Chapter title |
Compstatin: A Complement Inhibitor on its Way to Clinical Application
|
---|---|
Chapter number | 20 |
Book title |
Current Topics in Complement II
|
Published in |
Advances in experimental medicine and biology, November 2008
|
DOI | 10.1007/978-0-387-78952-1_20 |
Pubmed ID | |
Book ISBNs |
978-0-387-78951-4, 978-0-387-78952-1
|
Authors |
Ricklin D, Lambris JD, Daniel Ricklin, John D. Lambris, Ricklin, Daniel, Lambris, John D. |
Abstract |
Therapeutic modulation of the human complement system is considered a promising approach for treating a number of pathological conditions. Owing to its central position in the cascade, component C3 is a particularly attractive target for complement-specific drugs. Compstatin, a cyclic tridecapeptide, which was originally discovered from phage-display libraries, is a highly potent and selective C3 inhibitor that demonstrated clinical potential in a series of experimental models. A combination of chemical, biophysical, and computational approaches allowed a remarkable optimization of its binding affinity towards C3 and its inhibitory potency. With the recent announcement of clinical trials with a compstatin analog for the treatment of age-related macular degeneration, another important milestone has been reached on its way to a drug. Furthermore, the release of a co-crystal structure of compstatin with C3c allows a detailed insight into the binding mode and paves the way to the rational design of peptides and mimetics with improved activity. Considering the new incentives and the promising pre-clinical results, compstatin seems to be well equipped for the challenges on its way to a clinical therapeutic. |
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Geographical breakdown
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Unknown | 117 | 96% |
Demographic breakdown
Readers by professional status | Count | As % |
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Student > Ph. D. Student | 29 | 24% |
Student > Master | 13 | 11% |
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Professor > Associate Professor | 8 | 7% |
Other | 16 | 13% |
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Chemistry | 8 | 7% |
Other | 22 | 18% |
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