Abstract

The overall goal of our research program is to understand some of the factors involved in the modulation of human immune responses so that desirable functions might be enhanced, to both prevent the development of a disease state (as in infection or cancer) and to enhance the body's ability to cope with challenges under conditions in which some part of the defense system is compromised, either by genetic deficiencies or immunosuppression. It has been demonstrated previously that interaction of the complement subcomponent C1q with specific cells of the immune system enhances the phagocytic and killing capacity of those cells. We have isolated candidate C1q receptor molecules by ligand affinity chromatography. This protein was used to produce monoclonal antibodies, two of which inhibit the C1q-mediated enhancement of phagocytosis in monocytes. Amino acid sequencing of the 126,000 Mr molecule recognized by the inhibitory antibodies has led to the isolation of a cDNA fragment encoding part of this molecule. We now intend to clone and sequence the full length cDNA coding for the 126,000 Mr component of the C1q receptor that mediates the enhancement of phagocytosis. Suitable expression systems for this C1qRp will subsequently be developed to further characterize the structure and function of this receptor using both molecular and biochemical approaches. The structural requirements and amino acid sequences of C1q involved in the molecular interaction with the phagocytosis-enhancing C1q Receptor will be delineated. This will facilitate the development of reagents that will enhance the human immune responses to prevent the development of disease or regulate detrimental responses. Finally, we will explore both the relationship of the C1q receptor system with other reported C1q-mediated functions and the possible coreceptor molecules involved in this innate immune response. Individuals genetically deficient in C1q are prone to bacterial infections and/or develop autoimmune disorders. In addition, antibodies to the collagen-like region (that contains the cell binding domain) of C1q are found in sera of patients with SLE, rheumatoid vasculitis and hypocomplementemic urticarial vasculitis syndrome. The research proposed here will provide necessary information for future development of therapeutic strategies for these conditions and other immunodeficient states.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI041090-04
Application #
2887415
Study Section
Special Emphasis Panel (ZRG2-ALY (01))
Program Officer
Jones, Melinda
Project Start
1996-07-01
Project End
2000-06-30
Budget Start
1999-07-01
Budget End
2000-06-30
Support Year
4
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of California Irvine
Department
Biochemistry
Type
Schools of Arts and Sciences
DUNS #
161202122
City
Irvine
State
CA
Country
United States
Zip Code
92697

  Publications

Clarke, Elizabeth V; Weist, Brian M; Walsh, Craig M et al. (2015) Complement protein C1q bound to apoptotic cells suppresses human macrophage and dendritic cell-mediated Th17 and Th1 T cell subset proliferation. J Leukoc Biol 97:147-60
Clarke, Elizabeth V; Tenner, Andrea J (2014) Complement modulation of T cell immune responses during homeostasis and disease. J Leukoc Biol 96:745-56
Ueno, Norikiyo; Harker, Katherine S; Clarke, Elizabeth V et al. (2014) Real-time imaging of Toxoplasma-infected human monocytes under fluidic shear stress reveals rapid translocation of intracellular parasites across endothelial barriers. Cell Microbiol 16:580-95
Benoit, Marie E; Hernandez, Michael X; Dinh, Minhan L et al. (2013) C1q-induced LRP1B and GPR6 proteins expressed early in Alzheimer disease mouse models, are essential for the C1q-mediated protection against amyloid-? neurotoxicity. J Biol Chem 288:654-65
Stephan, Alexander H; Madison, Daniel V; Mateos, José María et al. (2013) A dramatic increase of C1q protein in the CNS during normal aging. J Neurosci 33:13460-74
Clarke, Elizabeth V; Benoit, Marie E; Tenner, Andrea J (2013) Purification of Human Monocytes and Lymphocyte Populations by Counter Current Elutriation- A Short Protocol. Bio Protoc 3:
Benoit, Marie E; Clarke, Elizabeth V; Tenner, Andrea J (2013) C1q Binding to and Uptake of Apoptotic Lymphocytes by Human Monocyte-derived Macrophages. Bio Protoc 3:
Benoit, Marie E; Clarke, Elizabeth V; Morgado, Pedro et al. (2012) Complement protein C1q directs macrophage polarization and limits inflammasome activity during the uptake of apoptotic cells. J Immunol 188:5682-93
Benoit, Marie E; Tenner, Andrea J (2011) Complement protein C1q-mediated neuroprotection is correlated with regulation of neuronal gene and microRNA expression. J Neurosci 31:3459-69
Fraser, Deborah A; Pisalyaput, Karntipa; Tenner, Andrea J (2010) C1q enhances microglial clearance of apoptotic neurons and neuronal blebs, and modulates subsequent inflammatory cytokine production. J Neurochem 112:733-43

Showing the most recent 10 out of 35 publications