4.7 Article

Phosphorylated Osteopontin Secreted from Cancer Cells Induces Cancer Cell Motility

期刊

BIOMOLECULES
卷 11, 期 9, 页码 -

出版社

MDPI
DOI: 10.3390/biom11091323

关键词

osteopontin; phosphorylation; cancer; migration

资金

  1. Japan Society for Promotion of Science KAKENHI [17K08665]
  2. Japan Intractable Diseases Research Foundation [SO23016]
  3. Ichiro Kanehara Foundation [SO28035]
  4. Grants-in-Aid for Scientific Research [17K08665] Funding Source: KAKEN

向作者/读者索取更多资源

Phosphorylated OPN secreted from cancer cells plays a regulatory role in cancer cell motility, with higher OPN expression levels correlating with increased cell migration capability. The presence of phosphorylated OPN in cell culture media affects cancer cell motility, indicating a potential mechanism for regulating cancer cell migration through the secretion of phosphorylated OPN.
Osteopontin (OPN) plays a pivotal role in cancer cell invasion and metastasis. Although OPN has a large number of phosphorylation sites, the functional significance of OPN phosphorylation in cancer cell motility remains unclear. In this study, we attempted to investigate whether phosphorylated OPN secreted from cancer cells affect cancer cell migration. Quantitative PCR and Western blot analyses revealed that MDA-MB435S, A549, and H460 cells highly expressed OPN, whereas the OPN expression levels in H358, MIAPaca-2, and Panc-1 cells were quite low or were not detected. Compared with the cancer cell lines with a low OPN expression, the high OPN-expressing cancer cell lines displayed a higher cell migration, and the cell migration was suppressed by the anti-OPN antibody. This was confirmed by the OPN overexpression in H358 cancer cells with a low endogenous OPN. Phos-tag ELISA showed that phosphorylated OPN was abundant in the cell culture media of A549 and H460 cells, but not in those of MDA-MB435S cells. Moreover, the A549 and H460 cell culture media, as well as the MDA-MB435S cell culture media with a kinase treatment increased cancer cell motility, both of which were abrogated by phosphatase treatment or anti-OPN antibodies. These results suggest that phosphorylated OPN secreted from cancer cells regulates cancer cell motility.

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