alpha (TGF-alpha) and epidermal growth factor (EGF), exert mitogenic activities in epithelial cells. Hence, the overall aim of this work was delineation of the EGF receptor system in head and neck carcinomas, which in the majority of cases are epithelial derived tumours. Chapter 1 is a general introduction to head and neck carcinomas and the relevance of the EGF receptor system in this context. Chapter 2 focuses on the immunohistochemical distribution of TGF-alpha in normal human tissues, while previous studies dealing with the growth factor in head and neck carcinomas revealed other localizations in normal cells. TGF-alpha was detected with monoclonal as well as polyclonal antibodies. The results showed that the growth factor is widely distributed in normal human tissues and thus not limited to malignant cells. Chapter 3 describes the immunohistochemical localization of the EGF receptor in 55 patients with squamous cell carcinoma in the head and neck region. The study included adjacent normal mucosa and in 12 cases additional dysplastic areas were present. The EGF receptor was found in the basal cell layer in normal oral and laryngeal mucosa. In sections from patients who had received preoperative irradiation the receptor was in addition seen on the spinous cells. In dysplastic epithelial all cells stained for the EGF receptor. The majority of the head and neck carcinomas expressed the EGF receptor. In poorly differentiated tumours almost all cells were positive for the receptor. Sections from moderately and well differentiated tumours demonstrated a reduction in the extent of stained areas, paralleling the situation observed in the differentiated upper layers of normal oral and laryngeal mucosa. Furthermore, this chapter describes the EGF receptor quantitatively in 60 patients with head and neck carcinoma. This study was performed in order to evaluate if overexpression of the EGF receptor was a common motif for head and neck carcinomas. The level in tumour biopsies was compared with the level in the patients' corresponding normal mucosa. An enzyme-linked immunosorbent assay detecting protein epitopes of the receptor was employed. Overexpression of the receptor was found in the majority of cases. The overexpression was further correlated to clinicopathological parameters. However, no significant correlations were found although the mean values increased with increased tumour size and advanced clinical stage. The use of quantitative assays are further discussed and limitations are emphasized with respect to heterogeneity at the EGF receptor level and the varying stromal components in malignant tissues. Despite these problems the relevance of the EGF receptor a therapeutic situation is illustrated with e.g. EGF receptor antibodies and tyrosine-kinase inhibitors. Chapter 4 focuses on the immunohistochemical expression of EGF and TGF-alpha in carcinomas from same 55 patients. This study included adjacent normal mucosa in which the growth factors were expressed above the basal cell layer. The majority of the tumours expressed both growth factors and none of the sections were negative for both EGF and TGF-alpha. In biopsies from moderately and well differentiated tumours the growth factors were demonstrated in the more differentiated cells. However, in poorly differentiated tumours the cells were positive for EGF and TGF-alpha. Chapter 5 describes immunohistochemical and quantitative changes of salivary EGF, amylase and haptocorrin following radiotherapy for oral cancer. This study was initiated because irradiated oral and laryngeal mucosa have demonstrated staining for the receptor in the basal cell layer as well as in the spinous cells, indicating an upregulation of the receptor in response to lack of EGF. In normal biopsies from the glandula submandibularis and glandula parotis, EGF and amylase were demonstrated in the serous acini, whereas haptoc
表皮生长因子受体(EGF受体)以及两种配体,即转化生长因子α(TGF-α)和表皮生长因子(EGF),在上皮细胞中发挥促有丝分裂活性。因此,本研究的总体目标是描绘头颈部癌中的EGF受体系统,在大多数情况下,头颈部癌是上皮来源的肿瘤。第1章是对头颈部癌以及在此背景下EGF受体系统相关性的概述。第2章重点关注TGF-α在正常人体组织中的免疫组化分布,而之前关于头颈部癌中该生长因子的研究揭示了其在正常细胞中的其他定位。使用单克隆抗体和多克隆抗体检测TGF-α。结果表明,该生长因子在正常人体组织中广泛分布,因此不限于恶性细胞。第3章描述了55名头颈部鳞状细胞癌患者中EGF受体的免疫组化定位。该研究包括相邻的正常黏膜,并且在12例中存在额外的发育异常区域。在正常口腔和喉黏膜的基底细胞层中发现了EGF受体。在接受术前放疗患者的切片中,此外在棘细胞上也可见到该受体。在发育异常的上皮中,所有细胞均对EGF受体染色。大多数头颈部癌表达EGF受体。在低分化肿瘤中,几乎所有细胞均为该受体阳性。中分化和高分化肿瘤的切片显示染色区域范围减小,这与正常口腔和喉黏膜分化上层中观察到的情况相似。此外,本章对60名头颈部癌患者的EGF受体进行了定量分析。进行这项研究是为了评估EGF受体的过表达是否是头颈部癌的常见特征。将肿瘤活检组织中的水平与患者相应正常黏膜中的水平进行比较。采用了一种检测该受体蛋白表位的酶联免疫吸附测定法。在大多数病例中发现了该受体的过表达。该过表达进一步与临床病理参数相关。然而,尽管平均值随着肿瘤大小增加和临床分期进展而升高,但未发现显著相关性。进一步讨论了定量测定法的使用,并强调了在EGF受体水平的异质性以及恶性组织中不同的基质成分方面的局限性。尽管存在这些问题,但通过例如EGF受体抗体和酪氨酸激酶抑制剂说明了EGF受体在治疗情况下的相关性。第4章重点关注来自同一55例患者的癌组织中EGF和TGF-α的免疫组化表达。该研究包括相邻的正常黏膜,其中生长因子在基底细胞层以上表达。大多数肿瘤同时表达这两种生长因子,并且没有切片对EGF和TGF-α均呈阴性。在中分化和高分化肿瘤的活检组织中,生长因子在分化程度较高的细胞中显示出来。然而,在低分化肿瘤中,细胞对EGF和TGF-α均呈阳性。第5章描述了口腔癌放疗后唾液EGF、淀粉酶和运钴胺素的免疫组化和定量变化。开展这项研究是因为照射后的口腔和喉黏膜在基底细胞层以及棘细胞中显示出对该受体的染色,表明受体因EGF缺乏而上调。在来自下颌下腺和腮腺的正常活检组织中,EGF和淀粉酶在浆液性腺泡中显示出来,而运钴胺素……
