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正常和转化的小鼠乳腺上皮细胞在体外复制形成基底膜。

Basal lamina formation by normal and transformed mouse mammary epithelial cells duplicated in vitro.

作者信息

David G, Van der Schueren B, Bernfield M

出版信息

J Natl Cancer Inst. 1981 Sep;67(3):719-28.

PMID:6944539
Abstract

Cells from low-passage (LP) cultures of a mouse mammary epithelial line (NMuMG cells) form a basal lamina when they are cultured on a type I collagen gel substratum. A high-passage (HP) strain of this line maintained the morphologic, serologic, and karyologic properties of the LP cells. For the determination of whether transformation of the NMuMG cells might lead to defects in the basal lamina, cells from LP cultures were compared in vivo and in vitro with cells of HP cultures for tumorigenicity, growth characteristics, and ability to form a lamina. The LP NMuMG cells had a typical epithelial morphology and showed no cytologic evidence of cancer. They formed an ultrastructurally normal continuous basal lamina in vivo when they were injected into athymic nude mice. In contrast, the HP cells were pleomorphic and highly invasive when injected into nude mice where they showed frequent and large basal lamina defects. These cells also accumulated only traces of lamina-like materials when cultured on a collagen gel, indicating that neoplastic transformation had markedly reduced the ability of NMuMG cells to form a basal lamina both in vivo and in vitro. Because the collagen gel culture system duplicated the in vivo situation with regard to basal lamina integrity, the basis for this lack of in vitro basal lamina formation may be physiologically relevant for the mechanism of malignant invasion.

摘要

从小鼠乳腺上皮细胞系(NMuMG细胞)的低代(LP)培养物中获取的细胞,在I型胶原凝胶基质上培养时会形成基底膜。该细胞系的高代(HP)菌株保持了LP细胞的形态学、血清学和核型特征。为了确定NMuMG细胞的转化是否会导致基底膜缺陷,将LP培养物中的细胞与HP培养物中的细胞在体内和体外进行比较,以观察其致瘤性、生长特性和形成基底膜的能力。LP NMuMG细胞具有典型的上皮形态,未显示出癌症的细胞学证据。当将它们注射到无胸腺裸鼠体内时,它们在体内形成了超微结构正常的连续基底膜。相反,HP细胞在注射到裸鼠体内时具有多形性且具有高度侵袭性,在那里它们显示出频繁且大的基底膜缺陷。当在胶原凝胶上培养时,这些细胞也仅积累了痕量的类基底膜物质,这表明肿瘤转化显著降低了NMuMG细胞在体内和体外形成基底膜的能力。由于胶原凝胶培养系统在基底膜完整性方面模拟了体内情况,这种体外缺乏基底膜形成的基础可能与恶性侵袭机制在生理上相关。

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