2009
DOI: 10.1016/j.dci.2008.07.006
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Functional characterization of human C3/cobra venom factor hybrid proteins for therapeutic complement depletion

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Cited by 28 publications
(43 citation statements)
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“…To address this issue, we engineered a hybrid protein in which a portion of the ␣ chain at the C terminus of human C3 is replaced with homologous regions of the CVF ␤ chain crucial to activity (HC3-1496). 20,30 Using both CVF and HC3-1496, we found that depletion of complement in the 38C13 model improved the efficacy of mAb therapy. Complement depletion after CVF lasted longer than that seen with HC3-1496; however, the enhanced therapeutic response was similar for both agents, suggesting prolonged depletion of complement may not be necessary to enhance the therapeutic response to mAb therapy.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…To address this issue, we engineered a hybrid protein in which a portion of the ␣ chain at the C terminus of human C3 is replaced with homologous regions of the CVF ␤ chain crucial to activity (HC3-1496). 20,30 Using both CVF and HC3-1496, we found that depletion of complement in the 38C13 model improved the efficacy of mAb therapy. Complement depletion after CVF lasted longer than that seen with HC3-1496; however, the enhanced therapeutic response was similar for both agents, suggesting prolonged depletion of complement may not be necessary to enhance the therapeutic response to mAb therapy.…”
Section: Discussionmentioning
confidence: 99%
“…The plasmid preparation, protein expression, and purification were performed essentially as previously described. 20 …”
Section: Antibodies and Reagentsmentioning
confidence: 99%
“…One of the limits of this treatment alternative in the clinic is the high immunogenicity of this compound (28). However, a human C3 hybrid, containing crucial regions of the CVF b chain (so-called humanized CVF or HC3-1496), has been created for this purpose (29). It will be of great interest to test other complement inhibitors currently in development in various solid tumor models to determine whether sustained treatment will favor the induction of an improved tumorspecific immune response and promote CD8 þ T-cell expansion.…”
Section: The Complement System Limits Systemic T-cell Activationmentioning
confidence: 99%
“…The structure showed that all the four modules of factor H interact with the C3b molecule in a discontinuous manner. On the basis of the structure (51) and previous studies (50,52), it was proposed that factor I inactivates C3b by interacting with the C3b-factor H complex at sites formed by the modules 1-3 of factor H, and C345C and complement C1r-C1s, UEGF, BMP1 domains of C3b. The VCP domains 1-4 are structurally and functionally similar to factor H modules 1-4.…”
Section: Vcp Domains Critical For Factor I Cfasmentioning
confidence: 99%