Tenascin-C is Associated With Coronary Plaque Instability in Patients With Acute Coronary Syndromes
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概要
- 論文の詳細を見る
Background Tenascin-C (TNC) is an extracellular matrix glycoprotein that increases after inflammation and injury. In cultured cells TNC has been reported to markedly induce the expression of matrix metalloproteinase-9, which stimulates collagen degradation in the fibrous cap of human atherosclerotic plaque. Methods and Results Immunohistochemical techniques were used to analyze the expression of TNC protein in 51 coronary atherectomy specimens obtained from patients with stable angina pectoris (SAP, n=23) or acute coronary syndromes (ACS) (n=28; unstable angina pectoris, n=20, acute myocardial infarction, n=8). Immunostaining for a-smooth muscle actin, CD68, CD45, and CD31 was also performed in serial sections to identify the cell types that express TNC protein. The %TNC+area (percentage of the area of immunostaining for TNC protein in the total surface area of the plaque) was larger in coronary samples with the plaque characteristics of thrombus, angiogenesis, intraplaque hemorrhage, and macrophage (CD68+), and lymphocyte (CD45+) clusters than in coronary samples without them (52±3.4 vs 39±4.8, p<0.05; 57±3.7 vs 36±3.7, p<0.01; 51±3.6 vs 39±4.8, p<0.05; 53±3.4 vs 33±4.5, p<0.01; 56±4.1 vs 37±3.6, p<0.01, respectively). The presence of other components, such as dense fibrous tissue, neointimal hyperplasia, atheromatous gruel and calcification, was not significantly correlated with the %TNC + area. The %TNC + area was larger in coronary samples from patients with ACS than in samples from patients with SAP (56±3.2% vs 34±4.3%, p<0.01). Conclusions The results suggest that TNC may have specific functions in coronary plaque formation and may be involved in the pathogenesis of coronary lesions in ACS.
- 社団法人日本循環器学会の論文
- 2004-02-20
著者
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YAMAMOTO Hideya
Department of Cardiovascular Medicine, Graduate School of Biomedical Sciences, Hiroshima University
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KOHNO Nobuoki
Department of Molecular and Internal Medicine, Graduate School of Biomedical Sciences, Hiroshima Uni
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Kajiwara kenji
Department of Molecular Medicine, Hiroshima University Graduate School
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Yamamoto Hideya
Department Of Cardiovascular Medicine Graduate School Of Biomedical Sciences Hiroshima University
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Imazu Michinori
Division Of Cardiology Tsuchiya General Hospital
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Imazu Michinori
Department Of Medicine Ajina Tsuchiya Hospital
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Hayashi Yasuhiko
Department Of Cardiovascular Physiology And Medicine Hiroshima University Graduate School Of Biomedi
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Kajiwara Kenji
Department Of Molecular Medicine Hiroshima University Graduate School
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Kohno Nobuoki
Department Of Molecular And Internal Medicine Graduate School Of Biomedical Sciences Hiroshima Unive
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Kohno Nobuoki
Department Of Molecular And Internal Medicine Hiroshima University Graduate School Of Biomedical Sci
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Ueda Hironori
Department of Cardiology, Akane-kai, Tsuchiya General Hospital
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Kajiwara Kenji
Department Of Applied Physics Faculty Of Engineering University Of Tokyo
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Kohno Nobuoki
Department Of Internal Medicine Hiroshima University Graduate School Of Medicine
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Kohno Nobuoki
Second Department Of Internal Medicine Hiroshima University School Of Medicine
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Ueda Hironori
Department Of Cardiology Tsuchiya General Hospital
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Yamamoto Hideya
Department Of Molecular And Internal Medicine Hiroshima University
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Kohno Nobuoki
Department Of Molecular And Internal Medicine Division Of Clinical Medical Science Programs For Appl
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Imazu Michinori
Second Department Of Internal Medicine Hiroshima University School Of Medicine
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Hayashi Yasuhiko
Department Of Cardiology Tsuchiya General Hospital
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Yamamoto Hideya
Department Of Molecular And Internal Medicine Graduate School Of Biomedical Sciences Hiroshima Unive
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Hayashi Yasuhiko
Department Of Cardiology Cardiovascular Center Tsuchiya General Hospital
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