59 research outputs found

    Innovative Cyanine-Based Fluorescent Dye for Targeted Mitochondrial Imaging and Its Utility in Whole-Brain Visualization

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    Conducting in vivo brain imaging can be a challenging task due to the complexity of brain tissue and the strict requirements for safe and effective imaging agents. However, a new fluorescent dye called Cy5-PEG2 has been developed that selectively accumulates in mitochondria, enabling the visualization of these essential organelles in various cell lines. This dye is versatile and can be used for the real-time monitoring of mitochondrial dynamics in living cells. Moreover, it can cross the blood-brain barrier, making it a promising tool for noninvasive in vivo brain imaging. Based on the assessment of glial cell responses in the hippocampus and neocortex regions using GFAP and Iba1 biomarkers, Cy5-PEG2 seems to have minimal adverse effects on brain immune response or neuronal health. Therefore, this mitochondria-targeting fluorescent dye has the potential to advance our understanding of mitochondrial dynamics and function within the broader context of whole-brain physiology and disease progression. However, further research is needed to evaluate the safety and efficacy of Cy5-PEG2

    Induction of Neuroinflammation and Brain Oxidative Stress by Brain-Derived Extracellular Vesicles from Hypertensive Rats

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    Neuroinflammation and brain oxidative stress are recognized as significant contributors to hypertension including salt sensitive hypertension. Extracellular vesicles (EVs) play an essential role in intercellular communication in various situations, including physiological and pathological ones. Based on this evidence, we hypothesized that EVs derived from the brains of hypertensive rats with salt sensitivity could trigger neuroinflammation and oxidative stress during hypertension development. To test this hypothesis, we compared the impact of EVs isolated from the brains of hypertensive Dahl Salt-Sensitive rats (DSS) and normotensive Sprague Dawley (SD) rats on inflammatory factors and mitochondrial reactive oxygen species (mtROS) production in primary neuronal cultures and brain cardiovascular relevant regions, including the hypothalamic paraventricular nucleus (PVN) and lamina terminalis (LT). We found that brain-derived DSS-EVs significantly increased the mRNA levels of proinflammatory cytokines (PICs) and chemokines, including TNFĪ±, IL1Ī², CCL2, CCL5, and CCL12, as well as the transcriptional factor NF-ĪŗB in neuronal cultures. DSS-EVs also induced oxidative stress in neuronal cultures, as evidenced by elevated NADPH oxidase subunit CYBA coding gene mRNA levels and persistent mtROS elevation. When DSS-EVs were injected into the brains of normal SD rats, the mRNA levels of PICs, chemokines, and the chronic neuronal activity marker FOSL1 were significantly increased in the PVN and LT. Furthermore, DSS-EVs caused mtROS elevation in brain PVN and LT, particularly in neurons. Our study reveals a novel role for brain-derived EVs from hypertensive rats in triggering neuroinflammation, upregulating chemokine expression, and inducing excessive ROS production. These findings provide insight into the complex interactions between EVs and hypertension-associated processes, offering potential therapeutic targets for hypertension-linked neurological complications

    Modulate Molecular Interaction between Hole Extraction Polymers and Lead Ions toward Hysteresis-Free and Efficient Perovskite Solar Cells

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    Herein three polymeric hole extraction materials (HEMs), poly(benzeneā€dithiophene) (PB2T)ā€O, PB2Tā€S, and PB2Tā€SO are presented for pā€“iā€“n perovskite solar cells (PVSCs). This study reveals that the perovskite device hysteresis and performance heavily rely on the perovskite grain boundary conditions. More specifically, they are predetermined through the molecular interaction between Lewis base atoms of HEMs and perovskites. It is revealed that only changing the side chain terminals (-OCH_3, -SCH_3, and ā€“SOCH_3) of HEMs results in effective modulating PVSC performance and hysteresis, due to the effective tune of interaction strength between HEM and perovskite. With an in situ grown perovskiteā€HEM bulk heterojunction structure, PB2Tā€O with weak binding group (-OCH_3, āˆ’78.9 kcal mol^(āˆ’1) bonding energy) to lead ions allows delivering hysteresisā€free and efficient devices, which is sharp contrast to the strong binding PB2Tā€SO (āˆ’119.3 kcal mol^(āˆ’1) bonding energy). Overall, this work provides new insights on PVSC hysteresis and the related curing methods via multifunctional HEM design in PVSCs

    Conductive 3D nano-biohybrid systems based on densified carbon nanotube forests and living cells

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    Conductive biohybrid cell-material systems have applications in bioelectronics and biorobotics. To date, conductive scaffolds are limited to those with low electrical conductivity or 2D sheets. Here, 3D biohybrid conductive systems are developed using fibroblasts or cardiomyocytes integrated with carbon nanotube (CNT) forests that are densified due to interactions with a gelatin coating. CNT forest scaffolds with a height range of 120ā€“240 Āµm and an average electrical conductivity of 0.6 S/cm are developed and shown to be cytocompatible as evidenced from greater than 89% viability measured by live-dead assay on both cells on day 1. The cells spread on top and along the height of the CNT forest scaffolds. Finally, the scaffolds have no adverse effects on the expression of genes related to cardiomyocyte maturation and functionality, or fibroblast migration, adhesion, and spreading. The results show that the scaffold could be used in applications ranging from organ-on-a-chip systems to muscle actuators. Graphical abstract: [Figure not available: see fulltext.
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