63 results on '"Sung Il Yang"'
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2. AI-Empowered Database Management Platform for New Materials Discovery for Consumer Electronics
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Taeyeop Kim, JaeSeong Lee, Jaeho Song, Dongwoo Lee, Jun-Chae Na, Sung-Il Yang, Kyong-Jin Park, Young-Jin Yoo, Juhye Lee, and Won-Yong Shin
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- 2023
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3. Improved waveform design for radar target classification
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Sung-Il Yang, Nathan A. Goodman, H. S. Kim, and Chankil Lee
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Computer science ,020206 networking & telecommunications ,02 engineering and technology ,Frequency deviation ,Radar lock-on ,01 natural sciences ,Upper and lower bounds ,010305 fluids & plasmas ,law.invention ,Continuous-wave radar ,Adaptive filter ,Radar engineering details ,law ,0103 physical sciences ,0202 electrical engineering, electronic engineering, information engineering ,Waveform ,Electrical and Electronic Engineering ,Radar ,Algorithm - Abstract
The information-theoretic waveform for target classification based on spectral variance has been studied, and its advantages have been shown. The waveform design algorithm has a low computational load and can be applied to real-time applications. In looking for more sophisticated methods while keeping the advantages of an information-based approach, a new design algorithm by deriving a strict lower bound of the information measure is developed. The proposed design algorithm requires a small amount of calculation and shows better classification performance in terms of percentage of correct detection. The proposed method is compared with other methods, and the improved performance is shown in numerically generated graphs.
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- 2017
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4. A parallel migration scheme for fast virtual machine relocation on a cloud cluster
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Chang-Ho Jeon, Chang-Hyeon Kim, Won Joo Lee, and Sung-Il Yang
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Scheme (programming language) ,Computer science ,business.industry ,Cloud computing ,Parallel computing ,computer.software_genre ,Theoretical Computer Science ,Hardware and Architecture ,Virtual machine ,Operating system ,Cluster (physics) ,business ,Relocation ,computer ,Software ,Information Systems ,computer.programming_language ,Live migration - Abstract
The paper proposes a method for parallelizing migrations to reduce the time required for virtual machine (VM) relocation. During VM relocation, VMs need to wait for their migrations in a chain due to the limited resource of the physical machines (PMs), lengthening the VM relocation time. The essence of the proposed scheme is to break off the VMs' chained migration wait and enables VM migrations to be performed in parallel. The VMs' chained migration wait can be broken off by allowing some VMs, called breakup VMs, to migrate without waiting. A breakup VM is the first VM in a chain of migrations with which the total migration time is reduced when the chain is split at that VM and performed in parallel. Breakup VMs are selected recursively from all the split migration chains until the total migration time can no longer be reduced. After all breakup VMs are selected, VMs' chained migrations are parallelized by temporarily migrating the breakup VMs to spare PMs regardless of their initial migration order. The performance of the proposed scheme is evaluated through simulation. The VM relocation time is affected by the number of VMs and PM utilization in a cluster. Therefore, we simulate relocations of 100---800 VMs in clusters with different average CPU and memory utilizations of PMs. The simulation results show that the proposed scheme reduces VM relocation time by 21.9---62.0 % while using 1.6---5.8 % spare PMs to parallelize the chained migrations.
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- 2015
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5. Synergistic activation of lipopolysaccharide-stimulated glial cells by propofol
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Hyun Myung Ko, Jae Hoon Cheong, Sung-Il Yang, So Yeon Kim, Bon Nyeo Koo, Chan Young Shin, and So Hyun Joo
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Lipopolysaccharides ,Programmed cell death ,Lipopolysaccharide ,Cell Survival ,MAP Kinase Kinase 4 ,p38 mitogen-activated protein kinases ,Interleukin-1beta ,Cell ,Biophysics ,Nitric Oxide Synthase Type II ,Pharmacology ,Nitric Oxide ,p38 Mitogen-Activated Protein Kinases ,Biochemistry ,Rats, Sprague-Dawley ,chemistry.chemical_compound ,medicine ,Animals ,Propofol ,Molecular Biology ,Cells, Cultured ,Cerebral Cortex ,Neurons ,Cell Death ,Dose-Response Relationship, Drug ,Interleukin-6 ,Cell Biology ,Rats ,medicine.anatomical_structure ,Matrix Metalloproteinase 9 ,chemistry ,Cell culture ,Astrocytes ,Immunology ,Anesthetic ,Cytokines ,Neuron ,Reactive Oxygen Species ,Neuroglia ,Anesthetics, Intravenous ,medicine.drug - Abstract
Despite the extensive use of propofol in general anesthetic procedures, the effects of propofol on glial cell were not completely understood. In lipopolysaccharide (LPS)-stimulated rat primary astrocytes and BV2 microglial cell lines, co-treatment of propofol synergistically induced inflammatory activation as evidenced by the increased production of NO, ROS and expression of iNOS, MMP-9 and several cytokines. Propofol augmented the activation of JNK and p38 MAPKs induced by LPS and the synergistic activation of glial cells by propofol was prevented by pretreatment of JNK and p38 inhibitors. When we treated BV2 cell culture supernatants treated with LPS plus propofol on cultured rat primary neuron, it induced a significant neuronal cell death. The results suggest that the repeated use of propofol in immunologically challenged situation may induce glial activation in brain.
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- 2013
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6. A Role of CPEB1 in the Modulation of Proliferation and Neuronal Maturation of Rat Primary Neural Progenitor Cells
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Sung-Il Yang, Ki Chan Kim, Jae Hoon Cheong, Chang Soon Choi, Seol-Heui Han, Sun Young Han, Geon Ho Bahn, Ji-Woon Kim, and Chan Young Shin
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Polyadenylation ,Aurora A kinase ,RNA-binding protein ,Biology ,Biochemistry ,Rats, Sprague-Dawley ,Cellular and Molecular Neuroscience ,Neural Stem Cells ,Pregnancy ,Animals ,Cyclin B1 ,Cells, Cultured ,Cell Proliferation ,DNA Primers ,Neurons ,Base Sequence ,Reverse Transcriptase Polymerase Chain Reaction ,Cell growth ,RNA-Binding Proteins ,Translation (biology) ,General Medicine ,Transfection ,Rats ,Cell biology ,Phosphorylation ,Female - Abstract
Cytoplasmic polyadenylation binding protein 1 (CPEB1) is a RNA binding protein, which regulates translation of target mRNAs by regulating polyadenylation status. CPEB1 plays important roles in the regulation of germline cell development by modulating cell cycle progression through the polyadenylation of target mRNAs such as cyclin B1. Similar mechanism is reported in proliferating astrocytes by us, although CPEB1 is involved in the transport of target mRNAs as well as local translation at dendritic spines. In this study, we found the expression of CPEB1 in cultured rat primary neural progenitor cells (NPCs). EGF stimulation of cultured NPCs induced rapid phosphorylation of CPEB1, a hallmark of CPEB1-dependent translational control along with cyclin B1 polyadenylation and translation. EGF-induced activation of ERK1/2 and Aurora A kinase was responsible for CPEB1 phosphorylation. Pharmacological inhibition studies suggested that ERK1/2 is involved in the activation of Aurora A kinase and regulation of CPEB1 phosphorylation in cultured NPCs. Long-term incubation in EGF resulted in the down-regulation of CPEB1 expression, which further increased expression of cyclin B1 and cell cycle progression. When we down-regulated the expression of CPEB1 in NPCs by siRNA transfection, the proliferation of NPCs was increased. Increased NPCs proliferation by down-regulation of CPEB1 resulted in eventual up-regulation of neuronal differentiation with increase in both pre- and post-synaptic proteins. The results from the present study may suggest the importance of translational control in the regulation of neuronal development, an emerging concept in many neurodevelopmental and psychiatric disorders such as autism spectrum disorder.
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- 2013
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7. Hepatitis B virus inhibits liver regeneration via epigenetic regulation of urokinase-type plasminogen activator
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Kyun-Hwan Kim, Kwang Pyo Kim, Baik Lin Seong, Seung Hwa Park, So Young Kwon, Sung Hyun Ahn, Keo Heun Lim, Yong Kwang Park, Doo Hyun Kim, Chan Young Shin, Eun Sook Park, and Sung Il Yang
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Male ,Hepatitis B virus ,medicine.medical_specialty ,viruses ,medicine.medical_treatment ,Mice, Transgenic ,In Vitro Techniques ,Biology ,medicine.disease_cause ,Cell Line ,DNA Methyltransferase 3A ,Epigenesis, Genetic ,Mice ,Internal medicine ,medicine ,Animals ,Hepatectomy ,Viral Regulatory and Accessory Proteins ,DNA (Cytosine-5-)-Methyltransferases ,Cell Proliferation ,Mice, Inbred BALB C ,Hepatology ,Hepatocyte Growth Factor ,Liver cell ,Hepatitis B ,Urokinase-Type Plasminogen Activator ,digestive system diseases ,Liver regeneration ,Liver Regeneration ,Disease Models, Animal ,HBx ,DNA, Viral ,Hepatocytes ,Trans-Activators ,Cancer research ,Hepatocyte growth factor ,Plasminogen activator ,Signal Transduction ,medicine.drug - Abstract
Liver regeneration after liver damage caused by toxins and pathogens is critical for liver homeostasis. Retardation of liver proliferation was reported in hepatitis B virus (HBV) X protein (HBx)-transgenic mice. However, the underlying mechanism of the HBx-mediated disturbance of liver regeneration is unknown. We investigated the molecular mechanism of the inhibition of liver regeneration using liver cell lines and a mouse model. The mouse model of acute HBV infection was established by hydrodynamic injection of viral DNA. Liver regeneration after partial hepatectomy was significantly inhibited in the HBV DNA-treated mice. Mechanism studies have revealed that the expression of urokinase-type plasminogen activator (uPA), which regulates the activation of hepatocyte growth factor (HGF), was significantly decreased in the liver tissues of HBV or HBx-expressing mice. The down-regulation of uPA was further confirmed using liver cell lines transiently or stably transfected with HBx and the HBV genome. HBx suppressed uPA expression through the epigenetic regulation of the uPA promoter in mouse liver tissues and human liver cell lines. Expression of HBx strongly induced hypermethylation of the uPA promoter by recruiting DNA methyltransferase (DNMT) 3A2. Conclusion: Taken together, these results suggest that infection of HBV impairs liver regeneration through the epigenetic dysregulation of liver regeneration signals by HBx. (Hepatology 2013;58:762–776)
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- 2013
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8. Valproic Acid Regulates α-Synuclein Expression through JNK Pathway in Rat Primary Astrocytes
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Kyu Suk Cho, Min Kyeong Kim, Jung Nam Kim, Sung Il Yang, Chan Young Shin, Seol Heui Han, Seung Hwa Park, So Hyun Joo, Chang Soon Choi, Jin Hee Park, He Jin Lee, Geon Ho Bahn, and Kyoung Ja Kwon
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animal diseases ,Pharmacology ,Biochemistry ,Neuroprotection ,chemistry.chemical_compound ,α-synuclein ,mental disorders ,Drug Discovery ,Valproic acid ,medicine ,Alpha-synuclein ,Valproic Acid ,business.industry ,JNK Pathway ,Acetylation ,Articles ,nervous system diseases ,medicine.anatomical_structure ,nervous system ,chemistry ,Molecular Medicine ,Phosphorylation ,lipids (amino acids, peptides, and proteins) ,α synuclein ,JNK ,Neuron ,business ,Stability ,medicine.drug - Abstract
Although the role of α-synuclein aggregation on Parkinson's disease is relatively well known, the physiological role and the regulatory mechanism governing the expression of α-synuclein are unclear yet. We recently reported that α-synuclein is expressed and secreted from cultured astrocytes. In this study, we investigated the effect of valproic acid (VPA), which has been suggested to provide neuroprotection by increasing α-synuclein in neuron, on α-synuclein expression in rat primary astrocytes. VPA concentrationdependently increased the protein expression level of α-synuclein in cultured rat primary astrocytes with concomitant increase in mRNA expression level. Likewise, the level of secreted α-synuclein was also increased by VPA. VPA increased the phosphorylation of Erk1/2 and JNK and pretreatment of a JNK inhibitor SP600125 prevented the VPA-induced increase in α-synuclein. Whether the increased α-synuclein in astrocytes is involved in the reported neuroprotective effects of VPA awaits further investigation.
