骨髓增生异常综合征的转化研究。

Azra Raza, Huma Qawi, Murtaza Mehdi, Muhammad Mumtaz, Naomi Galili
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摘要

近年来,随着对骨髓增生异常综合征(MDS)生物学的研究取得了巨大进展,MDS正受到越来越多的关注。认识到过度细胞因子诱导的细胞凋亡在大多数患者的细胞减少中起着重要作用,为抗细胞因子治疗打开了大门,沙利度胺在大约20%的患者中成功使用。已经出现的其他治疗方法包括沙利度胺类似物来那度胺,它对5q患者以及低或中危MDS的非5q患者特别有益。其他靶向治疗包括维生素、细胞保护剂、分化诱导剂、抗血管生成剂或免疫调节剂。此外,蛋白酶体、甲基化、组蛋白去乙酰化、法尼化、受体酪氨酸激酶、拓扑异构酶和基质金属蛋白酶的抑制剂在部分患者中产生了令人鼓舞的反应。针对导致融合基因(tel - pdgfr - β,或fip1l1 - pdgfr - α)的遗传异常,或由于突变/功能失活(FLT3),表达失调(EVI-1)而导致的异常蛋白,也开发了特异性治疗方法。在短短十年的时间里,这个领域已经从没有有效的治疗方法来为大多数MDS患者提供化疗,到有一个FDA批准的药物,几个正在批准的过程中,以及一些新的药物产生令人兴奋的临床结果。本章总结了快速发展的MDS治疗领域的新靶点和靶向治疗。
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Translational research in myelodysplastic syndromes.

The myelodysplastic syndromes (MDS) are receiving unusual attention recently as great strides have been made in understanding the biology. Recognition that excessive cytokine-induced apoptosis plays a significant role in the cytopenias of the majority of patients opened the doors to anti-cytokine therapy, with thalidomide being used with success in approximately 20% patients. Other therapies that have emerged include the thalidomide analog lenalidomide which is particularly beneficial for 5q- patients as well as a subset of non-5q- patients with low or intermediate-1 risk MDS. Other targeted therapies include vitamins, agents that are cytoprotective, differentiation inducers, anti-angiogenic, or immune modulatory. In addition, inhibitors of proteasome, methylation, histone deacetylation, farnesylation, receptor tyrosine kinases, topoisomerase, and matrix mettaloproteinases have yielded encouraging responses in subsets of patients. Specific therapies have also been developed for genetic abnormalities that lead to fusion genes (TEL-PDGFR-beta, or FIP1L1-PDGFR-alpha), or abnormal proteins due to mutations/functional inactivation (FLT3), dysregulated expression (EVI-1). In a short span of ten years, the field has evolved from having no effective therapy to offer the majority of MDS patients save chemotherapy, to having one FDA approved drug, several on the way to approval, and a number of novel agents producing exciting clinical results. This chapter summarizes the novel targets and targeted therapies in the rapidly evolving therapeutic landscape of MDS.

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