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1. Differential susceptibility of cells infected with defective and intact HIV proviruses to killing by obatoclax and other small molecules

Author

Kadiyala, Gayatri Nikhila, Telwatte, Sushama, Wedrychowski, Adam, Janssens, Julie, Kim, Sun Jin, Kim, Peggy, Deeks, Steven, Wong, Joseph K, and Yukl, Steven A

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Infectious Diseases, Sexually Transmitted Infections, Genetics, 5.1 Pharmaceuticals, 6.1 Pharmaceuticals, Infection, Humans, Indoles, HIV Infections, Pyrroles, Leukocytes, Mononuclear, Proviruses, apoptosis, Bcl-2, DNA, HIV, IAP, interferon, mTOR, PD-1, proteasome, RIG-I, TLR7, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Virology, Biomedical and clinical sciences, Health sciences
Abstract

ObjectivesSome drugs that augment cell-intrinsic defenses or modulate cell death/survival pathways have been reported to selectively kill cells infected with HIV or Simian Immunodeficiency Virus (SIV), but comparative studies are lacking. We hypothesized that these drugs may differ in their ability to kill cells infected with intact and defective proviruses.DesignTo investigate this hypothesis, drugs were tested ex vivo on peripheral blood mononuclear cells (PBMC) from nine antiretroviral therapy (ART)-suppressed individuals.MethodsWe tested drugs currently in clinical use or human trials, including auranofin (p53 modulator), interferon alpha2A, interferon gamma, acitretin (RIG-I inducer), GS-9620/vesatolimod (TLR7 agonist), nivolumab (PD-1 blocker), obatoclax (Bcl-2 inhibitor), birinapant [inhibitor of apoptosis proteins (IAP) inhibitor], bortezomib (proteasome inhibitor), and INK128/sapanisertib [mammalian target of rapamycin mTOR] [c]1/2 inhibitor). After 6 days of treatment, we measured cell counts/viabilities and quantified levels of total, intact, and defective HIV DNA by droplet digital PCR (Intact Proviral DNA Assay).ResultsObatoclax reduced intact HIV DNA [median = 27-30% of dimethyl sulfoxide control (DMSO)] but not defective or total HIV DNA. Other drugs showed no statistically significant effects.ConclusionObatoclax and other Bcl-2 inhibitors deserve further study in combination therapies aimed at reducing the intact HIV reservoir in order to achieve a functional cure and/or reduce HIV-associated immune activation.

Published
2024

2. Digital Protein Detection in Bulk Solutions

Author

Beck, Sungjun, Shin, Donghae, Kim, Sun Jin, Hedde, Per Niklas, and Zhao, Weian

Subjects
Analytical Chemistry, Chemical Sciences, Biotechnology, Infection, Chemical Engineering, Materials Engineering, Macromolecular and materials chemistry, Physical chemistry, Chemical engineering
Abstract

Quick and accurate molecular diagnostics in protein detection can greatly benefit medicine in disease diagnosis and lead to positive patient outcomes. However, specialized equipment used in clinical laboratories often comes with trade-offs between operation and function serving a single role for very specific needs. For example, to achieve high analytical sensitivity and specificity, instruments such as high-performance liquid chromatography and/or liquid chromatography-mass spectrometry use a complex instrument design and require thorough training of the users. On the other hand, simple tests such as protein detection in urinary tract infection using dip-stick assays provide very quick results but suffer from poor analytical sensitivity. Here, we present an application study for the 3D particle counter technology, which is based on optical confocal detection in order to scan large sample volumes (0.5-3 mL) in glass cuvettes, that aims to close the gap between analytical sensitivity and turnover assay time and simplify protein detection by adopting bead-based immunoassays. Combining the 3D particle counter technology with bead-based immunoassays, a subpicomolar limit of detection-ranging from 119 to 346 fM-was achieved within 3.5-hour assay time for recombinant mouse interleukin 6 detection. As an alternative instrument to a flow cytometer, the 3D particle counter takes advantages of bead-based immunoassays and provides unique accessibility and flexibility for users.

Published
2022

3. A Protein Microarray-Based Respiratory Viral Antigen Testing Platform for COVID-19 Surveillance.

Author

Beck, Sungjun, Nakajima, Rie, Jasinskas, Algis, Abram, Timothy J, Kim, Sun Jin, Bigdeli, Nader, Tifrea, Delia F, Hernandez-Davies, Jenny, Huw Davies, D, Hedde, Per Niklas, Felgner, Philip L, and Zhao, Weian

Subjects
SARS-CoV-2, antibody microarray, antigen test, immunofluorescence assay, portable imager, protein biotinylation, tyramide signal amplification, Vaccine Related, Biodefense, Health Services, Emerging Infectious Diseases, Biotechnology, Prevention, Clinical Research, Infectious Diseases, Immunization, Pneumonia & Influenza, Lung, Influenza, 5.1 Pharmaceuticals, 4.2 Evaluation of markers and technologies, Development of treatments and therapeutic interventions, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, Infection
Abstract

