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Aramchol : ウィキペディア英語版
Aramchol
Aramchol is an investigational drug being developed by Galmed Pharmaceuticals as a first-in-class, potentially disease modifying treatment for nonalcoholic steatohepatitis, or NASH, a more advanced condition of non-alcoholic fatty liver disease.〔(【引用サイトリンク】url=http://www.ncbi.nlm.nih.gov/pubmed/24815326 )〕〔(【引用サイトリンク】url=http://www.jewocity.com/blog/fast-growing-israel-pharma-companies/13970 )〕〔(【引用サイトリンク】url=http://www.fiercebiotech.com/story/az-strikes-alderley-cancer-pact-cerenis-mulls-ipo-4d-start-microbiome-trial/2014-09-04 )〕〔(【引用サイトリンク】url=http://www.jwatch.org/na36528/2014/12/17/aramchol-nonalcoholic-fatty-liver-disease )
Aramchol, a conjugate of Cholic acid and Arachidic acid, is a first in class member of a novel family of synthetic Fatty-Acid / Bile-Acid Conjugates (FABACs). FABACs are composed of endogenic compounds, orally administrated with potentially good safety and tolerability parameters.〔(【引用サイトリンク】url=http://www.healio.com/hepatology/steatohepatitis-metabolic-liver-disease/news/online/%7B9413578d-4f31-4aaa-847c-4cae3a6784b8%7D/endopat-to-be-used-in-trial-with-potential-nash-drug-aramchol )
Aramchol affects liver fat metabolism and has been shown in a Phase IIa clinical study to significantly reduce liver fat content as well as improve metabolic parameters associated with fatty liver disease. Furthermore, it has been shown to be safe for use, and with no severe adverse effects.〔(【引用サイトリンク】url=http://www.rttnews.com/2387951/galmed-liver-drug-aramchol-gets-fda-s-fast-track-review.aspx )〕〔(【引用サイトリンク】url=http://www.sciencedaily.com/releases/2014/11/141121102825.htm )
Aramchol was initially intended to combine a cholesterol solubilising moiety (a saturated fatty acid) with a bile acid (cholic acid) acting as a vehicle to enable secretion into bile and entry into the enterohepatic circulation to solubilise bile stones.〔Gilat, T., Somjen G.J., et al. (2001). Fatty acid bile acid conjugates (FABACs)–new molecules for the prevention of cholesterol crystallisation in bile. '' 48(1),'' 75-79.〕 However, early in the development, it was observed that Aramchol reduced liver fat infiltration in animals fed a high fat, lithogenic diet.〔Gilat, T., Leikin-Frenkel, A., et al. (2003). Prevention of diet-induced fatty liver in experimental animals by the oral administration of a fatty acid bile acid conjugate (FABAC). Hepatology'' 48(1),'' 75-79.〕 This effect was confirmed in other animal models and the development plan was modified according to these findings, as fatty liver is an unmet need.
Aramchol has been shown to work by two parallel pathways, leading to synergistic effects:
==The SCD1 pathway==

Aramchol inhibits the activity of Stearoyl Coenzyme A Desaturase 1 (SCD1) in the liver. This is likely a direct effect since the mRNA of this and other lipogenic genes or the activities of nuclear receptors are not affected. The physiologic effects of SCD1 inhibition are: decreased synthesis of fatty acids, resulting in a decrease in storage triglycerides and other esters of fatty acids. This reduces liver fat (including triglycerides and free fatty acids), and results in an improvement in insulin resistance.〔Leikin-Frenkel A., Goldiner I., et al., (2008). Treatment of preestablished diet-induced fatty liver by oral fatty acid-bile acid conjugates in rodents, Eur J GastroenterolHepatol'' 20(12), 1205-13.〕 Aramchol’s mechanism of action, inhibition of the SCD1 enzyme, has been confirmed in human liver microsomes2 and in animal studies by showing a reduction of the SCD1 activity marker, the fatty acid ratio 16:1/16:0, following Aramchol treatment1. These studies showed that the SCD1 inhibition effect of Aramchol is partial (can reach to 70 to 83%). Unlike other SCD1 inhibitors, it was shown that Aramchol’s effects are non- atherogenic.〔 There are at present no known inhibitors of SCD1 with the established safety and efficacy profile of Aramachol.

抄文引用元・出典: フリー百科事典『 ウィキペディア(Wikipedia)
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