期刊论文详细信息
Diabetology & Metabolic Syndrome
Human resistin and the RELM of Inflammation in diabesity
Kevin Gerard Culligan1  Fatima Al Hannan2 
[1] Royal College of Surgeons in Ireland – Bahrain, Adliya, Kingdom of Bahrain;Department of Biomedical Sciences, Royal College of Surgeons in Ireland – Bahrain, Building No. 2441, Road 2835, Busaiteen, Kingdom of Bahrain
关键词: RELMβ;    Resistin;    Inflammation;    Diabetes;    Obesity;    Diabesity;   
Others  :  1220760
DOI  :  10.1186/s13098-015-0050-3
 received in 2015-02-20, accepted in 2015-06-05,  发布年份 2015
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【 摘 要 】

The initial discovery of resistin and resistin-like molecules (RELMs) in rodents suggested a role for these adipocytokines in molecular linkage of obesity, Type 2 Diabetes mellitus and metabolic syndrome. Since then, it became apparent that the story of resistin and RELMs was very much of mice and men. The putative role of this adipokine family evolved from that of a conveyor of insulin resistance in rodents to instigator of inflammatory processes in humans. Structural dissimilarity, variance in distribution profiles and a lack of corroborating evidence for functional similarities separate the biological functions of resistin in humans from that of rodents. Although present in gross visceral fat deposits in humans, resistin is a component of inflammation, being released from infiltrating white blood cells of the sub-clinical chronic low grade inflammatory response accompanying obesity, rather than from the adipocyte itself. This led researchers to further explore the functions of the resistin family of proteins in inflammatory-related conditions such as atherosclerosis, as well as in cancers such as endometrial and gastric cancers. Although elevated levels of resistin have been found in these conditions, whether it is causative or as a result of these conditions still remains to be determined.

【 授权许可】

   
2015 Al Hannan and Culligan.

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