Department of Medical Oncology, the First Affiliated Hospital of Wenzhou Medical University, 1 Xuefubei Street, Ouhai District, Wenzhou, 325000, Zhejiang Province, China.
Wenzhou Institute, University of Chinese Academy of Sciences, 1 Jinlian Road, Longwan District, Wenzhou, 325000, Zhejiang Province, China.
Acta Biomater. 2022 Jun;145:246-259. doi: 10.1016/j.actbio.2022.04.005. Epub 2022 Apr 8.
Selective BCL2 inhibitor ABT-199 has been approved to treat hematological malignancies including acute myeloid leukemia (AML). However, acquired drug resistance and severe side effects occur after extended treatment limiting the clinical usage of ABT-199. Here, we successfully encapsulated pure ABT-199 in amphiphilic mPEG-b-PTMC block copolymer, forming mPEG-b-PTMC@ABT-199 nanoparticles (abbreviated as PEG-ABT-199), which presented better aqueous dispersion and higher efficiency of loading and encapsulation than pure ABT-199. We then compared the anti-leukemic ability of pure ABT-199 and PEG-ABT-199 in vitro and in vivo. PEG-ABT-199 had a lower IC50 value compared with pure ABT-199 in MV4-11 and MOLM-13 cell lines. In addition, PEG-ABT-199 significantly induced apoptosis and decreased colony number than pure ABT-199. Most importantly, PEG-ABT-199 markedly reduced leukemic burden, inhibited the infiltration of leukemic blasts in the spleen, and extended the overall survival (OS) in MLL-AF9-transduced murine AML compared with free ABT-199. Meanwhile, the blank PEG169 NP was non-toxic to normal hematopoiesis in vitro and in vivo, suggesting that PEG169 NP is a safe carrier. Mechanistically, PEG-ABT-199 enhanced mitochondria-targeted delivery of ABT-199 to trigger the collapse of mitochondrial membrane potential (MMP), the release of cytochrome c (cyt-c), and mitochondria-based apoptosis. In conclusion, our results suggest that PEG-ABT-199 has more vital anti-leukemic ability than pure ABT-199. PEG-ABT-199 has potential application in clinical trials to alleviate side effects and improve anti-leukemia ability. STATEMENT OF SIGNIFICANCE: ATB-199, an orally selective inhibitor for BCL2 protein, presents marked activity in relapsed or refractory AML, T-ALL, and CLL patients. However, ABT-199 resistance severely limits the further clinical usage because of off-target effects, non-specific toxicities, and low delivery of drugs. To reduce the side-effects and improve the solubility and bioavailability, ABT-199 was encapsulated into the amphiphilic mPEG-b-PTMC block copolymer by co-assembly method to obtain mPEG-b-PTMC@ABT-199 nanoparticles (PEG-ABT-199). PEG-ABT-199 has several advantages compared with pure ABT-199. 1.PEG-ABT-199 presents better aqueous dispersion and higher efficiencies of loading and encapsulation than pure ABT-199. 2. PEG-ABT-199 substantially enhances the anti-leukemic ability in vitro and in vivo compared with pure ABT-199. 3. PEG-ABT-199 has little effects on normal cells. 4. PEG-ABT-199 can reduce treatment cost.
选择性 BCL2 抑制剂 ABT-199 已被批准用于治疗包括急性髓细胞白血病(AML)在内的血液系统恶性肿瘤。然而,在延长治疗后,会出现获得性耐药和严重的副作用,限制了 ABT-199 的临床应用。在这里,我们成功地将纯 ABT-199 包裹在两亲性 mPEG-b-PTMC 嵌段共聚物中,形成 mPEG-b-PTMC@ABT-199 纳米颗粒(简称 PEG-ABT-199),与纯 ABT-199 相比,PEG-ABT-199 具有更好的水分散性和更高的载药量和包封率。然后,我们比较了纯 ABT-199 和 PEG-ABT-199 在体外和体内的抗白血病能力。与纯 ABT-199 相比,PEG-ABT-199 在 MV4-11 和 MOLM-13 细胞系中的 IC50 值更低。此外,PEG-ABT-199 比纯 ABT-199 更能显著诱导细胞凋亡和减少集落数量。最重要的是,与游离 ABT-199 相比,PEG-ABT-199 能显著降低白血病负担,抑制白血病细胞在脾脏中的浸润,并延长 MLL-AF9 转导的小鼠 AML 的总生存期(OS)。同时,空白 PEG169 NP 在体外和体内对正常造血无毒性,表明 PEG169 NP 是一种安全的载体。在机制上,PEG-ABT-199 增强了 ABT-199 对线粒体的靶向递送,从而引发线粒体膜电位(MMP)崩溃、细胞色素 c(cyt-c)释放和基于线粒体的细胞凋亡。总之,我们的结果表明,PEG-ABT-199 比纯 ABT-199 具有更强的抗白血病能力。PEG-ABT-199 具有在临床试验中减轻副作用和提高抗白血病能力的潜力。意义:ATB-199 是一种口服选择性 BCL2 蛋白抑制剂,在复发或难治性 AML、T-ALL 和 CLL 患者中表现出显著的活性。然而,由于靶外作用、非特异性毒性和药物递送率低,ABT-199 耐药严重限制了其进一步的临床应用。为了降低副作用,提高溶解度和生物利用度,ABT-199 被包裹在两亲性 mPEG-b-PTMC 嵌段共聚物中,通过共组装方法得到 mPEG-b-PTMC@ABT-199 纳米颗粒(PEG-ABT-199)。与纯 ABT-199 相比,PEG-ABT-199 具有以下几个优点。1. PEG-ABT-199 具有更好的水分散性和更高的载药量和包封率。2. 与纯 ABT-199 相比,PEG-ABT-199 大大增强了体外和体内的抗白血病能力。3. PEG-ABT-199 对正常细胞影响较小。4. PEG-ABT-199 可以降低治疗成本。