High-throughput and rapid screening testing is highly desirable to effectively combat the rapidly evolving COVID-19 pandemic co-presents with influenza and seasonal common cold epidemics. Here, we present a general workflow for iterative development and validation of an antibody-based microarray assay for the detection of a respiratory viral panel: (a) antibody screening to quickly identify optimal reagents and assay conditions, (b) immunofluorescence assay design including signal amplification for low viral titers, (c) assay characterization with recombinant proteins, inactivated viral samples and clinical samples, and (d) multiplexing to detect a panel of common respiratory viruses. Using RT-PCR-confirmed SARS-CoV-2 positive and negative pharyngeal swab samples, we demonstrated that the antibody microarray assay exhibited a clinical sensitivity and specificity of 77.2% and 100%, respectively, which are comparable to existing FDA-authorized antigen tests. Moreover, the microarray assay is correlated with RT-PCR cycle threshold (Ct) values and is particularly effective in identifying high viral titers. The multiplexed assay can selectively detect SARS-CoV-2 and influenza virus, which can be used to discriminate these viral infections that share similar symptoms. Such protein microarray technology is amenable for scale-up and automation and can be broadly applied as a both diagnostic and research tool.

Published
2022

12. A homogeneous split-luciferase assay for rapid and sensitive detection of anti-SARS CoV-2 antibodies

Author

Yao, Zhong, Drecun, Luka, Aboualizadeh, Farzaneh, Kim, Sun Jin, Li, Zhijie, Wood, Heidi, Valcourt, Emelissa J., Manguiat, Kathy, Plenderleith, Simon, Yip, Lily, Li, Xinliu, Zhong, Zoe, Yue, Feng Yun, Closas, Tatiana, Snider, Jamie, Tomic, Jelena, Drews, Steven J., Drebot, Michael A., McGeer, Allison, Ostrowski, Mario, Mubareka, Samira, Rini, James M., Owen, Shawn, and Stagljar, Igor

Published
2021
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13. Increased 90-Day Mortality and Morbidity Among Patients Recovering From Elective Primary Arthroplasty During the COVID-19 Pandemic in New York City.

Author

Mizera, Megan M., Seref-Ferlengez, Zeynep, Tarasova, Anna, Mostafa, Evan, Kamara, Eli, and Kim, Sun Jin

Subjects
MEDICAL research, HEALTH care industry, ARTHROPLASTY, COVID-19 pandemic
Abstract

All elective procedures were stopped in March 2020 because of the coronavirus disease 2019 (COVID-19) pandemic. We report the 90-day mortality and complications of patients who underwent primary arthroplasty before the stopping of elective procedures at a single academic medical center. A retrospective cohort study was conducted including patients who underwent elective primary arthroplasty between December 2019 and mid-March 2020. Their 90-day postoperative mortality and medical complications were statistically compared with those of a historical cohort from the same operative period in 2019. The 2020 and 2019 cohorts included 372 and 410 patients, respectively. Except for the prevalence of diabetes, there was no significant difference between the two cohorts regarding baseline characteristics or preoperative health. The 2020 cohort had statistically significant higher rates of pneumonia (2.7% vs 0.7%; P=.03), readmission (9.1% vs 5.4%; P=.04), pulmonary embolism (1.6% vs 0.2%; P=.04), and 90-day mortality (1.1% vs 0%; P=.04). The 2020 cohort also had a trend for increased rates of deep venous thrombosis (1.1% vs 0.7%; P=.7) and cardiac complications (1.9% vs 0.5%; P=.07) and no change in emergency department visits (14.0% vs 11.7%; P=.3). There were 7 confirmed cases of COVID-19 in the 2020 cohort and 1 death. This study demonstrates that patients who underwent primary arthroplasty procedures at our institution close to the time of the first wave of the COVID-19 pandemic experienced a statistically significant increase in mortality, pneumonia, pulmonary embolism, and readmission compared with a historical cohort. As elective procedures have resumed during the ongoing pandemic, providers and patients should be aware of these increased risks. [Orthopedics. 2024;47(3):135–140.] [ABSTRACT FROM AUTHOR]

Published
2024
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22. Supplementary Figure 3 from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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23. Supplementary Table and Figures from Characterization of CD45−/CD31+/CD105+ Circulating Cells in the Peripheral Blood of Patients with Gynecologic Malignancies

Author

Yu, Hyun-Kyung, primary, Lee, Ho-Jeong, primary, Choi, Ha-Na, primary, Ahn, Jin-Hyung, primary, Choi, Ji-Young, primary, Song, Haeng-Seok, primary, Lee, Ki-Heon, primary, Yoon, Yeup, primary, Yi, Lee S. H., primary, Kim, Jang-Seong, primary, Kim, Sun Jin, primary, and Kim, Tae Jin, primary

