Minimizing the non-specific binding of nanoparticles to the brain enables active targeting of Fn14-positive glioblastoma cells

Schneider, Craig S.; Perez, Jimena G.; Cheng, Emily H.; Zhang, Clark; Mastorakos, Panagiotis; Hanes, Justin; Winkles, Jeffrey A.; Woodworth, Graeme F.; Kim, Anthony J.

doi:10.1016/j.biomaterials.2014.11.054

Cited by 60 publications

(95 citation statements)

References 54 publications

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“…These nanoparticles successfully penetrated brain parenchyma, but specifically bound glioblastoma cells, without significant off-target effects. 62 Additionally, the nanoparticles showed reduced nonspecific binding of the brain extracellular matrix. By specifically targeting cancer cells, as demonstrated via Fn14 conjugation in the Schneider et al study, 62 it is possible that nanoparticles that specifically target cancer cells could be effectively used to deliver drugs to remote tumor cells that otherwise escape resection.…”

Section: Intramedullary Metastasesmentioning

confidence: 99%

“…However, there have been promising results from nanomedicine approaches to brain tumors. For instance, Schneider et al 62 show that the use of drug-loaded nanoparticles can be targeted to specifically bind glioblastoma cells via conjugation with the protein fibroblast growth factor-inducible 14 (Fn14). These nanoparticles successfully penetrated brain parenchyma, but specifically bound glioblastoma cells, without significant off-target effects.…”

Section: Intramedullary Metastasesmentioning

confidence: 99%

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Intramedullary spinal cord tumors: a review of current and future treatment strategies

Tobin¹,

Geraghty²,

Engelhard³

et al. 2015

FOC

150

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Intramedullary spinal cord tumors have low incidence rates but are associated with difficult treatment options. The majority of patients with these tumors can be initially treated with an attempted resection. Unfortunately, those patients who cannot undergo gross-total resection or have subtotal resection are left with few treatment options, such as radiotherapy and chemotherapy. These adjuvant treatments, however, are associated with the potential for significant adverse side effects and still leave patients with a poor prognosis. To successfully manage these patients and improve both their quality of life and prognosis, novel treatment options must be developed to supplement subtotal resection. New research is underway investigating alternative therapeutic approaches for these patients, including directed, localized drug delivery and nanomedicine techniques. These and other future investigations will hopefully lead to promising new therapies for these devastating diseases.

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Section: Intramedullary Metastasesmentioning

confidence: 99%

Section: Intramedullary Metastasesmentioning

confidence: 99%

Intramedullary spinal cord tumors: a review of current and future treatment strategies

Tobin¹,

Geraghty²,

Engelhard³

et al. 2015

FOC

150

View full text Add to dashboard Cite

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“…NPs targeted to Fn14-positive GBM cells using a monoclonal antibody improved NP tumor localization and internalization. 48,68 Thus, a similar targeting strategy may enhance the delivery of platinum compounds specifically to GBM cells, improving efficacy and minimizing toxicity.…”

Section: Reduced Side-effects Through Enhanced Site-specific Deliverymentioning

confidence: 99%

“…53 NPs may improve the delivery of therapeutics to invasive GBM cells by overcoming such drug delivery challenges. 48 Furthermore, a major reason for failure of platinumbased chemotherapeutics in GBM patients is off-target toxicity. NP formulations may effectively address this issue; indeed, NPs have been shown to reduce toxicity compared to free drug.…”

Section: Reduced Side-effects Through Enhanced Site-specific Deliverymentioning

confidence: 99%

“…These strategies include (a) increasing BBB permeability, 45 (b) delivering cisplatin within biodegradable polymer implants in the tumor bed of patients, 46 and (c) bypassing the BBB via delivery under low sustained pressure ('convection') directly into the brain through an implanted catheter(s), an approach termed as convection enhanced delivery (CED). 47 The expanding field of nanomedicine offers a variety of drug formulation options to improve platinum-based therapies, such as (a) increased solubility and increased blood half-life, (b) reduced side-effects through targeted delivery and broader tissue distribution in mouse intracranial glioma models, 48 (c) controlled and sustained drug release, and (d) simultaneous incorporation and delivery of other anticancer drugs for combination therapy. 49 …”

