Development of Effective Therapeutics Targeting HER3 for Cancer Treatment

被引:0
|
作者
Xiaolong Liu
Shuang Liu
Hui Lyu
Adam I. Riker
Yamin Zhang
Bolin Liu
机构
[1] Tianjin First Central Hospital,Department of Hepatobiliary Surgery
[2] School of Medicine,Department of Genetics, Stanley S. Scott Cancer Center
[3] Louisiana State University Health Sciences Center,Department of Surgery, Section of Surgical Oncology, Stanley S. Scott Cancer Center, School of Medicine
[4] Louisiana State University Health Sciences Center,undefined
来源
Biological Procedures Online | 2019年 / 21卷
关键词
HER3; Cell signaling; Targeted therapy; Epigenetic approach; miRNA;
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学科分类号
摘要
HER3 is the third member of the human epidermal growth factor receptor (HER/EGFR) family, and unlike its other family members, is unique due to its minimal intrinsic kinase activity. As a result, HER3 has to interact with another receptor tyrosine kinase (RTK), such as EGFR or HER2, in order to activate the PI-3 K/Akt, MEK/MAPK, Jak/Stat pathways, as well as Src kinase. Over-expression of HER3 in various human cancers promotes tumor progression by increasing metastatic potential and acting as a major cause of treatment failure. Effective inhibition of HER3, and/or the key downstream mediators of HER3 signaling, is thought to be required to overcome resistance and enhance therapeutic efficacy. To date, there is no known HER3-targeted therapy that is approved for breast cancer, with a number of anti-HER3 antibodies current in various stages of development and clinical testing. Recent data suggests that the epigenetic strategy of using a histone deacetylase (HDAC) inhibitor, or functional cooperative miRNAs, may be an effective way to abrogate HER3 signaling. Here, we summarize the latest advances in our understanding of the mechanism of HER3 signaling in tumor progression, with continuing research towards the identification of therapeutic anti-HER3 antibodies. We will also examine the potential to develop novel epigenetic approaches that specifically target the HER3 receptor, along with important key downstream mediators that are involved in cancer treatment.
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