The two new studies could help 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.
Previously, Professor Arne Akbar's group at University College London (UCL) showed that ageing 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.
In a study published in the journal 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 research provides a prototype mechanism of how nutrient and senescence signals converge to regulate the function of T lymphocytes.
The study conducted at UCL alongside colleagues from Complejo Hospitalario de Navarra, Pamplona, Spain also suggests that the function of old T lymphocytes could be reconstituted by blocking one of several molecules involved in the process.
Extra energy for the cell to divide was generated by the recycling of intracellular molecules, a process known as autophagy, researchers from UCL, Cancer Research UK, University of Oxford and University of Tor Vergata, Rome, Italy found.
This highlights the existence of a common signalling pathway in old/senescent T lymphocytes that controls their immune function as well as metabolism, further underscoring the intimate association between ageing and metabolism of T lymphocytes.
"It is therefore essential to understand reasons why immunity decreases and whether it is possible to counteract some of these changes," Akbar said.
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