Section: Augmenting Delivery To Improve Platinum-based Therapymentioning

confidence: 99%

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Repurposing platinum-based chemotherapies for multi-modal treatment of glioblastoma

et al. 2016

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Glioblastoma (GBM) is a fatal brain cancer for which new treatment options are sorely needed. Platinumbased drugs have been investigated extensively for GBM treatment but few have shown significant efficacy without major central nervous system (CNS) and systemic toxicities. The relative success of platinum drugs for treatment of non-CNS cancers indicates great therapeutic potential when effectively delivered to the tumor region(s). New insights into the broad anticancer effects of platinum drugs, particularly immunomodulatory effects, and innovative delivery strategies that can maximize these multimodal effects and minimize toxicities may promote the re-purposing of this chemotherapeutic drug class for GBM treatment.

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Treatment of Malignant Brain Tumor by Tumor‐Triggered Programmed Wormlike Micelles with Precise Targeting and Deep Penetration

Zeng

Zou

et al. 2016

Adv Funct Materials

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The effi cient and specifi c drug delivery to brain tumor is a crucial challenge for successful systemic chemotherapy. To overcome these limitations, here a tumor-triggered programmed wormlike micelle is reported with precise targeting and deep penetration to treat malignant gliomas, which is composed of pH-responsive mPEG-b -PDPA copolymer and bioreducible cyclic RGD peptide targeted cytotoxic emtansine (DM1) conjugates (RGD-DM1). The RGD-DM1 loaded nanoscaled wormlike micelles (RNW) exhibit nanometer-sized wormlike assemblies with the transverse diameter of 21.3±1.8 nm and length within 60-600 nm, and the RGD targeting peptide in RNW is 4.2% % in weight. RNW can be dissociated at intracellular acidic environments to release RGD-DM1, and be further degraded into DM1 by cleavage of disulfi de bonds in the reductive milieu. In particular, by exploiting the unique wormlike structure and the RGD targeting peptide modifi cation, RNW can be endowed with obviously enhanced drug delivery to brain, precise targeting to brain tumor, deep penetration into tumor mass, and effi cient internalization into glioma cells in a programmed manner, thereby surprisingly leading to an 88.9% % inhibition on tumor progression in an orthotopic brain tumor model. Therefore, the properly designed RNW can provide a promising delivery platform for systemic chemotherapy of brain tumor. the characteristics of BBB, and the new blood vessels in brain tumor are not as leaky as the angiogenic vessels observed in other cancer types, thereby signifi cantly restricting the delivery of nanosystems to the tumor sites. [ 19,21 ] To improve the transport of nanosystem across these barriers, various approaches including disrupting the integrity, convection enhanced delivery and ligand-modifi ed active targeting methods, have been investigated. [ 7,8,16,22 ] However, most nanosystems are mainly located in the perivascular space of tumor areas or around the tumor vessels, and cannot penetrate into the deep sites of brain tumors. [ 23 ] Even after successful targeting to brain tumors, the drug molecules have to be released from the nanosystem into cytoplasma with suffi cient drug concentration for chemotherapy. Thereby, the nanosystems should be properly designed to offer a promising delivery system for systemic chemotherapy of brain tumor. DOIWith this in mind, we herein designed a novel tumor-triggered programmed wormlike micelles with precise targeting, deep tumor penetration and on-demand drug release capability to treat malignant gliomas ( Scheme 1 ). The wormlike system is composed of pH-responsive amphiphilic polymer of methoxypoly (ethylene glycol)-block -poly(2-diisopropyl methacrylate) (mPEG-b -PDPA) and a bioreducible cyclic [RGDfK]C peptide (RGD) targeted cytotoxic emtansine (DM1) conjugates (RGD-S-S-DM1, further shorten as RGD-DM1). By combining the unique wormlike structure and RGD targeting peptide modifi cation, the RGD-DM1 loaded nanoscaled wormlike micelles (RNW) is supposed to be effi ciently and progressively targeted to brain tumor afte...

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Minimizing the non-specific binding of nanoparticles to the brain enables active targeting of Fn14-positive glioblastoma cells

Cited by 60 publications

References 54 publications

Intramedullary spinal cord tumors: a review of current and future treatment strategies

Intramedullary spinal cord tumors: a review of current and future treatment strategies

Repurposing platinum-based chemotherapies for multi-modal treatment of glioblastoma

Treatment of Malignant Brain Tumor by Tumor‐Triggered Programmed Wormlike Micelles with Precise Targeting and Deep Penetration

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