Published
2023
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24. Supplementary Figure 4 from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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25. Supplementary Figure 1 from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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26. Supplementary Figure 6 from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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27. Supplementary Figure 5 from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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28. Supplementary Figure 2 from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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29. Supplementary Figure Legends from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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30. Data from Macitentan, a Dual Endothelin Receptor Antagonist, in Combination with Temozolomide Leads to Glioblastoma Regression and Long-term Survival in Mice

Author

Kim, Sun-Jin, primary, Lee, Ho Jeong, primary, Kim, Mark Seungwook, primary, Choi, Hyun Jin, primary, He, Junqin, primary, Wu, Qiuyu, primary, Aldape, Kenneth, primary, Weinberg, Jeffrey S., primary, Yung, W.K. Alfred, primary, Conrad, Charles A., primary, Langley, Robert R., primary, Lehembre, François, primary, Regenass, Urs, primary, and Fidler, Isaiah J., primary

Published
2023
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31. Data from Gain of Glucose-Independent Growth upon Metastasis of Breast Cancer Cells to the Brain

Author

Chen, Jinyu, primary, Lee, Ho-Jeong, primary, Wu, Xuefeng, primary, Huo, Lei, primary, Kim, Sun-Jin, primary, Xu, Lei, primary, Wang, Yan, primary, He, Junqing, primary, Bollu, Lakshmi R., primary, Gao, Guang, primary, Su, Fei, primary, Briggs, James, primary, Liu, Xiaojing, primary, Melman, Tamar, primary, Asara, John M., primary, Fidler, Isaiah J., primary, Cantley, Lewis C., primary, Locasale, Jason W., primary, and Weihua, Zhang, primary

Published
2023
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32. Supplemental Table 1 from Gain of Glucose-Independent Growth upon Metastasis of Breast Cancer Cells to the Brain

Author

Chen, Jinyu, primary, Lee, Ho-Jeong, primary, Wu, Xuefeng, primary, Huo, Lei, primary, Kim, Sun-Jin, primary, Xu, Lei, primary, Wang, Yan, primary, He, Junqing, primary, Bollu, Lakshmi R., primary, Gao, Guang, primary, Su, Fei, primary, Briggs, James, primary, Liu, Xiaojing, primary, Melman, Tamar, primary, Asara, John M., primary, Fidler, Isaiah J., primary, Cantley, Lewis C., primary, Locasale, Jason W., primary, and Weihua, Zhang, primary

Published
2023
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33. Supplementary Figure S2 from Gain of Glucose-Independent Growth upon Metastasis of Breast Cancer Cells to the Brain

Author

Chen, Jinyu, primary, Lee, Ho-Jeong, primary, Wu, Xuefeng, primary, Huo, Lei, primary, Kim, Sun-Jin, primary, Xu, Lei, primary, Wang, Yan, primary, He, Junqing, primary, Bollu, Lakshmi R., primary, Gao, Guang, primary, Su, Fei, primary, Briggs, James, primary, Liu, Xiaojing, primary, Melman, Tamar, primary, Asara, John M., primary, Fidler, Isaiah J., primary, Cantley, Lewis C., primary, Locasale, Jason W., primary, and Weihua, Zhang, primary

Published
2023
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36. Supplementary Figure 1 from Gain of Glucose-Independent Growth upon Metastasis of Breast Cancer Cells to the Brain

Author

Chen, Jinyu, primary, Lee, Ho-Jeong, primary, Wu, Xuefeng, primary, Huo, Lei, primary, Kim, Sun-Jin, primary, Xu, Lei, primary, Wang, Yan, primary, He, Junqing, primary, Bollu, Lakshmi R., primary, Gao, Guang, primary, Su, Fei, primary, Briggs, James, primary, Liu, Xiaojing, primary, Melman, Tamar, primary, Asara, John M., primary, Fidler, Isaiah J., primary, Cantley, Lewis C., primary, Locasale, Jason W., primary, and Weihua, Zhang, primary

Published
2023
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45. Route Selection and Rate Allocation Using Evolutionary Computation Algorithms in Multirate Multicast Networks

Author

Kim, Sun-Jin, Choi, Mun-Kee, Hutchison, David, editor, Kanade, Takeo, editor, Kittler, Josef, editor, Kleinberg, Jon M., editor, Mattern, Friedemann, editor, Mitchell, John C., editor, Naor, Moni, editor, Nierstrasz, Oscar, editor, Pandu Rangan, C., editor, Steffen, Bernhard, editor, Sudan, Madhu, editor, Terzopoulos, Demetri, editor, Tygar, Dough, editor, Vardi, Moshe Y., editor, Weikum, Gerhard, editor, Carbonell, Jaime G., editor, Siekmann, Jörg, editor, Gelbukh, Alexander, editor, and Reyes-Garcia, Carlos Alberto, editor

Published
2006
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