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Chronobiologic study of the GH-IGF1 axis and the ageing immune system
Gianluigi Mazzoccoli, Francesco Giuliani, Michele Inglese, Nunzia Marzulli, Mariangela Pia Dagostino, Angelo De Cata, Antonio Greco, Stefano Carughi, Roberto Tarquini
Jazyk angličtina Země Česko
NLK
Free Medical Journals
od 2003 do 2013
Freely Accessible Science Journals
od 2003 do 2013
ROAD: Directory of Open Access Scholarly Resources
od 2002
- MeSH
- biomedicínský výzkum MeSH
- chronobiologické jevy MeSH
- cirkadiánní rytmus MeSH
- endokrinní systém enzymologie imunologie metabolismus MeSH
- experimenty na lidech MeSH
- imunitní systém enzymologie imunologie metabolismus MeSH
- imunologické faktory imunologie izolace a purifikace metabolismus MeSH
- insulinu podobný růstový faktor I imunologie izolace a purifikace metabolismus MeSH
- lidé středního věku MeSH
- lidé MeSH
- lidský růstový hormon imunologie izolace a purifikace metabolismus MeSH
- lymfocyty fyziologie imunologie metabolismus MeSH
- nervový systém enzymologie imunologie metabolismus MeSH
- proliferace buněk MeSH
- senioři MeSH
- stárnutí fyziologie genetika imunologie MeSH
- statistika jako téma MeSH
- Check Tag
- lidé středního věku MeSH
- lidé MeSH
- senioři MeSH
One of the many systems that weakens as we age is our immune system and there is a reduction in the GH-IGF1 axis activity with increasing age. In this study we evaluated the immune system and the GH-IGF1 axis function in healthy ageing. CD3, CD4, CD20, CD25, HLA-DR and GH showed acrophase during the night, whereas CD8, CD16 and TCRgamma delta expressing cells showed acrophase during the day. MESOR of CD3 was higher in the old aged subjects, MESOR of CD20 and CD20 values at 14:00h and at 02:00h were higher in the young middle aged subjects, MESOR of CD25 and CD25 values at 10:00 were higher in the elderly subjects, MESOR of HLA-DR was higher in the young middle aged subjects, whereas MESOR of DR+ T cells and HLA-DR at 02:00h were higher in the elderly subjects, MESOR of TCRgamma delta bearing cells was higher in the elderly subjects, GH value at 18:00h was also higher in the elderly subjects, and MESOR of IGF1 was higher in the young middle aged subjects. There was a statistically significant difference for the acrophases of CD25, HLA-DR and IGF1. There were different and opposing correlations among lymphocyte subpopulations and GH-IGF1 axis hormones in young and middle aged subjects in comparison with old aged subjects. Linear regression evidenced a statistically significant positive trend between age and the 24h mean of CD3 and CD25 and a statistically significant negative trend between age and the 24h mean of CD20 and GH. In conclusion, ageing is associated with an altered GH and IGF1 secretion, with decreased peripheral B cell compartment, increased peripheral T cell compartment and alterations of circadian rhythmicity.
Citace poskytuje Crossref.org
Lit.: 51
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- $a Lit.: 51
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- $a One of the many systems that weakens as we age is our immune system and there is a reduction in the GH-IGF1 axis activity with increasing age. In this study we evaluated the immune system and the GH-IGF1 axis function in healthy ageing. CD3, CD4, CD20, CD25, HLA-DR and GH showed acrophase during the night, whereas CD8, CD16 and TCRgamma delta expressing cells showed acrophase during the day. MESOR of CD3 was higher in the old aged subjects, MESOR of CD20 and CD20 values at 14:00h and at 02:00h were higher in the young middle aged subjects, MESOR of CD25 and CD25 values at 10:00 were higher in the elderly subjects, MESOR of HLA-DR was higher in the young middle aged subjects, whereas MESOR of DR+ T cells and HLA-DR at 02:00h were higher in the elderly subjects, MESOR of TCRgamma delta bearing cells was higher in the elderly subjects, GH value at 18:00h was also higher in the elderly subjects, and MESOR of IGF1 was higher in the young middle aged subjects. There was a statistically significant difference for the acrophases of CD25, HLA-DR and IGF1. There were different and opposing correlations among lymphocyte subpopulations and GH-IGF1 axis hormones in young and middle aged subjects in comparison with old aged subjects. Linear regression evidenced a statistically significant positive trend between age and the 24h mean of CD3 and CD25 and a statistically significant negative trend between age and the 24h mean of CD20 and GH. In conclusion, ageing is associated with an altered GH and IGF1 secretion, with decreased peripheral B cell compartment, increased peripheral T cell compartment and alterations of circadian rhythmicity.
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