The Use of Lymphocyte Function–Associated Antigen (Lfa)-1–Deficient Mice to Determine the Role of Lfa-1, Mac-1, and α4 Integrin in the Inflammatory Response of Neutrophils

Henderson, Robert B.; Lim, Lina H.K.; Tessier, Philippe A.; Gavins, Felicity N. E.; Mathies, Meg; Perretti, Mauro; Hogg, Nancy

doi:10.1084/jem.194.2.219

Cited by 160 publications

(186 citation statements)

References 32 publications

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“…Gamma delta (c d) T cells, which also express high levels of LFA-1, are particularly abundant in the resident lymphocyte population of the liver (47) and have been shown to be important for priming of CD8 + T cells in response to infection (48). In addition, many of the effectors of innate immunity such as neutrophils and macrophages rely on LFA-1 for vascular adhesion and rolling prior to emigration into tissues (49)(50)(51). Such effectors of innate immunity which comprise early inflammatory events can significantly influence T-cell recruitment and acute allograft rejection (52).…”

Section: Discussionmentioning

confidence: 99%

Targeting LFA-1 Synergizes with CD40/CD40L Blockade for Suppression of Both CD4-Dependent and CD8-Dependent Rejection

Wang

Gao

Lunsford

et al. 2003

American Journal of Transplantation

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Allogeneic hepatocytes elicit CD4-dependent and (CD4-independent) CD8 + T-cell-initiated graft rejection. The (CD4-independent) CD8 + T-cell pathway is resistant to immunosuppressive strategies that readily and indefinitely suppress CD4 + T-cell-dependent rejection responses. Consequently, successful immunoregulation of hepatocyte-initiated immune responses requires a strategy which regulates both CD4-dependent and CD8-dependent rejection responses. Interference with CD40/CD40 ligand (CD40L) costimulation only transiently suppresses CD4-and CD8-dependent hepatocyte rejection. Interference with CD28/B7 costimulation transiently suppresses CD4-dependent hepatocyte rejection, but is ineffective for suppression of CD8-dependent hepatocyte rejection. To date, hepatocyte survival > 60 days post-transplant has not been achieved by any immunotherapeutic strategy. In the current study, we evaluated a novel immunosuppressive strategy which targets both LFA-1 and CD40L-mediated signals. Targeting LFA-1 suppressed (CD4-independent) CD8 + T-cell-initiated hepatocyte rejection such that allogeneic hepatocyte survival > 60 days was achieved in 70% of CD4 KO mice. Targeting both LFA-1-mediated signals and CD40/CD40L costimulation resulted in synergistic effects, such that hepatocellular survival > 60 days was achieved in 100% of C57BL/6 mice (which have both CD4-and CD8-dependent T-cell pathways available).

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Section: Discussionmentioning

confidence: 99%

Targeting LFA-1 Synergizes with CD40/CD40L Blockade for Suppression of Both CD4-Dependent and CD8-Dependent Rejection

Wang

Gao

Lunsford

et al. 2003

American Journal of Transplantation

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“…There is some evidence for other integrins that certain conformational states are likely to be more suited for a transient adhesion like cell spreading, rolling, and migration, whereas other conformations favor a more stable adhesion. For example, it has been demonstrated that the integrin ␣L␤2 can support such a transient adhesion of leukocytes (namely rolling), together with selectins and ␣4 integrins, during inflammation in vivo (52). More recently, this observation could be linked to a certain conformational state of ␣L␤2.…”

Section: Discussionmentioning

confidence: 99%

Two Functional Active Conformations of the Integrin α2β1, Depending on Activation Condition and Cell Type

Walle

Vanhoorelbeke

Májer

et al. 2005

Journal of Biological Chemistry

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“…Fully activated LFA-1 mediates the stop of rolling and makes firm adhesion along with Mac-1 (175). Deficiency of b 2 integrin chain causes Leukocyte Adhesion Deficiency Type 1, an inherited disorder that is characterized by inability of leukocytes to undergo adhesion-dependent migration (49).…”

Section: B Integrinsmentioning

confidence: 99%

Reactive Oxygen Species in Inflammation and Tissue Injury

Mittal

Siddiqui

Tran

et al. 2014

Antioxidants & Redox Signaling

3,201

2,198

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Reactive oxygen species (ROS) are key signaling molecules that play an important role in the progression of inflammatory disorders. An enhanced ROS generation by polymorphonuclear neutrophils (PMNs) at the site of inflammation causes endothelial dysfunction and tissue injury. The vascular endothelium plays an important role in passage of macromolecules and inflammatory cells from the blood to tissue. Under the inflammatory conditions, oxidative stress produced by PMNs leads to the opening of inter-endothelial junctions and promotes the migration of inflammatory cells across the endothelial barrier. The migrated inflammatory cells not only help in the clearance of pathogens and foreign particles but also lead to tissue injury. The current review compiles the past and current research in the area of inflammation with particular emphasis on oxidative stress-mediated signaling mechanisms that are involved in inflammation and tissue injury. Antioxid. Redox Signal. 20, 1126-1167.

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The Use of Lymphocyte Function–Associated Antigen (Lfa)-1–Deficient Mice to Determine the Role of Lfa-1, Mac-1, and α4 Integrin in the Inflammatory Response of Neutrophils

Cited by 160 publications

References 32 publications

Targeting LFA-1 Synergizes with CD40/CD40L Blockade for Suppression of Both CD4-Dependent and CD8-Dependent Rejection

Targeting LFA-1 Synergizes with CD40/CD40L Blockade for Suppression of Both CD4-Dependent and CD8-Dependent Rejection

Two Functional Active Conformations of the Integrin α2β1, Depending on Activation Condition and Cell Type

Reactive Oxygen Species in Inflammation and Tissue Injury

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