Enhanced endosomal escape of siRNA-incorporating hybrid nanoparticles from calcium phosphate and PEG-block charge-conversional polymer for efficient gene knockdown with negligible cytotoxicity

Pittella, Frederico; Zhang, Mingzhen; Lee, Yan; Kim, Hyun Jin; Tockary, Theofilus A.; Osada, Kensuke; Ishii, Takehiko; Miyata, Kanjiro; Nishiyama, Nobuhiro; Kataoka, Kazunori

doi:10.1016/j.biomaterials.2010.12.057

Cited by 157 publications

(118 citation statements)

References 33 publications

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“…To overcome these problems, nanoparticles will be effective, because they are able to escape from endosomes into the cytosol, where these nanoparticles release drugs. Based on this strategy, delivery of siRNA-containing nanoparticles into HeLa cells and human pancreatic carcinoma PanC-1 cells is reported to be successful [69,70].…”

Section: Pattern Recognition-mediated Inflammatory Responsesmentioning

confidence: 99%

Endocytosis of Particle Formulations by Macrophages and Its Application to Clinical Treatment

Hirota¹,

Terada²

2012

Molecular Regulation of Endocytosis

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Section: Pattern Recognition-mediated Inflammatory Responsesmentioning

confidence: 99%

Endocytosis of Particle Formulations by Macrophages and Its Application to Clinical Treatment

Hirota¹,

Terada²

2012

Molecular Regulation of Endocytosis

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“…The drawbacks are low throughput, inability to detect metabolites, and difficulty in achieving precise quantification of fluorescence intensity on IF-stained tissue sections. There are examples of applying such histological methods to investigate siRNA deposition in the liver (Shi et al 2011), tumor (Yoshizawa et al 2008;Mikhaylova et al 2009), lung (Tayyari et al 2011), or even subcellular compartments (Akita et al 2010;Basha et al 2011;Pittella et al 2011). …”

Section: Analysis Of Sirna At Cell and Subcellular Levelsmentioning

confidence: 99%

“…Others (Akita et al 2010;Pittella et al 2011) have applied confocal microscopy where they labeled siRNA with Cy5 (red) and stained siRNA-treated cells with LysoTracker (green), and they calculated the ratio of yellow pixels (co-localization of siRNA with LysoTracker), which was equal to yellow pixels divided by the sum of yellow and red pixels. If more yellow perinuclear signals were observed and the yellow co-localization ratio was higher, it indicated more endosomal/lysosomal captured siRNAs.…”

Section: Analyses Of Sirna Endosomal Escape and Riscloaded Sirnamentioning

confidence: 99%

Technologies for Investigating the Physiological Barriers to Efficient Lipid Nanoparticle–siRNA Delivery

Shu¹,

Abrams²

2013

J Histochem Cytochem.

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Small interfering RNA (siRNA) therapeutics have advanced from bench to clinical trials in recent years, along with new tools developed to enable detection of siRNA delivered at the organ, cell, and subcellular levels. Preclinical models of siRNA delivery have benefitted from methodologies such as stem-loop quantitative polymerase chain reaction, histological in situ immunofluorescent staining, endosomal escape assay, and RNA-induced silencing complex loading assay. These technologies have accelerated the detection and optimization of siRNA platforms to overcome the challenges associated with delivering therapeutic oligonucleotides to the cytosol of specific target cells. This review focuses on the methodologies and their application in the biodistribution of siRNA delivered by lipid nanoparticles.

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“…The charge response between particles and cells is an important basis for these biological performances. 54 The experimental results of Tang et al showed that when the nanoparticles are dispersed in the culture medium, only positively charged particles can be ingested by the cells; if the particles are connected to the protein, the electrostatic difference between the positively and negatively charged particles can be almost completely eliminated. 55 Although protein-coated particles may help identify antigens or receptors, they are not very important in determining particle-to-cell attraction.…”

mentioning

confidence: 99%

Effects of major parameters of nanoparticles on their physical and chemical properties and recent application of nanodrug delivery system in targeted chemotherapy

Zhang¹,

Tang²,

Liu³

et al. 2017

IJN

120

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Chemotherapy is still one of the main cancer therapy treatments, but the curative effect of chemotherapy is relatively low, as such the development of a new cancer treatment is highly desirable. The gradual maturation of nanotechnology provides an innovative perspective not only for cancer therapy but also for many other applications. There are a diverse variety of nanoparticles available, and choosing the appropriate carriers according to the demand is the key issue. The performance of nanoparticles is affected by many parameters, mainly size, shape, surface charge, and toxicity. Using nanoparticles as the carriers to realize passive targeting and active targeting can improve the efficacy of chemotherapy drugs significantly, reduce the mortality rate of cancer patients, and improve the quality of life of patients. In recent years, there has been extensive research on nanocarriers. In this review, the effects of several major parameters of nanoparticles on their physical and chemical properties are reviewed, and then the recent progress in the application of several commonly used nanoparticles is presented.

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Enhanced endosomal escape of siRNA-incorporating hybrid nanoparticles from calcium phosphate and PEG-block charge-conversional polymer for efficient gene knockdown with negligible cytotoxicity

Cited by 157 publications

References 33 publications

Endocytosis of Particle Formulations by Macrophages and Its Application to Clinical Treatment

Endocytosis of Particle Formulations by Macrophages and Its Application to Clinical Treatment

Technologies for Investigating the Physiological Barriers to Efficient Lipid Nanoparticle–siRNA Delivery

Effects of major parameters of nanoparticles on their physical and chemical properties and recent application of nanodrug delivery system in targeted chemotherapy

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