Literature DB >> 22172291

Stability of lyophilized siRNA nanosome formulations.

Anup K Kundu1, Partha K Chandra, Sidhartha Hazari, Grace Ledet, Yashoda V Pramar, Srikanta Dash, Tarun K Mandal.   

Abstract

The goal of this study is to evaluate the stability of lyophilized siRNA formulations. The gene silencing efficiency of a stored lyophilized siRNA formulation (i.e. siRNA nanosomes) was evaluated in interferon-α (IFN-α) resistant hepatitis C virus (HCV) at different time points up to three months in an in vitro cell culture model and compared with freshly prepared siRNA formulations. Novel siRNA sequences were encapsulated within nanosize liposomes following condensation with protamine sulfate. The siRNA encapsulated nanosomes were lyophilized and stored at 4 °C for 3 months, along with liquid liposomes (L) and lyophilized liposome powder (P) which were subsequently used to prepare siRNA nanosomes (L) and siRNA nanosomes (P), respectively at different time points. Physiochemical and biological properties of all three formulations were compared at different time points up to 3 months. The particle size of the stored siRNA nanosomes (642 ± 25 nm) was considerably larger initially in comparison with the liquid liposomes (134 ± 5 nm) and lyophilized liposomes (118 ± 3). However, the particle size gradually became smaller over time (413 ± 128 nm by the third month). The zeta potential of all three formulations was initially very high (> +40 mV), followed by a gradual decrease over time. The amount of siRNA in the stored siRNA nanosomes decreased ∼18 % during the 3 month storage period (1.16 ± 0.03 nmol initially on day 1 vs. 0.95 ± 0.04 nmol after 3 months). With respect to biological potency, all three formulations were significantly effective to knock-down HCV throughout the storage time. The cell viability was well-maintained throughout this period. Thus, this study indicates that the stored lyophilized siRNA formulation is as effective as the fresh preparation and that long-term storage could be a viable option to treat deadly diseases such as cancer and viral infection.
Copyright © 2011 Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 22172291      PMCID: PMC3298087          DOI: 10.1016/j.ijpharm.2011.11.040

Source DB:  PubMed          Journal:  Int J Pharm        ISSN: 0378-5173            Impact factor:   5.875


  35 in total

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Authors:  Morten Ø Andersen; Kenneth A Howard; Søren R Paludan; Flemming Besenbacher; Jørgen Kjems
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2.  Liver target delivery of small interfering RNA to the HCV gene by lactosylated cationic liposome.

Authors:  Tsunamasa Watanabe; Takuya Umehara; Fumihiko Yasui; Shin-Ichiro Nakagawa; Junichi Yano; Tadaaki Ohgi; Satoru Sonoke; Kenichi Satoh; Kazuaki Inoue; Makoto Yoshiba; Michinori Kohara
Journal:  J Hepatol       Date:  2007-07-26       Impact factor: 25.083

3.  Freeze-dried nifedipine-lipid nanoparticles with long-term nano-dispersion stability after reconstitution.

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4.  Impaired antiviral activity of interferon alpha against hepatitis C virus 2a in Huh-7 cells with a defective Jak-Stat pathway.

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5.  Degradation of lyophilized lipid/DNA complexes during storage: the role of lipid and reactive oxygen species.

Authors:  Marion D C Molina; Thomas J Anchordoquy
Journal:  Biochim Biophys Acta       Date:  2008-04-10

6.  Effect of lyophilization and freeze-thawing on the stability of siRNA-liposome complexes.

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Journal:  AAPS PharmSciTech       Date:  2007-12-29       Impact factor: 3.246

Review 7.  Nonviral methods for siRNA delivery.

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Authors:  Marion D C Molina; Thomas J Anchordoquy
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10.  Lyophilized HER2-specific PEGylated immunoliposomes for active siRNA gene silencing.

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  9 in total

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3.  Formulation of Biocompatible Targeted ECO/siRNA Nanoparticles with Long-Term Stability for Clinical Translation of RNAi.

Authors:  Nadia R Ayat; Zhanhu Sun; Da Sun; Michelle Yin; Ryan C Hall; Amita M Vaidya; Xujie Liu; Andrew L Schilb; Josef H Scheidt; Zheng-Rong Lu
Journal:  Nucleic Acid Ther       Date:  2019-05-28       Impact factor: 5.486

4.  Inhibition of hepatitis C virus replication by intracellular delivery of multiple siRNAs by nanosomes.

Authors:  Partha K Chandra; Anup K Kundu; Sidhartha Hazari; Sruti Chandra; Lili Bao; Tara Ooms; Gilbert F Morris; Tong Wu; Tarun K Mandal; Srikanta Dash
Journal:  Mol Ther       Date:  2012-05-22       Impact factor: 11.454

5.  Achieving long-term stability of lipid nanoparticles: examining the effect of pH, temperature, and lyophilization.

Authors:  Rebecca L Ball; Palak Bajaj; Kathryn A Whitehead
Journal:  Int J Nanomedicine       Date:  2016-12-30

6.  Novel siRNA formulation to effectively knockdown mutant p53 in osteosarcoma.

Authors:  Anup K Kundu; Swathi V Iyer; Sruti Chandra; Amit S Adhikari; Tomoo Iwakuma; Tarun K Mandal
Journal:  PLoS One       Date:  2017-06-21       Impact factor: 3.240

7.  Effect of pre‑freezing and saccharide types in freeze‑drying of siRNA lipoplexes on gene‑silencing effects in the cells by reverse transfection.

Authors:  Min Tang; Subin Hu; Yoshiyuki Hattori
Journal:  Mol Med Rep       Date:  2020-08-05       Impact factor: 2.952

8.  Induction of osteogenic differentiation of stem cells via a lyophilized microRNA reverse transfection formulation on a tissue culture plate.

Authors:  Kaimin Wu; Jie Xu; Mengyuan Liu; Wen Song; Jun Yan; Shan Gao; Lingzhou Zhao; Yumei Zhang
Journal:  Int J Nanomedicine       Date:  2013-05-03

9.  Lyophilization and stability of antibody-conjugated mesoporous silica nanoparticle with cationic polymer and PEG for siRNA delivery.

Authors:  Worapol Ngamcherdtrakul; Thanapon Sangvanich; Moataz Reda; Shenda Gu; Daniel Bejan; Wassana Yantasee
Journal:  Int J Nanomedicine       Date:  2018-07-10
  9 in total

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