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Both age and gender affect thymic output: more recent thymic migrants in females than males as they age

机译:年龄和性别都会影响胸腺输出:随着年龄的增长女性中的胸腺迁徙者多于男性

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摘要

The thymus undergoes age-associated involution, with studies showing thymic size decreasing from birth at a rate of approximately 3% per year until middle age, and at a rate of 1% per year thereafter. The aim of this study was to determine the effect of thymic atrophy on T-lymphocyte production by the thymus, and to clarify the ongoing uncertainty regarding gender differences in thymic function. We quantified recent thymic emigrants (RTEs) in blood through the measurement of signal joint T-cell receptor rearrangement excision circles (sjTRECs), and showed that the decline in the number of RTEs in the blood with increasing age is gender-linked. Peripheral blood from females contained significantly higher levels of sjTRECs per CD3+ T cell than blood from males (P = 0·002), despite there being no significant gender difference in the absolute number of CD3+ T cells in the populations analysed (P > 0·10). Our findings suggest better thymic function in females compared with males, providing females with a higher number of recent thymic emigrants for longer periods of life. Such a finding provides a plausible explanation for the immunological gender differences observed in previous studies and possibly, for the general longer life expectancy in females compared with males.
机译:胸腺经历与年龄相关的对合,研究表明,胸腺从出生到现在,以每年大约3%的速度减少,直到中年为止,以每年1%的速度减少。这项研究的目的是确定胸腺萎缩对胸腺产生T淋巴细胞的影响,并阐明关于胸腺功能性别差异的不确定性。我们通过测量信号关节T细胞受体重排切除环(sjTRECs)量化了血液中的近期胸腺迁徙者(RTE),并显示随着年龄的增长血液中RTE数量的下降与性别有关。尽管CD3 的绝对数量没有明显的性别差异,但女性的外周血每个CD3 + T细胞的sjTRECs水平明显高于男性(P = 0·002)。分析人群中的+ T细胞(P> 0·10)。我们的发现表明,与男性相比,女性的胸腺功能更好,从而为女性提供了更长寿命的近期胸腺迁徙者。这一发现为以前的研究中观察到的免疫学性别差异提供了合理的解释,并且有可能为女性与男性相比普遍的预期寿命更长。

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