In Situ Forming of Nitric Oxide and Electric Stimulus for Nerve Therapy by Wireless Chargeable Gold Yarn‐Dynamos

Chiang, Min‐Ren; Lin, Ya‐Hui; Zhao, Wei‐Jie; Liu, Hsiu‐Ching; Hsu, Ru‐Siou; Chou, Tsu‐Chin; Lu, Tsai‐Te; Lee, I‐Chi; Liao, Lun‐De; Chiou, Shih‐Hwa; Chu, Li‐An; Hu, Shang‐Hsiu

doi:10.1002/advs.202303566

Cited by 4 publications

(1 citation statement)

References 77 publications

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“…The cytotoxic T cells are often hampered by tumor heterogeneity constituted of high interstitial fluid pressure (IFP) and the presence of cancer-associated fibroblasts. They limit transport and immune escape of therapeutic agents, especially in the brain. − To address these issues, one potential strategy is to use specific particles to create gaps between cancer cells, called nanoparticle-induced endothelial leakage (NanoEL). − It induces extravasation of cancer cells into the surrounding vascular areas. The NanoEL gaps also allowed for nanomedicine to pass through, which has been reported recently. − It is intended to kill tumors, but it may also inadvertently cause leakage in tumor vasculature, thereby lowering the intravascular barrier for viable cancer cells to enter the circulation. , Furthermore, utilizing NanoEL gold particles leads to increased leakage of larger sized nanoparticles and could bring about complete regression of primary tumors and attack against the secondary metastatic tumor when it is at the micrometastasis stage .…”

Section: Introductionmentioning

confidence: 99%

A Self-Cascade Penetrating Brain Tumor Immunotherapy Mediated by Near-Infrared II Cell Membrane-Disrupting Nanoflakes via Detained Dendritic Cells

Yalamandala,

Chen,

Lin

et al. 2024

ACS Nano

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Immunotherapy can potentially suppress the highly aggressive glioblastoma (GBM) by promoting T lymphocyte infiltration. Nevertheless, the immune privilege phenomenon, coupled with the generally low immunogenicity of vaccines, frequently hampers the presence of lymphocytes within brain tumors, particularly in brain tumors. In this study, the membrane-disrupted polymer-wrapped CuS nanoflakes that can penetrate delivery to deep brain tumors via releasing the cell−cell interactions, facilitating the near-infrared II (NIR II) photothermal therapy, and detaining dendritic cells for a self-cascading immunotherapy are developed. By convection-enhanced delivery, membrane-disrupted amphiphilic polymer micelles (poly(methoxypoly(ethylene glycol)-benzoic imineoctadecane, mPEG-b-C18) with CuS nanoflakes enhances tumor permeability and resides in deep brain tumors. Under low-power NIR II irradiation (0.8 W/cm 2 ), the intense heat generated by well-distributed CuS nanoflakes actuates the thermolytic efficacy, facilitating cell apoptosis and the subsequent antigen release. Then, the positively charged polymer after hydrolysis of the benzoic-imine bond serves as an antigen depot, detaining autologous tumorassociated antigens and presenting them to dendritic cells, ensuring sustained immune stimulation. This selfcascading penetrative immunotherapy amplifies the immune response to postoperative brain tumors but also enhances survival outcomes through effective brain immunotherapy.

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Section: Introductionmentioning

confidence: 99%

A Self-Cascade Penetrating Brain Tumor Immunotherapy Mediated by Near-Infrared II Cell Membrane-Disrupting Nanoflakes via Detained Dendritic Cells

Yalamandala,

Chen,

Lin

et al. 2024

ACS Nano

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Magnetically Controlled Strategies for Enhanced Tissue Vascularization

Zhu,

Xu,

Zhang

et al. 2024

Adv Funct Materials

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Tissue vascularization plays a critical role in the regeneration and repair of damaged tissues. However, in certain instances of tissue injury, the pace and effectiveness of vascularization can be limited. Innovative strategies leveraging magnetic fields and magnetic nanoparticles (MNPs) are devised to enhance the efficacy of tissue vascularization. This review explores the potential of magnetic field‐assisted strategies in augmenting tissue vascularization and repair. Direct application of static or dynamic magnetic fields, alone or in combination with MNPs, offers a means to modulate cellular behaviors and gene expression, thereby promoting angiogenesis and tissue regeneration. Techniques such as cell labeling, gene delivery using MNPs, and magnetic targeting have shown promise in efficiently repairing various ischemic tissue injuries by enhancing tissue vascularization. These strategies have broad applications in bone and skin tissue regeneration, limb ischemia treatment, myocardial injury treatment, and diabetic wound therapy. By summarizing recent advancements in magnetically controlled strategies, this review aims to shed light on their future prospects in tissue regeneration and clinical treatment.

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Reprogrammed Lung Metastasis Immunodeficiency via Targeted Penetrated Delivery of M1 Macrophage‐Wrapped NanoCubes‐Mediated T Cell Infiltration

Wang,

Li,

Huang

et al. 2024

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The infiltration of cytotoxic T lymphocytes holds promise for suppressing even the most resilient metastatic tumors in immunotherapy. Polarizing tumor‐associated macrophages (TAMs) and remodeling the immune‐deficient tumor microenvironment (TME) can enhance T lymphocyte recruitment and infiltration. However, the immune privilege and low immunogenic responses of these aggressive tumor clusters often limit lymphocyte recruitment. Here, an M1 macrophage membrane‐coated iron oxide nanoparticle (IO@MM) double as a tumor‐penetrated agent and naïve M0 macrophage to M1 polarizer is developed for lung metastatic colorectal cancer (CRC) immunotherapy. At the tumor site, IO@MM combined with resiquimod (R848) increased the immune cell infiltration, turning the “Cold” TME into an immune‐activating “Hot” one. Together with self‐cascade immunotherapy, IO@MM with R848 promotes tumor release of damage‐associated molecular patterns (DAMPs). At the same time, IO@MM uses the membrane as an antigen reservoir and provides autologous DAMPs to retain dendritic cells. This IO@MM effectively inhibits tumors and improves survival rate as an immunomodulator in lung metastasis.

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In Situ Forming of Nitric Oxide and Electric Stimulus for Nerve Therapy by Wireless Chargeable Gold Yarn‐Dynamos

Cited by 4 publications

References 77 publications

A Self-Cascade Penetrating Brain Tumor Immunotherapy Mediated by Near-Infrared II Cell Membrane-Disrupting Nanoflakes via Detained Dendritic Cells

A Self-Cascade Penetrating Brain Tumor Immunotherapy Mediated by Near-Infrared II Cell Membrane-Disrupting Nanoflakes via Detained Dendritic Cells

Magnetically Controlled Strategies for Enhanced Tissue Vascularization

Reprogrammed Lung Metastasis Immunodeficiency via Targeted Penetrated Delivery of M1 Macrophage‐Wrapped NanoCubes‐Mediated T Cell Infiltration

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