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- 2013
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9. Transcriptional Upregulation of Plasminogen Activator Inhibitor-1 in Rat Primary Astrocytes by a Proteasomal Inhibitor MG132
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Jae Hoon Cheong, Sung-Il Yang, Kyu Suk Cho, Seol Heui Han, Geon Ho Bahn, Chan Young Shin, So Hyun Joo, Kyoung Ja Kwon, Ki Chan Kim, Se Jin Jeon, and Hahn Young Kim
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Pharmacology ,MAPK/ERK pathway ,MG132 ,Tissue plasminogen activator ,Lactacystin ,p38 ,Articles ,Biology ,Biochemistry ,Molecular biology ,Cell biology ,Plasminogen activator inhibitor-1 ,chemistry.chemical_compound ,chemistry ,Drug Discovery ,Proteasome inhibitor ,medicine ,Molecular Medicine ,Plasminogen activator ,Protein kinase B ,medicine.drug - Abstract
Plasminogen activator inhibitor-1 (PAI-1) is a member of serine protease inhibitor family, which regulates the activity of tissue plasminogen activator (tPA). In CNS, tPA/PAI-1 activity is involved in the regulation of a variety of cellular processes such as neuronal development, synaptic plasticity and cell survival. To gain a more insights into the regulatory mechanism modulating tPA/PAI-1 activity in brain, we investigated the effects of proteasome inhibitors on tPA/PAI-1 expression and activity in rat primary astrocytes, the major cell type expressing both tPA and PAI-1. We found that submicromolar concentration of MG132, a cell permeable peptide-aldehyde inhibitor of ubiquitin proteasome pathway selectively upregulates PAI-1 expression. Upregulation of PAI-1 mRNA as well as increased PAI-1 promoter reporter activity suggested that MG132 transcriptionally increased PAI-1 expression. The induction of PAI-1 downregulated tPA activity in rat primary astrocytes. Another proteasome inhibitor lactacystin similarly increased the expression of PAI-1 in rat primary astrocytes. MG132 activated MAPK pathways as well as PI3K/Akt pathways. Inhibitors of these signaling pathways reduced MG132-mediated upregulation of PAI-1 in varying degrees and most prominent effects were observed with SB203580, a p38 MAPK pathway inhibitor. The regulation of tPA/PAI-1 activity by proteasome inhibitor in rat primary astrocytes may underlie the observed CNS effects of MG132 such as neuroprotection.
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- 2013
10. Positive feedback regulation of Akt-FMRP pathway protects neurons from cell death
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Kwang Ho Ko, Sung-Il Yang, David G. Wells, Jong Hoon Ryu, Seung Hwa Park, Seol-Heui Han, Hahn Young Kim, Kyoung Ja Kwon, Chan Young Shin, Se Jin Jeon, Ji Woong Choi, and Jae Hoon Cheong
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congenital, hereditary, and neonatal diseases and abnormalities ,Programmed cell death ,biology ,Glutamate receptor ,Bcl-xL ,Biochemistry ,FMR1 ,nervous system diseases ,Cellular and Molecular Neuroscience ,medicine.anatomical_structure ,Apoptosis ,medicine ,biology.protein ,Neuron ,Protein kinase B ,Neuroscience ,PI3K/AKT/mTOR pathway - Abstract
J. Neurochem. (2012) 123, 226–238. Abstract Fragile X syndrome (FXS), the most common single genetic cause of mental retardation and autistic spectrum disease, occurs when FMR1 gene is mutated. FMR1 encodes fragile X mental retardation protein (FMRP) which regulates translation of mRNAs playing important roles in the development of neurons as well as formation and maintenance of synapses. To examine whether FMRP regulates cell viability, we induced apoptosis in rat primary cortical neurons with glutamate in vitro and with middle cerebral artery occlusion (MCAO) in striatal neurons in vivo. Both conditions elicited a rapid, but transient FMRP expression in neurons. This up-regulated FMRP expression was abolished by pre-treatment with PI3K and Protein Kinase B (Akt) inhibitors: LY294002, Akt inhibitor IV, and VIII. Reduced FMRP expression in vitro or in vivo using small hairpin Fmr1 virus exacerbated cell death by glutamate or MCAO, presumably via hypophosphorylation of Akt and reduced expression of B-cell lymphoma-extra large (Bcl-xL). However, over-expression of FMRP using enhanced green fluorescent protein (eGFP)-FMRP constructs alleviated cell death, increased Akt activity, and enhanced Bcl-xL production. The pro-survival role of Akt-dependent up-regulation of FMRP in glutamate-stimulated cultured neuron as well as in ischemic brain may have a clinical importance in FXS as well as in neurodegenerative disorders and traumatic brain injury.
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- 2012
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11. Oroxylin A Induces BDNF Expression on Cortical Neurons through Adenosine A2AReceptor Stimulation: A Possible Role in Neuroprotection
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Se Jin Jeon, Kyoung Ja Kwon, Jae Hoon Cheong, So Min Han, Sung Hoon Lee, Seung Hwa Park, Chan Young Shin, Ji Woong Choi, Jung-eun Seo, Seol-Heui Han, Haerang Bak, Kwang Ho Ko, Sung-Il Yang, and Jong Hoon Ryu
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Oroxylin A ,Synaptogenesis ,Adenosine A2A receptor ,Pharmacology ,CREB ,Biochemistry ,Neuroprotection ,chemistry.chemical_compound ,Drug Discovery ,Brain-derived neurotrophic factor ,biology ,Chemistry ,Articles ,Cell biology ,BDNF ,nervous system ,biology.protein ,Molecular Medicine ,Signal transduction ,CGS21680 ,ZM241385 ,Neurotrophin - Abstract
Oroxylin A is a flavone isolated from a medicinal herb reported to be effective in reducing the inflammatory and oxidative stresses. It also modulates the production of brain derived neurotrophic factor (BDNF) in cortical neurons by the transactivation of cAMP response element-binding protein (CREB). As a neurotrophin, BDNF plays roles in neuronal development, differentiation, synaptogenesis, and neural protection from the harmful stimuli. Adenosine A2A receptor colocalized with BDNF in brain and the functional interaction between A2A receptor stimulation and BDNF action has been suggested. In this study, we investigated the possibility that oroxylin A modulates BDNF production in cortical neuron through the regulation of A2A receptor system. As ex-pected, CGS21680 (A2A receptor agonist) induced BDNF expression and release, however, an antagonist, ZM241385, prevented oroxylin A-induced increase in BDNF production. Oroxylin A activated the PI3K-Akt-GSK-3β signaling pathway, which is inhibited by ZM241385 and the blockade of the signaling pathway abolished the increase in BDNF production. The physiological roles of oroxylin A-induced BDNF production were demonstrated by the increased neurite extension as well as synapse formation from neurons. Overall, oroxylin A might regulate BDNF production in cortical neuron through A2A receptor stimulation, which promotes cellular survival, synapse formation and neurite extension.
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- 2012
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12. Research on Characteristics of Field Uniformity in Reverberation Chamber Using Two TX Antennas
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Junghoon Kim, Sung-Kuk Lim, Songjun Lee, Sung-Il Yang, and Tae-Heon Jang
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Computer Networks and Communications ,Computer science ,business.industry ,Acoustics ,Electrical and Electronic Engineering ,Telecommunications ,business ,Software ,Field uniformity ,Electromagnetic reverberation chamber - Published
- 2012
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13. Energy Sensitive Bandpass Filter to Protect Ku-Band LNAs from HPEM Threats
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Jong-Wook Lee, Werner Arriola, Tae Heon Jang, Ihn Seok Kim, Sung Il Yang, and Kiho Kim
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Attenuator (electronics) ,Engineering ,HFSS ,business.industry ,Frequency band ,Amplifier ,Electrical engineering ,Condensed Matter Physics ,Ku band ,Band-pass filter ,Insertion loss ,Electrical and Electronic Engineering ,business ,Electronic circuit - Abstract
This letter introduces an energy sensitive bandpass filter (ESBPF) to protect Ku-band low noise amplifiers (LNAs) from high power electromagnetic (HPEM) threats. The ESBPF circuit has anti-parallel Schottky Barrier diodes mounted on a planar bandpass filter (BPF) circuit. The ESBPF operates as a BPF at a power level below the maximum permissible power level (MPPL) of the LNAs. However, the circuit works like a variable attenuator at the power level equal to or higher than the MPPL of the LNAs. To increase attenuation and selectivity functions, a 63 $^{\circ}$ line section between two planar filter circuits loaded transversely along WR-75 waveguide has been inserted to cascade. The development of the circuit model has been started with lumped elements under the condition of a 0 dBm MPPL of LNA. Then, the model has been simulated, optimized with HFSS, and fabricated. Measurement results show that the ESBPF has insertion loss less than 1.27 dB at the power level lower than $-$ 2 dBm for the frequency range from 11.8 to 12.3 GHz. At the power level higher than $-$ 2 dBm, the circuit provides different levels of attenuation depending on the input power within the identical frequency band; 31 dB insertion loss, which provides isolation characteristic, has been measured at the power level of 30 dBm.
