Your search keyword '"Kuro-O M"' showing total 357 results

351. Expression of myosin isozymes during the developmental stage and their redistribution induced by pressure overload.

Author

Tsuchimochi H, Kuro-o M, Takaku F, Yoshida K, Kawana M, Kimata S, and Yazaki Y

Subjects

Animals, Cattle, Heart embryology, Humans, Hypertension metabolism, Myocardium metabolism, Myosins metabolism

Abstract

Cardiac muscles contain at least two isozymes--referred to as alpha(HC alpha) and beta(HC beta)--of the myosin heavy chain. The proportional ratio of these isozymes varies depending upon the developmental stage and the physiological and/or the hormonal milieu of the cell. Using monoclonal antibodies (MoAb) specific for human cardiac HC alpha and HC beta, we have examined the expression of these isozymes in fetal through adult cardiac tissues and investigated whether isozymic redistribution occurs in pressure overloaded human ventricles. We found that although HC alpha was expressed in the atrium from the early embryonic stage, in embryonic ventricular myofibers, only HC beta was expressed without expression of HC alpha, but some myofibers replace HC beta by HC alpha after birth, and these HC alpha containing ventricular myofibers were found to be decreased by pressure overload, which suggested that isozymic redistribution from HC alpha to HC beta also occurred in the ventricles, as well as the atrium. In addition, we also found two subtypes of HC beta (beta 1, beta 2) in the human heart. In the ventricle, both beta 1 and beta 2 was present in all myofibers; in contrast, some myofibers contained beta 1 or beta 2 or both with or without expression of HC alpha in the atrium. beta 1 and beta 2 were distinctive in their expression during the developmental stage, since beta 1 was present in the embryonic heart from the early developmental stage, whereas beta 2 was not present in the early embryonic heart, but began to be expressed in the late embryonic stage.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1986

352. Distribution of cardiac myosin isozymes in human conduction system. Immunohistochemical study using monoclonal antibodies.

Author

Kuro-o M, Tsuchimochi H, Ueda S, Takaku F, and Yazaki Y

Subjects

Antibodies, Monoclonal, Atrioventricular Node analysis, Bundle of His analysis, Fluorescent Antibody Technique, Heart Atria analysis, Heart Ventricles analysis, Histocytochemistry, Humans, Purkinje Fibers analysis, Sinoatrial Node analysis, Tissue Distribution, Heart Conduction System analysis, Myosins analysis

Abstract

To determine the presence and distribution of cardiac myosin isozymes in the human conduction system, we performed an immunohistochemical study using monoclonal antibodies CMA19 and HMC14, which are specific for myosin heavy chains of human atrial type (alpha-type) and ventricular type (beta-type), respectively. Serial frozen sections of human hearts were obtained from autopsy samples and examined by indirect immunofluorescence. Alpha-type was found in all myofibers of sinus node and atrio-ventricular node, and in 55.2 +/- 10.2% (mean +/- SD, n = 5) of the myofibers of ventricular conduction tissue, which consists of the bundle of His, bundle branches, and the Purkinje network. In contrast, beta-type was found in all myofibers of the atrio-ventricular node and ventricular conduction tissue, whereas almost all myofibers of the sinus node were unlabeled by HMC14. Although the number of ventricular myofibers labeled by CMA19 was small, the labeled myofibers were more numerous in the subepicardial region than in the subendocardial region. These findings show that the gene coding for alpha-type is expressed predominantly in specialized myocardium compared with the adjacent ordinary working myocardium.

Published

1986

353. [Coronary artery sclerosis and major causes of death in the aged].

