Your search keyword '"Tsuji, Masato"' showing total 7 results

1. Sexual dimorphisms of mRNA and miRNA in human/murine heart disease.

Author

Tsuji, Masato, Kawasaki, Takanori, Matsuda, Takeru, Arai, Tomio, Gojo, Satoshi, and Takeuchi, Jun K.

Subjects

*SEXUAL dimorphism, *MICRORNA, *MESSENGER RNA, *HEART diseases, *THERAPEUTICS, *GENE ontology, *HOMEOSTASIS

Abstract

Background: Sexual dimorphisms are well recognized in various cardiac diseases such as ischemic cardiomyopathy (ICM), hypertrophic cardiomyopathy (HCM) and dilated cardiomyopathy (DCM). Thorough understanding of the underlying genetic programs is crucial to optimize treatment strategies specified for each gender. By performing meta-analysis and microarray analysis, we sought to comprehensively characterize the sexual dimorphisms in the healthy and diseased heart at the level of both mRNA and miRNA transcriptome. Results: Existing mRNA microarray data of both mouse and human heart were integrated, identifying dozens/ hundreds of sexually dimorphic genes in healthy heart, ICM, HCM, and DCM. These sexually dimorphic genes overrepresented gene ontologies (GOs) important for cardiac homeostasis. Further, microarray of miRNA, isolated from mouse sham left ventricle (LV) (n = 6 & n = 5 for male & female) and chronic MI LV (n = 19 & n = 19) and from human normal LV (n = 6 & n = 6) and ICM LV (n = 4 & n = 5), was conducted. This revealed that 13 mouse miRNAs are sexually dimorphic in MI and 6 in normal heart. In human, 3 miRNAs were sexually dimorphic in ICM and 15 in normal heart. These data revealed miRNA-mRNA networks that operate in a sexually-biased fashion. Conclusions: mRNA and miRNA transcriptome of normal and disease heart show significant sex differences, which might impact the cardiac homeostasis. Together this study provides the first comprehensive picture of the genome-wide program underlying the heart sexual dimorphisms, laying the foundation for gender specific treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2017

2. Conductance through a multiorbital quantum dot coupled to ferromagnetic leads

Author

Tsuji, Masato and Suga, Sei-ichiro

Subjects

*SEMICONDUCTORS, *CRYSTALS, *ELECTRIC conductivity, *ELECTRICAL engineering materials

Abstract

Abstract: We investigate the Kondo effect of a multiorbital quantum dot coupled to spin polarized leads, using the noncrossing approximation. It is shown that as the spin polarization is increased, the Kondo peak splits into three peaks and the middle one is located close to the Fermi energy. The results indicate that the Kondo effect caused by the orbital degrees of freedom survives, while the Kondo effect by the spin degrees of freedom is suppressed. In the temperature dependence of the conductance, the hump structure emerges owing to the contribution from the orbital and spin degrees of freedom. [Copyright &y& Elsevier]

Published

2007

3. Contribution of cell surface protein antigen PAc of Streptococcus mutans to bacteremia

Author

Nakano, Kazuhiko, Tsuji, Masato, Nishimura, Kaoru, Nomura, Ryota, and Ooshima, Takashi

Subjects

*STREPTOCOCCUS mutans, *ANTIGEN-antibody reactions, *PHAGOCYTOSIS, *CELL membranes

