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      KCI등재 SCOPUS SCIE

      Thymosin Beta4 Regulates Cardiac Valve Formation Via Endothelial-Mesenchymal Transformation in Zebrafish Embryos

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      https://www.riss.kr/link?id=A103928238

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      다국어 초록 (Multilingual Abstract)

      Thymosin beta4 (TB4) has multiple functions in cellular response in processes as diverse as embryonic organ development and the pathogeneses of disease, especially those associated with cardiac coronary vessels. However, the specific roles played by TB4 during heart valve development in vertebrates are largely unknown. Here, we identified a novel function of TB4 in endothelial-mesenchymal transformation (EMT) in cardiac valve endocardial cushions in zebrafish. The expressions of thymosin family members in developing zebrafish embryos were determined by whole mount in situ hybridization. Of the thymosin family members only zTB4 was expressed in the developing heart region. Cardiac valve development at 48 h post fertilization was defected in zebrafish TB4 (zTB4) morpholino-injected embryos (morphants). In zTB4 morphants, abnormal linear heart tube development was observed. The expressions of bone morphogenetic protein (BMP) 4, notch1b, and hyaluronic acid synthase (HAS) 2 genes were also markedly reduced in atrio-ventricular canal (AVC). Endocardial cells in the AVC region were stained with anti-Zn5 antibody reactive against Dm-grasp (an EMT marker) to observe EMT in developing cardiac valves in zTB4 morphants. EMT marker expression in valve endothelial cells was confirmed after transfection with TB4 siRNA in the presence of transforming growth factor β (TGFβ) by RT-PCR and immunofluorescent assay. Zn5-positive endocardial AVC cells were not observed in zTB4 morphants, and knockdown of TB4 suppressed TGF--induced EMT in ovine valve endothelial cells. Taken together, our results demonstrate that TB4 plays a pivotal role in cardiac valve formation by increasing EMT.
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      Thymosin beta4 (TB4) has multiple functions in cellular response in processes as diverse as embryonic organ development and the pathogeneses of disease, especially those associated with cardiac coronary vessels. However, the specific roles played by T...

      Thymosin beta4 (TB4) has multiple functions in cellular response in processes as diverse as embryonic organ development and the pathogeneses of disease, especially those associated with cardiac coronary vessels. However, the specific roles played by TB4 during heart valve development in vertebrates are largely unknown. Here, we identified a novel function of TB4 in endothelial-mesenchymal transformation (EMT) in cardiac valve endocardial cushions in zebrafish. The expressions of thymosin family members in developing zebrafish embryos were determined by whole mount in situ hybridization. Of the thymosin family members only zTB4 was expressed in the developing heart region. Cardiac valve development at 48 h post fertilization was defected in zebrafish TB4 (zTB4) morpholino-injected embryos (morphants). In zTB4 morphants, abnormal linear heart tube development was observed. The expressions of bone morphogenetic protein (BMP) 4, notch1b, and hyaluronic acid synthase (HAS) 2 genes were also markedly reduced in atrio-ventricular canal (AVC). Endocardial cells in the AVC region were stained with anti-Zn5 antibody reactive against Dm-grasp (an EMT marker) to observe EMT in developing cardiac valves in zTB4 morphants. EMT marker expression in valve endothelial cells was confirmed after transfection with TB4 siRNA in the presence of transforming growth factor β (TGFβ) by RT-PCR and immunofluorescent assay. Zn5-positive endocardial AVC cells were not observed in zTB4 morphants, and knockdown of TB4 suppressed TGF--induced EMT in ovine valve endothelial cells. Taken together, our results demonstrate that TB4 plays a pivotal role in cardiac valve formation by increasing EMT.

