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Shingo Kajimura

UCSF Diabetes Center and Department of Cell and Tissue Biology

University of California, San Francisco

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PUBLICATIONS

Effects of insulin-like growth factors (IGF-I and -II) on growth hormone and prolactin release and gene expression in euryhaline tilapia, Oreochromis mossambicus.

General and comparative endocrinology Jul, 2002 | Pubmed ID: 12225763

Effects of environmental osmolality on release of prolactin, growth hormone and ACTH from the tilapia pituitary.

General and comparative endocrinology Sep, 2002 | Pubmed ID: 12392682

In vitro effects of cortisol on the release and gene expression of prolactin and growth hormone in the tilapia, Oreochromis mossambicus.

General and comparative endocrinology Jan, 2004 | Pubmed ID: 14644651

Insulin-like growth factor-binding protein-1 (IGFBP-1) mediates hypoxia-induced embryonic growth and developmental retardation.

Proceedings of the National Academy of Sciences of the United States of America Jan, 2005 | Pubmed ID: 15644436

Physiological concentrations of ouabain rapidly inhibit prolactin release from the tilapia pituitary.

General and comparative endocrinology Sep, 2005 | Pubmed ID: 15922343

Understanding hypoxia-induced gene expression in early development: in vitro and in vivo analysis of hypoxia-inducible factor 1-regulated zebra fish insulin-like growth factor binding protein 1 gene expression.

Molecular and cellular biology Feb, 2006 | Pubmed ID: 16428465

Prolactin receptor and proliferating/apoptotic cells in esophagus of the Mozambique tilapia (Oreochromis mossambicus) in fresh water and in seawater.

General and comparative endocrinology Jun-Jul, 2007 | Pubmed ID: 17418192

Transcriptional control of brown fat determination by PRDM16.

Cell metabolism Jul, 2007 | Pubmed ID: 17618855

Regulation of the brown and white fat gene programs through a PRDM16/CtBP transcriptional complex.

Genes & development May, 2008 | Pubmed ID: 18483224

PRDM16 controls a brown fat/skeletal muscle switch.

Nature Aug, 2008 | Pubmed ID: 18719582

Modulation of PGC-1 coactivator pathways in brown fat differentiation through LRP130.

The Journal of biological chemistry Nov, 2008 | Pubmed ID: 18728005

Transcriptional control of brown adipocyte development and physiological function--of mice and men.

Genes & development Apr, 2009 | Pubmed ID: 19339685

Initiation of myoblast to brown fat switch by a PRDM16-C/EBP-beta transcriptional complex.

Nature Aug, 2009 | Pubmed ID: 19641492

Transcriptional control of brown fat development.

Cell metabolism Apr, 2010 | Pubmed ID: 20374957

Anti-diabetic drugs inhibit obesity-linked phosphorylation of PPARgamma by Cdk5.

Nature Jul, 2010 | Pubmed ID: 20651683

Prdm16 determines the thermogenic program of subcutaneous white adipose tissue in mice.

The Journal of clinical investigation Jan, 2011 | Pubmed ID: 21123942

Role of IGF signaling in catch-up growth and accelerated temporal development in zebrafish embryos in response to oxygen availability.

Development (Cambridge, England) Feb, 2011 | Pubmed ID: 21266413

A PGC1-Î±-dependent myokine that drives brown-fat-like development of white fat and thermogenesis.

Nature Jan, 2012 | Pubmed ID: 22237023

PPARÎ³ agonists induce a white-to-brown fat conversion through stabilization of PRDM16 protein.

Cell metabolism Mar, 2012 | Pubmed ID: 22405074

A novel therapeutic approach to treating obesity through modulation of TGFÎ² signaling.

Endocrinology Jul, 2012 | Pubmed ID: 22549226

Relevance of brown adipose tissue in infancy and adolescence.

Pediatric research Jan, 2013 | Pubmed ID: 23090604

Human BAT possesses molecular signatures that resemble beige/brite cells.

PloS one , 2012 | Pubmed ID: 23166672

Regulation of early adipose commitment by zfp521.

PLoS biology Nov, 2012 | Pubmed ID: 23209378

INSTITUTIONS

University of California, San Francisco

JOVE ARTICLES

Isolation and Differentiation of Stromal Vascular Cells to Beige/Brite Cells

Ulrike Liisberg Aune^1,2,3,

Lauren Ruiz¹,

Shingo Kajimura¹

¹UCSF Diabetes Center and Department of Cell and Tissue Biology, University of California, San Francisco ,

²Department of Biology, University of Copenhagen, Denmark,

³, National Institute of Nutrition and Seafood Research, Bergen, Norway

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Shingo Kajimura

.css-o250i3{font-size:18px;font-family:Open Sans,sans-serif;line-height:21.6px;}UCSF Diabetes Center and Department of Cell and Tissue Biology

University of California, San Francisco

Isolation and Differentiation of Stromal Vascular Cells to Beige/Brite Cells

UCSF Diabetes Center and Department of Cell and Tissue Biology