Abstract

Expression of endothelial-leukocyte adhesion molecule is dramatically induced by inflammatory cytokines. This increased expression occurs at the transcriptional level and requires activation of the nuclear factor-kappaB (NF-kB) system. Recent studies indicate that the p65 component of NF-kB, like many signal dependent transcriptional activators, interacts with the transcriptional co-activator CREB-binding protein (CBP). In this continuing project, we will investigate whether CBP is part of a novel level of nuclear regulation linking diverse signaling systems in endothelial cells and test the hypothesis that competition for limiting amounts of CBP facilitates the activation of some signal dependent genes at the expense of others. In the renewal period we propose to determine if this regulatory system is relevant to the process of endothelial activation during inflammatory responses.
In Specific Aim #1, the antagonistic interactions between p65 and other signal-dependent transcription factors occur because for limiting amounts of the common transcriptional co-activator, CBP. These studies will examine the levels of CBP expression in quiescent and cytokine-activated cultured endothelial cells, determine if levels of the co-activator limit NF-kappaB dependent gene expression, and will explore the molecular basis of the antagonistic interaction.
In Specific Aim #2, the pathophysiologic consequences of CBP over- expression in endothelial cells will be examined in a transgenic model of endothelial activation. In this defined genetic context, we will determine if CBP over expression increases induction of NF-kappaB dependent genes and diminishes the negative regulatory effects of the activated nuclear receptors on the induction of kappaB-dependent genes. Like the induction process, decreased expression of the endothelial adhesion molecules following cytokine exposure is an active process that occurs at the transcriptional level. This level of negative regulation my be key in preventing inappropriate or prolonged expression of some adhesion molecule genes.
In Specific Aim #3, the mechanisms responsible for the post-induction transcriptional repression of E-selectin will continue to be investigated. These studies will determine the role of the dual specificity phosphatases in limiting the expression of this adhesion molecule gene using tools developed in this project, as well as unique cellular and animal reagents developed by collaborators. Collectively, the findings from these studies should provide insights into two new endothelial regulatory systems: first, they should indicate if CBP serves an integration function for interactions between p65 and other classes of CBP dependent transcription factors during cytokine-induced gene expression; and second, they should define the mechanisms which tightly control the post-induction transcriptional repression of the E- selectin gene.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL036028-17
Application #
6469266
Study Section
Project Start
2001-07-01
Project End
2002-06-30
Budget Start
Budget End
Support Year
17
Fiscal Year
2001
Total Cost
$68,666
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Zahr, Alisar; Alcaide, Pilar; Yang, Jinling et al. (2016) Endomucin prevents leukocyte-endothelial cell adhesion and has a critical role under resting and inflammatory conditions. Nat Commun 7:10363
Venkatesh, Deepak; Mruk, Dolores; Herter, Jan M et al. (2016) AKAP9, a Regulator of Microtubule Dynamics, Contributes to Blood-Testis Barrier Function. Am J Pathol 186:270-84
Milstone, David S; Ilyama, Motoi; Chen, Mian et al. (2015) Differential role of an NF-?B transcriptional response element in endothelial versus intimal cell VCAM-1 expression. Circ Res 117:166-77
Cullere, Xavier; Plovie, Eva; Bennett, Paul M et al. (2015) The cerebral cavernous malformation proteins CCM2L and CCM2 prevent the activation of the MAP kinase MEKK3. Proc Natl Acad Sci U S A 112:14284-9
Luscinskas, Francis W; Imhof, Beat A (2014) Introduction for the special issue on new paradigms in leukocyte trafficking, lessons for therapeutics. Semin Immunopathol 36:133-6
Brown, Jonathan D; Lin, Charles Y; Duan, Qiong et al. (2014) NF-?B directs dynamic super enhancer formation in inflammation and atherogenesis. Mol Cell 56:219-231
Mayadas, Tanya N; Cullere, Xavier; Lowell, Clifford A (2014) The multifaceted functions of neutrophils. Annu Rev Pathol 9:181-218
Massaad, Michel J; Oyoshi, Michiko K; Kane, Jennifer et al. (2014) Binding of WIP to actin is essential for T cell actin cytoskeleton integrity and tissue homing. Mol Cell Biol 34:4343-54
Leick, Marion; Azcutia, Veronica; Newton, Gail et al. (2014) Leukocyte recruitment in inflammation: basic concepts and new mechanistic insights based on new models and microscopic imaging technologies. Cell Tissue Res 355:647-56
Azcutia, Veronica; Routledge, Matthew; Williams, Marcie R et al. (2013) CD47 plays a critical role in T-cell recruitment by regulation of LFA-1 and VLA-4 integrin adhesive functions. Mol Biol Cell 24:3358-68

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