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      참고문헌 (Reference)

      1 Huff, T., "β-Thymosins, small acidic peptides with multiple functions" 33 : 205-220, 2001

      2 Bakkers, J., "Zebrafish as a model to study cardiac development and human cardiac disease" 91 : 279-288, 2011

      3 Lee, Y. M., "Vascular endothelial growth factor receptor signaling is required for cardiac valve formation in zebrafish" 235 : 29-37, 2006

      4 Stankunas, K., "VEGF signaling has distinct spatiotemporal roles during heart valve development" 347 : 325-336, 2010

      5 Thatcher, J. E., "Thymosin β4 sustained release from poly(lactide‐co‐glycolide)microspheres : synthesis and implications for treatment of myocardial ischemia" 1270 : 112-119, 2012

      6 Bock-Marquette, I., "Thymosin β4 mediated PKC activation is essential to initiate the embryonic coronary developmental program and epicardial progenitor cell activation in adult mice in vivo" 46 : 728-738, 2009

      7 Bock-Marquette, I., "Thymosin β4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repair" 432 : 466-472, 2004

      8 Malinda, K. M., "Thymosin β4 accelerates wound healing" 113 : 364-368, 1999

      9 Goldstein, A. L., "Thymosin β4 : a multi-functional regenerative peptide. Basic properties and clinical applications" 12 : 37-51, 2012

      10 Li, Q., "Thymosin beta4 regulation, expression and function in aortic valve interstitial cells" 11 : 726-735, 2002

      1 Huff, T., "β-Thymosins, small acidic peptides with multiple functions" 33 : 205-220, 2001

      2 Bakkers, J., "Zebrafish as a model to study cardiac development and human cardiac disease" 91 : 279-288, 2011

      3 Lee, Y. M., "Vascular endothelial growth factor receptor signaling is required for cardiac valve formation in zebrafish" 235 : 29-37, 2006

      4 Stankunas, K., "VEGF signaling has distinct spatiotemporal roles during heart valve development" 347 : 325-336, 2010

      5 Thatcher, J. E., "Thymosin β4 sustained release from poly(lactide‐co‐glycolide)microspheres : synthesis and implications for treatment of myocardial ischemia" 1270 : 112-119, 2012

      6 Bock-Marquette, I., "Thymosin β4 mediated PKC activation is essential to initiate the embryonic coronary developmental program and epicardial progenitor cell activation in adult mice in vivo" 46 : 728-738, 2009

      7 Bock-Marquette, I., "Thymosin β4 activates integrin-linked kinase and promotes cardiac cell migration, survival and cardiac repair" 432 : 466-472, 2004

      8 Malinda, K. M., "Thymosin β4 accelerates wound healing" 113 : 364-368, 1999

      9 Goldstein, A. L., "Thymosin β4 : a multi-functional regenerative peptide. Basic properties and clinical applications" 12 : 37-51, 2012

      10 Li, Q., "Thymosin beta4 regulation, expression and function in aortic valve interstitial cells" 11 : 726-735, 2002

      11 Dube, K. N., "Thymosin beta4 protein therapy for cardiac repair" 18 : 799-806, 2012

      12 Smart, N., "Thymosin beta4 induces adult epicardial progenitor mobilization and neovascularization" 445 : 177-182, 2006

      13 Sosne, G., "Thymosin beta 4 stimulates laminin-5 production independent of TGF-beta" 293 : 175-183, 2004

      14 Malinda, K., "Thymosin beta 4 stimulates directional migration of human umbilical vein endothelial cells" 11 : 474-481, 1997

      15 Sosne, G., "Thymosin beta 4 promotes corneal wound healing and decreases inflammation in vivo following alkali injury" 74 : 293-299, 2002

      16 Westerfield, M., "The zebrafish book: a guide for the laboratory use of zebrafish (Brachydanio rerio)" University of Oregon Press 1993

      17 Lee, S. I., "The role of thymosin beta 4 on odontogenic differentiation in human dental pulp cells" 8 : e61960-, 2013

      18 Markwald, R. R., "Structural development of endocardial cushions" 148 : 85-119, 1977

      19 Kim, S. H., "Specification of an anterior neuroectoderm patterning by Frizzled8a-mediated Wnt8b signalling during late gastrulation in zebrafish" 129 : 4443-4455, 2002