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- 2015
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14. A retrospective study of 220 cases of keratocystic odontogenic tumor (KCOT) in 181 patients
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Chin-Soo Kim, Young-In Park, Jinwook Kim, Sung-Il Yang, and So-Young Choi
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medicine.medical_specialty ,business.industry ,medicine.medical_treatment ,Enucleation ,Nevoid basal-cell carcinoma syndrome ,Decortication ,medicine.disease ,Marsupialization ,Curettage ,Surgery ,Odontogenic cyst ,medicine ,Orthopedics and Sports Medicine ,Keratocystic Odontogenic Tumor ,Oral Surgery ,Keratocyst ,medicine.symptom ,business - Abstract
Odontogenic keratocyst is one of the most aggressive odontogenic cyst due to its relatively high recurrence rate, fast growth, and its tendency to invade adjacent tissue. The aim of the present study is to analyze retrospectively the clinico-pathological characteristics of the 220 KCOTs cases in 181 and find the relationship among the various factors. And the following data were obtained: patient age ranged from 8 to 77 years with an average of 33.06 years. There were 111 male and 70 female patients. The mandibular angle and ascending ramus was the most frequent site of KCOTs. Swelling, the most presenting sign, was noted in 97 cases, followed by the pain, 85 cases, and 78 cases showed no presenting signs and symptoms. On radiologic findings, the primary KCOTs appeared as a unilocular in 59 cases or multilocular in 39 cases. The KCOTs can achieve the size of which may vary from 1.0 cm to 13.0 cm, and the mean size was 4.07 cm. The KCOTs were associated with the displacement of impacted teeth, the mandibular third molar; 47 cases, was the most frequent impacted teeth. Four patients (2.21%) were confirmed to be associated with nevoid basal cell carcinoma syndrome. Enucleation or curettage was the most common employed treatment modality (164 cases), followed by marsupialization or decompression (17 cases), and lateral decortication (13 cases). The recurrence rate was 10.78%. Most of the recurrences (21 cases) were found during the first 5 years after the first treatment for the KCOTs.
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- 2011
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15. The critical period of valproate exposure to induce autistic symptoms in Sprague–Dawley rats
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Jae Hoon Cheong, Sung-Il Yang, Hyo Sang Go, Kwang Ho Ko, Ki Chan Kim, Pitna Kim, Chang Soon Choi, and Chan Young Shin
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medicine.medical_specialty ,Period (gene) ,Toxicology ,Rats, Sprague-Dawley ,Glycogen Synthase Kinase 3 ,Fetus ,Receptors, GABA ,Pregnancy ,Internal medicine ,medicine ,Animals ,Neural Tube Defects ,Autistic Disorder ,Social Behavior ,Psychiatry ,Prenatal exposure ,Electroshock ,Valproic Acid ,Glycogen Synthase Kinase 3 beta ,business.industry ,Neural tube ,General Medicine ,medicine.disease ,Rats ,Disease Models, Animal ,Endocrinology ,medicine.anatomical_structure ,Autism ,Anticonvulsants ,Female ,lipids (amino acids, peptides, and proteins) ,Live birth ,business ,Reproductive toxicity ,Social behavior ,medicine.drug - Abstract
Prenatal exposure to valproic acid (VPA) induces neural tube defects and impairment in social behaviors related to autistic spectrum disorder in newborns, which make it a useful animal model of autism. In this study, we compared the effects of different time window of prenatal valproic acid exposure for inducing the altered social behaviors relevant to autism from embryonic day 7 to embryonic day 15 in Sprague–Dawley rats to determine the critical periods for the impairment. Compared to E7, E9.5 and E15 exposure, VPA exposure at E12 showed most significant changes in behaviors over control animals with reduced sociability and social preference. E9.5 exposure to valproic acid showed strong reproductive toxicity including decrease in the number of live birth. In general, exposure at E15 showed only marginal effects on reproduction and social behaviors. Finally, VPA-exposed rats at E12 were more sensitive to electric shock than VPA-exposed rats at any other periods. These results suggested that E12 is the critical period in rats when valproate exposure has prominent effects for inducing the altered social behavior similar to human autistic behavior.
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- 2011
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16. The Field Uniformity Analysis in a Triangular Prism Reverberation Chamber with a QRD
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Junghoon Kim, Eugene Rhee, Hye-Kwang Kim, and Sung-Il Yang
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Electromagnetic field ,Electromagnetic testing ,Anechoic chamber ,Computer Networks and Communications ,Computer science ,Acoustics ,Finite-difference time-domain method ,Electromagnetic compatibility ,Reverberation room ,Diffuser (thermodynamics) ,Electric field ,Prism ,Triangular prism ,Electrical and Electronic Engineering ,Software ,Electromagnetic reverberation chamber - Abstract
This letter presents the field uniformity characteristics of a triangular prism reverberation chamber. A reverberation chamber that generally uses a stirrer to create a uniform electric field inside is an alternative to the semi-anechoic chamber for an electromagnetic compatibility test. To overcome the size and maintenance problems of a stirrer, we propose to replace it with a Quadratic Residue Diffuser which is commonly used in acoustics. To confirm that the diffuser is a valid alternative to the stirrer, a diffuser and an equilateral triangular prism reverberation chamber are designed and fabricated for 2.3-3.0GHz operation. To investigate the field uniformity characteristics by varying the location of the transmitting antenna, both simulation and measurement in the triangular prism reverberation chamber were also done at its two positions, respectively. A commercial program XFDTD 6.2, engaging the finite difference time domain (FDTD), is used for simulation and a cumulative probability distribution, which the IEC 61000-4-21 recommends, is used to evaluate the field uniformity. Both simulation and measurement results show that the field uniformity in the chamber satisfies the international standard requirement of ±6dB tolerance and ±3dB standard deviation, which means that a diffuser can be substituted for a stirrer.
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- 2011
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17. Influence of Land Use and Meteorological Factors for Evapotranspiration Estimation in the Coastal Urban Area
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Sung-Il Yang, Byung-Woo Kim, Dong-Hwan Kang, and Byung-Hyuk Kwon
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Hydrology ,Coefficient of determination ,Correlation coefficient ,Evapotranspiration ,Air temperature ,Environmental science ,Precipitation ,Longitude ,Atmospheric sciences ,Wind speed ,Latitude - Abstract
Actual evapotranspiration (AET) in the Suyeong-gu was estimated and correlations between AET and meteorological factors were analyzed. The study area was Suyeong-gu lay at the east longitude 05' 40" ~ 129 08' 08" and north latitude 07' 59" ~ 11' 01". The Kumryun mountain, the Bae mountain, the Suyeong river and the Suyeong bay are located on west, north, northeaster and south side in the study area, respectively. AET was estimated using precipitation (P), potential evapotranspiration (PET) and plant-available water coefficient. Meteorological factors to estimate PET were air temperature, dewpoint temperature, atmospheric pressure, duration of sunshine and mean wind speed (MWS). PET and AET were estimated by a method of Allen et al. (1998) and Zhang et al. (2001), respectively. PET was the highest value (564.45 mm/yr) in 2002 year, while it was the lowest value (449.95 mm/yr) in 2003 year. AET was estimated highest value (554.14 mm/yr) in 2002 year and lowest value (427.91 mm/yr) in 2003 year. Variations of PET and AET were similar. The linear regression function of AET as PET using monthly data was AET=0.87PET+3.52 and coefficient of determination was high, 0.75. In order to analyze relationship between the evapotranspiration and meteorological factors, correlation analysis using monthly data were accomplished. Correlation coefficient of AET-PET was 0.96 high, but they of AET-P and PET-P were very low. Correlation coefficients of AET-MWS and PET-MWS were 0.67 and 0.73, respectively. Thus, correlation between evapotranspiration and MWS was the highest among meteorological factors in Suyong-gu. This means that meteorological factor to powerfully effect for the variation of evapotranspiration was MWS. The linear regression function of AET as MWS was AET=84.73MWS+223.05 and coefficient of determination was 0.54. The linear regression function of PET as MWS was PET=83.83MWS+203.62 and coefficient of determination was 0.45.
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- 2010
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18. Optimization of Field Uniformity in a Reverberation Chamber Using Quadratic Residue Diffusers
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Junghoon Kim, Sung-Il Yang, and Joong-Geun Rhee
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Quadratic residue ,Computer Networks and Communications ,Computer science ,Acoustics ,Electrical and Electronic Engineering ,Software ,Electromagnetic reverberation chamber ,Field uniformity - Published
- 2010
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19. A Method of Expanding Operating Frequency Band in a Reverberating TEM Cell by Using a Wire Septum
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Eugene Rhee, Hye-Kwang Kim, Junghoon Kim, and Sung-Il Yang
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Optics ,Computer Networks and Communications ,business.industry ,Computer science ,Electric field ,Operating frequency ,Electromagnetic compatibility ,Maximum usable frequency ,Electrical and Electronic Engineering ,business ,Tem cell ,Software ,Transverse mode - Abstract
This paper presents a method of expanding the operating frequency band of a Reverberating TEM Cell (RTC) for electromagnetic compatibility (EMC) testing. To expand the operating frequency band of an RTC, this paper places a wire septum inside the cell instead of a solid septum. The maximum usable frequency (MUF) for TEM cell operation and the lowest usable frequency (LUF) for reverberating chamber operation with the wire septum are studied and compared with a conventional solid septum. The E field strengths inside the RTC are measured and evaluated. The measurement results show that the RTC with the wire septum have similar MUF to the RTC with a solid septum at TEM mode, but have much lower LUF at a reverberating mode, which proves that the operating frequency band of the RTC can be expanded by using the wire septum.
