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首页> 外文期刊>Life sciences >ZINC AND METALLOTHIONEINS ON CELLULAR IMMUNE EFFECTIVENESS DURING LIVER REGENERATION IN YOUNG AND OLD MICE
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ZINC AND METALLOTHIONEINS ON CELLULAR IMMUNE EFFECTIVENESS DURING LIVER REGENERATION IN YOUNG AND OLD MICE

机译:锌和金属硫蛋白对幼鼠和老鼠肝脏再生过程中细胞免疫功能的影响

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摘要

Partial hepatectomy in young mice (pHx) induces thymic atrophy, disregulation of thymocytes subsets and a strong accumulation of zinc in thymic tissue after 1-2 days of liver regeneration. Zinc is relevant for good immune functioning. Restoration of zinc into both the thymus and thymocytes subsets in the late period of liver regeneration is observed in young pHx mice. These findings have suggested a link between the thymus and the liver influencing T-cell functions and involving zinc. This kind of link could be relevant in aging because thymic involution, negative crude zinc balance and crippled immune functions are constant events. The preminence of a liver extrathymic T-cell pathway after pHx or during aging has been suggested. Thus the study of pHx in young and old mice may offer a good model to better understand the role played both by thymic involution and by liver extrathymic T-cell pathway and the role of zinc in these physiological processes during aging. Young pHx mice after 1-2 days of liver regeneration show: reduced thymic endocrine activity, increment of double negative (DN) thymocytes subsets, impairment of peripheral immune efficiency (PHA, NK activity and IL-2) and negative crude zinc balance, which are all restored in the late period of liver regeneration. By contrast the thymic and peripheral immune defects and the negative crude zinc balance, already present in old sham mice, are not modified during liver regeneration in old pHx mice. Circulating leukocytes and lymphocytes are not significantly modified both in young and old pHx mice as compared to respective sham controls. Zinc may also be crucial for extrathymic T-cells pathway, being preminent in aging, rather than in young age, due to its metallothioneins (MT) binding capacity. MT are significantly increased in young pHx and in aging inducing a low zinc-free quota for thymic and peripheral immune efficiency in young pHx mice, and for extrathymic T-cell pathway, in old age. Thus low zinc bioavailability, due to MT, may play a pivotal role, not only for thymocytes but also for liver extrathymic T-cell pathway. [References: 63]
机译:肝脏再生1-2天后,幼鼠部分肝切除术(pHx)引起胸腺萎缩,胸腺细胞亚群失调以及胸腺组织中锌的大量积累。锌与良好的免疫功能有关。在年轻的pHx小鼠中,观察到在肝再生后期锌可恢复到胸腺和胸腺细胞亚群中。这些发现表明胸腺和肝脏之间存在联系,影响T细胞功能并涉及锌。这种联系可能与衰老有关,因为胸腺退化,负的粗锌平衡和免疫功能受损是持续的事件。有人建议在pHx之后或衰老过程中存在肝脏胸腺T细胞通路的优势。因此,对年幼小鼠和年老小鼠进行pHx的研究可以提供一个很好的模型,以更好地了解胸腺退化和肝胸腺T细胞途径在衰老过程中锌的作用。肝脏再生1-2天后的年轻pHx小鼠显示:胸腺内分泌活性降低,双阴性(DN)胸腺细胞亚群增加,外周免疫效率(PHA,NK活性和IL-2)受损以及粗锌平衡阴性,这在肝脏再生的后期都恢复了。相比之下,旧假小鼠中已经存在的胸腺和外周免疫缺陷以及负的粗锌平衡,在旧pHx小鼠的肝脏再生过程中没有被改变。与相应的假对照组相比,在年轻和年老的pHx小鼠中循环白细胞和淋巴细胞均未显着改变。锌对于胸腺T细胞途径也可能至关重要,由于其金属硫蛋白(MT)的结合能力,锌在衰老而不是年轻人中占优势。 MT在年轻的pHx和衰老中显着增加,从而导致年轻的pHx小鼠的胸腺和外周免疫效率以及年老的胸腺T细胞途径的无锌配额较低。因此,由于MT而导致的低锌生物利用度可能不仅对胸腺细胞而且对肝胸腺T细胞途径都起关键作用。 [参考:63]

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