Role of anatomical location, cellular phenotype and perfusion of adipose tissue in intermediary metabolism: A narrative review

StefaniaCamastra; EleFerrannini

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Role of anatomical location, cellular phenotype and perfusion of adipose tissue in intermediary metabolism: A narrative review

机译：Role of anatomical location, cellular phenotype and perfusion of adipose tissue in intermediary metabolism: A narrative review

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Abstract It is well-established that adipose tissue accumulation is associated with insulin resistance through multiple mechanisms. One major metabolic link is the classical Randle cycle: enhanced release of free fatty acids (FFA) from hydrolysis of adipose tissue triglycerides impedes insulin-mediated glucose uptake in muscle tissues. Less well studied are the different routes of this communication. First, white adipose tissue depots may be regionally distant from muscle (i.e., gluteal fat and diaphragm muscle) or contiguous to muscle but separated by a fascia (Scarpa’s fascia in the abdomen, fascia lata in the thigh). In this case, released FFA outflow through the venous drainage and merge into arterial plasma to be transported to muscle tissues. Next, cytosolic triglycerides can directly, i.e., within the cell, provide FFA to myocytes (but also pancreatic ?-cells, renal tubular cells, etc.). Finally, adipocyte layers or lumps may be adjacent to, but not anatomically segregated, from muscle, as is typically the case for epicardial fat and cardiomyocytes. As regulation of these three main delivery paths is different, their separate contribution to substrate competition at the whole-body level is uncertain.?Another important link between fat and muscle is vascular. In the resting state, blood flow is generally higher in adipose tissue than in muscle. In the insulinized state, fat blood flow is directly related to whole-body insulin resistance whereas muscle blood flow is not; consequently, fractional (i.e., flow-adjusted) glucose uptake is stimulated in muscle but not fat. Thus, reduced blood supply is a major factor for the impairment of in vivo insulin-mediated glucose uptake in both subcutaneous and visceral fat. In contrast, the insulin resistance of glucose uptake in resting skeletal muscle is predominantly a cellular defect.

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《Reviews in endocrine & metabolic disorders》 |2022年第1期|43-50|共8页
作者
StefaniaCamastra; EleFerrannini;
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作者单位

Department of Clinical & Experimental Medicine,University of Pisa;

Institute of Clinical Physiology,CNR;

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原文格式 PDF
正文语种英语
中图分类内分泌腺疾病及代谢病;
关键词
Adipose tissue; Adipocytes; Insulin sensitivity; Blood flow; FFA; Glucose metabolism;

Role of anatomical location, cellular phenotype and perfusion of adipose tissue in intermediary metabolism: A narrative review

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