Publications by authors named "Digigow R"

Article Synopsis
  • The study examines how intravenous (IV) nanomedicines interact with endothelial cells (ECs) that line blood vessels, focusing on the importance of shear stress in experimental designs for testing nanoparticle responses.
  • Researchers developed a flow-induced endothelium model that simulates real blood flow conditions over 14 days, leading to a more stable and less reactive cell layer.
  • Results showed that when exposed to iron sucrose under dynamic conditions, the mature endothelium had reduced nanoparticle uptake and less cytotoxicity, largely due to the presence of glycocalyx, ultimately suggesting that this model helps better understand how nanomedicines behave immediately after injection.
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Article Synopsis
  • Iron deficiency and anemia are major global health issues, and intravenous iron carbohydrate nanoparticles are vital for effective treatment.
  • Our study used advanced cryogenic Scanning Transmission Electron Microscopy (cryo-STEM) to analyze the physical structure of these nanoparticles, revealing they typically have iron cores about 2 nm in size and distinct cluster-like shapes in various products.
  • By employing this sophisticated imaging technique, we not only preserved the specimens' structural integrity but also contributed insights that could enhance understanding of how these nanoparticles function, including the development of a machine learning tool for better image analysis.
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Intravenous (IV) iron-carbohydrate complexes are widely used nanoparticles (NPs) to treat iron deficiency anaemia, often associated with medical conditions such as chronic kidney disease, heart failure and various inflammatory conditions. Even though a plethora of physicochemical characterisation data and clinical studies are available for these products, evidence-based correlation between physicochemical properties of iron-carbohydrate complexes and clinical outcome has not fully been elucidated yet. Studies on other metal oxide NPs suggest that early interactions between NPs and blood upon IV injection are key to understanding how differences in physicochemical characteristics of iron-carbohydrate complexes cause variance in clinical outcomes.

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Iron-carbohydrate complexes are widely used to treat iron deficiencies. Macrophages play a crucial role in the uptake and fate of these nanomedicines, however, how complexed iron carbohydrates are taken up and metabolized by macrophages is still not fully understood. Using a (phospho-)proteomics approach, we assessed differences in protein expression and phosphorylation in M2 macrophages triggered by iron sucrose (IS).

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Intravenously administered iron-carbohydrate nanoparticle complexes are widely used to treat iron deficiency. This class includes several structurally heterogeneous nanoparticle complexes, which exhibit varying sensitivity to the conditions required for the methodologies available to physicochemically characterize these agents. Currently, the critical quality attributes of iron-carbohydrate complexes have not been fully established.

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Intravenous iron-carbohydrate nanomedicines are widely used to treat iron deficiency and iron deficiency anemia across a wide breadth of patient populations. These colloidal solutions of nanoparticles are complex drugs which inherently makes physicochemical characterization more challenging than small molecule drugs. There have been advancements in physicochemical characterization techniques such as dynamic light scattering and zeta potential measurement, that have provided a better understanding of the physical structure of these drug products in vitro.

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Intravenous iron-carbohydrate complexes are nanomedicines that are commonly used to treat iron deficiency and iron deficiency anemia of various etiologies. Many challenges remain regarding these complex drugs in the context of fully understanding their pharmacokinetic parameters. Firstly, the measurement of the intact iron nanoparticles versus endogenous iron concentration fundamentally limits the availability of data for computational modeling.

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Autoimmune diseases are caused by adaptive immune responses to self-antigens. The development of antigen-specific therapies that suppress disease-related, but not unrelated immune responses in general, is an important goal of biomedical research. We have previously shown that delivery of myelin peptides to liver sinusoidal endothelial cells (LSECs) using LSEC-targeting nanoparticles provides effective protection from CD4 T-cell-driven autoimmune encephalomyelitis.

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Microreactors have attracted wide attention in the nano- and biotechnology fields because they offer many advantages over standard liquid phase reactions. We report the development of a magnetic microreactor for reliable, fast and efficient surface functionalization of superparamagnetic iron oxide nanoparticles (SPIONs). A comprehensive study of the development process in terms of setup, loading capacity and efficiency is described.

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