2008
DOI: 10.1093/protein/gzm067
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Anti-serum albumin domain antibodies for extending the half-lives of short lived drugs

Abstract: We have used phage display to isolate a range of human domain antibodies (dAbs) that bind to mouse, rat and/or human serum albumin (SA) and can be expressed at very high levels in bacterial, yeast or mammalian cell culture. In contrast to non-SA-binding dAbs, which have terminal half-lives of less than 45 min, the half-lives of these 12 kDa 'AlbudAbs' can match the half-life of SA itself. To demonstrate the use of AlbudAbs for extending the half-lives of therapeutic drugs, we created a fusion of the interleuki… Show more

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Cited by 177 publications
(124 citation statements)
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“…As shown in Fig. 5A, the cytotoxic activity triggered by sdAb C17-Fc was lower than that of bsFab C21, both in terms of EC 50 (values in the nmol/L range) and of maximal lysis (< 50%), despite its bivalent binding to CEA. This result is likely due to the weaker interaction of the Fc portion of sdAb C17-Fc with FcgRIIIa, as compared with bsFab C21.…”
Section: Sensitivity To Fcgriiia Polymorphismmentioning
confidence: 82%
See 1 more Smart Citation
“…As shown in Fig. 5A, the cytotoxic activity triggered by sdAb C17-Fc was lower than that of bsFab C21, both in terms of EC 50 (values in the nmol/L range) and of maximal lysis (< 50%), despite its bivalent binding to CEA. This result is likely due to the weaker interaction of the Fc portion of sdAb C17-Fc with FcgRIIIa, as compared with bsFab C21.…”
Section: Sensitivity To Fcgriiia Polymorphismmentioning
confidence: 82%
“…Nevertheless, the bsFab format authorizes the linker-free addition of single-domain antibodies at the C-terminus of CH1 or Ck domains (data not shown). It can therefore be envisaged to construct trispecific formats by adding an anti-human serum albumin sdAb, a method that has been shown to significantly increase tumor retention and half-life (50,51).…”
Section: Discussionmentioning
confidence: 99%
“…Phage particles from a large synthetic Vk dAb repertoire (24) based on a fully human scaffold encoded by germline k L chain genes O12/O2/DPK9 and Jk1 with the side chain diversity incorporated at positions in the Ag binding site were prepared and purified as described (25). This library was selected against recombinant biotinylated monomeric human CD28 fragment in solution, matured, and expressed as previously described (26). Surface plasmon resonance method for affinity measurements.…”
Section: Methodsmentioning
confidence: 99%
“…One interesting programme is the fusion of an anti-HSA dAb (GSK2374697) to GLP-1 for the possible treatment of diabetes. The inclusion of an anti-HSA dAb as part of this drug formulation has validated the approach of 'piggybacking' on the long-lived serum protein as a method of increasing the half-life of biologically active but short-lived peptides in the body [89,90].…”
Section: Antibody-based Biologicsmentioning
confidence: 99%