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老人不宜经常节食或天天素食 精选

已有 4727 次阅读 2014-8-26 10:26 |个人分类:期刊论文|系统分类:论文交流| 长寿, 老人, 节食

过去已有无数证据表明节食即热量限制(calorie restriction)能延长动物寿命,也能改善人的代谢状况,如增强胰岛素敏感性,避免发生糖尿病和心血管病,还能降低患癌风险。至于节食对于免疫系统尤其是免疫细胞功能的影响,目前还所知甚少。

最近,英国伦敦大学学院与西班牙科学家在《自然—免疫学》(Nature Immunology)上发表论文称,营养、代谢和免疫均参与衰老过程,并证明营养与衰老信号共同调节T淋巴细胞功能,从而打消了人们长期以来对它们是否有关联的疑虑。

当人衰老时,免疫功能下降,患传染病和得癌症的机会增大,而且严重程度也增加。同时,接种疫苗的抗病效果会随年龄增长而降低。导致这个现象的根本原因是T细胞的衰老,而采用丝裂原激活蛋白的激酶(MAPK)p38 抑制剂可以逆转T细胞衰老,提示可以通过药物控制免疫功能因衰老而下降。

该研究发现,T细胞中的p38可被低水平营养和DNA损伤信号所激活,从而自动发生磷酸化。低营养与基因损伤对p38的活化依赖AMP激酶(AMPK)及骨架蛋白TAB1的共同作用,从而抑制端粒酶活性、T细胞增殖和T细胞抗原受体(TCR)表达。

英国癌症研究院、伦敦大学学院、牛津大学意大利科学家在《临床调查杂志》(JCI)发表的一篇最新论文也表明,抑制p38的激活可以恢复衰老T细胞的免疫功能,包括促进线粒体增殖和细胞分裂,而这得益于自噬活性增强。

由此可见,p38的活性可以通过药物或食物进行控制。现在已有制药公司研制出p38抑制剂,用于缓解慢性炎症。但是,通过食物调节p38的活性更健康和更简便。由于p38可被低营养(饥饿)激活,故在日常生活中老年人应注意加强营养,而不是经常节食或天天素食。


Are you as old as what you eat? Researchers learn how to rejuvenate aging immune cells

Date:
August 24, 2014
Source:
Biotechnology and Biological Sciences Research Council
Summary:
Researchers have demonstrated how an interplay between nutrition, metabolism and immunity is involved in the process of aging. It has been suspected for a long time that these are linked, and this paper provides a prototype mechanism of how nutrient and senescence signals converge to regulate the function of T lymphocytes.


Researchers from UCL (University College London) have demonstrated how an interplay between nutrition, metabolism and immunity is involved in the process of aging.

The two new studies, supported by the Biotechnology and Biological Sciences Research Council (BBSRC), could help to enhance our immunity to disease through dietary intervention and help make existing immune system therapies more effective.

As we age our immune systems decline. Older people suffer from increased incidence and severity of both infections and cancer. In addition, vaccination becomes less efficient with age.

In previous BBSRC funded work, Professor Arne Akbar's group at UCL showed that aging in immune system cells known as 'T lymphocytes' was controlled by a molecule called 'p38 MAPK' that acts as a brake to prevent certain cellular functions.

They found that this braking action could be reversed by using a p38 MAPK inhibitor, suggesting the possibility of rejuvenating old T cells using drug treatment.

In a new study published in Nature Immunology the group shows that p38 MAPK is activated by low nutrient levels, coupled with signals associated with age, or senescence, within the cell.

It has been suspected for a long time that nutrition, metabolism and immunity are linked and this paper provides a prototype mechanism of how nutrient and senescence signals converge to regulate the function of T lymphocytes.

The study also suggests that the function of old T lymphocytes could be reconstituted by blocking one of several molecules involved in the process. The research was conducted at UCL alongside colleagues from Complejo Hospitalario de Navarra, Pamplona, Spain.

The second paper, published in The Journal of Clinical Investigation, showed that blocking p38 MAPK boosted the fitness of cells that had shown signs of aging; improving the function of mitochondria (the cellular batteries) and enhancing their ability to divide.

Extra energy for the cell to divide was generated by the recycling of intracellular molecules, a process known as autophagy. This highlights the existence of a common signaling pathway in old/senescent T lymphocytes that controls their immune function as well as metabolism, further underscoring the intimate association between aging and metabolism of T lymphocytes.

This study was conducted by researchers from UCL, Cancer Research UK, University of Oxford and University of Tor Vergata, Rome, Italy.

Professor Arne Akbar said: "Our life expectancy at birth is now twice as long as it was 150 years ago and our lifespans are on the increase. Healthcare costs associated with aging are immense and there will be an increasing number of older people in our population who will have a lower quality of life due in part to immune decline. It is therefore essential to understand reasons why immunity decreases and whether it is possible to counteract some of these changes.

"An important question is whether this knowledge can be used to enhance immunity during aging. Many drug companies have already developed p38 inhibitors in attempts to treat inflammatory diseases. One new possibility for their use is that these compounds could be used to enhance immunity in older subjects. Another possibility is that dietary instead of drug intervention could be used to enhance immunity since metabolism and senescence are two sides of the same coin."

Story Source:

The above story is based on materials provided by Biotechnology and Biological Sciences Research Council. Note: Materials may be edited for content and length.

Journal Reference:

  1. Alessio Lanna, Sian M Henson, David Escors, Arne N Akbar. The kinase p38 activated by the metabolic regulator AMPK and scaffold TAB1 drives the senescence of human T cells. Nature Immunology, 2014; DOI: 10.1038/ni.2981




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