2012
DOI: 10.1182/blood-2012-03-416859
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IL-7–producing stromal cells are critical for lymph node remodeling

Abstract: Nonhematopoietic stromal cells of secondary lymphoid organs form important scaffold and fluid transport structures, such as lymph node (LN) trabeculae, lymph vessels, and conduits. Furthermore, through the production of chemokines and cytokines, these cells generate a particular microenvironment that determines lymphocyte positioning and supports lymphocyte homeostasis. IL-7 is an important stromal cell-derived cytokine that has been considered to be derived mainly from T-cell zone fibroblastic reticular cells… Show more

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Cited by 148 publications
(154 citation statements)
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“…We identifi ed stromal ECM modifi cations as a potential common denominator for this event and focused on the matricellular protein SPARC as a key regulator of relevant stromal changes. The end targets of ECM regulation in SLO are the lymphoid populations, as stromal cells support the survival of different subsets of T and B cells, providing prototypical homeostatic factors and functioning as antigen-presenting cells ( 47 ). During immune responses, SLO undergo profound architectural changes that are driven by stromal cells and involve the synthesis of ECM molecules, including matricellular proteins and collagens, which are somewhat unexpectedly implicated in the response outcome.…”
Section: Discussionmentioning
confidence: 99%
“…We identifi ed stromal ECM modifi cations as a potential common denominator for this event and focused on the matricellular protein SPARC as a key regulator of relevant stromal changes. The end targets of ECM regulation in SLO are the lymphoid populations, as stromal cells support the survival of different subsets of T and B cells, providing prototypical homeostatic factors and functioning as antigen-presenting cells ( 47 ). During immune responses, SLO undergo profound architectural changes that are driven by stromal cells and involve the synthesis of ECM molecules, including matricellular proteins and collagens, which are somewhat unexpectedly implicated in the response outcome.…”
Section: Discussionmentioning
confidence: 99%
“…The two conditions, (15) and continuity of C(x) at x = X, allow us to find the two unknowns,x and c 0 . In Figure 8, we compare the steady-state values of the mean number of cells,n, and the mean IL-7 level,x, obtained from numerical solution of the heterogeneous population model introduced in Section 3, with the following approximation, obtained using only the first term in (15) and (16) …”
Section: B the Steady State Of The Heterogeneous Population Modelmentioning
confidence: 99%
“…The T-cell zones of lymph nodes (LN), where the encounters between T cells and antigen-presenting cells that initiate immune responses occur [9,10], is also the site where T-cells access the IL-7 resource they need to survive in the absence of infection. One subset of lymph node stromal cells, the fibroblastic reticular cells in the T-cell zone, produce IL-7 [11][12][13][14][15][16]. Within a T-cell population, IL-7 receptor expression varies from cell to cell; those with higher expression are believed to be more likely to divide [17,18].…”
Section: Introductionmentioning
confidence: 99%
“…The stromal cells responsible for IL-7 production in secondary lymphoid organs are mainly fibroblastic reticular cells (FRCs) and lymphatic endothelial cells (36), which can both be identified as CD45 2 gp38 + cells (37). Because we were unable to use CD45 as a marker for stromal cell discrimination, we developed a lineage mix (CD11b, CD11c, NK1.1, CD4, and CD8) that labeled virtually all of the CD45 + cells in the lymph nodes of RAGKO mice.…”
Section: Innate Immune Cell Cd45 Regulates Il-7 Production By Stromalmentioning
confidence: 99%