靶向黑色素瘤中的 KIT:分子医学和靶向治疗的范例。
Targeting KIT in melanoma: a paradigm of molecular medicine and targeted therapeutics.
机构信息
Departments of Melanoma Medical Oncology and Systems Biology, University of Texas, MD Anderson Cancer Center, Houston, TX 77030, USA.
出版信息
Biochem Pharmacol. 2010 Sep 1;80(5):568-74. doi: 10.1016/j.bcp.2010.04.032. Epub 2010 May 8.
Abstract
Despite multiple clinical trials utilizing a spectrum of therapeutic modalities, melanoma remains a disease with dismal outcomes in patients with advanced disease. However, it is now clear that melanoma is not a single entity, but can be molecularly divided into subtypes that generally correspond to the anatomical location of the primary melanoma. Melanomas from acral lentiginous, mucosal, and chronic sun-damaged sites frequently harbor activating mutations and/or increased copy number in the KIT tyrosine kinase receptor gene, which are very rare in the more common cutaneous tumors. Multiple case reports and early observations from clinical trials suggest that targeting mutant KIT with tyrosine kinase inhibitors is efficacious in KIT mutant melanoma. This review recounts what is known about the role of KIT in melanocyte maturation, our current understanding of KIT genetic aberrations in melanoma, and how this knowledge is being translated into clinical oncology.
摘要
尽管进行了多项临床试验,采用了多种治疗方法,但黑色素瘤仍然是一种疾病,晚期患者的预后仍然很差。然而,现在很明显,黑色素瘤不是一个单一的实体,而是可以在分子上分为亚型,通常与原发性黑色素瘤的解剖位置相对应。来自肢端雀斑样、黏膜和慢性日光损伤部位的黑色素瘤经常携带 KIT 酪氨酸激酶受体基因的激活突变和/或拷贝数增加,而在更常见的皮肤肿瘤中则非常罕见。多项病例报告和临床试验的早期观察结果表明,用酪氨酸激酶抑制剂靶向突变的 KIT 在 KIT 突变黑色素瘤中是有效的。这篇综述回顾了 KIT 在黑素细胞成熟中的作用、我们目前对黑色素瘤中 KIT 遗传异常的认识,以及如何将这些知识转化为临床肿瘤学。
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