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- 2010
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20. Essential role of mitogen-activated protein kinase pathways in protease activated receptor 2-mediated nitric-oxide production from rat primary astrocytes
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Jae Ryun Ryu, Sung-Il Yang, Se Jin Jeon, Jong Hoon Ryu, Jae Hoon Cheong, Min Sik Choi, Chan Young Shin, Seol-Heui Han, Kwang Ho Ko, and Gyu Hwan Park
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MAPK/ERK pathway ,Cancer Research ,Cell Survival ,MAP Kinase Signaling System ,Physiology ,p38 mitogen-activated protein kinases ,Clinical Biochemistry ,Nitric Oxide Synthase Type II ,Biology ,Nitric Oxide ,Biochemistry ,Rats, Sprague-Dawley ,NF-KappaB Inhibitor alpha ,Animals ,Receptor, PAR-2 ,Trypsin ,Receptor ,Nitrites ,Protein Kinase C ,Protease-activated receptor 2 ,Protein kinase C ,Analysis of Variance ,Kinase ,NF-kappa B ,Proteolytic enzymes ,Molecular biology ,Rats ,Cell biology ,Astrocytes ,Mitogen-activated protein kinase ,biology.protein ,I-kappa B Proteins ,Mitogen-Activated Protein Kinases - Abstract
Protease-activated receptors (PARs) play important roles in the regulation of brain function such as neuroinflammation by transmitting the signal from proteolytic enzymes such as thrombin and trypsin. We and others have reported that a member of the family, PAR-2 is activated by trypsin, whose involvement in the neurophysiological process is increasingly evident, and is involved in the neuroinflammatory processes including morphological changes of astrocytes. In this study, we investigated the role of PAR-2 in the production of nitric oxide (NO) in rat primary astrocytes. Treatment of PAR-2 agonist trypsin increased NO production in a dose-dependent manner, which was mediated by the induction of inducible nitric-oxide synthase. The trypsin-mediated production of NO was mimicked by PAR-2 agonist peptide and reduced by either pharmacological PAR-2 antagonist peptide or by siRNA-mediated inhibition of PAR-2 expression, which suggests the critical role of PAR-2 in this process. NO production by PAR-2 was mimicked by PMA, a PKC activator, and was attenuated by Go6976, a protein kinase C (PKC) inhibitor. PAR-2 stimulation activated three subtypes of mitogen-activated protein kinases (MAPKs): extracellular signal-regulated kinase (ERK), c-Jun N-terminal kinase (JNK), and p38 MAPK. NO production by PAR-2 was blocked by inhibition of ERK, p38, and JNK pathways. PAR-2 stimulation also activated nuclear factor-kappaB (NF-kappaB) DNA binding and transcriptional activity as well as IkappaBalpha phosphorylation. Inhibitors of NF-kappaB pathway inhibited PAR-2-mediated NO production. In addition, inhibitors of MAPK pathways prevented transcriptional activation of NF-kappaB reporter constructs. These results suggest that PAR-2 activation-mediated NO production in astrocytes is transduced by the activation of MAPKs followed by NF-kappaB pathways.
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- 2009
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21. Speech Enhancement by Overweighting Gain with Nonlinear Structure in Wavelet Packet Transform
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Sung-Ill Jung, Sung-Il Yang, and Younghun Kwon
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Signal processing ,Computer Networks and Communications ,Computer science ,Speech recognition ,Noise reduction ,Intelligibility (communication) ,Speech processing ,Wavelet packet decomposition ,Speech enhancement ,Signal-to-noise ratio ,Wavelet ,Electrical and Electronic Engineering ,Sound quality ,Algorithm ,Software - Abstract
A sound quality enhancement method by overweighting gain of a nonlinear structure in a wavelet packet area is provided to restrain the generation of musical noise efficiently and ensure reliable intelligibility in an enhanced voice. A sound quality enhancement method by overweighting gain of a nonlinear structure in a wavelet packet area comprises the following steps of: generating a converting signal that a voice signal polluted by noise is converted by UWPT(Uniform Wavelet Packet Transform); calculating a relative size difference, which is an identifier for calculating a relative difference between the amount of noise existing in a sub band and the amount of a voice polluted by noise; calculating the overweighting gain of the nonlinear structure from the relative size difference; calculating a transformed time-varying gain function based on an LSL(Least-Squares Line) algorithm; and performing spectral subtraction using the transformed time-varying gain function.
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- 2007
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22. Automatically Extracting Unknown Translations Using Phrase Alignment
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Sung Il Yang and Jae Hoon Kim
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Phrase ,Computer science ,business.industry ,Speech recognition ,media_common.quotation_subject ,computer.software_genre ,Translation (geometry) ,Parallel corpora ,Quality (business) ,Language model ,Objective evaluation ,Artificial intelligence ,business ,computer ,Natural language processing ,media_common - Abstract
In this paper, we propose an automatic extraction model for unknown translations and implement an unknown translation extraction system using the proposed model. The proposed model as a phrase-alignment model is incorporated with three models: a phrase-boundary model, a language model, and a translation model. Using the proposed model we implement the system for extracting unknown translations, which consists of three parts: construction of parallel corpora, alignment of Korean and English words, extraction of unknown translations. To evaluate the performance of the proposed system we have established the reference corpus for extracting unknown translation, which comprises of 2,220 parallel sentences including about 1,500 unknown translations. Through several experiments, we have observed that the proposed model is very useful for extracting unknown translations. In the future, researches on objective evaluation and establishment of parallel corpora with good quality should be performed and studies on improving the performance of unknown translation extraction should be kept up.
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- 2007
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23. Power scheduling for distributed multiple-hypothesis detection by task-specific information
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Sung-Il Yang and Hyoung-soo Kim
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Mathematical optimization ,Multiple hypothesis ,Computer science ,Specific-information ,Pairwise comparison ,Fading ,Transmitter power output ,Scheduling (computing) ,Communication channel ,Power optimization - Abstract
We introduce a new information theoretic power allocation scheme applicable to distributed multiple-hypothesis detection systems communicating over slow fading channels. In earlier work, it was demonstrated that performance could be improved by adjusting transmit power to maximize the J-divergence measure of a binary detection system and the J-divergence method is extended for a distributed multiple-hypothesis detection system by defining pairwise sums of the J-divergences. However, the pairwise sum measure does not provide a tight bound. Basically, the more hypotheses we adopt, the less efficient the optimization is. Thus, we derive a more efficient classification-oriented information measure for power optimization of distributed multiple-hypothesis system by introducing a virtual decider variable. The virtual decider variable is directly related with classification task. Various numerical results are also shown to compare the performances.
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- 2015
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24. Adaptive Noise Estimation Using Least-Squares Line in Wavelet Packet Transform Domain
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Sung-il Jung, Sung-Il Yang, and Younghun Kwon
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Noise measurement ,Speech recognition ,Wavelet packet decomposition ,Background noise ,Gradient noise ,Noise ,symbols.namesake ,Signal-to-noise ratio ,Artificial Intelligence ,Hardware and Architecture ,Gaussian noise ,symbols ,Computer Vision and Pattern Recognition ,Value noise ,Electrical and Electronic Engineering ,Algorithm ,Software ,Mathematics - Abstract
In this letter, we suggest a noise estimation method which can be applied for speech enhancement in various noise environments. The proposed method consists of the following two main processes to analyze and estimate efficiently the noise from the noisy speech. First, a least-squares line is used, which is obtained by applying coefficient magnitudes in node with a uniform wavelet packet transform to a least squares method. Next, a differential forgetting factor and a correlation coefficient per subband are applied, where each subband consists of several nodes with the uniform wavelet packet transform. In particular, this approach has the ability to update noise estimation by using the estimated noise at the previous frame only instead of employing the statistical information of long past frames and explicit nonspeech frames detection consisted of noise signals. In objective assessments, we observed that the performance of the proposed method was better than that of the compared methods. Furthermore, our method showed a reliable result even at low SNR.
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- 2006
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25. Long-range correlations in Korean literary corpora
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Jongkwang Kim, Sowoon Kim, Younghun Kwon, Jaemi Bhan, Kunsang Lee, and Sung-Il Yang
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Grammar ,General Mathematics ,Applied Mathematics ,media_common.quotation_subject ,Existential quantification ,General Physics and Astronomy ,Statistical and Nonlinear Physics ,Arithmetic ,Linguistics ,Mathematics ,media_common ,Range (computer programming) - Abstract
Recently, Montemurro et al. showed that there would be a long-range correlation in Shakespeare’s 36 plays written in English. However it is not clear that similar result can be found in other language which has very different grammar structure from English. So we examine whether there exists a long-range correlation in Shakespeare’s plays translated into Korean which would have very different syntactic rules from English. Additionally, we perform the same experiment for 12 novels written by four Korean popular writers in order to see the difference due to the styles of the writers. As a result, we find Hurst’s exponents of 0.632 ± 0.03 in Shakespeare’s plays translated in Korean. Also we find the similar values of Hurst’s exponent even to the novels of the Korean popular writers. It implies that regardless of languages, there exists a long-range correlation in literary corpora.
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- 2006
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26. Identification and characterization of four novel peptide motifs that recognize distinct regions of the transcription factor CP2
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Bo Mee Chung, Ho Chul Kang, Chul Geun Kim, Ji Hyung Chae, Chan Gil Kim, and Sung-Il Yang
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Zinc finger ,Genetics ,Phage display ,RNA-binding protein ,Cell Biology ,Biology ,Biochemistry ,Protein–protein interaction ,Cell biology ,Globin ,Peptide library ,Molecular Biology ,Gene ,Peptide sequence - Abstract
Although ubiquitously expressed, the transcriptional factor CP2 also exhibits some tissue- or stage-specific activation toward certain genes such as globin in red blood cells and interleukin-4 in T helper cells. Because this specificity may be achieved by interaction with other proteins, we screened a peptide display library and identified four consensus motifs in numerous CP2-binding peptides: HXPR, PHL, ASR and PXHXH. Protein-database searching revealed that RE-1 silencing factor (REST), Yin-Yang1 (YY1) and five other proteins have one or two of these CP2-binding motifs. Glutathione S-transferase pull-down and coimmunoprecipitation assays showed that two HXPR motif-containing proteins REST and YY1 indeed were able to bind CP2. Importantly, this binding to CP2 was almost abolished when a double amino acid substitution was made on the HXPR sequence of REST and YY1 proteins. The suppressing effect of YY1 on CP2's transcriptional activity was lost by this point mutation on the HXPR sequence of YY1 and reduced by an HXPR-containing peptide, further supporting the interaction between CP2 and YY1 via the HXPR sequence. Mapping the sites on CP2 for interaction with the four distinct CP2-binding motifs revealed at least three different regions on CP2. This suggests that CP2 recognizes several distinct binding motifs by virtue of employing different regions, thus being able to interact with and regulate many cellular partners.