Abstract

Abstract: Streptococcus mutans, a major cariogenic bacterium, is occasionally isolated from the blood of patients with bacteremia and infective endocarditis. Mutant strains of S. mutans MT8148, defective in the major surface proteins glucosyltransferase (GTF) B-, C-, and D-, and protein antigen c (PAc), were constructed by insertional inactivation of each respective gene with an antibiotic resistant cassette. Susceptibility to phagocytosis was determined by analyses of interactions of the bacteria with human polymorphonuclear leukocytes, and the PAc-defective mutant strain (PD) showed the lowest rate of phagocytosis. Further, when PD and MT8148 were separately injected into the jugular veins of Sprague–Dawley rats, PD was recovered in significantly larger numbers and for a longer duration, and caused more severe systemic inflammation than MT8148, indicating that S. mutans PAc is associated with its systemic virulence in blood. Next, 100 S. mutans clinical isolates from 100 Japanese children and adolescents were analyzed by Western blotting using antisera raised against recombinant PAc, generated based on the pac sequence of MT8148. Four of the 100 strains showed no positive band and each exhibited a significantly lower phagocytosis rate than that of 25 randomly selected clinical strains (P <0.01). In addition, three of the 100 strains possessed a lower molecular weight PAc and a significantly lower rate of phagocytosis than the 25 reference strains (P <0.05). These results suggest that S. mutans PAc may be associated with phagocytosis susceptibility to human polymorphonuclear leukocytes, with approximately 7% of S. mutans clinical isolates possible high-risk strains for the development of bacteremia. [Copyright &y& Elsevier]

Published

2006

4. Inhibitory effects of cacao bean husk extract on plaque formation in vitro and in vivo.

Author

Matsumoto, Michiyo, Tsuji, Masato, Okuda, Jumpei, Sasaki, Hidekazu, Nakano, Kazuhiko, Osawa, Kenji, Shimura, Susumu, and Ooshima, Takashi

Subjects

*CACAO beans, *PLANT extracts, *DENTAL plaque, *ANTIBACTERIAL agents, *STREPTOCOCCUS mutans, *DENTAL hygiene

Abstract

Matsumoto M, Tsuji M, Okuda J, Sasaki H, Nakano K, Osawa K, Shimura S, Ooshima T. Inhibitory effects of cacao bean husk extract on plaque formation in vitro and in vivo. Eur J Oral Sci 2004; 112: 249–252. ©Eur J Oral Sci, 2004 Cacao bean husk extract (CBH) has been shown to possess antibacterial and antiglucosyltransferase activities through its unsaturated fatty acids and epicatechin polymers, respectively. In the present study, the antiplaque activities of CBH were examined in vitro and in vivo. The extract inhibited the adherence of Streptococcus mutans MT8148 to saliva-coated hydroxyapatite and reduced the accumulation of artificial dental plaque by S. mutans MT8148 on orthodontic wire. The number of mutans streptococci in dental plaque was also significantly reduced when human dental plaque was exposed to CBH from 21 children at 37°C for 1 h. For the in vivo study, 28 volunteers aged 19–29 yr old rinsed their mouth with CBH, before and after each intake of food and before sleeping at night for 4 d without using other oral hygiene procedures. Plaque depositions and the numbers of mutans streptococci were reduced in the subjects, compared with rinsing with 1% ethanol alone. These results indicate that CBH possesses significant antiplaque activity in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2004

5. Correction: Sexual dimorphisms of mRNA and miRNA in human/murine heart disease.

Author

Tsuji, Masato, Kawasaki, Takanori, Matsuda, Takeru, Arai, Tomio, Gojo, Satoshi, and Takeuchi, Jun K.

Subjects

*SEXUAL dimorphism, *HEART diseases, *MICRORNA, *MESSENGER RNA, *LIFE sciences

Published

2020

6. Spatial and temporal diversity of DCLK1 isoforms in developing mouse brain.

Author

Bergoglio, Emilia, Suzuki, Ikuo K., Togashi, Kazuya, Tsuji, Masato, Takeuchi, Shunsuke, Koizumi, Hiroyuki, and Emoto, Kazuo

