Synthesis and characterization of degradable multivalent cationic lipids with disulfide-bond spacers for gene delivery

Shirazi, Rahau S.; Ewert, Kai K.; Leal, Cecı́lia; Majzoub, Ramsey N.; Bouxsein, Nathan F.; Safinya, Cyrus R.

doi:10.1016/j.bbamem.2011.04.020

Cited by 73 publications

(74 citation statements)

References 64 publications

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“…[14][15][16][17][18][19][20][21][22][23][24] Among the existing nonviral vectors, the cationic liposome, representing an attractive, alternative approach for gene delivery has a broad varity of advantages, such as biodegradability, easy preparation, good repeatability and potential clinical applications. [25][26][27][28][29] Cationic lipids generally consist of polar head group and hydrophobic tails connected through the backbone (Fig.…”

mentioning

confidence: 99%

Preparation, Physicochemical Properties, and Transfection Activities of Tartaric Acid-Based Cationic Lipids as Effective Nonviral Gene Delivery Vectors

Wan

Jia

Hou

et al. 2016

Biological & Pharmaceutical Bulletin

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confidence: 99%

Preparation, Physicochemical Properties, and Transfection Activities of Tartaric Acid-Based Cationic Lipids as Effective Nonviral Gene Delivery Vectors

Wan

Jia

Hou

et al. 2016

Biological & Pharmaceutical Bulletin

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“…cleavage of single-strand crgD-sirNa conjugates in a reductive environment According to the reported concentrations of DTT (10-300 mM); [35][36][37][38][39][40] we used 100 mM of DTT to detect the cleavage of disulfide bond. The reaction was allowed to proceed at 37°C for 2 h, which was stopped by immediately storing the conjugates at -80°C until analysis.…”

Section: Western Blot Analysismentioning

confidence: 99%

Reductive nanocomplex encapsulation of cRGD-siRNA conjugates for enhanced targeting to cancer cells

Zhou¹,

Liu²,

Zhang³

et al. 2017

IJN

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In this study, through covalent conjugation and lipid material entrapment, a combined modification strategy was established for effective delivery of small interfering RNA (siRNA). Single strands of siRNA targeting to BRAF V600E gene (siMB3) conjugated with cRGD peptide at 3′-terminus or 5′-terminus via cleavable disulfide bond was synthesized and then annealed with corresponding strands to obtain single and bis-cRGD-siRNA conjugates. A cationic lipid material (CLD) developed by our laboratory was mixed with the conjugates to generate nanocomplexes; their uniformity and electrical property were revealed by particle size and zeta potential measurement. Compared with CLD/siBraf, CLD/cRGD-siBraf achieved higher cell uptake and more excellent tumor-targeting ability, especially 21 (sense-5′/antisense-3″-cRGD-congjugate) nanocomplex. Moreover, they can regulate multiple pathways to varying degree and reduce acidification of endosome. Compared with the gene silencing of different conjugates, single or bis-cRGD-conjugated siRNA showed little differences except 22 (5/5) which cRGD was conjugated at 5′-terminus of antisense strand and sense strand. However bis-cRGD conjugate 21 nanocomplex exhibited better specific target gene silencing at multiple time points. Furthermore, the serum stabilities of the bis-cRGD conjugates were higher than those of the single-cRGD conjugates. In conclusion, all these data suggested that CLD/bis-conjugates, especially CLD/ 21 , can be an effective system for delivery of siRNA to target BRAF V600E gene for therapy of melanoma.

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“…After 24 hours, the culture medium was replaced by 100 μL of complete DMEM involving blank NPs (HP and SHP), plain fasudil, and coloaded NPs ( Fasudil HP miR195 , Fasudil SHP miR195 ) for 24 hours. Also, 100 nM miR195 was constantly used, and fasudil was loaded at three different drug concentrations (10,30, and 60 μM) as low-, moderate-, and high-dose fasudil groups. Cells treated with the same amount of PBS were used as control.…”

Section: In Vitro Cytotoxicity Assaymentioning

confidence: 99%

Aptamer-functionalized peptide H<sub>3</sub>CR<sub>5</sub>C as a novel nanovehicle for codelivery of fasudil and miRNA-195 targeting hepatocellular carcinoma

Liu¹,

Wu²,

Gao³

et al. 2016

IJN

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Liver cancer is the fifth most commonly diagnosed malignancy, of which hepatocellular carcinoma (HCC) represents the dominating histological subtype. Antiangiogenic therapy aimed at vascular endothelial growth factor (VEGF) has shown promising but deficient clinical prospects on account of vasculogenic mimicry, a highly patterned vascular channel distinguished from the endothelium-dependent blood vessel, which may function as blood supply networks occurring in aggressive tumors including HCC. In this study, we used a new cationic peptide, disulfide cross-linked stearylated polyarginine peptide modified with histidine (H 3 R 5 ), as a reducible vector, cell penetrating peptide-modified aptamer (ST21) with specific binding to HCC cells to conjugate to peptide H 3 R 5 as the targeting probe, miRNA-195 (miR195) as a powerful gene drug to inhibit VEGF, and fasudil to suppress vasculogenic mimicry by blocking ROCK2, all of which were simultaneously encapsulated in the same nanoparticles. Fasudil was loaded by ammonium sulfate-induced transmembrane electrochemical gradient and miR195 was condensed through electrostatic interaction. ST21-H 3 R 5 -polyethylene glycol (PEG) exhibited excellent loading capacities for both fasudil and miR195 with adjustable dosing ratios. Western blot analysis showed that Fasudil ST21-H 3 R 5 -PEG miR195 had strong silencing activity of ROCK2 and VEGF, as compared with Fasudil H 3 R 5 -PEG miR195 . In vitro and in vivo experiments confirmed that ST21-modified nanoparticles showed significantly higher cellular uptake and therapeutic efficacy in tumor cells or tumor tissues than the unmodified counterparts. These findings suggest that aptamer-conjugated peptide holds great promise for delivering chemical drugs and gene drugs simultaneously to overcome HCC.

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Synthesis and characterization of degradable multivalent cationic lipids with disulfide-bond spacers for gene delivery

Cited by 73 publications

References 64 publications

Preparation, Physicochemical Properties, and Transfection Activities of Tartaric Acid-Based Cationic Lipids as Effective Nonviral Gene Delivery Vectors

Preparation, Physicochemical Properties, and Transfection Activities of Tartaric Acid-Based Cationic Lipids as Effective Nonviral Gene Delivery Vectors

Reductive nanocomplex encapsulation of cRGD-siRNA conjugates for enhanced targeting to cancer cells

Aptamer-functionalized peptide H<sub>3</sub>CR<sub>5</sub>C as a novel nanovehicle for codelivery of fasudil and miRNA-195 targeting hepatocellular carcinoma

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