Your search keyword '"Moo Yeol Lee"' showing total 7 results

1. Arsenic May Act as a Pro-Metastatic Carcinogen Through Promoting Tumor Cell-Induced Platelet Aggregation

Author

Ok-Nam Bae, Keunyoung Kim, Soyoung Chun, Kyung Min Lim, Yoon-Kyung Heo, Chang-Hwan Kim, Moo-Yeol Lee, Yiying Bian, and Jin Ho Chung

Subjects

Blood Platelets, 0301 basic medicine, Platelet Aggregation, Platelet Glycoprotein GPIIb-IIIa Complex, Toxicology, medicine.disease_cause, Arsenic, Metastasis, Mice, 03 medical and health sciences, 0302 clinical medicine, In vivo, Cell Line, Tumor, Cell Adhesion, Animals, Medicine, Platelet, Platelet activation, Neoplasm Metastasis, Melanoma, Carcinogen, Aspirin, business.industry, Platelet Activation, medicine.disease, Extravasation, Mice, Inbred C57BL, 030104 developmental biology, Metalloproteases, Cancer research, business, Carcinogenesis, Platelet Aggregation Inhibitors, 030217 neurology & neurosurgery

Abstract

Arsenic-associated carcinogenesis and related mortality are a major public health concern worldwide; however, the underlying mechanism of action remains unclear. Here, we demonstrated that arsenic promotes tumor metastasis by stimulating tumor cell-platelet aggregation (TCPA), which can ultimately increase cancer-related mortality. In freshly isolated human platelets in vitro, arsenic potentiated TCPA prompted by diverse cancer cell lines, which was attributable to increased platelet reactivity to TCPA with respect to thrombin generation and P-selectin, GPIIb/IIIa expression. Consistently, the co-existence of platelets and arsenic significantly enhanced tumor cell adhesion, extravasation and invasion along with increased metastasis-related markers like metallo-matrix proteinase-2 and -9 in vitro, which was attenuated by platelet activation blockers. Importantly, the exposure to arsenic-contaminated drinking water (2 ppm, 3 weeks) in mice in vivo significantly increased the metastasis of intravenously injected melanoma cells into lung. Furthermore, the exposure to arsenic-contaminated drinking water significantly reduced the survival of melanoma cell-injected mice, which was attenuated by the pretreatment of platelet-activation blockers; aspirin and eptifibatide. All these results provide an important clue to understand the mechanism underlying arsenic-associated cancer mortality and its prevention.

Published

2018

2. Dysfunction of Vascular Smooth Muscle and Vascular Remodeling by Simvastatin

Author

Ok-Nam Bae, Keunyoung Kim, Jin Ho Chung, Moo-Yeol Lee, Young Min Bae, Seojin Kang, Kyung Min Lim, Ji-Yoon Noh, and Hyang-Hwa Woo

Subjects

Male, Simvastatin, medicine.medical_specialty, Time Factors, Contraction (grammar), RHOA, Vascular smooth muscle, Endothelium, Myocytes, Smooth Muscle, Primary Cell Culture, Aorta, Thoracic, Toxicology, Muscle, Smooth, Vascular, Rats, Sprague-Dawley, medicine.artery, Internal medicine, medicine, Animals, cardiovascular diseases, Cells, Cultured, Aorta, Dose-Response Relationship, Drug, biology, nutritional and metabolic diseases, Rats, Endocrinology, medicine.anatomical_structure, Vasoconstriction, biology.protein, Calcium, lipids (amino acids, peptides, and proteins), Hydroxymethylglutaryl-CoA Reductase Inhibitors, medicine.symptom, Muscle Contraction, Muscle contraction, medicine.drug

