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一种对淋巴结具有高转移性的人胃癌细胞系的建立与鉴定

Establishment and characterization of a human gastric carcinoma cell line that is highly metastatic to lymph nodes.

作者信息

Yamaguchi K, Ura H, Yasoshima T, Shishido T, Denno R, Hirata K

机构信息

First Dept. of Surgery, Sapporo Medical University School of Medicine, Japan.

出版信息

J Exp Clin Cancer Res. 2000 Mar;19(1):113-20.

Abstract

The actual mechanisms by which carcinoma cells metastasize to lymph nodes are still unclear, and there is a need to establish in vivo experimental models suitable for the investigation of lymph node metastasis. For the purpose, we established a highly lymph node-metastasizing line, designated AZL5G, derived from a human gastric cancer cell line, AZ521, which had low capacity for lymph node metastasis. AZL5G cells transplanted orthotopically in the nude mouse stomach metastasize predominantly to the regional lymph nodes, showing little potential for hematogenous metastasis. AZL5G tumors developing in the stomach and regional lymph nodes showed poorly differentiated adenocarcinoma with medullary growth, and their histologic appearance strongly resembled that of parental AZ521. The growth activities in vitro of low-metastatic AZ521 and high-metastatic AZL5G were almost the same, but the tumorigenicity in vivo of AZL5G was significantly higher than that of AZ521. AZL5G cells also showed clearly higher abilities of cell locomotion and adhesion to type IV collagen and fibronectin in vitro as compared with AZ521 cells. Flow cytometric analysis demonstrated that the expression of integrin beta1 subfamily except for alpha6 integrin was generally increased in AZL5G cells than in AZ521 cells. Especially, the expression of alpha1 and alpha2 integrins in AZL5G cells was clearly higher than in AZ521, while alpha(v)beta3 integrin, E-cadherin, ICAM-1 and CD44H were not expressed by either cell line. The cell adhesion blocking assay showed that DGEA-containing peptide, which is composed of alpha2 integrin recognition sequence, significantly reduced the adhesiveness of AZL5G cells to type IV collagen as well as to type I collagen and laminin. Furthermore, the administration of anti-alpha2 integrin mAb or DGEA peptide in AZL5G-transplanted nude mice produced a significant reduction in the number of lymph node metastases. These data suggest that the up-regulation of alpha2 integrin expression by gastric cancer cells may play a critical role in the process of lymph node metastasis through the increased adhesiveness to type IV collagen. In conclusion, we established a gastric cancer cell line, AZL5G, with a highly metastatic potential to lymph nodes. This well-characterized line and its in vivo experimental model should be useful for investigation of the mechanisms of lymph node metastasis and for establishment of a new therapeutic approach for human gastric cancer.

摘要

癌细胞转移至淋巴结的实际机制仍不清楚,因此需要建立适合研究淋巴结转移的体内实验模型。为此,我们从低淋巴结转移能力的人胃癌细胞系AZ521中建立了一个高淋巴结转移细胞系,命名为AZL5G。原位移植到裸鼠胃内的AZL5G细胞主要转移至区域淋巴结,血行转移潜能较小。在胃和区域淋巴结中生长的AZL5G肿瘤表现为低分化腺癌伴髓样生长,其组织学外观与亲代AZ521极为相似。低转移的AZ521和高转移的AZL5G在体外的生长活性几乎相同,但AZL5G在体内的致瘤性明显高于AZ521。与AZ521细胞相比,AZL5G细胞在体外对IV型胶原和纤连蛋白的细胞运动和黏附能力也明显更高。流式细胞术分析表明,除α6整合素外,整合素β1亚家族在AZL5G细胞中的表达普遍高于AZ521细胞。特别是,AZL5G细胞中α1和α2整合素的表达明显高于AZ521,而两种细胞系均不表达α(v)β3整合素、E-钙黏蛋白、细胞间黏附分子-1和CD44H。细胞黏附阻断试验表明,由α2整合素识别序列组成的含DGEA肽显著降低了AZL5G细胞对IV型胶原以及I型胶原和层粘连蛋白的黏附性。此外,在移植了AZL5G的裸鼠中给予抗α2整合素单克隆抗体或DGEA肽可显著减少淋巴结转移数量。这些数据表明,胃癌细胞α2整合素表达上调可能通过增加对IV型胶原的黏附性在淋巴结转移过程中起关键作用。总之,我们建立了一个对淋巴结具有高转移潜能的胃癌细胞系AZL5G。这个特征明确的细胞系及其体内实验模型对于研究淋巴结转移机制和建立人类胃癌新的治疗方法应该是有用的。

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