首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Nanoscale liposomal formulation of a SYK P-site inhibitor against B-precursor leukemia.
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Nanoscale liposomal formulation of a SYK P-site inhibitor against B-precursor leukemia.

机译:纳米级脂质体配制Syk对B-前体白血病的Syk P-Paine抑制剂。

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摘要

We report preclinical proof of principle for effective treatment of B-precursor acute lymphoblastic leukemia (ALL) by targeting the spleen tyrosine kinase (SYK)-dependent antiapoptotic blast cell survival machinery with a unique nanoscale pharmaceutical composition. This nanoscale liposomal formulation (NLF) contains the pentapeptide mimic 1,4-Bis (9-O dihydroquinidinyl) phthalazine/hydroquinidine 1,4-phathalazinediyl diether (C61) as the first and only selective inhibitor of the substrate binding P-site of SYK. The C61 NLF exhibited a very favorable pharmacokinetic and safety profile in mice, induced apoptosis in primary B-precursor ALL blast cells taken directly from patients as well as in vivo clonogenic ALL xenograft cells, destroyed the in vivo clonogenic fraction of ALL blast cells, and, at nontoxic dose levels, exhibited potent in vivo antileukemic activity against patient-derived ALL cells in xenograft models of aggressive B-precursor ALL. Our findings establish SYK as an attractive molecular target for therapy of B-precursor ALL. Further development of the C61 NLF may provide the foundation for therapeutic innovation against therapy-refractory B-precursor ALL.
机译:我们通过靶向脾酪氨酸激酶(SYK) - 依赖性抗曝光爆炸细胞存活机械与独特的纳米级药物组合物来报告B-前体急性淋巴细胞白血病(All)的有效治疗突出的原则证明。该纳米级脂质体制剂(NLF)含有五肽模拟1,4-双(9-O二氢喹啉基)酞嗪/氢醌1,4- phathalazineIyl Diather(C61),作为Syk的底物结合P-Site的第一和唯一选择性抑制剂。 C61 NLF在小鼠中表现出非常有利的药代动力学和安全性曲线,诱导的原发性B-前体的凋亡所有爆炸细胞直接从患者以及体内克隆到所有异种移植细胞中,摧毁了所有爆炸细胞的体内克隆核酸部分,和在无毒剂量水平下,在患者衍生出异种移植模型中的患者衍生的患者的患者的体内抗血吸虫活性效果。我们的调查结果将Syk建立为诱人的分子靶标,用于治疗B-前体。 C61 NLF的进一步发展可以为治疗 - 难治性B-前体的治疗创新提供基础。

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