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肿瘤细胞上整合素α5的表达水平影响其向肾脏转移的速率。

Expression level of integrin alpha 5 on tumour cells affects the rate of metastasis to the kidney.

作者信息

Tani N, Higashiyama S, Kawaguchi N, Madarame J, Ota I, Ito Y, Ohoka Y, Shiosaka S, Takada Y, Matsuura N

机构信息

Division of Structutral Cell Biology, Nara Institute of Science and Technology, Ikoma, Japan.

出版信息

Br J Cancer. 2003 Jan 27;88(2):327-33. doi: 10.1038/sj.bjc.6600710.

Abstract

Tumour metastasis is known clinically to have organ specificity. We hypothesised that integrins might be involved in determining the organ specificity of tumour metastasis. Here, we report the results of spontaneous metastasis tested in nude mice that were inoculated with Chinese hamster ovary (CHO) cells expressing integrin alpha 5 beta 1 at various levels. The growth of the primary tumour inversely correlated with the alpha 5 expression level on CHO cells, which is consistent with a previous report (Schreiner et al, 1991). The rates of pulmonary, lymph node, and adrenal metastases that developed in nude mice were not related to changes of the alpha 5 expression level on CHO cells. Kidney metastasis developed in 40% of nude mice inoculated with alpha 5B2 cells (CHO cells overexpressing alpha 5) and in 20% of mice with CHO-K1 cells (CHO cells expressing native alpha 5), whereas inoculation with CHO-B2 cells (alpha 5-defective mutants) and alpha 5CHO cells with the highest expression of alpha 5 did not lead to development of kidney metastasis. Furthermore, alpha 5CHO, which shows the slowest growth of these cell types, did not lead to primary tumours in nude mice. These findings suggest that there is an appropriate level of alpha 5 expression on tumour cells that leads to metastasis. Microscopic observations revealed that micrometastasis in the kidney was formed in glomeruli. An adhesion assay using frozen sections of the kidney demonstrated that alpha 5B2 cells, but not CHO-B2 cells, effectively adhered to glomeruli. Kidney metastasis in vivo and the adhesion of alpha 5B2 to glomeruli shown ex vivo were significantly suppressed by the administration of GRGDS peptide. Finally, we conclude that the interaction of alpha 5 beta 1 on tumour cells with fibronectin in kidney glomeruli is involved in kidney metastasis and that the tumour has appropriate levels of integrins crucial for metastasis.

摘要

临床上已知肿瘤转移具有器官特异性。我们推测整合素可能参与决定肿瘤转移的器官特异性。在此,我们报告了在接种了不同水平表达整合素α5β1的中国仓鼠卵巢(CHO)细胞的裸鼠中进行的自发转移测试结果。原发性肿瘤的生长与CHO细胞上α5的表达水平呈负相关,这与之前的一份报告(施赖纳等人,1991年)一致。裸鼠中发生的肺、淋巴结和肾上腺转移率与CHO细胞上α5表达水平的变化无关。接种α5B2细胞(过表达α5的CHO细胞)的裸鼠中有40%发生了肾转移,接种CHO-K1细胞(表达天然α5的CHO细胞)的裸鼠中有20%发生了肾转移,而接种CHO-B2细胞(α5缺陷突变体)和α5表达最高的α5CHO细胞并未导致肾转移。此外,在这些细胞类型中生长最慢的α5CHO细胞,在裸鼠中并未形成原发性肿瘤。这些发现表明,肿瘤细胞上存在一个导致转移的α5表达的适当水平。显微镜观察显示,肾中的微转移形成于肾小球。使用肾脏冰冻切片进行的黏附试验表明,α5B2细胞而非CHO-B2细胞能有效黏附于肾小球。给予GRGDS肽可显著抑制体内的肾转移以及体外显示的α5B2细胞与肾小球的黏附。最后,我们得出结论,肿瘤细胞上的α5β1与肾小球中的纤连蛋白之间的相互作用参与了肾转移,并且肿瘤具有对转移至关重要的适当水平的整合素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/34d3/2377056/33256a5d48d7/88-6600710f1.jpg

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