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- 2005
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27. Similar speaker recognition using nonlinear analysis
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Min-Hye Kim, Kunsang Lee, Sung-Il Yang, Y.H Kwon, Jung-Pa Seo, In-Chan Baek, and Sungwook Chang
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Computer science ,General Mathematics ,Applied Mathematics ,Feature vector ,Speech recognition ,General Physics and Astronomy ,Spectral space ,Word error rate ,Computer Science::Computation and Language (Computational Linguistics and Natural Language and Speech Processing) ,Statistical and Nonlinear Physics ,Speaker recognition ,Speaker diarisation ,Correlation ,Identification (information) ,Nonlinear system ,Computer Science::Sound - Abstract
Speech features of the conventional speaker identification system, are usually obtained by linear methods in spectral space. However, these methods have the drawback that speakers with similar voices cannot be distinguished, because the characteristics of their voices are also similar in spectral space. To overcome the difficulty in linear methods, we propose to use the correlation exponent in the nonlinear space as a new feature vector for speaker identification among persons with similar voices. We show that our proposed method surprisingly reduces the error rate of speaker identification system to speakers with similar voices.
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- 2004
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28. Synthesis andin vitro cytotoxicity of 2-alkylaminosubstituted quinoline derivatives
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Sung Il Yang, Heesoon Lee, Jeeman Lee, Sang-Hun Jung, Yurngdong Jahng, Seoung Soo Hong, and Jungsook Cho
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Organic Chemistry ,Quinoline ,In vitro cytotoxicity ,Antineoplastic Agents ,Pharmacology ,In vitro ,Structure-Activity Relationship ,chemistry.chemical_compound ,chemistry ,Cell culture ,Drug Discovery ,Quinolines ,Tumor Cells, Cultured ,medicine ,Humans ,Molecular Medicine ,Structure–activity relationship ,Doxorubicin ,Cytotoxicity ,Human cancer ,medicine.drug - Abstract
Eight 2-alkylaminosubstituted 5,8-dimethoxy-4-methylquinolines and nine 2-alkylaminosubstituted or 2,6-disubstituted 4-methylquinoline-5,8-diones were synthesized and evaluated in vitro cytotoxicity against four human cancer cell lines (HOP62, SK-OV-3, HCT15 and SF295).
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- 2000
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29. Heat Shock-Induced, Caspase-3-Independent Rapid Breakdown of Akt and Consequent Alteration of Its Total Phosphorylation/Activity Level
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Sung-Il Yang, Heung-Soo Choi, Hyo-Jung Mo, and Hong-Chang Lee
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Activity level ,Proto-Oncogene Proteins c-akt ,Biophysics ,Caspase 3 ,Protein Serine-Threonine Kinases ,Biochemistry ,Proto-Oncogene Proteins ,medicine ,Animals ,Phosphorylation ,Heat shock ,Molecular Biology ,Protein kinase B ,COS cells ,Chemistry ,Cell Biology ,Cell biology ,Electroporation ,Caspases ,Shock (circulatory) ,COS Cells ,medicine.symptom ,Heat-Shock Response - Abstract
The immediate effect of a 15-min heat shock was examined on the level and the activity of Akt. Following heat shock, the Akt level decreased by 15-70% in a temperature-dependent and phosphorylation status-independent manner. This decrease of Akt level was not prevented by caspase inhibitors. At 48 degrees C, the extent of the breakdown was so immense that the total phosphorylation/activity level of Akt was not increased over the control level, implying that the total cellular activity of Akt governed by the level and the molar activity does not necessarily undergo the ensuing change.
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- 2000
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30. Synthesis andin vitro cytotoxicity of 1-azaanthraquinone-3-carboxamides
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Sung-Il Yang, Heesoon Lee, and Chang-wook Lee
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Chemotherapy ,Antibiotics, Antineoplastic ,Chemistry ,medicine.medical_treatment ,Organic Chemistry ,Anthraquinones ,Cell Count ,Drug resistance ,Pharmacology ,Amides ,In vitro ,Doxorubicin ,Cell culture ,Active compound ,Drug Discovery ,Tumor Cells, Cultured ,medicine ,Humans ,Molecular Medicine ,Cytotoxic T cell ,Cytotoxicity ,medicine.drug - Abstract
Five 1-azaanthraquinone-3-carboxamides were synthesized and evaluated in vitro cytotoxicity against four human cancer cell lines. The most active compound, 7b, exhibited cytotoxic activity comparable to doxorubicin.
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- 1999
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31. Synthesis and in vitro evaluation of 7-dialkylaminomethylbenzo[ g ]quinoxaline-5,10-diones
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Kwon Namgoong, Jae-Kyung Jung, Jungsook Cho, Heesoon Lee, Sung-Il Yang, and Sungmoon Cho
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Tertiary amine ,Stereochemistry ,Clinical Biochemistry ,Drug Evaluation, Preclinical ,Substituent ,Pharmaceutical Science ,Biochemistry ,Chemical synthesis ,chemistry.chemical_compound ,Quinoxaline ,Cell Line, Tumor ,Quinoxalines ,Drug Discovery ,medicine ,Humans ,Cytotoxic T cell ,Doxorubicin ,Cytotoxicity ,Molecular Biology ,Chemistry ,Organic Chemistry ,General Medicine ,In vitro ,Cell culture ,Active compound ,Molecular Medicine ,Human cancer ,medicine.drug - Abstract
A series of benzo[g]quinoxaline-5,10-dione derivatives carrying a 7-dialkylaminomethyl substituent was synthesized and their in vitro cytotoxic activities were evaluated against four human cancer cell lines (HCT-15, SK-OV-3, MD-MB-468 and T-47D). The most active compound 9d showed cytotoxic activity comparable to that of doxorubicin against HCT-15 cancer cell line.
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- 2004
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32. The protein kinase encoded by the Akt proto-oncogene is a target of the PDGF-activated phosphatidylinositol 3-kinase
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Andrius Kazlauskas, Philip N. Tsichlis, Deborah K. Morrison, Thomas F. Franke, David R. Kaplan, Sung-Il Yang, Ketaki Datta, and Tung O. Chan
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Phosphatidylinositol 4,5-Diphosphate ,AKT1 ,AKT2 ,Biology ,Protein Serine-Threonine Kinases ,Models, Biological ,General Biochemistry, Genetics and Molecular Biology ,AKT3 ,Gene Expression Regulation, Enzymologic ,Wortmannin ,chemistry.chemical_compound ,Mice ,Phosphatidylinositol 3-Kinases ,Phosphatidylinositol Phosphates ,Proto-Oncogene Proteins ,Proto-Oncogenes ,Animals ,Receptors, Platelet-Derived Growth Factor ,Enzyme Inhibitors ,Protein kinase B ,PI3K/AKT/mTOR pathway ,Cells, Cultured ,Oncogene Proteins ,Platelet-Derived Growth Factor ,Sequence Homology, Amino Acid ,Akt/PKB signaling pathway ,Biochemistry, Genetics and Molecular Biology(all) ,Cell biology ,Rats ,Androstadienes ,Enzyme Activation ,Phosphotransferases (Alcohol Group Acceptor) ,chemistry ,Enzyme Induction ,ras Proteins ,Proto-Oncogene Proteins c-akt ,Phosphoinositide-dependent kinase-1 ,Signal Transduction - Abstract
The serine/threonine protein kinase encoded by the Akt proto-oncogene is catalytically inactive in serum-starved primary and immortalized fibroblasts. Here we show that Akt and the Akt-related kinase AKT2 are activated by PDGF. The activation was rapid and specific, and it was abrogated by mutations in the Akt Pleckstrin homology (PH) domain. The Akt activation was also shown to depend on PDGFRβ tyrosines Y740 and Y751, which bind phosphatidylinositol 3-kinase (PI 3-kinase) upon phosphorylation. Moreover, Akt activation was blocked by the PI 3-kinase-specific inhibitor wortmanin and the dominant inhibitory N17Ras. Conversely, Akt activity was induced following the addition of phosphatidylinositol-3-phosphate to Akt immunoprecipitates from serum-starved cells in vitro. These results identify Akt as a novel target of PI 3-kinase and suggest that the Akt PH domain may be a mediator of PI 3-kinase signaling.
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- 1995
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33. AH/PH Domain-Mediated Interaction between Akt Molecules and Its Potential Role in Akt Regulation
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D. K. Morrison, Philip N. Tsichlis, Thomas F. Franke, Ketaki Datta, Erica A. Golemis, D. R. Kaplan, Antonios M. Makris, Sung-Il Yang, and Tung O. Chan
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Proto-Oncogene Proteins c-akt ,Molecular Sequence Data ,AKT1 ,AKT2 ,Saccharomyces cerevisiae ,Plasma protein binding ,Protein Serine-Threonine Kinases ,Biology ,Structure-Activity Relationship ,Proto-Oncogene Proteins ,Animals ,Amino Acid Sequence ,Protein kinase A ,Molecular Biology ,Protein kinase B ,Cells, Cultured ,Kinase ,Cell Biology ,Recombinant Proteins ,Enzyme Activation ,Pleckstrin homology domain ,Biochemistry ,Mutation ,Protein Binding ,Research Article - Abstract
The cytoplasmic serine-threonine protein kinase coded for by the c-akt proto-oncogene features a protein kinase C-like catalytic domain and a unique NH2-terminal domain (AH domain). The AH domain is a member of a domain superfamily whose prototype was observed in pleckstrin (pleckstrin homology, or PH, domain). In this communication, we present evidence that the AH/PH domain is a domain of protein-protein interaction which mediates the formation of Akt protein complexes. The interaction between c-akt AH/PH domains is highly specific, as determined by the failure of this domain to bind AKT2. The AH/PH domain-mediated interactions depend on the integrity of the entire domain. Akt molecules with deletions of the NH2-terminal portion (amino acids 11 to 60) and AH/PH constructs with deletions of the C-terminal portion of this domain (amino acids 107 to 147) fail to interact with c-akt. To determine the significance of these findings, we carried out in vitro kinase assays using Akt immunoprecipitates from serum-starved and serum-starved, platelet-derived growth factor-stimulated NIH 3T3 cells. Addition of maltose-binding protein-AH/PH fusion recombinant protein, which is expected to bind Akt, to the immunoprecipitates from serum-starved cells induced the activation of the Akt kinase.
