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Aging is an organ-specific process: changes in homeostasis of iron and redox proteins in the rat

机译:衰老是器官特定的过程:大鼠中铁和氧化还原蛋白体内稳态的变化

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摘要

Organ-specific changes of iron- and redox-related proteins occur with age in the rat. Ferritin, the major iron storage and detoxifying protein, as well as the proteins of the methionine-centered redox cycle (MCRC) were examined in old and young animals, and showed organ-dependent changes. In spleens and livers of aged rats, ferritin (protein) levels were greater than in young ones, and their iron saturation increased, rendering higher ferritin-bound iron (FtBI). Iron saturation of the ferritin molecule in the tongues and sternohyoids of old rats was lower but ferritin level was higher than in young rats, resulting in increased FtBI with age. Ferritin level in the esophagus of older rats was lower than in young rats but its molecular iron content higher thus the total FtBI remained the same. In the larynx, both ferritin and its iron content were the same in young and old animals. MCRC proteins were measured in livers and spleens only. With aging, methionine sulfoxide reductase A and B (MsrA and MsrB) levels in livers and spleens decreased. Thioredoxin1 (Trx) and Trx-reductase1 were elevated in old spleens, but reduced in livers. Aged spleens showed reduced Msr isozyme activity; but in the liver, its activity increased. mRNA changes with age were monitored and found to be organ specific. These organ-specific changes could reflect the different challenges and the selective pathways of each organ and its resultant capacity to cope with aging.
机译:铁和氧化还原相关蛋白的器官特异性变化随年龄的增长而发生。铁蛋白,主要的铁存储和解毒蛋白以及蛋氨酸中心氧化还原循环(MCRC)的蛋白已在成年和幼年动物中进行了检查,并显示了器官依赖性变化。在老年大鼠的脾脏和肝脏中,铁蛋白(蛋白质)水平高于年轻大鼠,并且铁饱和度增加,从而使铁蛋白结合铁(FtBI)升高。老老鼠的舌头和胸骨舌骨中的铁蛋白分子的铁饱和度较低,但铁蛋白水平却高于年轻大鼠,导致FtBI随着年龄的增长而增加。老年大鼠食管中的铁蛋白水平低于年轻大鼠,但其分子铁含量较高,因此总FtBI保持不变。在喉中,年轻动物和老年动物的铁蛋白及其铁含量均相同。仅在肝脏和脾脏中测量了MCRC蛋白。随着衰老,肝脏和脾脏中的蛋氨酸亚砜还原酶A和B(MsrA和MsrB)水平降低。硫氧还蛋白1(Trx)和Trx-还原酶1在老脾脏中升高,但在肝脏中降低。脾脏衰老表明Msr同工酶活性降低。但在肝脏中,其活性增加。监测随年龄的mRNA变化,发现是器官特异性的。这些特定于器官的变化可能反映了每个器官的不同挑战和选择性途径,以及由此产生的应对衰老的能力。

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