Integrin‐Targeted, Short Interfering RNA Nanocomplexes for Neuroblastoma Tumor‐Specific Delivery Achieve <i>MYCN</i> Silencing with Improved Survival

Tagalakis, Aristides D.; Jayarajan, Vignesh; Maeshima, Ruhina; Ho, Kin H.; Syed, Farhatullah; Wu, Lin; Aldossary, Ahmad M.; Munye, Mustafa M.; Mistry, Talisa; Ogunbiyi, Olumide; Sala, Arturo; Standing, Joseph F.; Moghimi, S. Moein; Stoker, Andrew W.; Hart, Stephen L.

doi:10.1002/adfm.202104843

Cited by 15 publications

(16 citation statements)

References 51 publications

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“…several strategies including targeting ligand modification, [5][6][7][8] size engineering, [9,10] tunable surface charge, [11][12][13] and sheddable polyethylene glycol (PEG) strategies, [14][15][16] which substantially enhance siRNA therapy effect. However, non-specific gene inhibition in normal tissues remains a limitation for siRNA therapy, which is due to the uncontrolled distribution of siRNA in vivo.…”

Section: Research Articlementioning

confidence: 99%

“…Small interfering RNA (siRNA) molecules have been extensively explored to treat many diseases including cancer and liver diseases due to their highly efficient target gene silencing. [ 1–4 ] siRNA delivery efficiency has been greatly improved through several strategies including targeting ligand modification, [ 5–8 ] size engineering, [ 9,10 ] tunable surface charge, [ 11–13 ] and sheddable polyethylene glycol (PEG) strategies, [ 14–16 ] which substantially enhance siRNA therapy effect. However, non‐specific gene inhibition in normal tissues remains a limitation for siRNA therapy, which is due to the uncontrolled distribution of siRNA in vivo.…”

Section: Introductionmentioning

confidence: 99%

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Unprotonatable and ROS‐Sensitive Nanocarrier for NIR Spatially Activated siRNA Therapy with Synergistic Drug Effect

Deng

Wang

Xiao

et al. 2022

Small

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Although small interfering RNA (siRNA) therapy has achieved great progress, unwanted gene inhibition in normal tissues severely limits its extensive clinical applications due to uncontrolled siRNA biodistribution. Herein, a spatially controlled siRNA activation strategy is developed to achieve tumor‐specific siRNA therapy without gene inhibition in the normal tissues. The quaternary ammonium moieties are conjugated to amphiphilic copolymers via reactive oxygen species (ROS)‐sensitive thioketal (TK) linkers for co‐delivery of siRNA and photosensitizer chlorin e6 (Ce6), showing excellent siRNA complexation capacity and near infrared (NIR)‐controlled siRNA release. In the normal tissue, siRNAs are trapped and degraded in the endo‐lysosomes due to the unprotonatable property of quaternary ammonium moiety, showing the siRNA activity “off” state. When NIR irradiation is spatially applied to the tumor tissue, the NIR irradiation/Ce6‐induced ROS trigger siRNA endo‐lysosomal escape and cytosolic release through the photochemical internalization effect and cleavage of TK bonds, respectively, showing the siRNA activity “on” state. The siRNA‐mediated glutathione peroxidase 4 gene inhibition enhances ROS accumulation. The synergistic antitumor activity of Ce6 photodynamic therapy and gene inhibition is confirmed in vivo. Spatially controlled tumor‐specific siRNA activation and co‐delivery with Ce6 using unprotonatable and ROS‐sensitive cationic nanocarriers provide a feasible strategy for tumor‐specific siRNA therapy with synergistic drug effects.

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Section: Research Articlementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Unprotonatable and ROS‐Sensitive Nanocarrier for NIR Spatially Activated siRNA Therapy with Synergistic Drug Effect

Deng

Wang

Xiao

et al. 2022

Small

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“…The newly developed structures demonstrated improved tissue penetration, enhanced dispersal, and more widespread cellular transfection than cationic systems. Similar anionic targeting hybrid nanocarriers have also shown promising results for siRNA delivery to neuroblastoma tumors with reduced systemic and cellular toxicity [129].…”

Section: Lipid-polymer Hybrid-based Delivery Systemsmentioning

confidence: 99%

New Applications of Lipid and Polymer-Based Nanoparticles for Nucleic Acids Delivery

2021

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Nucleic acids represent a promising lead for engineering the immune system. However, naked DNA, mRNA, siRNA, and other nucleic acids are prone to enzymatic degradation and face challenges crossing the cell membrane. Therefore, increasing research has been recently focused on developing novel delivery systems that are able to overcome these drawbacks. Particular attention has been drawn to designing lipid and polymer-based nanoparticles that protect nucleic acids and ensure their targeted delivery, controlled release, and enhanced cellular uptake. In this respect, this review aims to present the recent advances in the field, highlighting the possibility of using these nanosystems for therapeutic and prophylactic purposes towards combatting a broad range of infectious, chronic, and genetic disorders.

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“…There are several mechanisms by whichMYCN is overexpressed in tumors, ranging from induction ofMYCN transcriptional activation, increased MYCN protein stability due to dysregulated MYCN phosphorylation, and reduced proteasomal degradation to MYCN gene amplification [62][63][64][65][66][67]. Additionally, the aberrant expression of MYCN induces a unique cancer stem cell-like phenotype by enabling infinite self-renewal, apoptotic resistance, and metabolic reprogramming characterized by increased glycolysis with active oxidative phosphorylation [67][68][69][70][71].MYCN is one of the earliest genetic markers discovered in neuroblastoma, and MYCN amplification status is one of the strongest predictors of poor prognosis [72][73][74][75][76][77]. In high-risk neuroblastoma patients, MYCN amplification, if present, will always be present at diagnosis.…”

Section: Introductionmentioning

confidence: 99%

A systematic review of circulating-free MYCN amplification status as a noninvasive and prominent prognostic and recurrence monitoring indicator for neuroblastoma

Zhang

Liang

Zhang

et al. 2022

Preprint

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MYCN gene plays an important role in neuroblastoma cell growth, apoptosis, differentiation, tumor infiltration, metastasis, and angiogenesis. MYCN gene amplification status in tumor tissue is one of the important clinical indicators of neuroblastoma risk. However, there are several problems in detecting the MYCN gene in tumor tissues, such as complex procedures in detection approaches, high detection costs, and difficulty in obtaining tumor tissues. Studies have shown that circulating-free MYCN gene amplification in neuroblastoma is consistent with that in tumor tissue. Circulating-free MYCN gene amplification has the advantages of high sensitivity, high specificity, simple operation, and non-invasiveness as an indicator for prognosis and recurrence of neuroblastoma. Therefore, the application and future development of circulating-free MYCN gene amplification status in the prognosis and recurrence monitoring of neuroblastoma was examined in this article.

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Integrin‐Targeted, Short Interfering RNA Nanocomplexes for Neuroblastoma Tumor‐Specific Delivery Achieve MYCN Silencing with Improved Survival

Cited by 15 publications

References 51 publications

Unprotonatable and ROS‐Sensitive Nanocarrier for NIR Spatially Activated siRNA Therapy with Synergistic Drug Effect

Unprotonatable and ROS‐Sensitive Nanocarrier for NIR Spatially Activated siRNA Therapy with Synergistic Drug Effect

New Applications of Lipid and Polymer-Based Nanoparticles for Nucleic Acids Delivery

A systematic review of circulating-free MYCN amplification status as a noninvasive and prominent prognostic and recurrence monitoring indicator for neuroblastoma

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