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- 1995
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34. Positive feedback regulation of Akt-FMRP pathway protects neurons from cell death
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Se Jin, Jeon, Seol-Heui, Han, Sung-Il, Yang, Ji Woong, Choi, Kyoung Ja, Kwon, Seung Hwa, Park, Hahn Young, Kim, Jae Hoon, Cheong, Jong Hoon, Ryu, Kwang Ho, Ko, David G, Wells, and Chan Young, Shin
- Subjects
Feedback, Physiological ,Male ,Neurons ,Cell Death ,Cell Survival ,Apoptosis ,Infarction, Middle Cerebral Artery ,Rats ,Fragile X Mental Retardation Protein ,Animals ,Rats, Wistar ,Proto-Oncogene Proteins c-akt ,Cells, Cultured ,Signal Transduction - Abstract
J. Neurochem. (2012) 123, 226-238.Fragile X syndrome (FXS), the most common single genetic cause of mental retardation and autistic spectrum disease, occurs when FMR1 gene is mutated. FMR1 encodes fragile X mental retardation protein (FMRP) which regulates translation of mRNAs playing important roles in the development of neurons as well as formation and maintenance of synapses. To examine whether FMRP regulates cell viability, we induced apoptosis in rat primary cortical neurons with glutamate in vitro and with middle cerebral artery occlusion (MCAO) in striatal neurons in vivo. Both conditions elicited a rapid, but transient FMRP expression in neurons. This up-regulated FMRP expression was abolished by pre-treatment with PI3K and Protein Kinase B (Akt) inhibitors: LY294002, Akt inhibitor IV, and VIII. Reduced FMRP expression in vitro or in vivo using small hairpin Fmr1 virus exacerbated cell death by glutamate or MCAO, presumably via hypophosphorylation of Akt and reduced expression of B-cell lymphoma-extra large (Bcl-xL). However, over-expression of FMRP using enhanced green fluorescent protein (eGFP)-FMRP constructs alleviated cell death, increased Akt activity, and enhanced Bcl-xL production. The pro-survival role of Akt-dependent up-regulation of FMRP in glutamate-stimulated cultured neuron as well as in ischemic brain may have a clinical importance in FXS as well as in neurodegenerative disorders and traumatic brain injury.
- Published
- 2012
35. Comparison of heterotrimeric protein phosphatase 2A containing different B subunits
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Marc C. Mumby, Sung-Il Yang, R. Estes, R. L. Lickteig, Craig Kamibayashi, and Cheryl M. Craft
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Biochemistry ,Histone H1 ,Heterotrimeric G protein ,Protein subunit ,Phosphatase ,Alpha (ethology) ,Cell Biology ,Protein phosphatase 2 ,Biology ,Beta (finance) ,Molecular Biology ,G alpha subunit - Abstract
Protein phosphatase 2A (PP2A) is composed of structural (A), catalytic (C), and regulatory subunits (B). Immunological analyses identified B alpha/PR55 alpha as the major regulatory subunit of brain PP2A while a unique B' subunit was associated with the cardiac enzyme. Recombinant PP2A heterotrimers were purified from insect cells infected with baculoviruses expressing A and C, in combination with viruses expressing B alpha/PR55 alpha, B beta/PR55 beta, or SV40 small tumor antigen (st). Phosphatase activities of rAC-B alpha and rAC-B beta were similar to those for brain AC-B alpha, while rAC-st was 50-80% less active. Heparin had no effect on rAC-st myosin light chain phosphatase activity, while the B subunit-containing forms were stimulated 2-3-fold. Protamine caused a 3-4-fold increase in AC-B alpha and rAC-st activities and a marked activation of rAC-B beta (6-fold) and AC-B' (10.5-fold). When histone H1 was used as substrate, all of the heterotrimers were stimulated approximately 4-fold by heparin. The activity of AC-B' and rAC-B beta were increased 2-fold by Mn2+, while a 6-fold stimulation was observed with rAC-st. Chemical cross-linking of AC-B alpha and AC-B beta generated 200-kDa complexes, while AC-st was present as a 150-kDa complex. These results demonstrate that different regulatory proteins affect enzyme activity and the response to agents that modify PP2A activity in vitro. Different PP2A heterotrimers are likely to have distinct functions in vivo, and changes in subunit composition will have an important impact on signal transduction pathways.
- Published
- 1994
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36. Activation of adenosine A2A receptor up-regulates BDNF expression in rat primary cortical neurons
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Sung-Il Yang, Jong Hoon Ryu, Seol-Heui Han, Jongmin Lee, Chan Young Shin, So Young Rhee, Hahn Young Kim, Seung Hwa Park, Jae Hoon Cheong, Kwang Ho Ko, Kyung-Ja Kwon, and Se Jin Jeon
- Subjects
Adenosine ,Adenosine A2 Receptor Agonists ,Receptor, Adenosine A2A ,Excitotoxicity ,Synaptogenesis ,Adenosine A2A receptor ,Tropomyosin receptor kinase B ,medicine.disease_cause ,Biochemistry ,δ-opioid receptor ,Rats, Sprague-Dawley ,Cellular and Molecular Neuroscience ,Glycogen Synthase Kinase 3 ,Phenethylamines ,medicine ,Animals ,Cells, Cultured ,Brain-derived neurotrophic factor ,Cerebral Cortex ,Neurons ,Glycogen Synthase Kinase 3 beta ,biology ,Chemistry ,Brain-Derived Neurotrophic Factor ,General Medicine ,Adenosine A3 receptor ,Adenosine A2 Receptor Antagonists ,Rats ,Up-Regulation ,nervous system ,biology.protein ,Neuroscience ,Neurotrophin ,Signal Transduction - Abstract
As a member of neurotrophin family, brain derived neurotrophic factor (BDNF) plays critical roles in neuronal development, differentiation, synaptogenesis, and neural protection from the harmful stimuli. There have been reported that adenosine A2(A) receptor subtype is widely distributed in the brain regions, such as hippocampus, striatum, and cortex. Adenosine A2(A) receptor is colocalized with BDNF in brain regions and the functional interaction between A2(A) receptor stimulation and BDNF action has been suggested. In this study, we investigated the possibility that the activation of A2(A) receptor modulates BDNF production in rat primary cortical neuron. CGS21680, an adenosine A2(A) receptor agonist, induced BDNF expression and release. An antagonist against A2(A) receptor, ZM241385, prevented CGS21680-induced increase in BDNF production. A2(A) receptor stimulation induced the activation of Akt-GSK-3β signaling pathway and the blockade of the signaling pathway with specific inhibitors abolished the increase in BDNF production, possibly via modulation of ERK1/2-CREB pathway. The physiological roles of A2(A) receptor-induced BDNF production was demonstrated by the protection of neurons from the excitotoxicity and increased neurite extension as well as synapse formation from immature and mature neurons. Taken together, activation of A2(A) receptor regulates BDNF production in rat cortical neuron, which provides neuro-protective action.
- Published
- 2011
37. Cellular stress-induced up-regulation of FMRP promotes cell survival by modulating PI3K-Akt phosphorylation cascades
- Author
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Sung-Il Yang, Jung Eun Seo, Ji Woong Choi, Kwang Ho Ko, David G. Wells, Chan Young Shin, and Se Jin Jeon
- Subjects
congenital, hereditary, and neonatal diseases and abnormalities ,Cell Survival ,Endocrinology, Diabetes and Metabolism ,Clinical Biochemistry ,bcl-X Protein ,lcsh:Medicine ,Biology ,Small hairpin RNA ,chemistry.chemical_compound ,Fragile X Mental Retardation Protein ,Phosphatidylinositol 3-Kinases ,Stress, Physiological ,Gene silencing ,Humans ,Pharmacology (medical) ,Propidium iodide ,Protein kinase B ,Molecular Biology ,PI3K/AKT/mTOR pathway ,Etoposide ,Biochemistry, medical ,Research ,lcsh:R ,Biochemistry (medical) ,General Medicine ,Transfection ,Cell Biology ,FMR1 ,Antineoplastic Agents, Phytogenic ,nervous system diseases ,Up-Regulation ,chemistry ,Fragile X Syndrome ,Cancer research ,Signal transduction ,Proto-Oncogene Proteins c-akt ,HeLa Cells ,Signal Transduction - Abstract
Background Fragile X syndrome (FXS), the most commonly inherited mental retardation and single gene cause of autistic spectrum disorder, occurs when the Fmr1 gene is mutated. The product of Fmr1, fragile X linked mental retardation protein (FMRP) is widely expressed in HeLa cells, however the roles of FMRP within HeLa cells were not elucidated, yet. Interacting with a diverse range of mRNAs related to cellular survival regulatory signals, understanding the functions of FMRP in cellular context would provide better insights into the role of this interesting protein in FXS. Using HeLa cells treated with etoposide as a model, we tried to determine whether FMRP could play a role in cell survival. Methods Apoptotic cell death was induced by etoposide treatment on Hela cells. After we transiently modulated FMRP expression (silencing or enhancing) by using molecular biotechnological methods such as small hairpin RNA virus-induced knock down and overexpression using transfection with FMRP expression vectors, cellular viability was measured using propidium iodide staining, TUNEL staining, and FACS analysis along with the level of activation of PI3K-Akt pathway by Western blot. Expression level of FMRP and apoptotic regulator BcL-xL was analyzed by Western blot, RT-PCR and immunocytochemistry. Results An increased FMRP expression was measured in etoposide-treated HeLa cells, which was induced by PI3K-Akt activation. Without FMRP expression, cellular defence mechanism via PI3K-Akt-Bcl-xL was weakened and resulted in an augmented cell death by etoposide. In addition, FMRP over-expression lead to the activation of PI3K-Akt signalling pathway as well as increased FMRP and BcL-xL expression, which culminates with the increased cell survival in etoposide-treated HeLa cells. Conclusions Taken together, these results suggest that FMRP expression is an essential part of cellular survival mechanisms through the modulation of PI3K, Akt, and Bcl-xL signal pathways.
