The Microstructure of Secondary Lymphoid Organs That Support Immune Cell Trafficking

Overview

Journal Arch Histol Cytol

Specialties Anatomy & Histology
Cell Biology

Date 2011 Apr 8

PMID 21471663

Citations 14

Authors

Kenjiro Matsuno

Hisashi Ueta

Zhou Shu

Xu Xue-Dong

Yasushi Sawanobori

Yusuke Kitazawa

Yu Bin

Masaki Yamashita

Changde Shi

Affiliations

Soon will be listed here.

Abstract

Immune cell trafficking in the secondary lymphoid organs is crucial for an effective immune response. Recirculating T cells constantly patrol not only secondary lymphoid organs but also the whole peripheral organs. Thoracic duct lymphocytes represent an ideal cell source for analyzing T cell trafficking: high endothelial venules (HEVs) allow recirculating lymphocytes to transmigrate from the blood directly, and recirculating T cells form a cluster with dendritic cells (DCs) to survey antigen invasions even in a steady state. This cluster becomes an actual site for the antigen presentation when DCs have captured antigens. On activation, effector and memory T cells differentiate into several subsets that have different trafficking molecules and patterns. DCs also migrate actively in a manner depending upon their maturational stages. Danger signals induce the recruitment of several DC precursor subsets with different trafficking patterns and functions. In this review, we describe general and specialized structures of the secondary lymphoid organs for the trafficking of T cells and DCs by a multicolor immunoenzyme staining technique. The lymph nodes, spleen, and Peyer's patches of rats were selected as the major representatives. In vivo trafficking of subsets of T cells and DCs within these organs under steady or emergency states are shown and discussed, and unsolved questions and future prospects are also considered.

Citing Articles

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Kitazawa Y, Ueta H, Sawanobori Y, Katakai T, Yoneyama H, Ueha S Front Immunol. 2019; 10:1195.

PMID: 31191552 PMC: 6548820. DOI: 10.3389/fimmu.2019.01195.