Abstract

Recognition and removal of apoptotic cells is a critically important and highly conserved biologic process that is ?silent? with regard to local tissue responses. We have previously shown that the apoptotic cells induce an active anti-inflammatory response that is mediated in large part by the redistribution of phosphatidylserine (PS) from the inner to the outer leaflet of the plasma membrane and its subsequent recognition by responding phagocytes and other cells. More recently we have shown that PS on the apoptotic cells can also suppress the adaptive immune response. In the lung, as elsewhere in the body, these effects are suggested to mediate the resolution of normal, protective and self-limited inflammatory responses by removing apoptotic inflammatory cells, suppressing the ongoing inflammation while at the same time preventing inappropriate immune reactions. We have also shown that much of the inflammosuppression and immunosuppression initiated by recognition of the PS is mediated through the induction and effects of transforming growth factor beta (TGFa). Nevertheless, despite the information that we and others have gathered on the role of exposed PS, we still do not have an adequate understanding of the mechanisms and particularly, the receptors that recognize and respond to the PS, especially in its ability to drive the suppressive processes. Recently a number of candidate direct ?receptors? for PS have been identified to go along with previously described bridge molecules that bind on the one hand to PS on the apoptotic cells and on the other to receptors on the responding phagocyte. Accordingly, we suggest that the time is now ripe for a concerted approach to determine the receptors and mechanisms underlying the inflammosuppressive and immunosuppressive effects of PS-exposing apoptotic cells. These studies will be carried out in the pulmonary environment and following our usual approach will involve investigations both in vitro and in vivo. The proposal encompasses two specific aims, one on the inflammosuppression and one on immunosuppression, with major emphases on characterizing the role for TGFa and identifying the relevant receptors, first in vitro and then in vivo as well as exploring novel mechanisms by which immune responses in the lung are modulated. Implications and broader objectives of this work are the ability to use the knowledge obtained to deliberately block ongoing inflammatory and/or immunologic reactions in the lung and indeed the proposal includes early studies to explore this potential.

Public Health Relevance

The normal lung is constantly exposed to the external environment and needs to discriminate between relatively harmless exposure and potentially dangerous insults, mounting self-limiting inflammatory reactions and also local immune responses where necessary. Resolution of normal inflammation involves apoptosis of the recruited inflammatory cells, leading both to their removal as well as to stimulation of an active antiinflammatory response;events driven in part by exposure of phosphatidylserine (PS) on the apoptotic cells. In the first period of this grant we have addressed the role of the PS in suppressing the inflammation and have determined some of the mechanisms involved. However, the receptors that recognize the PS and drive the process have remained elusive. More recently, a number of candidates for this function have been described and we believe it is time to address in detail this crucial step in the process. In addition, we have also found that the PS on apoptotic cells can be immunosuppressive. This raises important questions about their effect on the immunogenicity of pathogens in the lung when in the context of many apoptotic cells, such as during resolution of the inflammation that was initiated as part of the innate immune to the pathogen. Accordingly, we propose also to address the mechanisms by which apoptotic cells and PS inhibit the pulmonary adaptive immune response. The long-term objective will be to develop approaches to manipulate these natural regulatory processes to suppress unwanted ongoing inflammation and to enhance the immunologic responses to pathogens or block those leading to disease ? for example in asthma or autoimmunity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
3R01HL081151-05A1S1
Application #
7995282
Study Section
Special Emphasis Panel (ZRG1-RES-C (02))
Program Officer
Reynolds, Herbert Y
Project Start
2005-07-01
Project End
2013-05-31
Budget Start
2010-01-01
Budget End
2010-05-31
Support Year
5
Fiscal Year
2010
Total Cost
$56,132
Indirect Cost

  Institution

Name
National Jewish Health
Department
Type
DUNS #
076443019
City
Denver
State
CO
Country
United States
Zip Code
80206

  Publications

Desch, A Nicole; Gibbings, Sophie L; Goyal, Rajni et al. (2016) Flow Cytometric Analysis of Mononuclear Phagocytes in Nondiseased Human Lung and Lung-Draining Lymph Nodes. Am J Respir Crit Care Med 193:614-26
Gibbings, Sophie L; Goyal, Rajni; Desch, A Nicole et al. (2015) Transcriptome analysis highlights the conserved difference between embryonic and postnatal-derived alveolar macrophages. Blood 126:1357-66
Kuan, Emma L; Ivanov, Stoyan; Bridenbaugh, Eric A et al. (2015) Collecting lymphatic vessel permeability facilitates adipose tissue inflammation and distribution of antigen to lymph node-homing adipose tissue dendritic cells. J Immunol 194:5200-10
Desch, A Nicole; Gibbings, Sophie L; Clambey, Eric T et al. (2014) Dendritic cell subsets require cis-activation for cytotoxic CD8 T-cell induction. Nat Commun 5:4674
Redente, Elizabeth F; Keith, Rebecca C; Janssen, William et al. (2014) Tumor necrosis factor-? accelerates the resolution of established pulmonary fibrosis in mice by targeting profibrotic lung macrophages. Am J Respir Cell Mol Biol 50:825-37
Aschner, Yael; Khalifah, Anthony P; Briones, Natalie et al. (2014) Protein tyrosine phosphatase ? mediates profibrotic signaling in lung fibroblasts through TGF-? responsiveness. Am J Pathol 184:1489-502
Henson, Peter M; Bratton, Donna L (2013) Antiinflammatory effects of apoptotic cells. J Clin Invest 123:2773-4
Jakubzick, Claudia; Gautier, Emmanuel L; Gibbings, Sophie L et al. (2013) Minimal differentiation of classical monocytes as they survey steady-state tissues and transport antigen to lymph nodes. Immunity 39:599-610
Frasch, S Courtney; Fernandez-Boyanapalli, Ruby F; Berry, Karin A Zemski et al. (2013) Neutrophils regulate tissue Neutrophilia in inflammation via the oxidant-modified lipid lysophosphatidylserine. J Biol Chem 288:4583-93
Xiong, Weipeng; Frasch, S Courtney; Thomas, Stacey M et al. (2013) Induction of TGF-?1 synthesis by macrophages in response to apoptotic cells requires activation of the scavenger receptor CD36. PLoS One 8:e72772

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