Takeshi Narita scite author profile

SummaryCaloric restriction (CR) can delay onset of several age‐related pathophysiologies and extend lifespan in various species, including rodents. CR also induces metabolic remodeling involved in activation of lipid metabolism, enhancement of mitochondrial biogenesis, and reduction of oxidative stress in white adipose tissue (WAT). In studies using genetically modified mice with extended lifespans, WAT characteristics influenced mammalian lifespans. However, molecular mechanisms underlying CR‐associated metabolic remodeling of WAT remain unclear. Sterol regulatory element‐binding protein‐1c (Srebp‐1c), a master transcription factor of fatty acid (FA) biosynthesis, is responsible for the pathogenesis of fatty liver (steatosis). Our study showed that, under CR conditions, Srebp‐1c enhanced mitochondrial biogenesis via increased expression of peroxisome proliferator‐activated receptor gamma coactivator‐1α (Pgc‐1α) and upregulated expression of proteins involved in FA biosynthesis within WAT. However, via Srebp‐1c, most of these CR‐associated metabolic alterations were not observed in other tissues, including the liver. Moreover, our data indicated that Srebp‐1c may be an important factor both for CR‐associated suppression of oxidative stress, through increased synthesis of glutathione in WAT, and for the prolongevity action of CR. Our results strongly suggested that Srebp‐1c, the primary FA biosynthesis‐promoting transcriptional factor implicated in fatty liver disease, is also the food shortage‐responsive factor in WAT. This indicated that Srebp‐1c is a key regulator of metabolic remodeling leading to the beneficial effects of CR.

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Improvement of 9Cr-ODS martensitic steel properties by controlling excess oxygen and titanium contents

Ohtsuka¹,

Ukai²,

Fujiwara³

et al. 2004

Journal of Nuclear Materials

111

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Improvement of Creep Strength of 9CrODS Martensitic Steel by Controlling Excess Oxygen and Titanium Concentrations

Ohtsuka¹,

Ukai²,

Fujiwara³

et al. 2005

Mater. Trans.

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The effects of chemical compositions (titanium, oxygen) and consolidation temperature on high-temperature mechanical properties of 9Cr-oxide dispersion strengthened steel (9CrODS steel) were investigated. A possible high-temperature strengthening mechanism of 9CrODS steel was discussed based on the experimental results. Creep strength of 9CrODS steel at 973 K was remarkably improved when titanium concentration was 0.35 mass%. A higher amount of added titanium than 0.2 mass% was effective for providing consistently reliable manufacturing of high strength 9CrODS steel because it reduced the effect of oxygen contamination on high-temperature strength. The fraction of elongated -ferrite grains, which had an ultra-fine oxide particle dispersion, tended to increase with increasing titanium. The elongated grains were considered to improve creep strength of 9CrODS steel. It was also found that creep strength was degraded by elevating the consolidation temperature from 1423 K to 1473 K.

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Caloric restriction-associated remodeling of rat white adipose tissue: effects on the growth hormone/insulin-like growth factor-1 axis, sterol regulatory element binding protein-1, and macrophage infiltration

Chujo

Fujii

Okita

et al. 2012

AGE

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The role of the growth hormone (GH)-insulin-like growth factor (IGF)-1 axis in the lifelong caloric restriction (CR)-associated remodeling of white adipose tissue (WAT), adipocyte size, and gene expression profiles was explored in this study. We analyzed the WAT morphology of 6-7-month-old wild-type Wistar rats fed ad libitum (WdAL) or subjected to CR (WdCR), and of heterozygous transgenic dwarf rats bearing an anti-sense GH transgene fed ad libitum (TgAL) or subjected to CR (TgCR). Although less effective in TgAL, the adipocyte size was significantly reduced in WdCR compared with WdAL. This CR effect was blunted in Tg rats. We also used high-density oligonucleotide microarrays to examine the gene expression profile of WAT of WdAL, WdCR, and TgAL rats. The gene expression profile of WdCR, but not TgAL, differed greatly from that of WdAL. The gene clusters with the largest changes induced by CR but not by Tg were genes involved in lipid biosynthesis and inflammation, particularly sterol regulatory element binding proteins (SREBPs)-regulated and macrophage-related genes, respectively. Real-time reverse-transcription polymerase chain reaction analysis confirmed that the expression of SREBP-1 and its downstream targets was upregulated, whereas the macrophage-related genes were downregulated in WdCR, but not in TgAL. In addition, CR affected the gene expression profile of Tg rats similarly to wild-type rats. Our findings suggest that CR-associated remodeling of WAT, which involves SREBP-1-mediated transcriptional activation and suppression of macrophage infiltration, is regulated in a GH-IGF-1-independent manner. AGE (2013) 35:1143-1156 DOI 10.1007 Yoshikazu Chujo, Namiki Fujii, Naoyuki Okita, and Tomokazu Konishi contributed equally to this work. Electronic supplementary materialThe online version of this article

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In situ synthesis of porous ceramics with a framework structure of aluminium borate whisker

Narita

Ogawa

et al. 1998

Journal of Materials Science

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Takeshi Narita

Sterol regulatory element-binding protein-1c orchestrates metabolic remodeling of white adipose tissue by caloric restriction

Improvement of 9Cr-ODS martensitic steel properties by controlling excess oxygen and titanium contents

Improvement of Creep Strength of 9CrODS Martensitic Steel by Controlling Excess Oxygen and Titanium Concentrations

Caloric restriction-associated remodeling of rat white adipose tissue: effects on the growth hormone/insulin-like growth factor-1 axis, sterol regulatory element binding protein-1, and macrophage infiltration

In situ synthesis of porous ceramics with a framework structure of aluminium borate whisker

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