Abstract

Statins, inhibitors of 3-hydroxy-3-methylglutaryl-coenzyme A reductase, are widely prescribed for hypercholesterolemia. With the increasing use of statins, numerous reports demonstrated that statins can cause damage to skeletal muscles. However, the toxicities of statins on vascular smooth muscle, which are essential to cardiovascular homeostasis, have not been previously described. Here, we examined the effects of simvastatin on the contractile function and the integrity of vascular smooth muscle in isolated rat thoracic aortic rings, primary cultured vascular smooth muscle cells (VSMCs) in vitro and rats in vivo. In aortic rings, simvastatin suppressed the normal agonist-induced contractile responses in time- and concentration-dependent manners (0.86 g ± 0.11 at 10 μM simvastatin for 24 h compared with 1.89 g ± 0.11 at control). The suppression persisted in the endothelium-denuded aortic rings and was irreversible even after wash-out of simvastatin. Simvastatin suppressed the contraction induced by Bay K8644, an activator of voltage-operated Ca²⁺ channel (VOCC) in rat aortic rings and abolished agonist-induced intracellular Ca²⁺ increase in VSMCs. The simvastatin-induced contractile dysfunction was reversed by the supplementation of mevalonate and geranylgeranylpyrophosphate, precursors for protein isoprenylation. Consistently, activation of RhoA, a representative isoprenylated protein, was disrupted by simvastatin in VSMCs and RhoA-mediated phosphorylation of MYPT1 and CPI-17, and tonic tension were also suppressed. Notably, prolonged treatment of simvastatin up to 48 h induced apoptosis of vascular smooth muscle in aortic rings. Most importantly, simvastatin treatment in vivo significantly attenuated the agonist-induced vasoconstriction in rats ex vivo and induced a decrease in luminal area of the vascular wall. Collectively, these results demonstrate that simvastatin can impair the normal vascular contractility by disturbing Ca²⁺ influx and RhoA activity, ultimately leading to apoptosis and structural remodeling.

Published

2014

3. U-shaped Dose Response in Vasomotor Tone: A Mixed Result of Heterogenic Response of Multiple Cells to Xenobiotics

Author

Seung-Min Chung, Byoung-In Jung, Moo-Yeol Lee, Jee-Yeon Han, Jin Ho Chung, Ok-Nam Bae, Kyung Min Lim, Jin Young Lee, Joo-Young Lee, and Ji-Yoon Noh

Subjects

Male, Luminescence, Myosin Light Chains, Endothelium, Blood Pressure, Vasodilation, Pharmacology, Biology, Toxicology, Muscle, Smooth, Vascular, Arsenic, Xenobiotics, Nitric oxide, Rats, Sprague-Dawley, chemistry.chemical_compound, In vivo, medicine, Animals, Humans, Phosphorylation, Cells, Cultured, chemistry.chemical_classification, Reactive oxygen species, Superoxide, Vitamin K 3, Rats, medicine.anatomical_structure, chemistry, Immunology, Calcium, medicine.symptom, Vasoconstriction, Muscle Contraction, Muscle contraction

Abstract

U-shaped response has been frequently encountered in various biological areas including epidemiology, toxicology, and oncology. Despite its frequent observation, the theory of U-shaped response has been crippled by the lack of a robust mechanism underlying and incomplete in vitro and in vivo correlation. In the present study, a novel mechanism is provided for a U-shaped response, based on the findings of agonist-induced vasomotor tone change affected by menadione (MEN) (synthetic vitamin K(3)), a reactive oxygen species generator, and arsenic, an environmental pollutant, which showed typical U-shaped responses in both in vitro aortic contractile response and in vivo blood pressure. U-shaped responses by MEN and arsenic were a combined result from heterogenic susceptibilities and responses of multiple target cells composing blood vessels, that is, endothelium and smooth muscle. Notably, endothelium, a regulator of vasomotor tone, was primarily affected by low-dose stimuli, whereas smooth muscle, an effector of vascular contraction, was affected later by high-dose. The dysfunction of smooth muscle was produced by high-dose MEN-induced hydrogen peroxide, resulting in the attenuation of vascular contractile reactivity, whereas low-dose MEN-induced superoxide led to the quenching of vasodilatory nitric oxide in endothelial cells, resulting in the enhancement of vasoconstriction. This mechanistic theory, the difference in susceptibilities and responses to a common stimulus between regulator and effector components of a system, could give a new insight into the explanation of various U-shaped responses and provide a new evidence for the need of the risk assessment of toxicants with a wider dose range.

