An activatable multimodal/multifunctional nanoprobe for direct imaging of intracellular drug delivery

Mitra, Riten; Doshi, Mona; Zhang, Xiaolei; Tyus, Jessica C.; Bengtsson, Niclas E.; Fletcher, Steven; Page, Brent D. G.; Turkson, James; Gesquiere, Andre J.; Gunning, Patrick T.; Walter, Glenn A.; Santra, Swadeshmukul

doi:10.1016/j.biomaterials.2011.10.068

Cited by 51 publications

(30 citation statements)

References 38 publications

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“…Transmission electron microscopy (TEM) analysis was carried out as described [30, 31] using one drop of a 1 mM or 5 μM Y 2 O 3 NP (Sigma-Aldrich Inc.) dispersion which was prepared under 10W ultrasonication at room temperature.…”

Section: Methodsmentioning

confidence: 99%

Yttrium oxide nanoparticles prevent photoreceptor death in a light-damage model of retinal degeneration

Mitra

Merwin

Han

et al. 2014

Free Radical Biology and Medicine

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Photoreceptor (PR) cells are prone to accumulation of reactive oxygen species (ROS) and oxidative stress. An imbalance between the production of ROS and cellular antioxidant defenses contributes to PR degeneration and blindness in many different ocular disease states. Yttrium oxide (Y2O3) nanoparticles (NPs) are excellent free radical scavengers due to their non-stoichiometric crystal defects. Here we utilize a murine light stress model to test the efficacy of Y2O3 NPs (~ 10–14 nm in diameter) in ameliorating retinal oxidative stress-associated degeneration. Our studies demonstrate that intravitreal injections of these NPs at doses ranging from 0.1 μM to 5.0 μM two weeks prior to acute light stress protects PRs from degeneration. This protection is reflected both structurally (i.e. decreased light-associated thinning of the outer nuclear layer) and functionally, i.e. in preservation of scotopic and photopic electroretinogram amplitudes. We also observe preservation of structure and function when NPs are delivered immediately after acute light stress, although the magnitude of the preservation is smaller, and only doses ranging from 1.0 μM to 5.0 μM were effective. We show that the Y2O3 NPs are non-toxic and well-tolerated after intravitreal delivery. Our results suggest that Y2O3 NPs have astonishing antioxidant benefits, and with further exploration, may be an excellent strategy for the treatment of oxidative stress associated with multiple forms of retinal degeneration.

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Section: Methodsmentioning

confidence: 99%

Yttrium oxide nanoparticles prevent photoreceptor death in a light-damage model of retinal degeneration

Mitra

Merwin

Han

et al. 2014

Free Radical Biology and Medicine

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“…for fluorescence resonance energy transfer, FRET) [12], ligands for colloidal stability or for targeting, or therapeutic compounds [13,14], and thus permits an exceptional tailoring in the design of these systems. In case magnetic nanoparticles are used as carriers the same system could act magnetically guided as drug delivery carrier, which simultaneously monitors the delivered drug [15]. Also polyelectrolyte capsules are a very universal system toward the integration of many different functional units into one particle [16], in addition to the actual ion-sensitive fluorophores [17].…”

Section: Potential Of Particles-based Ion-sensitive Fluorescence Sensorsmentioning

confidence: 99%

Fluorescence-based ion-sensing with colloidal particles

Ashraf

Carrillo‐Carrión

Zhang

et al. 2014

Current Opinion in Pharmacology

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“…The increased QD fluorescence could be used to track STAT3 release from the nanocomposite and the iron oxide core allowed MRI analysis of the nanocomposite in the cell cytoplasm. [209] In addition to following drug release from polymer conjugates or polymer nanomedicines, a second important challenge is to monitor endosomal escape of polymer nanomedicines and/or their cargo. The use of CLSM and suitable labels allows to monitor either drug or carrier.…”

Section: Monitoring Cytosolic Deliverymentioning

confidence: 99%

Controlling and Monitoring Intracellular Delivery of Anticancer Polymer Nanomedicines

Battistella

Klok

2017

Macromolecular Bioscience

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Polymer nanomedicines are very attractive to improve the delivery of chemotherapeutics. Polymer conjugates and other polymer‐based nanocarriers allow to increase plasma half‐life and drug bioavailability and can also be guided toward tumors using passive and active targeting strategies. Since many chemotherapeutics act on targets that are located in well‐defined subcellular compartments, other important factors that contribute to an efficient therapy include cellular internalization and subsequent intracellular trafficking of the polymer nanomedicines and/or its payload to the appropriate organelle in the cytoplasm. This article provides an overview of the different approaches that have been developed to control intracellular delivery of polymer nanomedicines and discusses the different techniques that can be used to monitor these processes.

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An activatable multimodal/multifunctional nanoprobe for direct imaging of intracellular drug delivery

Cited by 51 publications

References 38 publications

Yttrium oxide nanoparticles prevent photoreceptor death in a light-damage model of retinal degeneration

Yttrium oxide nanoparticles prevent photoreceptor death in a light-damage model of retinal degeneration

Fluorescence-based ion-sensing with colloidal particles

Controlling and Monitoring Intracellular Delivery of Anticancer Polymer Nanomedicines

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