      20 Derynck, R., "Smad-dependent and Smadindependent pathways in TGF-beta family signalling" 425 : 577-584, 2003

      21 Bakkers, J., "Shaping the zebrafish heart : from left-right axis specification to epithelial tissue morphogenesis" 330 : 213-220, 2009

      22 Sribenja, S., "Roles and mechanisms of β-thymosins in cell migration and cancer metastasis : an update" 31 : 103-110, 2013

      23 Yelon, D., "Restricted expression of cardiac myosin genes reveals regulated aspects of heart tube assembly in zebrafish" 214 : 23-37, 1999

      24 양정희, "Opposing actions of Notch1 and VEGF in post-natal cardiac valve endothelial cells" ACADEMIC PRESS INC ELSEVIER SCIENCE 374 (374): 512-516, 2008

      25 Milan, D. J., "Notch1b and neuregulin are required for specification of central cardiac conduction tissue" 133 : 1125-1132, 2006

      26 Johnson, E. N., "NFATc1 mediates vascular endothelial growth factor-induced proliferation of human pulmonary valve endothelial cells" 278 : 1686-1692, 2003

      27 Gomez-Marquez, J., "High levels of mouse thymosin β4 mRNA in differentiating P19 embryonic cells and during evelopment of cardiovascular tissues" 1306 : 187-193, 1996

      28 Armstrong, E. J., "Heart valve development : endothelial cell signaling and differentiation" 95 : 459-470, 2004

      29 Huang, C. J., "Germ‐line transmission of a myocardium‐specific GFP transgene reveals critical regulatory elements in the cardiac myosin light chain 2 promoter of zebrafish" 228 : 30-40, 2003

      30 Beis, D., "Genetic and cellular analyses of zebrafish atrioventricular cushion and valve development" 132 : 4193-4204, 2005

      31 Ji, Y. I., "Expression patterns of Thymosin β4 and cancer stem cell marker CD133 in ovarian cancers" 19 : 237-245, 2013

      32 Stainier, D. Y., "Endocardial cushion formation in zebrafish" 67 : 49-56, 2002

      33 Jang, G. H., "Differential functions of genes regulated by VEGF-NFATc1 signaling pathway in the migration of pulmonary valve endothelial cells" ELSEVIER SCIENCE BV 584 : 141-146, 2010

      34 Smart, N., "De novo cardiomyocytes from within the activated adult heart after injury" 474 : 640-644, 2011

      35 진석원, "Cellular and molecular analyses of vascular tube and lumen formation in zebrafish" COMPANY OF BIOLOGISTS LTD 132 (132): 5199-5209, 2005

      36 Paranya, G., "Aortic valve endothelial cells undergo transforming growth factor-beta-mediated and non-transforming growth factor-beta-mediated transdifferentiation in vitro" 159 : 1335-1343, 2001

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      2023 평가예정 해외DB학술지평가 신청대상 (해외등재 학술지 평가)
      2020-01-01 평가 등재학술지 유지 (해외등재 학술지 평가) KCI등재
      2012-11-07 학술지명변경 한글명 : 분자와 세포 -> Molecules and Cells KCI등재
      2008-01-01 평가 SCI 등재 (등재유지) KCI등재
      2006-01-01 평가 등재학술지 유지 (등재유지) KCI등재
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      2001-01-01 평가 등재학술지 선정 (등재후보2차) KCI등재
      1998-07-01 평가 등재후보학술지 선정 (신규평가) KCI등재후보
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      기준연도 WOS-KCI 통합IF(2년) KCIF(2년) KCIF(3년)
      2016 2.77 0.19 1.85
      KCIF(4년) KCIF(5년) 중심성지수(3년) 즉시성지수
      1.37 1.11 0.379 0.03
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