Abstract
Polo-like kinase 4 (PLK4) is indispensable for precise control of centriole duplication. Abnormal expression of PLK4 has been reported in many human cancers, and inhibition of PLK4 activity results in their mitotic arrest and apoptosis. Therefore, PLK4 may be a valid therapeutic target for antitumor therapy. However, clinically available small-molecule inhibitors targeting PLK4 are deficient and their underlying mechanisms still remain not fully clear. Herein, the effects of YLT-11 on breast cancer cells and the associated mechanism were investigated. In vitro, YLT-11 exhibited significant antiproliferation activities against breast cancer cells. Meanwhile, cells treated with YLT-11 exhibited effects consistent with PLK4 kinase inhibition, including dysregulated centriole duplication and mitotic defects, sequentially making tumor cells more vulnerable to chemotherapy. Furthermore, YLT-11 could strongly regulate downstream factors of PLK4, which was involved in cell cycle regulation, ultimately inducing apoptosis of breast cancer cell. In vivo, oral administration of YLT-11 significantly suppressed the tumor growth in human breast cancer xenograft models at doses that are well tolerated. In summary, the preclinical data show that YLT-11 could be a promising candidate drug for breast tumor therapy.
Highlights
Breast cancer is the second most common cancer among women worldwide; it is the fifth most common cause of death from cancer in women
Knocking down Polo-like kinase 4 (PLK4) expression inhibits cancer cell proliferation To study the effects of PLK4 on breast cancer cells proliferation, three independent small interfering RNAs specific to PLK4 were designed and transfected into MDA-MB-231 cells
These results indicated that the proliferation of cancer cells conspicuously decreased in a manner dependent on the expression of PLK4 (Fig. 1b and Supplementary Fig 1B), suggesting that PLK4 played an important role in the growth of breast cancer cells
Summary
Breast cancer is the second most common cancer among women worldwide; it is the fifth most common cause of death from cancer in women The incidence of this disease in China is growing rapidly and is estimated to reach 2.5 million cases by the end of year 20211–3. The polo-like kinases (PLKs) are identified as a family with essential roles in mitosis, including mitotic entry, spindle formation, centrosome duplication, and cytokinesis[7,8,9,10]. Among this family, PLK4 ( called Sak) is the most structurally divergent polo family member, which only contains one polo-box domain in the C-terminal noncatalytic region[11,12].
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