Abstract

In the absence of antigen, memory T helper (Th) cells are maintained in a resting state. Recently it has been shown that bone marrow (BM) is a major reservoir of resting memory Th cells. In a given immune response, less than 10% of the activated CD4 T cells are recruited to the pool of resting BM memory Th cells. Here we review recent evidence that CD69 and CD49b control homing of memory Th cell precursors to the BM. During the effector phase of an immune response, about 10% of activated CD4 T cells in the spleen express both CD69 and CD49b, and thus qualify as precursors of resting memory Th cells of BM. Loss or blockade of CD69 and CD49b expression on CD4 T cells impairs the generation of resting memory Th cells in the BM. Moreover, in the absence of BM memory Th cells in CD69-deficient mice, T-cell help for B cells is impaired, confirming the central role of BM memory Th cells in the maintenance of immunological memory.

Highlights

  • The immune system can memorize previously encountered specific antigens for many years, both by the secretion of specific antibodies and by long-lived, pre-activated cells

  • We review recent evidence that CD69 and CD49b control homing of memory T helper (Th) cell precursors to the bone marrow (BM)

  • It is still debated whether immunological memory is dependent on persistent antigen [1, 2] and whether it is dependent on long-lived effector cells as opposed to dedicated memory cells [3]

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Summary

Introduction

The immune system can memorize previously encountered specific antigens for many years, both by the secretion of specific antibodies (humoral memory) and by long-lived, pre-activated cells (reactive memory). During the effector phase of an immune response, about 10% of activated CD4 T cells in the spleen express both CD69 and CD49b, and qualify as precursors of resting memory Th cells of BM. Loss or blockade of CD69 and CD49b expression on CD4 T cells impairs the generation of resting memory Th cells in the BM.

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