研究者業績

東 顕二郎

ヒガシ ケンジロウ  (Kenjirou Higashi)

基本情報

所属
千葉大学 大学院薬学研究院製剤工学研究室 准教授
学位
博士(薬学)(2011年3月 千葉大学)

連絡先
ken-hfaculty.chiba-u.jp
研究者番号
40451760
ORCID ID
 https://orcid.org/0000-0003-2899-4724
J-GLOBAL ID
202101011267763513
researchmap会員ID
R000020204

外部リンク

論文

 183
  • Keisuke Ueda, Yui Sakagawa, Tomoki Saito, Fumie Sakuma, Hiroki Tanaka, Hidetaka Akita, Kenjirou Higashi, Kunikazu Moribe
    Journal of controlled release : official journal of the Controlled Release Society 373 738-748 2024年8月2日  
    This study aimed to assess the applicability of solution-state 1H NMR for molecular-level characterization of siRNA-loaded lipid nanoparticles (LNP). Dilinoleylmethyl-4-dimethylaminobutyrate (DLin-MC3-DMA, MC3) was used as an ionizable lipid, and siRNA-loaded LNPs were prepared by pre-mixing and post-mixing methods. The pre-mixing method involved mixing an acidic solution containing siRNA with an ethanolic lipid solution using a microfluidic mixer. The pre-mixed LNP was prepared by dialyzing the mixed solution into the phosphate buffered saline (PBS, pH 7.4). The post-mixed LNP was prepared by mixing the siRNA solution with empty LNP in an acidic condition with and without ethanol, resulting in post-mixed LNP (A) and (B), respectively. Both pre-mixed and post-mixed LNPs formed LNP particles with an average diameter of approximately 50 nm. Moreover, the ratio of encapsulated siRNA to lipid content in each LNP particle remained constant regardless of the preparation method. However, small-angle X-ray scattering measurements indicated structural variations in the siRNA-MC3 stacked bilayer structure formed in the LNPs, depending on the preparation method. Solution-state 1H NMR analysis suggested that the siRNA was incorporated uniformly into the LNP core for pre-mixed LNP compared to post-mixed LNPs. In contrast, the post-mixed LNPs contained siRNA-empty regions with local enrichment of siRNA in the LNP core. This heterogeneity was more pronounced in post-mixed LNP (B) than in post-mixed LNP (A), suggesting that ethanol facilitated the homogeneous mixing of siRNA with LNP lipids. The silencing effect of each siRNA-loaded LNP was reduced in the order of pre-mixed LNP, post-mixed LNP (A), and post-mixed LNP (B). This suggested that the heterogeneity of the siRNA-loaded LNP could cause a reduction in the silencing effect of the incorporated siRNA inside LNPs. The present study highlighted that NMR-based characterization of siRNA-loaded LNP can reveal the molecular-level heterogeneity of siRNA-loaded LNP, which helps to optimize the preparation conditions of siRNA-loaded LNP formulations.
  • Takeshi Morita, Yusuke Torii, Hiroshi Imamura, Teruki Kadota, Fumie Sakuma, Kenjirou Higashi, Tomonari Sumi
    The Journal of Physical Chemistry Letters 7909-7915 2024年7月27日  
  • Fumie Sakuma, Kenjirou Higashi, Keisuke Ueda, Takeshi Morita, Daisuke Iohara, Fumitoshi Hirayama, Kunikazu Moribe
    Langmuir 2024年7月16日  
  • 齊藤 智輝, 植田 圭祐, 東 顕二郎, 奥脇 弘次, 古石 誉之, 福澤 薫, 米持 悦生, 森部 久仁一
    日本薬剤学会年会講演要旨集 39年会 137-137 2024年5月  
  • Etsushi Yoshikawa, Keisuke Ueda, Rei Hakata, Kenjirou Higashi, Kunikazu Moribe
    Molecular Pharmaceutics 2024年4月1日  

MISC

 341

書籍等出版物

 10

共同研究・競争的資金等の研究課題

 18

産業財産権

 7