Published

2008

4. Association of Quinone-Induced Platelet Anti-Aggregation with Cytotoxicity

Author

Moo-Yeol Lee, Joo-Young Lee, Jin Ho Chung, Ok-Nam Bae, Se-Ryun Kim, and Seung-Min Chung

Subjects

Blood Platelets, Vitamin K, Platelet Aggregation, Cell Survival, Chloranil, Toxicology, Dithiothreitol, Rats, Sprague-Dawley, chemistry.chemical_compound, Menadione, Dinitrochlorobenzene, Animals, Platelet, Sulfhydryl Compounds, Cytotoxicity, chemistry.chemical_classification, L-Lactate Dehydrogenase, Proteins, Glutathione, Rats, Enzyme, chemistry, Biochemistry, Toxicity, Female, Intracellular, Naphthoquinones

Abstract

Various anti-platelet drugs, including quinones, are being investigated as potential treatments for cardiovascular disease because of their ability to prevent excessive platelet aggregation. In the present investigation 3 naphthoquinones (2,3-dimethoxy-1,4-naphthoquinone [DMNQ], menadione, and 1,4-naphthoquinone [4-NQ]) were compared for their abilities to inhibit platelet aggregation, deplete glutathione (GSH) and protein thiols, and cause cytotoxicity. Platelet-rich plasma, isolated from Sprague-Dawley rats, was used for all experiments. The relative potency of the 3 quinones to inhibit platelet aggregation, deplete intracellular GSH and protein thiols, and cause cytotoxicity was 1,4-NQ > menadione > > DMNQ. Experiments using 2 thiol-modifying agents, dithiothreitol (DTT) and 1-chloro-2,4-dintrobenzene (CDNB), confirmed the key roles for GSH in quinone-induced platelet anti-aggregation and for protein thiols in quinone-induced cytotoxicity. Furthermore, the anti-aggregative effects of a group of 12 additional quinone derivatives were positively correlated with their ability to cause platelet cytotoxicity. Quinones that had a weak anti-aggregative effect did not induce cytotoxicity (measured as LDH leakage), whereas quinones that had a potent anti-aggregative effect resulted in significant LDH leakage (84-96%). In one instance, however, p-chloranil demonstrated a potent anti-aggregative effect, but did not induce significant LDH leakage. This can be explained by the inability of p-chloranil to deplete protein thiols, even though intracellular GSH levels decreased rapidly. These results suggest that quinones that deplete GSH in platelets demonstrate a marked anti-aggregative effect. If this anti-aggregative effect is subsequently followed by depletion of protein thiols, cytotoxicity results.

Published

2001

5. Vascular Smooth Muscle Dysfunction and Remodeling Induced by Ginsenoside Rg3, a Bioactive Component of Ginseng.

Author

Jin-Young Lee, Kyung-Min Lim, Sun-Young Kim, Ok-Nam Bae, Ji-Yoon Noh, Seung-Min Chung, Keunyoung Kim, Yoo-Sun Shin, Moo-Yeol Lee, and Jin-Ho Chung

Subjects

THERAPEUTIC use of ginseng, CARDIOVASCULAR diseases, VASCULAR smooth muscle, MUSCLE cells, CALCIUM

Abstract

Ginseng, one of most well-known herbal medicines, is widely and indiscreetly used among the patients with cardiovascular disorders, raising concern over abuse of this medicine and unwanted effects. In this study, we investigated the effects of ginsenoside Rg3 (Rg3), an active ingredient of ginseng, on vascular contractility and structural integrity to explore its potential vascular toxicity. In isolated rat aorta, Rg3 suppressed the normal agonist-induced contractile response. This suppression persisted even after a rigorous washout. In the endothelium-denuded aortic ring, impairment of vascular contractility by Rg3 was retained, suggesting that vascular smooth muscle was affected. In primary vascular smooth muscle cells, Rg3 abolished agonist-induced Ca2+ increase, indicating that Ca2+ regulation was disrupted. Rg3 suppressed the contraction induced by Bay K8644, an L-type Ca2+ channel activator, whereas store-operated Ca2+ channel or intracellular Ca2+ store-mediated contraction was not affected, suggesting that the L-type Ca2+ channel was selectively impaired by Rg3. These in vitro results were further confirmed in vivo where Rg3 treatment significantly attenuated the agonist-induced pressor response. More importantly, 4-week repeated treatment with Rg3 in normal animals induced eutrophic outward remodeling in the thoracic aorta, that is, it brought about an increased luminal area without changes in the wall area. These results suggest that Rg3 can induce the vascular smooth muscle dysfunction by disturbing Ca2+ influx from the L-type Ca2+ channel, ultimately leading to impaired vascular contractility and structural remodeling. [ABSTRACT FROM AUTHOR]

