Aging Is Associated with Low Thyroid State and Organ-Specific Sensitivity to Thyroxine

内科学 内分泌学 甲状腺 脱碘酶 激素 三碘甲状腺素 医学 促甲状腺激素
作者
Helena Rakov,Meri De Angelis,Kostja Renko,Georg Sebastian Hönes,Denise Zwanziger,Lars C. Moeller,Karl‐Werner Schramm,Dagmar Führer
出处
期刊:Thyroid [Mary Ann Liebert, Inc.]
卷期号:29 (12): 1723-1733 被引量:22
标识
DOI:10.1089/thy.2018.0377
摘要

Background: Serum thyroid state in older adults correlates with extended longevity. We hypothesized that age impacts not only systemic but also organ-specific thyroid state and response to thyroxine (T4). Methods: Young (3 months) and old (23 months) male mice were analyzed at baseline and after acute T4 challenge. Age effects on circulating thyrotropin (TSH) and thyroid hormone (TH) concentrations, transcript expression in the pituitary and thyroid were compared with organ-specific responses characterized by hepatic and cardiac content of TH and TH metabolites and expression of TH-target genes, as well as hepatic deiodinase 1 activity. Results: Circulating TH concentrations and hepatic and cardiac TH content were lower in old versus young mice. After injection with T4, conversion of T4 to triiodothyronine was decreased in old mice while TH transport in liver and heart was not affected. Organ-specific TH response was augmented in old mice in liver but not heart, indicating age- and tissue-specific sensitivity to TH. A compensatory increase of thyroid stimulating hormone subunit beta expression in the pituitary and increased serum TSH concentrations, but reduced expression of thyroid differentiation markers were found in old mice. Conclusions: We suggest that a reduced activity of the aged thyroid is responsible for the systemic low TH state in old mice. Further, divergent TH metabolism and tissue response in liver and heart occur after T4 treatment in an aged organism. These rodent data are in agreement with a much narrower window for T4 substitution in the older adults to avoid overtreatment.
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