Polyvalent Oligonucleotide Gold Nanoparticle Conjugates as Delivery Vehicles for Platinum(IV) Warheads

Dhar, Shanta; Daniel, Weston L.; Giljohann, David A.; Mirkin, Chad A.; Lippard, Stephen J.

doi:10.1021/ja9071282

Cited by 474 publications

(395 citation statements)

References 20 publications

Supporting

Mentioning

384

Contrasting

Unclassified

Order By: Relevance

“…Cisplatin and c;t;c-½PtðNH 3 Þ 2 ðO 2 CCH 2 CH 2 COOHÞðOHÞCl 2 (4) were prepared as previously described (45). N,N′-dicylcohexylcarbodiimide (DCC), O-benzyl-Lserine, p-toluenesulfonic acid, sodium nitrite, NHS, EDC, paraformaldehyde, and N,N-diisopropylethylamine were purchased from Aldrich.…”

Section: Methodsmentioning

confidence: 99%

Engineering of self-assembled nanoparticle platform for precisely controlled combination drug therapy

Kolishetti

Dhar

Valencia

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

536

429

View full text Add to dashboard Cite

The genomic revolution has identified therapeutic targets for a plethora of diseases, creating a need to develop robust technologies for combination drug therapy. In the present work, we describe a self-assembled polymeric nanoparticle (NP) platform to target and control precisely the codelivery of drugs with varying physicochemical properties to cancer cells. As proof of concept, we codelivered cisplatin and docetaxel (Dtxl) to prostate cancer cells with synergistic cytotoxicity. A polylactide (PLA) derivative with pendant hydroxyl groups was prepared and conjugated to a platinum(IV) [Pt(IV)] prodrug, c,t,c-½PtðNH 3 Þ 2 ðO 2 CCH 2 CH 2 COOHÞðOHÞCl 2 [PLAPt(IV)]. A blend of PLA-Pt(IV) functionalized polymer and carboxylterminated poly(D,L-lactic-co-glycolic acid)-block-poly(ethylene glycol) copolymer in the presence or absence of Dtxl, was converted, in microfluidic channels, to NPs with a diameter of ∼100 nm. This process resulted in excellent encapsulation efficiency (EE) and high loading of both hydrophilic platinum prodrug and hydrophobic Dtxl with reproducible EEs and loadings. The surface of the NPs was derivatized with the A10 aptamer, which binds to the prostatespecific membrane antigen (PSMA) on prostate cancer cells. These NPs undergo controlled release of both drugs over a period of 48-72 h. Targeted NPs were internalized by the PSMA-expressing LNCaP cells via endocytosis, and formation of cisplatin 1,2-d(GpG) intrastrand cross-links on nuclear DNA was verified. In vitro toxicities demonstrated superiority of the targeted dual-drug combination NPs over NPs with single drug or nontargeted NPs. This work reveals the potential of a single, programmable nanoparticle to blend and deliver a combination of drugs for cancer treatment.chemotherapy | drug delivery | polymer-drug conjugate | targeting | temporal release

show abstract

Section: Methodsmentioning

confidence: 99%

Engineering of self-assembled nanoparticle platform for precisely controlled combination drug therapy

Kolishetti

Dhar

Valencia

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

536

429

View full text Add to dashboard Cite

show abstract

“…Then, the acidic tumor extracellular pH (pH e ∼6.5-7.2) (35, 36) triggers the release of small PAMAM prodrugs (∼5 nm) that enable deep and uniform tumor penetration to reach more cancer cells. Finally, the PAMAM prodrugs can be rapidly reduced in the reductive cytosol to release active and potent cisplatin to kill cancer cells and lead to robust antitumor efficacy (37).…”

Section: Significancementioning

confidence: 99%

Stimuli-responsive clustered nanoparticles for improved tumor penetration and therapeutic efficacy

