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压力与皮肤白细胞迁移:双相过程

Stress and skin leukocyte trafficking as a dual-stage process.

机构信息

Neuroimmunology Research Unit, Department of Psychology, Tel Aviv University, Tel Aviv, Israel.

出版信息

Brain Behav Immun. 2012 Feb;26(2):267-76. doi: 10.1016/j.bbi.2011.09.007. Epub 2011 Sep 19.

Abstract

Stress responses are known to modulate leukocyte trafficking. In the skin, stress was reported both to enhance and reduce skin immunity, and the chronicity of stress exposure was suggested as a key determining factor. We here propose a dual-stage hypothesis, suggesting that stress, of any duration, reduces skin immunity during its course, while its cessation is potentially followed by a period of enhanced skin immunity. To start testing this hypothesis, rats were subcutaneously implanted with sterile surgical sponges for four-hours, during or after exposure to one of several acute stress paradigms, or to a chronic stress paradigm. Our findings, in both males and females, indicate that numbers of sponge-infiltrating leukocytes, and their specific subsets, were reduced during acute or chronic stress, and increased after stress cessation. Studying potential mediating mechanisms of the reduction in leukocyte numbers during acute stress, we found that neither adrenalectomy nor the administration of beta-adrenergic or glucocorticoid antagonists prevented this reduction. Additionally, administration of corticosterone or epinephrine to adrenalectomized rats did not impact skin leukocyte numbers, whereas, in the blood, these treatments did affect numbers of leukocytes and their specific subsets, as was also reported previously. Overall, our findings support the proposed dual-stage hypothesis, which can be evolutionally rationalized and accounts for most of the apparent inconsistencies in the literature regarding stress and skin immunity. Other aspects of the hypothesis should be tested, also using additional methodologies, and its predictions may bear clinical significance in treatment of skin disorders related to hyper- or hypo-immune function.

摘要

应激反应被认为可以调节白细胞的迁移。在皮肤中,应激既被报道可以增强也可以降低皮肤免疫力,并且应激暴露的慢性被认为是一个关键的决定因素。我们在此提出一个两阶段假说,即任何持续时间的应激都会在其过程中降低皮肤免疫力,而应激的停止可能随后会导致皮肤免疫力增强的时期。为了开始检验这个假说,我们将无菌手术海绵植入大鼠的皮下 4 小时,在暴露于几种急性应激范式之一期间或之后,或者在慢性应激范式之后。我们的发现表明,无论是雄性还是雌性大鼠,在急性或慢性应激期间,海绵浸润白细胞的数量及其特定亚群减少,而应激停止后则增加。研究急性应激期间白细胞数量减少的潜在介导机制,我们发现,肾上腺切除术或β-肾上腺素能或糖皮质激素拮抗剂的给药并不能预防这种减少。此外,向肾上腺切除大鼠给予皮质酮或肾上腺素并不影响皮肤白细胞数量,而在血液中,这些处理确实影响白细胞及其特定亚群的数量,这也与之前的报道一致。总的来说,我们的发现支持所提出的两阶段假说,该假说可以从进化的角度进行合理化,并解释了文献中关于应激和皮肤免疫之间的大多数明显不一致之处。该假说的其他方面也应该用其他方法进行测试,其预测可能在治疗与超免疫或低免疫功能相关的皮肤疾病方面具有临床意义。

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