In vivo bone marrow microenvironment siRNA delivery using lipid–polymer nanoparticles for multiple myeloma therapy

归巢(生物学) 骨髓 癌症研究 多发性骨髓瘤 硼替佐米 Cypa 体内 小干扰RNA 肿瘤微环境 医学 免疫学 化学 生物 细胞培养 转染 肿瘤细胞 人类免疫缺陷病毒(HIV) 生态学 遗传学 生物技术
作者
Pedro Pires Goulart Guimarães,Christian G. Figueroa‐Espada,Rachel Riley,Ningqiang Gong,Lulu Xue,Tomasz Sewastianik,Peter S. Dennis,Claudia Loebel,Amanda Chung,Sarah J. Shepherd,Rebecca M. Haley,Alex G. Hamilton,Rakan El‐Mayta,Karin Wang,Róbert Langer,Daniel G. Anderson,Ruben D. Carrasco,Michael J. Mitchell
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:120 (25) 被引量:18
标识
DOI:10.1073/pnas.2215711120
摘要

Multiple myeloma (MM), a hematologic malignancy that preferentially colonizes the bone marrow, remains incurable with a survival rate of 3 to 6 mo for those with advanced disease despite great efforts to develop effective therapies. Thus, there is an urgent clinical need for innovative and more effective MM therapeutics. Insights suggest that endothelial cells within the bone marrow microenvironment play a critical role. Specifically, cyclophilin A (CyPA), a homing factor secreted by bone marrow endothelial cells (BMECs), is critical to MM homing, progression, survival, and chemotherapeutic resistance. Thus, inhibition of CyPA provides a potential strategy to simultaneously inhibit MM progression and sensitize MM to chemotherapeutics, improving therapeutic response. However, inhibiting factors from the bone marrow endothelium remains challenging due to delivery barriers. Here, we utilize both RNA interference (RNAi) and lipid–polymer nanoparticles to engineer a potential MM therapy, which targets CyPA within blood vessels of the bone marrow. We used combinatorial chemistry and high-throughput in vivo screening methods to engineer a nanoparticle platform for small interfering RNA (siRNA) delivery to bone marrow endothelium. We demonstrate that our strategy inhibits CyPA in BMECs, preventing MM cell extravasation in vitro. Finally, we show that siRNA-based silencing of CyPA in a murine xenograft model of MM, either alone or in combination with the Food and Drug Administration (FDA)-approved MM therapeutic bortezomib, reduces tumor burden and extends survival. This nanoparticle platform may provide a broadly enabling technology to deliver nucleic acid therapeutics to other malignancies that home to bone marrow.
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