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胃癌和胰腺癌的新细胞系:独特的形态、生长特性、上皮和免疫调节抗原的表达

New cell lines of gastric and pancreatic cancer: distinct morphology, growth characteristics, expression of epithelial and immunoregulatory antigens.

作者信息

Heike M, Röhrig O, Gabbert H E, Moll R, Meyer zum Büschenfelde K H, Dippold W G, Knuth A

机构信息

I. Medizinische Klinik und Poliklinik, Johannes Gutenberg-Universität, Mainz, Germany.

出版信息

Virchows Arch. 1995;426(4):375-84. doi: 10.1007/BF00191347.

Abstract

Two new cell lines from stomach cancers and one from a pancreatic carcinoma are presented. MZ-GC-1 was established from a hepatic metastasis of a well differentiated gastric adenocarcinoma. MZ-GC-2 was derived from ascites induced by a poorly differentiated gastric adenocarcinoma. MZ-PC-1 originated from the pleural effusion of a moderately well differentiated pancreatic ductal adenocarcinoma. MZ-GC-1 cells were adherent and partially polarized, connected tightly via desmosomes. In contrast MZ-GC-2 cells consisted of slightly adherent or floating subpopulations and displayed no desmosomes. MZ-PC-1 cells were adherent and showed polarized growth, connected by apical junctional complexes. Cell doubling times were 7 days for MZ-GC-1 and 45 h for MZ-GC-2 and MZ-PC-1 cells. MZ-GC-2 and MZ-PC-1 gave rise to nude mouse tumours, resembling the original lesions. Chromosome analysis of the cell lines revealed a high range of numerical abnormalities. Each cell line had cytokeratin patterns fitting well to typical in vivo patterns. Furthermore the cell lines expressed a panel of antigens typical for gastrointestinal epithelia. Unique for MZ-PC-1 were high amounts of secreted Ca19-9. gamma-Interferon enhanced HLA-class I antigens up to twofold and induced ICAM-1 expression on each cell line. HLA-class II antigens were differentially enhanced by gamma-interferon. Due to their distinct characteristics the three tumour cell lines may be useful models in the investigation of the cell biology and immunogenicity of gastrointestinal tumours.

摘要

本文介绍了两个新的胃癌细胞系和一个胰腺癌细胞系。MZ-GC-1是从高分化胃腺癌的肝转移灶建立的。MZ-GC-2源自低分化胃腺癌诱导产生的腹水。MZ-PC-1起源于中分化胰腺导管腺癌的胸腔积液。MZ-GC-1细胞贴壁且部分极化,通过桥粒紧密连接。相比之下,MZ-GC-2细胞由轻度贴壁或漂浮的亚群组成,未显示桥粒。MZ-PC-1细胞贴壁并呈现极化生长,通过顶端连接复合体相连。MZ-GC-1细胞的倍增时间为7天,MZ-GC-2和MZ-PC-1细胞的倍增时间为45小时。MZ-GC-2和MZ-PC-1可在裸鼠体内形成肿瘤,与原发病变相似。对这些细胞系的染色体分析显示存在广泛的数值异常。每个细胞系的细胞角蛋白模式与典型的体内模式吻合良好。此外,这些细胞系表达一组胃肠道上皮典型的抗原。MZ-PC-1的独特之处在于分泌大量的Ca19-9。γ干扰素可使HLA-I类抗原增加两倍,并在每个细胞系上诱导ICAM-1表达。γ干扰素对HLA-II类抗原的增强作用存在差异。由于其独特的特性,这三个肿瘤细胞系可能是研究胃肠道肿瘤细胞生物学和免疫原性的有用模型。

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