Aurora kinase inhibitor nanoparticles target tumors with favorable therapeutic index in vivo

Ashton, Susan; Song, Young Ho; Nolan, Jim; Cadogan, Elaine; Murray, J.A.; Odedra, Rajesh; Foster, John R.; Hall, Peter A.; Low, Susan C.; Taylor, Paula; Ellston, Rebecca; Polanska, Urszula M.; Wilson, Joanne; Howes, Colin; Smith, Aaron; Goodwin, Richard J. A.; Swales, John G.; Strittmatter, Nicole; Takáts, Zoltán; Nilsson, Anna; Andrén, Per E.; Trueman, Dawn; Walker, Mike; Reimer, Corinne; Troiano, Greg; Parsons, Donald M.; Witt, David De; Ashford, Marianne; Hrkach, Jeff; Zale, Stephen E.; Jewsbury, Philip J.; Barry, Simon T.

doi:10.1126/scitranslmed.aad2355

Cited by 175 publications

(142 citation statements)

References 24 publications

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“…Recently, there has been a move away from cytotoxic cancer drugs towards molecularly targeted agents (MTAs) that have had little attention in the nanomedicine field. While highly efficacious, these drugs are associated with serious toxicity profiles on their own, and therefore the combination with nanoparticles may help to reduce toxicity and allow higher dosing (43). Next generation BIND micelles that incorporate kinase inhibitors as future drug therapeutics have been used to investigate efficacy against metastatic colon cancers, showing promising results in pre-clinical trials.…”

Section: Polymeric Micellesmentioning

confidence: 98%

Nanoparticle-Based Medicines: A Review of FDA-Approved Materials and Clinical Trials to Date

et al. 2016

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In this review we provide an up to date snapshot of nanomedicines either currently approved by the US FDA, or in the FDA clinical trials process. We define nanomedicines as therapeutic or imaging agents which comprise a nanoparticle in order to control the biodistribution, enhance the efficacy, or otherwise reduce toxicity of a drug or biologic. We identified 51 FDA-approved nanomedicines that met this definition and 77 products in clinical trials, with ~40% of trials listed in clinicaltrials.gov started in 2014 or 2015. While FDA approved materials are heavily weighted to polymeric, liposomal, and nanocrystal formulations, there is a trend towards the development of more complex materials comprising micelles, protein-based NPs, and also the emergence of a variety of inorganic and metallic particles in clinical trials. We then provide an overview of the different material categories represented in our search, highlighting nanomedicines that have either been recently approved, or are already in clinical trials. We conclude with some comments on future perspectives for nanomedicines, which we expect to include more actively-targeted materials, multi-functional materials ("theranostics") and more complicated materials that blur the boundaries of traditional material categories. A key challenge for researchers, industry, and regulators is how to classify new materials and what additional testing (e.g. safety and toxicity) is required before products become available.

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Section: Polymeric Micellesmentioning

confidence: 98%

Nanoparticle-Based Medicines: A Review of FDA-Approved Materials and Clinical Trials to Date

et al. 2016

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“…49 The release kinetics of encapsulated drug has significant impacts on the efficacies of drug delivery systems. 49, 50 Burst release would result in similar pharmacokinetics between encapsulated drug and a free form of drug, diminishing advantages of using NP as a drug carrier. Hence, the sustained release of Gi would benefit in vivo application.…”

Section: Resultsmentioning

confidence: 99%

Delayed Sequential Co-Delivery of Gefitinib and Doxorubicin for Targeted Combination Chemotherapy

et al. 2017

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There are an increasing number of studies showing the order of drug presentation plays a critical role in achieving optimal combination therapy. Here, a nanoparticle design is presented using ion pairing and drug-polymer conjugate for the sequential delivery of gefitinib (Gi) and doxorubicin (Dox) targeting epidermal growth factor receptor (EGFR) signaling applicable for the treatment of triple negative breast cancers. To realize this nanoparticle design, Gi complexed with dioleoyl phosphatidic acid (DOPA) via ion paring was loaded onto the nanoparticle made of Dox-conjugated poly(L-lactide)-block-polyethylene glycol (PLA-b-PEG) and with an encapsulation efficiency of ~90%. The nanoparticle system exhibited a desired sequential release of Gi followed by Dox, as verified through release and cellular uptake studies. The nanoparticle system demonstrated approximate fourfold and threefold increases in anti-cancer efficacy compared to a control group of Dox-PLA-PEG conjugate against MDA-MB-468 and A549 cell lines in terms of half maximal inhibitory concentration (IC50), respectively. High tumor accumulation of the nanoparticle system was also substantiated for potential in vivo applicability by non-invasive fluorescent imaging.

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“…Barasertib has entered clinical trials in elderly patients with acute myeloid leukaemia (AML) and has demonstrated clinically meaningful responses, including complete remission in some patients [36,37]. In 2013, an agreement was signed with BIND Therapeutics to further develop the active ingredient of AZD1152 (AZD1152-hQPA, recently designated AZD2811 (compound 18) [38] using Accurin 1 nanoparticle technology and offering the potential to adapt the therapeutic regimen to different tumours while achieving an improved therapeutic index. AZD2811 has recently commenced Phase I clinical testing in patients with advanced solid tumours.…”

Section: Inhibitor Of Aurora-b Kinase Barasertibmentioning

confidence: 99%

Standing on the shoulders of giants: a retrospective analysis of kinase drug discovery at AstraZeneca

Kettle

Wilson

2016

Drug Discovery Today

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Aurora kinase inhibitor nanoparticles target tumors with favorable therapeutic index in vivo

Cited by 175 publications

References 24 publications

Nanoparticle-Based Medicines: A Review of FDA-Approved Materials and Clinical Trials to Date

Nanoparticle-Based Medicines: A Review of FDA-Approved Materials and Clinical Trials to Date

Delayed Sequential Co-Delivery of Gefitinib and Doxorubicin for Targeted Combination Chemotherapy

Standing on the shoulders of giants: a retrospective analysis of kinase drug discovery at AstraZeneca

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