Identification of Complin, a Novel Complement Inhibitor that Targets Complement Proteins Factor B and C2

Kadam, Archana P. ; Sahu, Arvind (2010) Identification of Complin, a Novel Complement Inhibitor that Targets Complement Proteins Factor B and C2 The Journal of Immunology, 184 (12). pp. 7116-7124. ISSN 0022-1767

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Official URL: http://doi.org/10.4049/jimmunol.1000200

Related URL: http://dx.doi.org/10.4049/jimmunol.1000200

Abstract

Complement factor B (fB) is a key constituent of the alternative pathway (AP). Its central role in causing inflammation and tissue injury through activation of the AP urges the need for its therapeutic targeting. In the current study, we have screened phage-displayed random peptide libraries against fB and identified a novel cyclic hendecapeptide that inhibits activation of fB and the AP. Structure-activity studies revealed that: 1) the cysteine-constrained structure of the peptide is essential for its activity; 2) Ile5, Arg6, Leu7, and Tyr8 contribute significantly to its inhibitory activity; and 3) retro-inverso modification of the peptide results in loss of its activity. Binding studies performed using surface plasmon resonance suggested that the peptide has two binding sites on fB, which are located on the Ba and Bb fragments. Studies on the mechanism of inhibition revealed that the peptide does not block the interaction of fB with the activated form of C3, thereby suggesting that the peptide inhibits fB activation primarily by inhibiting its cleavage by factor D. The peptide showed a weak effect on preformed C3 and C5 convertases. Like inhibition of fB cleavage, the peptide also inhibited C2 cleavage by activated C1s and activation of the classical as well as lectin pathways. Based on its inhibitory activities, we named the peptide Complin.

Item Type:Article
Source:Copyright of this article belongs to American Association of Immunologists.
ID Code:123305
Deposited On:13 Sep 2021 07:58
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