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首页> 外文期刊>Advances in Experimental Medicine and Biology >Cellular Mechanisms Driving Sex Differences in Adipose Tissue Biology and Body Shape in Humans and Mouse Models
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Cellular Mechanisms Driving Sex Differences in Adipose Tissue Biology and Body Shape in Humans and Mouse Models

机译:在人类和小鼠模型中推动脂肪组织生物学和身体形状的性差异的细胞机制

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摘要

Abstract Sex differences in adipose tissue distribution and the metabolic, endocrine, and immune functions of different anatomical fat depots have been described, but they are incompletely documented in the literature. It is becoming increasingly clear that adipose depots serve distinct functions in males and females and have specific physiological roles. However, the mechanisms that regulate the size and function of specific adipose tissues in men and women remain poorly understood. New insights from mouse models have advanced our understanding of depot differences in adipose growth and remodeling via the proliferation and differentiation of adipose progenitors that can expand adipocyte number in the tissue or simply replace dysfunctional older and larger adipocytes. A limited ability of a depot to expand or remodel can lead to excessive adipocyte hypertrophy, which is often correlated with metabolic dysfunction. However, the relationship of adipocyte size and function varies by depot and sex. For example, femoral adipose tissues of premeno-pausal women appear to have a greater capacity for adipose expansion via hyperpla-sia and hypertrophy; although larger, these gluteal-femoral adipocytes remain insulin sensitive. The microenvironment of specific depots, including the composition of the extracellular matrix and cellular composition, as well as cell-autonomous genetic differences, influences sex- and depot-dependent metabolic and growth properties. Although there are some species differences, studies of the molecular and physiological determinants of sex differences in adipocyte growth and function in humans and rodents are both needed for understanding sex differences in health and disease.
机译:摘要已经描述了脂肪组织分布的性别差异以及不同解剖脂肪库的代谢,内分泌和免疫功能,但它们在文献中不完全记录。越来越清楚的是,脂肪仓库在雄性和女性中提供不同的功能,并且具有特异性的生理作用。然而,调节男性和女性特异性脂肪组织的大小和功能的机制仍然明白很差。来自小鼠模型的新见解已经提出了我们对脂肪生长和通过脂肪祖细胞的增殖和分化进行重塑的脂肪凋亡的理解,这可以扩大组织中的脂肪细胞数或仅取代功能障碍更老和较大的脂肪细胞。仓库扩张或重塑的有限能力可以导致过度的脂肪细胞肥大,这通常与代谢功能障碍相关。然而,脂肪细胞尺寸和功能的关系因仓库和性而异。例如,前高分妇女的股骨脂肪组织似乎通过超增性和肥大具有更大的脂肪扩增能力;虽然较大,这些臀部 - 股骨脂肪细胞仍然是胰岛素敏感性。特定贮库的微环境,包括细胞外基质和细胞组合物的组成,以及细胞 - 自主遗传差异,影响性别和储存依赖性代谢和生长性质。虽然有一些物种差异,但是对脂肪细胞生长和人类和啮齿动物功能的性差异的分子和生理决定因素都需要健康和疾病的性别差异。

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