Subjects

*NEURAL development, *MICE, *CELL migration, *KINASES, *DENDRITES, *CARP

Abstract

• In silico analysis of DCLK1 transcripts reveals developmental dynamics unique for each isoform. • DCLK1 isoforms are distributed in the partially distinct brain regions. • Overexpression of DCLK1-L in progenitors causes neural migration defects. • The migration defects by DCLK1-L overexpression requires its kinase activity Doublecortin-like kinase 1 (DCLK1) is a Doublecortin family kinase involved in a range of brain development processes including cell migration, axon/dendrite growth, and synapse development. The Dclk1 gene potentially generates multiple splicing isoforms, but the detailed expression patterns in the brain as well as in vivo functions of each isoform are still incompletely understood. Here we assessed expression patterns of DCLK1 isoforms using multiple platforms including in silico , in situ , and in vitro datasets in the developing mouse brain, and show quantitative evidence that among the four DCLK1 isoforms, DCLK1-L and DCL are mainly expressed in the embryonic cortex whereas DCLK1-L and CPG16 become dominant compared to DCL and CARP in the postnatal cortex. We also provide compelling evidence that DCLK1 isoforms are distributed in the partially distinct brain regions in the embryonic and the postnatal stages. We further show that overexpression of DCLK1-L, but not the other isoforms, in neural progenitors causes severe migration defects in the cortex, and that the migration defects are dependent on the kinase activity of DCLK1-L. Our data thus uncover partially segregated localization of DCLK1 isoforms in the developing mouse brain and suggest different roles for distinct DCLK1 isoforms in the brain development and function. [ABSTRACT FROM AUTHOR]

Published

2021

7. Drosophila miR-87 promotes dendrite regeneration by targeting the transcriptional repressor Tramtrack69.

Author

Kitatani, Yasuko, Tezuka, Akane, Hasegawa, Eri, Yanagi, Satoyoshi, Togashi, Kazuya, Tsuji, Masato, Kondo, Shu, Parrish, Jay Z., and Emoto, Kazuo

Subjects

*DENDRITES, *DROSOPHILA, *SENSORY neurons, *NERVOUS system, *GENETIC repressors, *GENETIC testing

Abstract

To remodel functional neuronal connectivity, neurons often alter dendrite arbors through elimination and subsequent regeneration of dendritic branches. However, the intrinsic mechanisms underlying this developmentally programmed dendrite regeneration and whether it shares common machinery with injury-induced regeneration remain largely unknown. Drosophila class IV dendrite arborization (C4da) sensory neurons regenerate adult-specific dendrites after eliminating larval dendrites during metamorphosis. Here we show that the microRNA miR-87 is a critical regulator of dendrite regeneration in Drosophila. miR-87 knockout impairs dendrite regeneration after developmentally-programmed pruning, whereas miR-87 overexpression in C4da neurons leads to precocious initiation of dendrite regeneration. Genetic analyses indicate that the transcriptional repressor Tramtrack69 (Ttk69) is a functional target for miR-87-mediated repression as ttk69 expression is increased in miR-87 knockout neurons and reducing ttk69 expression restores dendrite regeneration to mutants lacking miR-87 function. We further show that miR-87 is required for dendrite regeneration after acute injury in the larval stage, providing a mechanistic link between developmentally programmed and injury-induced dendrite regeneration. These findings thus indicate that miR-87 promotes dendrite regrowth during regeneration at least in part through suppressing Ttk69 in Drosophila sensory neurons and suggest that developmental and injury-induced dendrite regeneration share a common intrinsic mechanism to reactivate dendrite growth. Author summary: Dendrites are the primary sites for synaptic and sensory inputs. To remodel or repair neuronal connectivity, dendrites often exhibit large-scale structural changes that can be triggered by developmental signals, alterations in sensory inputs, or injury. Despite the importance of dendritic remodeling to nervous system function, the molecular basis for this remodeling is largely unknown. Here we used an unbiased genetic screen and in vivo imaging in Drosophila sensory neurons to demonstrate that the microRNA miR-87 is a critical factor required in neurons to reactivate dendritic growth both in developmental remodeling and following injury. Our work supports the model that miR-87 promotes dendrite regeneration by blocking expression of the transcriptional repressor Tramtrack69 in neurons. This study thus establishes a role for miRNAs in temporal control of dendrite regeneration. [ABSTRACT FROM AUTHOR]

Published

2020