Growth pattern of experimental squamous cell carcinoma in rat submandibular glands—An immunohistochemical evaluation

S. Sumitomo, K. Hashimura, M. Mori
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引用次数: 13

Abstract

Histopathological and immunohistochemical studies during carcinogenesis in rat submandibular glands (SMGs) using a carcinogen (9,10-dimethyl-1,2-benzanthracene: DMBA) were evaluated. For carcinogenesis, the carcinogen-containing sponge was surgically inserted into the gland. Histopathological features during carcinogenesis were as follows; dilatation of ductal segments, the presence of duct-like structures and cystic lesion around the sponge were observed within 3 weeks of the experiment, squamous metaplasia in duct-like structures and lining epithelium of the cystic structures around the sponge were observed at 4–6 weeks of the experiment, and finally well differentiated squamous cell carcinomas (SCCs) were observed after 8 weeks of the experiment. The immunoreactivity of K8.12 keration (K8.12), S-100 protein (S-100), epidermal growth factor (EGF), laminin, and proliferating cell nuclear antigen (PCNA) were evaluated. In the normal SMG, EGF was confined to the granular cells and S-100 to the pillar cells of granular convoluted tubules (GCTs). K8.12 was found in striated (SD) and excretory duct (ED) cells and laminin showed linear staining of the basement membrane around the ducts, acini and blood vessels. PCNA-positive nuclei were rarely observed in the normal glandular parenchyma. During carcinogenesis, during the first stage, EGF in granular cells and S-100 in pillar cells of GCT segments disappeared, and cytokeration K8.12 was observed in duct-like structures and cystic epithelium around the DMBA sponge. PCNA-positive nuclei in the first stage were mainly confined to basal cells of morphologically altered ducts. During the second stage, squamous metaplastic cells showed an intense K8.12 reaction. During the third stage, the well differentiated SCC showed strong reaction for K8.12, and the linear staining for laminin staining had disappeared at the invading fronts. The PCNA index was nearly 40% in the tumour cell component. The stem cells or the progenitor cells during experimental carcinoma were most likely to be the ductal basal cells, and carcinogenesis was initiated with an increase of proliferating activity in small cell clusters surrounding a necrotic area, basal cells of dilated excretory ducts and duct-like structures. Thus, all ductal segments undergoing squamous metaplasia may participate in the genesis of neoplasia during experimental carcinogenesis.

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实验性大鼠颌下腺鳞状细胞癌的生长模式——免疫组织化学评价
采用致癌物(9,10-二甲基-1,2-苯并蒽:DMBA)对大鼠颌下腺(SMGs)发生癌变过程中的组织病理学和免疫组织化学研究进行了评估。对于癌变,手术将含致癌物的海绵插入腺体。癌变过程中的组织病理学特征如下;实验3周内观察到导管段扩张、导管样结构及海绵周围囊性病变的存在,实验4-6周时观察到海绵周围导管样结构及囊性结构衬上皮的鳞状化生,实验8周后观察到高分化鳞状细胞癌(SCCs)。评价K8.12膜(K8.12)、S-100蛋白(S-100)、表皮生长因子(EGF)、层粘连蛋白(laminin)、增殖细胞核抗原(PCNA)的免疫反应性。在正常SMG中,EGF局限于颗粒细胞,S-100局限于颗粒卷曲小管(gct)柱细胞。K8.12在横纹(SD)和排泄管(ED)细胞中发现,层粘连蛋白在管道、腺泡和血管周围的基底膜上呈线性染色。正常腺体实质中很少见pcna阳性核。在癌变过程中,第一阶段GCT节段颗粒细胞中的EGF和柱细胞中的S-100消失,DMBA海绵周围的管状结构和囊性上皮中观察到细胞生成K8.12。第一阶段pcna阳性细胞核主要局限于形态改变的导管基底细胞。第二阶段,鳞状化生细胞表现出强烈的K8.12反应。在第三阶段,分化良好的SCC表现出强烈的K8.12反应,浸润前层粘连蛋白的线性染色消失。肿瘤细胞成分中PCNA指数接近40%。实验癌的干细胞或祖细胞最有可能是导管基底细胞,随着坏死区域周围的小细胞簇、扩张的排泄管和导管样结构的基底细胞增殖活性的增加,癌变开始发生。因此,在实验癌变过程中,所有发生鳞状化生的导管段都可能参与肿瘤的发生。
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