- Published
- 2010
38. ChemInform Abstract: Synthesis and in vitro Cytotoxicity of 3-Substituted-1,8-diazaanthraquinones Produced by Lewis-Acid Catalyzed Hetero Diels-Alder Reaction
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Sung-Il Yang, Seung-Il Lee, and Heesoon Lee
- Subjects
Chemistry ,In vitro cytotoxicity ,Regioselectivity ,General Medicine ,Medicinal chemistry ,In vitro ,Catalysis ,chemistry.chemical_compound ,medicine ,Doxorubicin ,Lewis acids and bases ,Diels–Alder reaction ,medicine.drug ,Methyl group - Abstract
A hetero Diels-Alder reaction of quinoline-5,8-dione with 1-(N,N-dimethylamino)-3-methyl-1-aza-1,3-butadiene proceeded to give 3-methyl-1,8-diazaanthraquinone (100% regioselectivity) in the presence of Lewis-acid catalyst (ZnCl2 or ZnBr2). Subsequent functionalizations of the benzylic methyl group resulted in the 1,8-diazaanthraquinone analogues as potential antitumor agents. The most active compound, 8, exhibited in vitro cytotoxic activity comparable to that of doxorubicin.
- Published
- 2010
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39. Akt regulates the expression of MafK, synaptotagmin I, and syntenin-1, which play roles in neuronal function
- Author
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Chul Geun Kim, Chan Young Shin, Eui U Park, Young-Tae Ro, Sung-Il Yang, and Bo-Kwang Jang
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Neurite ,Syntenins ,Endocrinology, Diabetes and Metabolism ,Clinical Biochemistry ,lcsh:Medicine ,Biology ,Small hairpin RNA ,Animals ,Pharmacology (medical) ,Molecular Biology ,Protein kinase B ,Cells, Cultured ,PI3K/AKT/mTOR pathway ,MafK Transcription Factor ,Neurons ,Biochemistry, medical ,Regulation of gene expression ,Oncogene ,Research ,lcsh:R ,Biochemistry (medical) ,Synaptotagmin I ,Cell Biology ,General Medicine ,Molecular biology ,Rats ,Cell biology ,Gene Expression Regulation ,nervous system ,Proto-Oncogene Proteins c-akt - Abstract
Background Akt regulates various cellular processes, including cell growth, survival, and metabolism. Recently, Akt's role in neurite outgrowth has also emerged. We thus aimed to identify neuronal function-related genes that are regulated by Akt. Methods We performed suppression subtractive hybridization on two previously established PC12 sublines, one of which overexpresses the wild-type (WT) form and the other, the dominant-negative (DN) form of Akt. These sublines respond differently to NGF's neuronal differentiation effect. Results A variety of genes was identified and could be classified into several functional groups, one of which was developmental processes. Two genes involved in neuronal differentiation and function were found in this group. v-Maf musculoaponeurotic fibrosarcoma oncogene homolog K (MafK) induces the neuronal differentiation of PC12 cells and immature telencephalon neurons, and synaptotagmin I (SytI) is essential for neurotransmitter release. Another gene, syntenin-1 (Syn-1) was also recognized in the same functional group into which MafK and SytI were classified. Syn-1 has been reported to promote the formation of membrane varicosities in neurons. Quantitative reverse transcription polymerase chain reaction analyses show that the transcript levels of these three genes were lower in PC12 (WT-Akt) cells than in parental PC12 and PC12 (DN-Akt) cells. Furthermore, treatment of PC12 (WT-Akt) cells with an Akt inhibitor resulted in the increase of the expression of these genes and the improvement of neurite outgrowth. These results indicate that dominant-negative or pharmacological inhibition of Akt increases the expression of MafK, SytI, and Syn-1 genes. Using lentiviral shRNA to knock down endogenous Syn-1 expression, we demonstrated that Syn-1 promotes an increase in the numbers of neurites and branches. Conclusions Taken together, these results indicate that Akt negatively regulates the expression of MafK, SytI, and Syn-1 genes that all participate in regulating neuronal integrity in some way or another.
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- 2010
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40. A novel T-shaped slot PIFA for MIMO applications
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Mian Abdul Razzaq, Joong-Geun Rhee, Sung-Il Yang, and Muhammad Shoaib Khalid
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Physics ,Microstrip antenna ,Channel capacity ,business.industry ,MIMO ,Bandwidth (signal processing) ,Electrical engineering ,Return loss ,Standing wave ratio ,Omnidirectional antenna ,business ,Radiation pattern - Abstract
Because of rapidly increasing demand for high capacity communication services compact antennas have become center of research interest nowadays and this reduction of size becomes much more important especially when we want to use the multiple-input multiple-output (MIMO) technology; to increase channel capacity, in modern compact devices. Microstrip antennas are an attractive option due to low cost, and small size. However to fulfill need for more compact and miniaturized devices; a dual feed dual element planar inverted-F antenna (PIFA) at 2.45GHz has been proposed on a very small PCB (60 mm × 20 mm × 0.8 mm), to be used for ISM 2.45 GHz band. While total volume occupied by two antennas is 10 mm × 20 mm × 2.5 mm. −10 dB return loss or VSWR=2 criterion for required bandwidth has been satisfied, only with help of designing a novel radiation structure. To miniaturize size of PIFA a novel T-shaped slot has been employed in radiation structure. Overall size is compact than small MIMO antennas, available in open literature. As the proposed design is suitable for different feeding environments, it can be used in different small size PCB devices, for different applications. Results show satisfactory bandwidth, and omnidirectional radiation pattern.
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- 2009
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41. Substitution at rt269 in Hepatitis B Virus Polymerase Is a Compensatory Mutation Associated with Multi-Drug Resistance
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Gu Choul Shin, Ah Ram Lee, Hong Seok Kang, Sung Il Yang, Kyun-Hwan Kim, Eun Sook Park, Sung Hyun Ahn, Sang Hoon Ahn, Yong Kwang Park, Doo Hyun Kim, Jin Kyu Rhee, Youhoon Chong, Beom Kyung Kim, and Soree Park
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Models, Molecular ,Hepatitis B virus ,Guanine ,Organophosphonates ,lcsh:Medicine ,Gene Products, pol ,Microbial Sensitivity Tests ,Drug resistance ,Biology ,Virus Replication ,medicine.disease_cause ,Antiviral Agents ,Hepatitis B, Chronic ,Drug Resistance, Multiple, Viral ,Cell Line, Tumor ,medicine ,Adefovir ,Humans ,Hepatitis B e Antigens ,lcsh:Science ,Tenofovir ,Hepatitis B Surface Antigens ,Multidisciplinary ,Adenine ,Point mutation ,lcsh:R ,Arabinofuranosyluracil ,Lamivudine ,Entecavir ,Hepatitis B ,medicine.disease ,Virology ,Molecular biology ,Amino Acid Substitution ,Clevudine ,lcsh:Q ,Research Article ,medicine.drug - Abstract
The emergence of compensatory mutations in the polymerase gene of drug resistant hepatitis B virus (HBV) is associated with treatment failure. We previously identified a multi-drug resistant HBV mutant, which displayed resistance towards lamivudine (LMV), clevudine (CLV), and entecavir (ETV), along with a strong replication capacity. The aim of this study was to identify the previously unknown compensatory mutations, and to determine the clinical relevance of this mutation during antiviral therapy. In vitro mutagenesis, drug susceptibility assay, and molecular modeling studies were performed. The rtL269I substitution conferred 2- to 7-fold higher replication capacity in the wild-type (WT) or YMDD mutation backbone, regardless of drug treatment. The rtL269I substitution alone did not confer resistance to LMV, ETV, adefovir (ADV), or tenofovir (TDF). However, upon combination with YMDD mutation, the replication capacity under LMV or ETV treatment was enhanced by several folds. Molecular modeling studies suggested that the rtL269I substitution affects template binding, which may eventually lead to the enhanced activity of rtI269-HBV polymerase in both WT virus and YMDD mutant. The clinical relevance of the rtL269I substitution was validated by its emergence in association with YMDD mutation in chronic hepatitis B (CHB) patients with sub-optimal response or treatment failure to LMV or CLV. Our study suggests that substitution at rt269 in HBV polymerase is associated with multi-drug resistance, which may serve as a novel compensatory mutation for replication-defective multi-drug resistant HBV.
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- 2015
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42. Speech Enhancement by Wavelet Packet Transform with Best Fitting Regression Line in Various Noise Environments
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Younghun Kwon, Sung-Il Yang, and Sung-il Jung
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Speech enhancement ,Noise ,Estimation theory ,business.industry ,Mean opinion score ,Detector ,Spectrogram ,Wavelet transform ,Pattern recognition ,Artificial intelligence ,business ,Wavelet packet decomposition ,Mathematics - Abstract
In this paper, we suggest a speech enhancement method which can be applied in various noise environments. This method uses a wavelet packet transform (WPT) and a best fitting regression line (BFRL) in order to accurately estimate parameters for the spectral subtraction method based on the time-varying gain function. It should be noted that our method does not use the statistical information of pause region detected by voice activity detector. The evaluation is performed on various environments where the noisy speech are between SNR -5 ∼ 15 dB, in various noises. We compare the performance of the proposed method, with that of magnitude spectral subtraction in WPT and nonlinear magnitude spectral subtraction in WPT. We can see that the performance of the proposed method is better than that of any other methods, with regard to objective test (segmental SNR, weighted spectral slope), spectrogram analysis, and subjective one (mean opinion score). Especially, our method showed reliable result even at low SNR.
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- 2006
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43. Identification and characterization of four novel peptide motifs that recognize distinct regions of the transcription factor CP2
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Ho Chul, Kang, Bo Mee, Chung, Ji Hyung, Chae, Sung-Il, Yang, Chan Gil, Kim, and Chul Geun, Kim
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Sequence Homology, Amino Acid ,Transcription, Genetic ,Recombinant Fusion Proteins ,Molecular Sequence Data ,RNA-Binding Proteins ,Zinc Fingers ,DNA ,Peptide Fragments ,DNA-Binding Proteins ,Repressor Proteins ,Amino Acid Substitution ,Gene Expression Regulation ,Peptide Library ,Mutagenesis, Site-Directed ,Erythroid-Specific DNA-Binding Factors ,Humans ,Immunoprecipitation ,Point Mutation ,Amino Acid Sequence ,Luciferases ,Cells, Cultured ,YY1 Transcription Factor ,Transcription Factors - Abstract
Although ubiquitously expressed, the transcriptional factor CP2 also exhibits some tissue- or stage-specific activation toward certain genes such as globin in red blood cells and interleukin-4 in T helper cells. Because this specificity may be achieved by interaction with other proteins, we screened a peptide display library and identified four consensus motifs in numerous CP2-binding peptides: HXPR, PHL, ASR and PXHXH. Protein-database searching revealed that RE-1 silencing factor (REST), Yin-Yang1 (YY1) and five other proteins have one or two of these CP2-binding motifs. Glutathione S-transferase pull-down and coimmunoprecipitation assays showed that two HXPR motif-containing proteins REST and YY1 indeed were able to bind CP2. Importantly, this binding to CP2 was almost abolished when a double amino acid substitution was made on the HXPR sequence of REST and YY1 proteins. The suppressing effect of YY1 on CP2's transcriptional activity was lost by this point mutation on the HXPR sequence of YY1 and reduced by an HXPR-containing peptide, further supporting the interaction between CP2 and YY1 via the HXPR sequence. Mapping the sites on CP2 for interaction with the four distinct CP2-binding motifs revealed at least three different regions on CP2. This suggests that CP2 recognizes several distinct binding motifs by virtue of employing different regions, thus being able to interact with and regulate many cellular partners.