Author

Kuro-o M, Okai Y, Matsushita S, and Kuramoto K

Subjects

Age Factors, Aged, Aged, 80 and over, Coronary Artery Disease complications, Humans, Myocardial Infarction complications, Myocardial Infarction mortality, Neoplasms complications, Neoplasms mortality, Pneumonia complications, Pneumonia mortality, Cause of Death, Coronary Artery Disease mortality

Published

1988

354. Developmentally regulated expression of vascular smooth muscle myosin heavy chain isoforms.

Author

Kuro-o M, Nagai R, Tsuchimochi H, Katoh H, Yazaki Y, Ohkubo A, and Takaku F

Subjects

Animals, Aorta, DNA Probes, Fluorescent Antibody Technique, Immunoblotting, Muscle, Smooth, Vascular metabolism, Nucleic Acid Hybridization, RNA Splicing, RNA, Messenger genetics, Rabbits, Gene Expression physiology, Muscle Development, Muscle, Smooth, Vascular growth & development, Myosins genetics

Abstract

Two types of smooth muscle myosin heavy chain (MHC) isoforms, SM1 and SM2, were recently identified to have different carboxyl termini (Nagai, R., Kuro-o, M., Babij, P., and Periasamy, M. (1989) J. Biol. Chem. 264, 9734-9737). SM1 and SM2 are considered to be generated from a single gene through alternative RNA splicing. In this study we investigated expression of vascular MHC isoforms during development in rabbits at the mRNA, protein, and histological levels. In adults, all smooth muscle cells reacted with both anti-SM1 and anti-SM2 antibodies on immunofluorescence, suggesting the coexpression of SM1 and SM2 in a single cell. In fetal and perinatal rabbits, however, only anti-SM1 antibody consistently reacted with smooth muscles. Reactivity with anti-SM2 antibody was negative in the fetal and neonatal blood vessels and gradually increased during 30 days after birth. These developmental changes in SM1 and SM2 expression at the histological level coincided with mRNA expression of each MHC isoform as determined by S1 nuclease mapping, indicating that expression of SM1 and SM2 is controlled at the level of RNA splicing. However, sodium dodecyl sulfate-polyacrylamide gel electrophoresis of myosin from fetal and perinatal aortas revealed the presence of large amount of SM2. Interestingly, fetal SM2 did not cross-react with our anti-SM2 antibody on immunoblotting. We conclude that expression of SM1 and SM2 are differentially regulated during development and that a third type of MHC isoform may exist in embryonic and perinatal vascular smooth muscles.

Published

1989

355. Differences in response of myosin isozyme transition of ordinary and specialized myocardium to overload.

Author

Nomoto K, Komuro I, Kuro-o M, Tsuchimochi H, Takaku F, Machii K, and Yazaki Y

Subjects

Animals, Heart physiopathology, Heart Atria, Heart Ventricles, Immunohistochemistry, Myocardium cytology, Pulmonary Valve Stenosis enzymology, Pulmonary Valve Stenosis physiopathology, Sinoatrial Node cytology, Sinoatrial Node enzymology, Tricuspid Valve Insufficiency enzymology, Tricuspid Valve Insufficiency physiopathology, Isoenzymes metabolism, Myocardium enzymology, Myosins metabolism

Abstract

To investigate the response of myosin isozyme transition in specialized myocardium to cardiac overload, we examined immunohistochemically the distribution of myosin isozymes in sinus node cells of overloaded canine atria, using the monoclonal antibodies CMA19 and HMC14, which are specific for atrial myosin heavy chain (alpha-HC) and ventricular myosin heavy chain (beta-HC), respectively. Overloading in canine right atria was induced by artificial tricuspid valve regurgitation and pulmonary stenosis. Right atrial mean pressure rose to 15-20 mm Hg (n = 4) 2 months after surgery. In the working myocardium, cardiac overload caused redistribution of myosin isozymes, alpha-HC to beta-HC. Compared with the normal right atria, fewer myocytes were labeled with CMA19, but more were labeled with HMC14. However, the reactivity of sinus node cells with CMA19 and HMC14 was not changed between normal and overloaded right atria, indicating no redistribution of myosin heavy chain isozymes, alpha-HC to beta-HC. These results suggest that isozymes in myosin heavy chains in the specialized myocardium are protected from overload effects by their firm cytoskeletal framework or other mechanisms.

