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衰老过程中致密体和脂褐素的定量分析:形态学家的视角

Quantifying dense bodies and lipofuscin during aging: a morphologist's perspective.

作者信息

Schmucker Douglas L, Sachs Howard

机构信息

Cell Biology and Aging Section, San Francisco Veterans Affairs Medical Center, CA 94121, USA.

出版信息

Arch Gerontol Geriatr. 2002 May-Jun;34(3):249-61. doi: 10.1016/s0167-4943(01)00218-7.

Abstract

Secondary lysosomes, residual or dense bodies containing lipofuscin or age pigment accumulate in post-mitotic and inter-mitotic cells during aging. The consensus is that the accumulation of this auto-fluorescent material is an index of cellular senescence. Biochemical and morphological studies have independently demonstrated marked age-related increases in the cell and tissue contents of lipofuscin. Most morphological studies on aging have been qualitative, have included only two or three age groups and have not yielded data that are easily correlated with biochemical analyses. One of the best documented age-related changes in hepatocytes and cardiac myocytes is the accumulation of dense bodies and lipofuscin inclusions. Independent stereologic studies reported two- to eightfold age-related increases in the dense body volume fraction of rat hepatocytes. Furthermore, we reported a fourfold increase in the dense body volume fraction of cardiac myocytes in rats between 6 and 30 months of age. These and other studies confirm the use of quantitative morphology to estimate the increases in dense body and lipofuscin inclusions as indices of age. Whether or not the accumulated lipofuscin compromises cell functions in senescent animals has not been adequately addressed. On the one hand, there is little evidence that several-fold increases in this subcellular compartment impair the functional capacities of either hepatocytes or cardiac myocytes. On the other hand, the age-related accumulation of immunoprecipitable, but catalytically inactive, lysosomal enzymes in both liver and heart muscle may be a reflection of increased lipofuscin deposits in the dense bodies.

摘要

次级溶酶体,即含有脂褐素或老年色素的残余体或致密体,在衰老过程中会在有丝分裂后和有丝分裂间期的细胞中积累。目前的共识是,这种自发荧光物质的积累是细胞衰老的一个指标。生化和形态学研究已分别证明,脂褐素的细胞和组织含量随年龄增长显著增加。大多数关于衰老的形态学研究都是定性的,只包括两三个年龄组,且未得出易于与生化分析相关联的数据。肝细胞和心肌细胞中记录最详实的与年龄相关的变化之一,就是致密体和脂褐素包涵体的积累。独立的体视学研究报告称,大鼠肝细胞致密体体积分数随年龄增长增加了2至8倍。此外,我们报告了6至30月龄大鼠心肌细胞致密体体积分数增加了4倍。这些研究以及其他研究证实,利用定量形态学来估计致密体和脂褐素包涵体的增加,可作为衰老的指标。衰老动物体内积累的脂褐素是否会损害细胞功能,尚未得到充分探讨。一方面,几乎没有证据表明这个亚细胞区室增加数倍会损害肝细胞或心肌细胞的功能能力。另一方面,肝脏和心肌中与年龄相关的可免疫沉淀但无催化活性的溶酶体酶的积累,可能反映了致密体中脂褐素沉积物的增加。

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