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The targeting effect of Hm2E8b–NCTD–liposomes on B-lineage leukaemia stem cells is associated with the HLF–SLUG axis

机译:HM2E8B-NCTD-脂质体对B族白血病干细胞的靶向效果与HLF-SLUI轴相关

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摘要

To identify an agent with specific activity against B-lineage leukaemia stem cells (B-LSCs), we generated norcantharidin (NCTD)-encapsulated liposomes modified with a novel humanised anti-human CD19 monoclonal antibody, Hm2E8b (Hm2E8b–NCTD–liposomes). These liposomes were specially designed to recognise and kill B-LSCs in vitro, and to decrease non-specific cytotoxicity to untargeted cells. Hm2E8b–NCTD–liposomes selectively ablated B-LSCs through targeting hepatic leukaemia factor (HLF), which is implicated in haematopoietic stem cell regulation and is overexpressed in LSCs. Hm2E8b–NCTD–liposomes decreased HLF protein levels and induced apoptosis in the HAL-01 cell line harbouring the oncoprotein E2A–HLF. This resulted in modulation of the expression of several molecules that govern survival pathways, including HLF, SLUG, NFIL3 and C-Myc, thereby causing the induction of p53 and the mitochondrial caspase cascade. Therefore, the potent in vitro effect of Hm2E8b–NCTD–liposomes on B-LSC activity and survival pathways have the potential to be exploited clinically with appropriate drug combinations. ? 2017 Informa UK Limited, trading as Taylor & Francis Group.
机译:为了鉴定具有针对B型白血病干细胞(B-LSCs)的特异性活性的试剂,我们产生了用新型人源化的抗人CD19单克隆抗体,HM2E8B(HM2E8B-NCTD-脂质体)改性的NORCantharidin(NCTD)的脂质体。这些脂质体被专门设计用于在体外识别和杀死B-LSC,并降低非特异性细胞毒性对未明确的细胞。 HM2E8B-NCTD-脂质体通过靶向肝白血病因子(HLF)选择性地烧蚀B-LSC,其涉及血液生成干细胞调节并在LSC中过表达。 HM2E8B-NCTD-脂质体降低了HLF蛋白水平,并诱导含癌蛋白E2A-HLF的HAL-01细胞中的细胞凋亡。这导致调节治疗存活途径的几种分子的表达,包括HLF,SLUG,NFIL3和C-MYC,从而引起P53和线粒体胱天蛋白酶级联的诱导。因此,HM2E8B-NCTD-脂质体对B-LSC活性和存活途径的有效体外效应具有临床上具有适当的药物组合的潜力。还2017年Informa UK Limited,贸易为泰勒&弗朗西斯集团。

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