Abstract

Complement (C') is important in normal biology but it is also a pathological factor in a large number of inflammatory diseases. C'-mediated tissue injury has been reported in a wide variety of diseases including but not limited to autoimmune diseases, adult respiratory distress syndrome, Alzheimer's disease, stroke, heart attack, burn injuries, organ transplantation, and in extracorporeal blood oxygenation. There is a critical need for a therapeutically applicable C inhibitor. Several C' inhibitors have been described; however, the low-molecular weight inhibitors have shown low activity and high toxicity and are therefore pharmacologically undesirable. Recombinant forms of C' regulatory proteins such as CR1, DAF, MCP and CD59, and a monoclonal antibody to C5 have shown promise, as they have been effective in experimental diseases. All these inhibitors however, are large molecular weight protein, require intravenous administration and most of them have only a short half-life in vivo. Recent studies are focused on a second generation of smaller molecular weight derivatives with more desirable properties, but none of these has yet been adopted as a therapeutic agent. We have taken the alternative approach of screening a universe of random peptide information for C3-interactive peptides. Screening of a random peptide phage library yielded a novel small molecular weight cyclic peptide, Compstatin, (ICVVQDWGHHRCT) that binds specifically to human and primate C3 and inhibits the activation of C' by both the classical and alternative pathways. The peptide effectively inhibits C' in clinically relevant in vitro, ex vivo and most importantly in vivo models of C' activation. This application has three aims:
In Aim 1, the structure of Compstatin bound to a C3 fragment will be determined and the relationships between the structure and function of Compstatin will be studied by use of random peptide libraries, peptide synthesis, and NMR analyses.
In aim 2, photoaffinity probes, genetically engineered C3 molecules, and expressed C3 fragments will be used to identify the Compstatin binding Sites on C3, which may give important information on the C3 convertase recognition site on C3, a significant control point in the C3 architecture. In addition, we will also attempt to investigate the mechanism(s) by which Compstatin modulates C' activation.
Aim 3 will examine the C' inhibiting properties of Compstatin in clinical interventions. Half-life measurements, its biotransformation, and the ability of Compstatin to inhibit C' will be assessed in in vitro and in vivo experimental models of cardiopulmonary bypass (CPB) and in an ex vivo xenotransplantation model. In addition, the contribution of individual C' activation products in these clinical situations will be assessed using Compstatin, anti-C5 and C' receptor specific inhibitors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM062134-01
Application #
6224890
Study Section
Immunological Sciences Study Section (IMS)
Program Officer
Marino, Pamela
Project Start
2001-03-01
Project End
2005-02-28
Budget Start
2001-03-01
Budget End
2002-02-28
Support Year
1
Fiscal Year
2001
Total Cost
$305,113
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Pathology
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Moll, Guido; Alm, Jessica J; Davies, Lindsay C et al. (2014) Do cryopreserved mesenchymal stromal cells display impaired immunomodulatory and therapeutic properties? Stem Cells 32:2430-42
Nilsson, Per H; Ekdahl, Kristina N; Magnusson, Peetra U et al. (2013) Autoregulation of thromboinflammation on biomaterial surfaces by a multicomponent therapeutic coating. Biomaterials 34:985-94
Landsem, A; Nielsen, E W; Fure, H et al. (2013) C1-inhibitor efficiently inhibits Escherichia?coli-induced tissue factor mRNA up-regulation, monocyte tissue factor expression and coagulation activation in human whole blood. Clin Exp Immunol 173:217-29
Qu, Hongchang; Ricklin, Daniel; Bai, Hongjun et al. (2013) New analogs of the clinical complement inhibitor compstatin with subnanomolar affinity and enhanced pharmacokinetic properties. Immunobiology 218:496-505
Brekke, O L; Waage, C; Christiansen, D et al. (2013) The effects of selective complement and CD14 inhibition on the E. coli-induced tissue factor mRNA upregulation, monocyte tissue factor expression, and tissue factor functional activity in human whole blood. Adv Exp Med Biol 735:123-36
Hajishengallis, George; Lambris, John D (2013) Complement-targeted therapeutics in periodontitis. Adv Exp Med Biol 735:197-206
Christiansen, D; Brekke, O L; Stenvik, J et al. (2012) Differential effect of inhibiting MD-2 and CD14 on LPS- versus whole E. coli bacteria-induced cytokine responses in human blood. Adv Exp Med Biol 946:237-51
Oikonomopoulou, Katerina; Ricklin, Daniel; Ward, Peter A et al. (2012) Interactions between coagulation and complement--their role in inflammation. Semin Immunopathol 34:151-65
Garcia, Brandon L; Ramyar, Kasra X; Ricklin, Daniel et al. (2012) Advances in understanding the structure, function, and mechanism of the SCIN and Efb families of Staphylococcal immune evasion proteins. Adv Exp Med Biol 946:113-33
Hajishengallis, George; Krauss, Jennifer L; Liang, Shuang et al. (2012) Pathogenic microbes and community service through manipulation of innate immunity. Adv Exp Med Biol 946:69-85

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