纳米载体
粒径
甘露醇
化学
体内分布
纳米颗粒
壳聚糖
冷冻干燥
纳米技术
材料科学
色谱法
生物化学
体外
物理化学
作者
S. P. Surya Teja,Damodharan Narayanasamy,Tamilanban Thamaraikani,Vetriselvan Subramaniyan,V. Chitra,Suresh V. Chinni,Ling Shing Wong,Neeraj Kumar Fuloria,Mahendran Sekar,Shivkanya Fuloria,Gobinath Ramachawolran,Siddharthan Selvaraj
标识
DOI:10.3389/fbioe.2023.1222693
摘要
The aim of this study was to investigate the influence of excipients on retaining the particle size of methotrexate (MTX) loaded chitosan nanocarriers (CsNP) during lyophilization, which relates to the ability to enlarge the particle size and target specific areas. The nanocarriers were prepared using the ionic gelation technique with tripolyphosphate as a crosslinker. Three lyophilized formulations were used: nanosuspension without Lyoprotectant (NF), with mannitol (NFM), and with sucrose (NFS). The lyophilized powder intended for injection (PI) was examined to assess changes in particle size, product integrity, and comparative biodistribution studies to evaluate targeting ability. After lyophilization, NFS was excluded from in-vivo studies due to the product melt-back phenomenon. The particle size of the NF lyophile significantly increased from 176 nm to 261 nm. In contrast, NFM restricted the nanocarrier size to 194 nm and exhibited excellent cake properties. FTIR, XRD, and SEM analysis revealed the transformation of mannitol into a stable β, δ polymorphic form. Biodistribution studies showed that the nanocarriers significantly increased MTX accumulation in tumor tissue (NF = 2.04 ± 0.27; NFM = 2.73 ± 0.19) compared to the marketed PI (1.45 ± 0.25 μg), but this effect was highly dependent on the particle size. Incorporating mannitol yielded positive results in restricting particle size and favoring successful tumor targeting. This study demonstrates the potential of chitosan nanocarriers as promising candidates for targeted tumor drug delivery and cancer treatment.
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