癌症和衰老的标志

M. Blagosklonny
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引用次数: 16

摘要

Gems和de magalh的一篇发人深省的文章指出,衰老的典型特征是癌症特征的表面模仿。我将他们的工作推进了一步,提出了基于等级原则和功能亢进理论的衰老特征。为了做到这一点,我首先重新审视了Hanahan和Weinberg在2000年提出的癌症特征。虽然癌症的六个特征是真实的,但它们并没有等级排列,即分子、细胞内、细胞、组织、有机体和有机体外。(如侵袭和血管生成是组织水平分子改变的表现;在机体水平上转移,而在宿主外观察到细胞不朽)。同样的分层方法也适用于老化。然而,与癌症不同,衰老不是一种分子疾病。其起源的最低水平是正常的细胞内信号通路,如mTOR,它驱动发育生长,并在以后的生活中变得功能亢进,导致与年龄有关的疾病,其总和是衰老。从蠕虫到人类,生物体衰老的关键标志是与年龄相关的疾病。此外,衰老的标志可以按照时间线排列,其中最初的功能亢进随后是功能障碍,器官损伤和功能下降。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hallmarks of cancer and hallmarks of aging
A thought-provoking article by Gems and de Magalhães suggests that canonic hallmarks of aging are superficial imitations of hallmarks of cancer. I took their work a step further and proposed hallmarks of aging based on a hierarchical principle and the hyperfunction theory. To do this, I first reexamine the hallmarks of cancer proposed by Hanahan and Weinberg in 2000. Although six hallmarks of cancer are genuine, they are not hierarchically arranged, i.e., molecular, intra-cellular, cellular, tissue, organismal and extra-organismal. (For example, invasion and angiogenesis are manifestations of molecular alterations on the tissue level; metastasis on the organismal level, whereas cell immortality is observed outside the host). The same hierarchical approach is applicable to aging. Unlike cancer, however, aging is not a molecular disease. The lowest level of its origin is normal intracellular signaling pathways such as mTOR that drive developmental growth and, later in life, become hyperfunctional, causing age-related diseases, whose sum is aging. The key hallmark of organismal aging, from worms to humans, are age-related diseases. In addition, hallmarks of aging can be arranged as a timeline, wherein initial hyperfunction is followed by dysfunction, organ damage and functional decline.
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