TNFR1-dependent pulmonary apoptosis during ischemic acute kidney injury

White, Laura E.; Santora, Rachel J.; Cui, Yan; Moore, Frederick A.; Hassoun, Heitham T.

doi:10.1152/ajplung.00301.2011

Cited by 33 publications

(49 citation statements)

References 36 publications

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“…In our model, we found infiltration of primarily CD8 + T lymphocytes into the lungs, but both CD4 + and CD8 + T cells expressed markers of activation, suggesting that CD4 + T cells may serve an important role in crosstalk by activating cytotoxic T lymphocytes in the lungs during ischemic + T cell expression of TNFR1 or TNF-a, our prior research has identified a prominent role for the TNF superfamily in the distant organ effects of kidney IRI (8,19). In addition, we have identified TNFR1-dependent pulmonary apoptosis and increased levels of circulatory TNF-a during ischemic AKI (19). Despite no evidence of increased TNFR1 or TNF-a expression on infiltrating T cells, T nu/nu mice demonstrated significant protection from pulmonary apoptosis and functional injury during ischemic AKI.…”

Section: Discussionmentioning

confidence: 56%

“…CD8 + T cells are generally implicated in direct cytotoxicity; however, they typically require costimulation by either dendritic cells or CD4 + T cells to differentiate from naive to activated cytotoxic CD8 + T cells (30). In our model, we found infiltration of primarily CD8 + T lymphocytes into the lungs, but both CD4 + and CD8 + T cells expressed markers of activation, suggesting that CD4 + T cells may serve an important role in crosstalk by activating cytotoxic T lymphocytes in the lungs during ischemic + T cell expression of TNFR1 or TNF-a, our prior research has identified a prominent role for the TNF superfamily in the distant organ effects of kidney IRI (8,19). In addition, we have identified TNFR1-dependent pulmonary apoptosis and increased levels of circulatory TNF-a during ischemic AKI (19).…”

Section: Discussionmentioning

confidence: 57%

“…However, at 24 h, we observed greater expression of activation markers and nearly a 3-fold increase in Lung T lymphocyte TNF-a production and TNFR expression during ischemic AKI Our previous studies have suggested a prominent role for TNFR1-dependent pulmonary apoptosis following kidney IRI (8,19). To determine whether infiltrating T cells are a source for TNFdependent apoptosis, infiltrating T lymphocytes were analyzed for intracellular TNF-a and TNFR1 (CD120a) expression, using FACS analysis.…”

Section: Activation Of Cd4mentioning

confidence: 78%

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Lung T Lymphocyte Trafficking and Activation during Ischemic Acute Kidney Injury

Lie

White

Santora

et al. 2012

The Journal of Immunology

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Despite advances in renal replacement therapy, the mortality rate for acute kidney injury (AKI) remains unacceptably high, likely owing to extrarenal organ dysfunction. Kidney ischemia–reperfusion injury (IRI) activates cellular and soluble mediators that facilitate organ crosstalk and induce caspase-dependent lung apoptosis and injury through a TNFR1-dependent pathway. Given that T lymphocytes mediate local IRI in the kidney and are known to drive TNFR1-mediated apoptosis, we hypothesized that T lymphocytes activated during kidney IRI would traffic to the lung and mediate pulmonary apoptosis during AKI. In an established murine model of kidney IRI, we identified trafficking of CD3+ T lymphocytes to the lung during kidney IRI by flow cytometry and immunohistochemistry. T lymphocytes were primarily of the CD3+CD8+ phenotype; however, both CD3+CD4+ and CD3+CD8+ T lymphocytes expressed CD69 and CD25 activation markers during ischemic AKI. The activated lung T lymphocytes did not demonstrate an increased expression of intracellular TNF-α or surface TNFR1. Kidney IRI induced pulmonary apoptosis measured by caspase-3 activation in wild-type controls, but not in T cell-deficient (Tnu/nu) mice. Adoptive transfer of murine wild-type T lymphocytes into Tnu/nu mice restored the injury phenotype with increased cellular apoptosis and lung microvascular barrier dysfunction, suggesting that ischemic AKI-induced pulmonary apoptosis is T cell dependent. Kidney–lung crosstalk during AKI represents a complex biological process, and although T lymphocytes appear to serve a prominent role in the interorgan effects of AKI, further experiments are necessary to elucidate the specific role of activated T cells in modulating pulmonary apoptosis.

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Section: Discussionmentioning

confidence: 56%

Section: Discussionmentioning

confidence: 57%

Section: Activation Of Cd4mentioning

confidence: 78%

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Lung T Lymphocyte Trafficking and Activation during Ischemic Acute Kidney Injury

Lie

White

Santora

et al. 2012

The Journal of Immunology

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“…A likely underlying reason is the heterogeneity of the disease, which might be associated with a direct insult by, e.g., infection, aspiration, or injurious ventilation, or an indirect one during situations of severe systemic inflammation, or, frequently, a combination thereof. Efforts to define endogenous pathways or molecules that protect from ALI have recently significantly contributed to our understanding of ALI pathophysiology (5,36,51,81,95,99,132,150,176,189,226,245,254,256,261). Imai et al (106) were the first to suggest that the signals impacting on the balance between angiotensin converting enzymes (ACE) 1 and 2 modulate the degree of inflammatory lung injury after sepsis, and ACE I/D polymorphism was recently associated with mortality risk of ALI/ ARDS in patients (152).…”

Section: Putative Candidates For Treatment Of Alimentioning

confidence: 99%

Novel concepts of acute lung injury and alveolar-capillary barrier dysfunction

Herold

Gabrielli

Vadász

2013

American Journal of Physiology-Lung Cellular and Molecular Phys

172

178

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Herold S, Gabrielli NM, Vadász I. Novel concepts of acute lung injury and alveolar-capillary barrier dysfunction. Am J Physiol Lung Cell Mol Physiol 305: L665-L681, 2013. First published September 13, 2013 doi:10.1152/ajplung.00232.2013In this review we summarize recent major advances in our understanding on the molecular mechanisms, mediators, and biomarkers of acute lung injury (ALI) and alveolar-capillary barrier dysfunction, highlighting the role of immune cells, inflammatory and noninflammatory signaling events, mechanical noxae, and the affected cellular and molecular entities and functions. Furthermore, we address novel aspects of resolution and repair of ALI, as well as putative candidates for treatment of ALI, including pharmacological and cellular therapeutic means. alveolar-capillary barrier dysfunction; molecular mechanism; pharmacological and cell-based therapy; pulmonary edema; zaacute lung injury/acute respiratory distress syndrome Immune Cells and Inflammatory Signaling Pathways in ALIOne of the central concepts in acute lung injury (ALI) and acute respiratory distress syndrome (ARDS) is that an unbalanced quantity or quality of the inflammatory response aggravates epithelial or endothelial injury. This includes a dysregulated recruitment of leukocytes and/or an exaggerated activation of these cells; inappropriate expression of cytokines, lipid mediators, or reactive oxygen species; enhanced activation of death receptor signaling (97,98,140,207,240); or an uncontrolled activity of platelets or the coagulation cascade (154). In general, these responses are initiated and maintained by recognition of danger-or pathogen-associated molecular patterns

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“…For example, experimental acute kidney injury (AKI) causes cardiac dysfunction and induces apoptotic cell death in cardiac muscle and lungs (Hassoun et al, 2007(Hassoun et al, , 2009White et al, 2012). Similarly, both lung and bowel ischemia/reperfusion induce acute liver injury (Horie and Ishii, 2001;Esme et al, 2006).…”

Section: Introductionmentioning

confidence: 99%