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血管活性肠肽受体的体外改变会改变小鼠T细胞的体内定位。

In vitro alteration of receptors for vasoactive intestinal peptide changes the in vivo localization of mouse T cells.

作者信息

Ottaway C A

出版信息

J Exp Med. 1984 Oct 1;160(4):1054-69. doi: 10.1084/jem.160.4.1054.

Abstract

The capacity of T lymphocytes exposed in vitro to the neuropeptide vasoactive intestinal peptide (VIP) to bind VIP in vitro and to migrate to different tissues in vivo has been studied. VIP treatment of T cells resulted in a time- and dose-dependent loss of the ability of T cells to specifically bind radioiodinated VIP. Altered binding was due to a decrease in the expression of cellular receptors for VIP on the treated cells rather than an alteration in the affinity of the cells for the neuropeptide. Alteration of VIP receptor expression was not associated with a change in the expression of Thy-1, Lyt-1, or Lyt-2 surface markers by the treated cells. VIP treatment of T cells in vitro resulted, however, in a dose-dependent decrease in the ability of the treated cells to localize in mesenteric lymph nodes (MLN) and Peyer's patches of recipient animals at early times after cell transfer, and this was due to a selective decrease in the rate of accumulation of the treated cells in these tissues. There was no alteration in the distribution of VIP-treated cells in the blood, spleen, liver, or other major organs of the recipient animals. It is concluded that the presence of VIP receptors on T cells facilitates the entry of T cells into MLN and Peyer's patches in vivo, and it is proposed that this effect is mediated by T cell-VIP interactions in the vicinity of the specialized endothelium of those tissues.

摘要

研究了体外暴露于神经肽血管活性肠肽(VIP)的T淋巴细胞在体外结合VIP以及在体内迁移至不同组织的能力。用VIP处理T细胞导致T细胞特异性结合放射性碘化VIP的能力出现时间和剂量依赖性丧失。结合改变是由于处理过的细胞上VIP细胞受体表达减少,而非细胞对神经肽亲和力的改变。VIP受体表达的改变与处理过的细胞上Thy-1、Lyt-1或Lyt-2表面标志物表达的变化无关。然而,体外用VIP处理T细胞导致处理过的细胞在细胞转移后早期定位于受体动物肠系膜淋巴结(MLN)和派尔集合淋巴结的能力出现剂量依赖性降低,这是由于处理过的细胞在这些组织中的积累速率选择性降低所致。VIP处理过的细胞在受体动物的血液、脾脏、肝脏或其他主要器官中的分布没有改变。结论是T细胞上VIP受体的存在促进T细胞在体内进入MLN和派尔集合淋巴结,并且推测这种效应是由那些组织的特化内皮附近的T细胞-VIP相互作用介导的。

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