抗CD38標的カルフィルゾミブ-loaded ハイブリッドナノコンポジットによる多発性骨髄腫療法：細胞毒性と生体内分布

Key Points

• This research aims to develop and characterize an anti-CD38 targeted nanotherapeutic system to enhance carfilzomib delivery for multiple myeloma treatment.
• Developed anti-CD38 mAb functionalized carfilzomib loaded PCL nanocomposites using nanoprecipitation.
• Characterized nanocomposites with FTIR, DLS, and entrapment efficiency assessments.
• Assessed in vitro drug release behavior at physiological and tumor-stimulating pH.
• Evaluated cytotoxicity and cellular uptake in multiple myeloma cells.
• Mean hydrodynamic diameter of CFZ-PCL-NPs was 103.6 nm, while anti-CD38 conjugates were 189.9 nm.
• Sustained drug release of 91.12% at pH 7.4 over 10 days; 96.78% at pH 5.5 over 4 days.
• Cellular uptake exceeded 85%, with cytotoxicity exceeding 90% in MM cells.
• Tumor growth inhibition greater than 85% compared to non-conjugated formulations.