Published

1988

356. Isozymic changes in myosin of human atrial myocardium induced by overload. Immunohistochemical study using monoclonal antibodies.

Author

Tsuchimochi H, Sugi M, Kuro-o M, Ueda S, Takaku F, Furuta S, Shirai T, and Yazaki Y

Subjects

Animals, Antibodies, Monoclonal, Antigen-Antibody Complex, Cattle, Enzyme-Linked Immunosorbent Assay, Heart Atria enzymology, Heart Ventricles enzymology, Humans, Hypertension enzymology, Isoenzymes metabolism, Myocardium enzymology, Myosins metabolism

Abstract

An immunohistochemical study using monoclonal antibodies specific for the heavy chains of either human atrial (HC alpha) or ventricular (HC beta) myosin was performed to clarify the distribution of each isozyme in normal as well as pressure-overloaded human hearts. In normal human ventricles, all muscle fibers were stained by a monoclonal antibody (HMC14) specific for HC beta, whereas a small number of fibers reacted with a monoclonal antibody (CMA19) specific for HC alpha. In contrast, in normal human atria, almost all muscle fibers were stained by CMA19, and a relatively larger number of muscle fibers also reacted with HMC14. Furthermore, in pressure-overloaded atria, muscle fibers reactive with HMC14 were strikingly increased while those reactive with CMA19 showed a corresponding decrease. The extent of this isozymic redistribution was in good correlation with atrial pressure. These results not only confirmed the existence of isoforms of myosin heavy chain in human hearts, but also demonstrated that redistribution of iso-myosins could occur as an adaptation to pressure overload.

Published

1984

357. Identification of two types of smooth muscle myosin heavy chain isoforms by cDNA cloning and immunoblot analysis.

Author

Nagai R, Kuro-o M, Babij P, and Periasamy M

Subjects

Amino Acid Sequence, Animals, Base Sequence, Chickens, Female, Genetic Vectors, Gizzard, Avian metabolism, Molecular Sequence Data, Myosin Subfragments, Rabbits, Sequence Homology, Nucleic Acid, Uterus metabolism, Cloning, Molecular, DNA genetics, Muscle, Smooth metabolism, Myosins genetics, Peptide Fragments genetics

Abstract

We previously reported the characterization of a rabbit uterus cDNA clone (SMHC29) which encoded part of the light meromyosin of smooth muscle myosin heavy chain (Nagai, R., Larson, D.M., and Periasamy, M. (1988) Proc. Natl. Acad. Sci. U. S. A. 85, 1047-1051). We have now characterized a second cDNA clone (SMHC40) which also encodes part of the light meromyosin but differs from SMHC29 in the following respects. Nucleotide sequence analysis demonstrates that the two myosin heavy chain mRNAs are identical over 1424 nucleotides but differ in part of the 3'-carboxyl coding region and a portion of the 3'-nontranslated sequence. Specifically, SMHC40 cDNA encodes a unique stretch of 43 amino acids at the carboxyl terminus, whereas SMHC29 cDNA contains a shorter carboxyl terminus of 9 unique amino acids which is the result of a 39-nucleotide insertion. Recent peptide mapping of smooth muscle myosin heavy chain identified two isotypes with differences in the light meromyosin fragment that were designated as SM1 (204 kDa) and SM2 (200 kDa) type myosin (Eddinger, T. J., and Murphy, R.A. (1988) Biochemistry 27, 3807-3811). In this study we present direct evidence that SMHC40 and SMHC29 mRNA encode the two smooth muscle myosin heavy chain isoforms, SM1 and SM2, respectively, by immunoblot analysis using antibodies against specific carboxyl terminus sequences deduced from SMHC40 and SMHC29 cDNA clones.

Published

1989