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对L-选择素和α4整合素的双重阻断消除了初始CD4细胞在肠道相关淋巴器官中的迁移及反应。

Blockade of both L-selectin and alpha4 integrins abrogates naive CD4 cell trafficking and responses in gut-associated lymphoid organs.

作者信息

Bradley L M, Malo M E, Fong S, Tonkonogy S L, Watson S R

机构信息

Department of Immunology, The Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

Int Immunol. 1998 Jul;10(7):961-8. doi: 10.1093/intimm/10.7.961.

Abstract

The recirculation of naive lymphocytes from blood to lymph that is initiated in high endothelial venules (HEV) of secondary lymphoid organs such as lymph nodes and Peyer's patches (PP) is regulated by multiple interactions of adhesion receptor/counter-receptor pairs involving both selectins and integrins. We showed previously that blocking of only L-selectin is sufficient to ablate trafficking of naive CD4 cells and the development of their responses in peripheral lymph nodes but not in PP where alpha4beta7 integrins are thought to primarily regulate entry. However, although antibody to alpha4 integrins partially inhibited homing of naive CD4 cells to PP and not to lymph nodes, there was no effect on the development primary responses in these tissues or spleens. Since previous studies indicate that both alpha4beta7 integrins and L-selectin regulate adhesion of naive cells to PP HEV, we examined the effect a blockade of both adhesion pathways on the recirculation of naive CD4 cells. There was no detectable homing of naive CD4 cells to PP or lymph nodes when interactions with both receptors were inhibited, resulting in a profound depletion of naive CD4 cells and loss of antigen responses in these sites. In contrast, increased numbers of naive CD4 cells and responses of higher magnitude were found in the spleen. The results demonstrate recirculation of naive CD4 cells through tissues where entry is controlled through HEV is essential for the local generation of primary responses.

摘要

幼稚淋巴细胞从血液再循环至淋巴的过程起始于二级淋巴器官(如淋巴结和派氏结(PP))的高内皮微静脉(HEV),该过程由涉及选择素和整合素的粘附受体/反受体对的多种相互作用所调控。我们之前表明,仅阻断L-选择素就足以消除幼稚CD4细胞在外周淋巴结中的归巢及其反应的发展,但在PP中则不然,在PP中α4β7整合素被认为主要调节细胞进入。然而,尽管抗α4整合素抗体部分抑制了幼稚CD4细胞归巢至PP而非淋巴结,但对这些组织或脾脏中初级反应的发展没有影响。由于先前的研究表明α4β7整合素和L-选择素均调节幼稚细胞与PP HEV的粘附,我们研究了阻断这两种粘附途径对幼稚CD4细胞再循环的影响。当与两种受体的相互作用均被抑制时,未检测到幼稚CD4细胞归巢至PP或淋巴结,导致幼稚CD4细胞大量耗竭以及这些部位抗原反应丧失。相反,在脾脏中发现幼稚CD4细胞数量增加且反应强度更高。结果表明,幼稚CD4细胞通过HEV控制进入的组织进行再循环对于局部产生初级反应至关重要。

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