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- 2005
44. Synthesis and in vitro cytotoxicity of- 1,3-dioxoindan-2-carboxylic acid arylamides
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Heesoon Lee, Jae-Kyung Jung, Sung Il Yang, Jungsook Cho, and Jinhyeong Ryu
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chemistry.chemical_classification ,Stereochemistry ,Cell Survival ,Carboxylic acid ,Organic Chemistry ,Pharmacology toxicology ,In vitro cytotoxicity ,Substituent ,Antineoplastic Agents ,Amides ,In vitro ,chemistry.chemical_compound ,Structure-Activity Relationship ,chemistry ,Cell culture ,Cell Line, Tumor ,Drug Discovery ,Indans ,Molecular Medicine ,Humans ,Drug Screening Assays, Antitumor ,Cytotoxicity ,Human cancer - Abstract
A series of 1,3-dioxoindan-2-carboxylic acid arylamides were synthesized and evaluated for in vitro cytotoxicity against four human cancer cell lines (HOP62, SK-OV-3, MD-MB-468 and T-47D). The most active was compound 3e (1.2 microM against SK-OV-3 cell line) bearing a 4-methyl substituent.
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- 2004
45. Transcription factor CP2 is involved in activating mBMP4 in mouse mesenchymal stem cells
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Ho Chul, Kang, Ji Hyung, Chae, Beom Sue, Kim, Su Youne, Han, Sung-Hyun, Kim, Chung-Kyoon, Auh, Sung-Il, Yang, and Chul Geun, Kim
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Base Sequence ,Transcription, Genetic ,Molecular Sequence Data ,RNA-Binding Proteins ,Cell Differentiation ,Mesenchymal Stem Cells ,Bone Morphogenetic Protein 4 ,DNA-Binding Proteins ,Mice ,Gene Expression Regulation ,Bone Morphogenetic Proteins ,Animals ,RNA ,Databases, Nucleic Acid ,Luciferases ,Promoter Regions, Genetic ,Transcription Factors - Abstract
CP2 is a member of a family of transcription factors that regulate genes involved in events from early development to terminal differentiation. In an effort to understand how it selects its target genes we carried out a database search, and located several CP2 binding motifs in the promoter region of bone morphogenetic protein-4 (BMP4). BMP4 is a key regulator of cell fate and body patterning throughout development. For the CP2 binding motifs in BMP4 promoter region to be relevant in vivo, CP2 and BMP4 should be expressed together. We found that CP2b and CP2c, two potent transcriptional activators, are expressed in a manner similar to BMP4 during osteoblast differentiation of C3H10T1/2 cells. In in vitro assays, the CP2 proteins bound to two CP2 binding motifs (-715 to -676 and -147 to -118) in the BMP4 promoter, and luciferase reporter assays indicated that this binding was essential for transcription of BMP4 during osteoblast differentiation. Taken together, our data indicate that CP2b and CP2c play important roles during bone development by activating BMP4 transcription.
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- 2004
46. Synthesis and in vitro Evaluation of 1,8-Diazaanthraquinones Bearing 3-Dialkylaminomethyl or 3-(N-Alkyl- or N-Aryl)carbamoyloxymethyl Substituent
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Sung-Il Yang, Sang Un Choi, Seung-Il Lee, Jungsook Cho, and Heesoon Lee
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Tertiary amine ,Stereochemistry ,Substituent ,Anthraquinones ,Antineoplastic Agents ,Chemical synthesis ,Inhibitory Concentration 50 ,Structure-Activity Relationship ,chemistry.chemical_compound ,Cell Line, Tumor ,Drug Discovery ,medicine ,Humans ,Topoisomerase II Inhibitors ,Structure–activity relationship ,Cytotoxic T cell ,Doxorubicin ,Cytotoxicity ,Pharmacology ,biology ,Topoisomerase ,Aryl ,Organic Chemistry ,General Medicine ,In vitro ,Biochemistry ,chemistry ,Cell culture ,biology.protein ,Drug Screening Assays, Antitumor ,Cell Division ,medicine.drug - Abstract
A series of 1,8-diazaanthraquinone derivatives carrying a 3-dialkylaminomethyl or a 3-(N-alkyl or aryl)carbamoyloxymethyl substituent was synthesised and their in vitro cytotoxic activities were evaluated against eight human cancer cell lines (HOP62, SK-OV-3, HCT-15, SF295, MCF7, SNU-354, KB-3-1 and KB-V-1). A number of compounds including 8c, 8d and 11c showed cytotoxic activity comparable to that of doxorubicin against all human cancer cell lines tested. The compounds 8c and 8d were 2-100 times more potent than doxorubicin against HCT-15, MCF7 and SNU-354 cancer cell lines. Furthermore, these compounds retained considerable cytotoxic activity against the doxorubicin-resistant cell line KB-V-1, implying their therapeutic potential to treat doxorubicin-resistant tumours. These compounds inhibited topoisomerase II-mediated DNA relaxation in vitro, suggesting that this inhibitory effect be attributable to their cytotoxicity.
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- 2004
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47. Speaker verification system using hybrid model with pitch detection by wavelets
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Hyoung-soo Kim, Hojung Nam, Y. Kwon, and Sung-Il Yang
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Discrete wavelet transform ,Computer science ,business.industry ,Speech recognition ,Second-generation wavelet transform ,Stationary wavelet transform ,Wavelet transform ,Pattern recognition ,Pitch detection algorithm ,Wavelet packet decomposition ,Wavelet ,Artificial intelligence ,Harmonic wavelet transform ,business - Abstract
For speaker-verification, we design a hybrid-recognizer composed of conventional methods (such as HMM, MLP, and DTW) as pre-recognizer and pitch-detection method through wavelet transforms as post-recognizer. Conventional methods have respectively 3 classes of feature vectors; LSF, cepstrum, and filter bank. The pitch carries information about speaker identification, which is obtained by wavelet analysis. Wavelet analysis has advantages over traditional Fourier methods in analyzing physical situations where a signal contains discontinuities and sharp spikes, etc. The pitches in speech analysis are composed of impulses, so that a wavelet transform for detection of the pitch period can be used. This system can analyze pitch period under various noisy environments.
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- 2002
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48. Real-time moving automotive vehicle identification system (AVIS)
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Myung-Ryul Choi, Seung-Ho Tak, Jin-Sung Park, Woo-Gyun Shin, Young-Jin Shin, Sung-Il Yang, Hyun Jin Kim, and Ho-Jun Lee
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Engineering ,Signal processing ,Scanner ,business.industry ,Automotive industry ,Image processing ,Vehicle identification ,Optical scanners ,Computer vision ,Artificial intelligence ,business ,Automatic vehicle identification ,Digital signal processing ,Computer hardware - Abstract
A real-time moving automotive vehicle identification system (AVIS) has been developed for intelligent vehicle highway systems (IVHS). AVIS consists of 3 major elements: invisible bar-code material, optical scanner, and DSP board. The invisible bar-code material reflects only the specific wavelength light (1500 nm). The optical scanner developed can read the invisible bar-code data only at the corresponding wavelength light. The TI TMS320C31 digital signal processing (DSP) board has been implemented. The DSP board processes the bar-code data obtained from the optical scanner through the invisible bar-code. The DSP board operates at 33 MHz with the image processing algorithm which includes error-detecting and error-correcting capabilities. The system has been tested and the results show that the AVIS performed successfully. The AVIS is expected to be applied to the non-stop toll gate and violation enforcement system.
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- 2002
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49. Denoising on adapted wavelet packets domain for robust speech recognition
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Sungwook Chang, Y. Kwon, and Sung-Il Yang
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symbols.namesake ,Wavelet ,Formant ,Additive white Gaussian noise ,Computer Science::Sound ,Computer science ,Robustness (computer science) ,Network packet ,Speech recognition ,Noise reduction ,symbols ,Wavelet transform ,Wavelet packet decomposition - Abstract
In a real environment, additive noise will corrupt input speech for speech recognition. In this paper, the authors propose a noise suppression method on the wavelet packet domain as a front-end pre-processor for robust speech recognition. They focus on the enhancement of the formant characteristic to input speech. Suppose, one has observations y/sub i/=f(t/sub i/)+ /spl sigma//spl middot/z/sub i/, i=0, 1, ..., n-1, where f(t/sub i/) is the speech signal and z/sub i/ is i.i.d. white Gaussian noise (AWGN). And assume that one has an available library L of orthogonal bases, such as wavelet packet bases. Using these assumptions, the authors enhance the formant characteristic as well as SNR by adjusting each node variance from adapted wavelet packet transform (AWPT) tree. Experimental result shows an enhancement of SNR from 3.58 dB to 8.66 dB. Also, phoneme recognition performance is improved more than 6%. It confirms the robustness of proposed noise suppression method against additive white Gaussian noise.
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- 2002
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50. Speech enhancement using adaptive wavelet shrinkage
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Sung-Il Yang, I-jae Kim, and Y. Kwon
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Threshold limit value ,business.industry ,Bayesian probability ,Wiener filter ,Wavelet transform ,Pattern recognition ,Speech enhancement ,symbols.namesake ,symbols ,Entropy (information theory) ,Artificial intelligence ,business ,Mathematics ,Shrinkage ,Active noise control - Abstract
In this paper, the authors propose an adaptive wavelet threshold for noise cancellation. For this, they use a threshold value which minimizes Bayesian risk. And using entropy, they part the noisy signal into an unvoiced signal section and the other signal section is used to apply each the threshold value for each section. Experimental results show that proposed algorithm is more efficient.
- Published
- 2002
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