Abstract

Complement is important in physiology, but it is also a pathogenic factor in a large number ofinflammatory diseases. Complement-mediated tissue injury has been reported in a wide variety ofdisorders, including but not limited to autoimmune diseases, adult respiratory distress syndrome,Alzheimer's disease, stroke, heart attack, burn injuries, organ transplantation, as well as inextracorporeal blood oxygenation. There is a critical need for a therapeutically applicablecomplement inhibitor. Several complement inhibitors have been described; however, the lowmolecular weight inhibitors designed in the past showed low activity and high toxicity and aretherefore pharmacologically undesirable. Recombinant forms of complement regulatory proteinssuch as CR1, DAF, MCP, and CD59, and a monoclonal antibody against C5, have shown promise,as they have been effective in disease models. All these inhibitors, however, are large molecularweight proteins and require intravenous administration; also, most of them have only a short half-lifein vivo. Recent studies have focused on a second generation of low molecular weight derivativeswith more desirable properties, but none of these have yet been adopted as a therapeutic agent.We have taken the alternative approach of screening a peptide phage-display library for C3-interactive peptides and have isolated a novel small molecular weight cyclic peptide, Compstatin,which binds specifically to human and primate C3 and inhibits the activation of complement by theclassical, lectin, and alternative pathways. This peptide effectively inhibits complement activation inclinically relevant in vitro, ex vivo and, most importantly, in vivo models. The activity of the parentpeptide has now been improved 256 times. This proposal has three aims:
In Aim 1, a) the in vivoactivity of the most potent Compstatin analogs will be assessed, b) their in vivo efficacy will beimproved, and c) a mouse transgenic model using a human-mouse chimeric C3 will be generated toassess Compstatin's activity in the in vivo models proposed in Projects 1 and 2.
In Aim 2, phagepeptide libraries will be screened to identify complement inhibitors targeting factor B, *MASP2* *,C3, and C1.
In Aim 3, in silico screening methodologies utilizing public and commercial compoundlibraries will be applied to identify compounds targeting C3, factor B, *MASP2* *, and C1.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI068730-02
Application #
7686419
Study Section
Special Emphasis Panel (ZAI1-QV-I (M1))
Project Start
2008-09-01
Project End
2012-08-31
Budget Start
2008-09-01
Budget End
2009-08-31
Support Year
2
Fiscal Year
2008
Total Cost
$414,093
Indirect Cost

  Institution

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

  Publications

Bostanci, Nagihan; Bao, Kai; Li, Xiaofei et al. (2018) Gingival Exudatome Dynamics Implicate Inhibition of the Alternative Complement Pathway in the Protective Action of the C3 Inhibitor Cp40 in Nonhuman Primate Periodontitis. J Proteome Res 17:3153-3175
Ricklin, Daniel; Mastellos, Dimitrios C; Reis, Edimara S et al. (2018) The renaissance of complement therapeutics. Nat Rev Nephrol 14:26-47
Kwak, Jeff W; Laskowski, Jennifer; Li, Howard Y et al. (2018) Complement Activation via a C3a Receptor Pathway Alters CD4+ T Lymphocytes and Mediates Lung Cancer Progression. Cancer Res 78:143-156
Mastellos, Dimitrios C; Reis, Edimara S; Yancopoulou, Despina et al. (2018) Expanding Complement Therapeutics for the Treatment of Paroxysmal Nocturnal Hemoglobinuria. Semin Hematol 55:167-175
Reis, Edimara S; Mastellos, Dimitrios C; Ricklin, Daniel et al. (2018) Complement in cancer: untangling an intricate relationship. Nat Rev Immunol 18:5-18
Sauter, Reinhard J; Sauter, Manuela; Reis, Edimara S et al. (2018) Functional Relevance of the Anaphylatoxin Receptor C3aR for Platelet Function and Arterial Thrombus Formation Marks an Intersection Point Between Innate Immunity and Thrombosis. Circulation 138:1720-1735
Reis, Edimara S; Berger, Nadja; Wang, Xin et al. (2018) Safety profile after prolonged C3 inhibition. Clin Immunol 197:96-106
Laabei, Maisem; Liu, Guanghui; Ermert, David et al. (2018) Short Leucine-Rich Proteoglycans Modulate Complement Activity and Increase Killing of the Respiratory Pathogen Moraxella catarrhalis. J Immunol 201:2721-2730
Huber-Lang, Markus; Lambris, John D; Ward, Peter A (2018) Innate immune responses to trauma. Nat Immunol 19:327-341
Chen, Lan-Sun; Kourtzelis, Ioannis; Singh, Rashim Pal et al. (2018) Endothelial Cell-Specific Overexpression of Del-1 Drives Expansion of Haematopoietic Progenitor Cells in the Bone Marrow. Thromb Haemost :

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