Background: Evolutionary theory and empirical evidence suggest that aging is a process of gradual accumulation of damage in cells and tissues of the body. The progressive loss of ability to interact effectively with environmental stimuli is accompanied by progressive modification and adaptations that are influenced by lifestyle and genetic background of the individual. These affect the ability to age successfully, defined both as longevity and/or escaping the major age-related diseases. Some of the most important characteristics of adaptive immunity in aging are compatible with this assumption. Actually, the antigenic load results in the progressive generation of a chronic low grade inflammatory response involved in body and brain aging. Methods: Data on genetic background and immune system have been obtained in the last 10 years studying Sicilian centenarians and subjects affected by aging related diseases. Results: Studies have been focused on the genetic background predisposing to aging related diseases. Data gathered on gene variants in cytokine, pathogen-related pattern receptors or acute phase response genes allow the research group to define a complex trait in which the antagonistic pleiotropy of regulating immune-inflammatory mechanisms might play a central role in predisposing to a large array of age-related diseases and in determining lifespan expectancy. Conclusions: These findings suggest that different alleles at different immune-related genes coding for pro- or anti-inflammatory molecules may affect individual life-span expectancy and might be useful markers for the evaluation of aging-associated disease risk.

Lio D. (2012). Senescence Markers. In 1st Joint Meeting of Pathology and Laboratory Diagnostics, 2012 September 12-15, Udine, Italy. (pp.00-00). Elsevier Health Sciences.

Senescence Markers

LIO, Domenico
2012-01-01

Abstract

Background: Evolutionary theory and empirical evidence suggest that aging is a process of gradual accumulation of damage in cells and tissues of the body. The progressive loss of ability to interact effectively with environmental stimuli is accompanied by progressive modification and adaptations that are influenced by lifestyle and genetic background of the individual. These affect the ability to age successfully, defined both as longevity and/or escaping the major age-related diseases. Some of the most important characteristics of adaptive immunity in aging are compatible with this assumption. Actually, the antigenic load results in the progressive generation of a chronic low grade inflammatory response involved in body and brain aging. Methods: Data on genetic background and immune system have been obtained in the last 10 years studying Sicilian centenarians and subjects affected by aging related diseases. Results: Studies have been focused on the genetic background predisposing to aging related diseases. Data gathered on gene variants in cytokine, pathogen-related pattern receptors or acute phase response genes allow the research group to define a complex trait in which the antagonistic pleiotropy of regulating immune-inflammatory mechanisms might play a central role in predisposing to a large array of age-related diseases and in determining lifespan expectancy. Conclusions: These findings suggest that different alleles at different immune-related genes coding for pro- or anti-inflammatory molecules may affect individual life-span expectancy and might be useful markers for the evaluation of aging-associated disease risk.
Settore MED/05 - Patologia Clinica
set-2012
1st Joint Meeting of Pathology and Laboratory Diagnostics
Udine Congress and Exhibition Centre, Udine, Italy
September 12-15, 2012
2012
1
Lio D. (2012). Senescence Markers. In 1st Joint Meeting of Pathology and Laboratory Diagnostics, 2012 September 12-15, Udine, Italy. (pp.00-00). Elsevier Health Sciences.
Proceedings (atti dei congressi)
Lio D.
File in questo prodotto:
File Dimensione Formato  
abstracts.pdf

Solo gestori archvio

Descrizione: fascicolo degli abstract
Dimensione 831.11 kB
Formato Adobe PDF
831.11 kB Adobe PDF   Visualizza/Apri   Richiedi una copia

I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.

Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10447/74743
Citazioni
  • ???jsp.display-item.citation.pmc??? ND
  • Scopus ND
  • ???jsp.display-item.citation.isi??? ND
social impact