Publications by authors named "Yebin Jung"

Colloidal porous AuAg alloyed nanoparticles (pAuAgNPs) were synthesized by galvanic replacement reaction from Ag nanocubes. pAuAgNPs have a 50 nm exterior diameter and half of their inner space consists of voids that have a bimodal size distribution with peaks at 21 and 8.3 nm.

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Article Synopsis
  • Recent advances in mass spectrometry imaging highlight the need for high-resolution techniques to better understand complex biomolecular interactions related to life and disease.
  • The study introduces a new multiplex protein imaging method using secondary ion mass spectrometry (SIMS) with metal oxide nanoparticle-conjugated antibodies, achieving less than 300 nm spatial resolution without damaging cells.
  • This technique was applied to hippocampal tissue samples from control and Alzheimer's disease model mice, revealing that the proximity of protein clusters in the brain is influenced by aging and disease progression, which could aid in understanding pathological mechanisms at the cellular level.
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In this study, we designed and synthesized far-red- and near-infrared-emitting Cu-doped InP-based quantum dots (QDs), and we also demonstrated their highly specific and sensitive biological imaging ability. Cu-doped InP/ZnS (core/shell) QDs were prepared using the hot colloidal synthesis method in the organic phase. The ZnS shell passivates the surface and improves the photoluminescence (PL) intensity.

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PbS/CdS core/shell quantum dots (QDs) that emit at the second near-infrared (NIR-II, 1000-1700 nm) window are synthesized. The PbS seed size and CdS shell thicknesses are carefully controlled to produce bright and narrow fluorescence that are suitable for multiplexing. A polymer encapsulation yields polymer-encapsulated NIR-II QDs (PQDs), which provides the QDs with long-term fluorescence stability over a week in biological media.

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RNA interference (RNAi) is a mechanism in which small interfering RNA (siRNA) silences a target gene. Herein, we describe a DNA hydrogel capable of producing siRNA and interfering with protein expression. This RNAi-exhibiting gel (termed I-gel for interfering gel) consists of a plasmid carrying the gene transcribing siRNA against the target mRNA as part of the gel scaffold.

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Article Synopsis
  • - Recent advancements in fluorescence imaging have progressed into the second near-infrared region (NIR-II), which allows for high-resolution imaging through deep tissues, although effective fluorophores are still limited in this region.
  • - The study introduces a new enzyme-activatable NIR-II probe that lights up in response to matrix metalloprotease activity within tumor environments, utilizing specially designed quantum dots (QDs) for enhanced brightness and stability.
  • - Experiments with a colon cancer mouse model showed that this probe provides targeted fluorescence signal activation at tumor sites, achieving a 3-fold increase in signal in just 10 minutes, outperforming traditional imaging dyes.
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Quantum dot (QD) imaging capability was investigated by the imaging depth at a near-infrared second optical window (SOW; 1000 to 1400 nm) using time-modulated pulsed laser excitations to control the effective fluence rate. Various media, such as liquid phantoms, tissues, and in vivo small animals, were used and the imaging depths were compared with our predicted values. The QD imaging depth under excitation of continuous 20 mW/cm(2) laser was determined to be 10.

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The detection of colon cancer using endoscopy is widely used, but the interpretation of the diagnosis is based on the clinician's naked eye. This is subjective and can lead to false detection. Here we developed a rapid and accurate molecular fluorescence imaging technique using antibody-coated quantum dots (Ab-QDs) sprayed and washed simultaneously on colon tumor tissues inside live animals, subsequently excited and imaged by endoscopy.

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Intravital imaging has provided molecular, cellular and anatomical insight into the study of tumor. Early detection and treatment of gastrointestinal (GI) diseases can be enhanced with specific molecular markers and endoscopic imaging modalities. We present a wide-field multi-channel fluorescence endoscope to screen GI tract for colon cancer using multiple molecular probes targeting matrix metalloproteinases (MMP) conjugated with quantum dots (QD) in AOM/DSS mouse model.

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