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

622

390

View full text Add to dashboard Cite

A principal goal of cancer nanomedicine is to deliver therapeutics effectively to cancer cells within solid tumors. However, there are a series of biological barriers that impede nanomedicine from reaching target cells. Here, we report a stimuli-responsive clustered nanoparticle to systematically overcome these multiple barriers by sequentially responding to the endogenous attributes of the tumor microenvironment. The smart polymeric clustered nanoparticle (iCluster) has an initial size of ∼100 nm, which is favorable for long blood circulation and high propensity of extravasation through tumor vascular fenestrations. Once iCluster accumulates at tumor sites, the intrinsic tumor extracellular acidity would trigger the discharge of platinum prodrug-conjugated poly(amidoamine) dendrimers (diameter ∼5 nm). Such a structural alteration greatly facilitates tumor penetration and cell internalization of the therapeutics. The internalized dendrimer prodrugs are further reduced intracellularly to release cisplatin to kill cancer cells. The superior in vivo antitumor activities of iCluster are validated in varying intractable tumor models including poorly permeable pancreatic cancer, drug-resistant cancer, and metastatic cancer, demonstrating its versatility and broad applicability.nanomedicine | particle size | tumor penetration | tumor extracellular pH | stimuli responsive

show abstract

“…In comparison, 11 hydrogels containing 2% PVA showed a moderate inhibition of cell growth by 45%, whereas hydrogels containing 4% PVA released the smallest amount of drug and induced an inhibition of cell growth by 20%. A large variation of cytotoxicity is seen in hydrogels of different PVA concentrations; the higher the PVA concentration, the lower the cytotoxicity, which is potentially from the slower rate of release of the drug.…”

Section: In Vitro Cytotoxicitymentioning

confidence: 89%

“…The first method is through better targeting of the drugs to tumours, thereby leaving healthy tissue unaffected [7]. A number of delivery systems, that target the tumour either passively or actively have been examined, such as: liposomes and micelles [8,9], polymers [10], nanoparticles [11][12][13], nanotubes [14] and dendrimers [15], as well as by the use of various targeting molecules, such as: folate and estrogen [16,17], aptamers [18], antibodies [19], magnetic fields [20] and DNA sequence selective agents [21,22] The second method by which the side effects of platinum drugs can be reduced is to change their pharmacokinetics (where and how a drug is transported and excreted in the body). The two biggest problems with platinum drug pharmacokinetics are their short blood serum halflifes (maximum concentration of cisplatin is achieved in less than 10 min before its serum 4 concentration drops significantly) and the extent of drug-protein binding (up to 90% of cisplatin is protein bound in the blood stream).…”

Section: Introductionmentioning

confidence: 99%

A cisplatin slow-release hydrogel drug delivery system based on a formulation of the macrocycle cucurbit[7]uril, gelatin and polyvinyl alcohol

Oun¹,

Plumb²,

Wheate³

2014

Journal of Inorganic Biochemistry

View full text Add to dashboard Cite

The anticancer drug cisplatin was encapsulated within the cucurbit [7]uril macrocycle to form the host-guest complex: cisplatin@CB [7]. This was then incorporated into gelatin and 0-4% w/v polyvinyl alcohol (PVA)-based hydrogels as slow release drug delivery vehicles. The hydrogels demonstrated predicable swelling and disintegration dependent on the PVA concentration. The hydrogel with the highest PVA content was slower to swell and release drug compared with lower concentrations of PVA. The effect of the hydrogel PVA concentration on in vitro cytotoxicity was examined using A2780/CP70 ovarian cancer cells. Over the 24 h drug exposure time used, hydrogels containing 4% PVA showed a 20% decrease in viable cells compared to the control, whereas hydrogels containing 0% and 2% PVA induced an 80% and 45% inhibition of cell growth, respectively. There was no measurable difference in the in vitro cytotoxicity of free cisplatin and cisplatin@CB [7] containing hydrogels. Finally, the in vivo effectiveness of a 2%-PVA hydrogel implanted under the skin of nude mice bearing A2780/CP70 xenografts showed that low dose hydrogels containing cisplatin@CB [7] (30 µg equivalent of drug) was just as effective as an intraperitoneal high dose administration of free cisplatin (150 µg) at inhibiting tumour growth.

show abstract

Polyvalent Oligonucleotide Gold Nanoparticle Conjugates as Delivery Vehicles for Platinum(IV) Warheads

Cited by 474 publications

References 20 publications

Engineering of self-assembled nanoparticle platform for precisely controlled combination drug therapy

Engineering of self-assembled nanoparticle platform for precisely controlled combination drug therapy

Stimuli-responsive clustered nanoparticles for improved tumor penetration and therapeutic efficacy

A cisplatin slow-release hydrogel drug delivery system based on a formulation of the macrocycle cucurbit[7]uril, gelatin and polyvinyl alcohol

Contact Info

Product

Resources

About