CEL-1000—a peptide with adjuvant activity for Th1 immune responses

Y Charoenvit, N Goel, M Whelan, KS Rosenthal… - Vaccine, 2004 - Elsevier
Y Charoenvit, N Goel, M Whelan, KS Rosenthal, DH Zimmerman
Vaccine, 2004Elsevier
CEL-1000 (derG, DGQEEKAGVVSTGLIGGG) is a small immunomodulatory peptide which
delivers demonstrated protective activity in two infectious disease challenge models (HSV
and malaria) and an allogenic tumor vaccine model. CEL-1000 and other activators
(defensin-β, CpG ODN, and imiquimod) of the innate immune system promote IFN-γ-
associated protective responses. CEL-1000 is an improved form of peptide G (a peptide
from human MHC II β chain second domain, aa 135–149) known to enhance immune …
CEL-1000 (derG, DGQEEKAGVVSTGLIGGG) is a small immunomodulatory peptide which delivers demonstrated protective activity in two infectious disease challenge models (HSV and malaria) and an allogenic tumor vaccine model. CEL-1000 and other activators (defensin-β, CpG ODN, and imiquimod) of the innate immune system promote IFN-γ-associated protective responses. CEL-1000 is an improved form of peptide G (a peptide from human MHC II β chain second domain, aa 135–149) known to enhance immune responses of other immunogenic peptides. Since defensin-β, CpG ODN, and imiquimod have been shown to possess adjuvant activity, we investigated the adjuvant effect of peptide G and CEL-1000 as conjugates with HIV and malaria peptides. Antibody titers and isotypes were evaluated on serum taken from select days following immunization. Results for CEL-1000 and G peptide conjugates were compared with results for KLH conjugates of the same HIV peptide from the p17 molecule (87–116) referred to as HGP-30. Studies demonstrated that comparable titers were seen on day 28, 42, 63, and 77 with either G or KLH-HGP-30 peptide conjugates. In another study, CEL-1000 conjugates (CEL-1000-HGP-30) demonstrated a 4–10-fold higher titer antibody response than seen with several other peptide conjugates of the same HGP-30 peptide. Improved adjuvant activity of CEL-1000 in peptide conjugates was also demonstrated by a shift in the antibody isotypes toward a Th1 response (IgG2a). The IgG2a/IgG1, ratio for G-HGP-30 HIV or KLH-HGP-30 HIV conjugates were lower than for the CEL-1000-HGP-30 HIV conjugate. A similar favoring of the IgG2a/IgG1 ratio was seen for a malaria peptide conjugate (CEL-1000-SF/GF) compared to the un-conjugated peptide (SF-GF). CEL-1000 also showed adjuvant activity in an allogenic tumor vaccine model. As expected for an adjuvant, CEL-1000 or G does not induce detectable self-directed or cross reactive antibodies. CEL-1000 is currently being investigated for use as an adjuvant with conventional vaccines. It is expected that IgG2a antibodies would be preferably generated by CEL-1000 adjuvancy and could enhance in vivo clearance of antigens or pathogens.
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