Published

2010

6. Association of Quinone-Induced Platelet Anti-Aggregation with Cytotoxicity.

Author

Se-Ryun Kim, Joo-Young Lee, Moo-Yeol Lee, Seung-Min Chung, Ok-Nam Bae, and Jin-Ho Chung

Subjects

QUINONE, BLOOD platelets, CELL-mediated cytotoxicity, CARDIOVASCULAR diseases, CELL aggregation, GLUTATHIONE, THIOLS

Abstract

Various anti-platelet drugs, including quinones, are being investigated as potential treatments for cardiovascular disease because of their ability to prevent excessive platelet aggregation. In the present investigation 3 naphthoquinones (2,3-dimethoxy-1,4-naphthoquinone [DMNQ], menadione, and 1,4-naphthoquinone [4-NQ]) were compared for their abilities to inhibit platelet aggregation, deplete glutathione (GSH) and protein thiols, and cause cytotoxicity. Platelet-rich plasma, isolated from Sprague-Dawley rats, was used for all experiments. The relative potency of the 3 quinones to inhibit platelet aggregation, deplete intracellular GSH and protein thiols, and cause cytotoxicity was 1,4-NQ > menadione >> DMNQ. Experiments using 2 thiol-modifying agents, dithiothreitol (DTT) and 1-chloro-2,4-dintrobenzene (CDNB), confirmed the key roles for GSH in quinone-induced platelet anti-aggregation and for protein thiols in quinone-induced cytotoxicity. Furthermore, the anti-aggregative effects of a group of 12 additional quinone derivatives were positively correlated with their ability to cause platelet cytotoxicity. Quinones that had a weak anti-aggregative effect did not induce cytotoxicity (measured as LDH leakage), whereas quinones that had a potent anti-aggregative effect resulted in significant LDH leakage (84–96%). In one instance, however, p-chloranil demonstrated a potent anti-aggregative effect, but did not induce significant LDH leakage. This can be explained by the inability of p-chloranil to deplete protein thiols, even though intracellular GSH levels decreased rapidly. These results suggest that quinones that deplete GSH in platelets demonstrate a marked anti-aggregative effect. If this anti-aggregative effect is subsequently followed by depletion of protein thiols, cytotoxicity results. [ABSTRACT FROM PUBLISHER]

Published

2001

7. U-shaped Dose Response in Vasomotor Tone: A Mixed Result of Heterogenic Response of Multiple Cells to Xenobiotics.

Author

Ok-Nam Bae, Kyung-Min Lim, Jee-Yeon Han, Byoung-In Jung, Jin-Young Lee, Ji-Yoon Noh, Seung-Min Chung, Moo-Yeol Lee, Joo-Young Lee, and Jin-Ho Chung

Subjects

VASOMOTOR system, XENOBIOTICS, CELLS, HEALTH risk assessment

Abstract

U-shaped response has been frequently encountered in various biological areas including epidemiology, toxicology, and oncology. Despite its frequent observation, the theory of U-shaped response has been crippled by the lack of a robust mechanism underlying and incomplete in vitro and in vivo correlation. In the present study, a novel mechanism is provided for a U-shaped response, based on the findings of agonist-induced vasomotor tone change affected by menadione (MEN) (synthetic vitamin K3), a reactive oxygen species generator, and arsenic, an environmental pollutant, which showed typical U-shaped responses in both in vitro aortic contractile response and in vivo blood pressure. U-shaped responses by MEN and arsenic were a combined result from heterogenic susceptibilities and responses of multiple target cells composing blood vessels, that is, endothelium and smooth muscle. Notably, endothelium, a regulator of vasomotor tone, was primarily affected by low-dose stimuli, whereas smooth muscle, an effector of vascular contraction, was affected later by high-dose. The dysfunction of smooth muscle was produced by high-dose MEN-induced hydrogen peroxide, resulting in the attenuation of vascular contractile reactivity, whereas low-dose MEN-induced superoxide led to the quenching of vasodilatory nitric oxide in endothelial cells, resulting in the enhancement of vasoconstriction. This mechanistic theory, the difference in susceptibilities and responses to a common stimulus between regulator and effector components of a system, could give a new insight into the explanation of various U-shaped responses and provide a new evidence for the need of the risk assessment of toxicants with a wider dose range. [ABSTRACT FROM AUTHOR]

Published

2008