AI Article Synopsis

  • Developing protein therapeutics requires optimizing their pharmacokinetic and pharmacodynamic properties, particularly to prolong their half-lives in the body.
  • A study compared various half-life extension technologies (PAS polypeptides, XTEN polypeptides, and an albumin binding domain) using an HER2 affibody-drug conjugate, revealing that while these extensions lowered HER2 affinity slightly, they maintained cytotoxic effectiveness.
  • The results indicated that the ABD-enhanced construct had the highest tumor uptake and the best overall performance, despite not having the longest half-life compared to others tested.

Article Abstract

A critical parameter during the development of protein therapeutics is to endow them with suitable pharmacokinetic and pharmacodynamic properties. Small protein drugs are quickly eliminated by kidney filtration, and in vivo half-life extension is therefore often desired. Here, different half-life extension technologies were studied where PAS polypeptides (PAS300, PAS600), XTEN polypeptides (XTEN288, XTEN576), and an albumin binding domain (ABD) were compared for half-life extension of an anti-human epidermal growth factor receptor 2 (HER2) affibody-drug conjugate. The results showed that extension with the PAS or XTEN polypeptides or the addition of the ABD lowered the affinity for HER2 to some extent but did not negatively affect the cytotoxic potential. The half-lives in mice ranged from 7.3 h for the construct including PAS300 to 11.6 h for the construct including PAS600. The highest absolute tumor uptake was found for the construct including the ABD, which was 60 to 160% higher than the PASylated or XTENylated constructs, even though it did not have the longest half-life (9.0 h). A comparison of the tumor-to-normal-organ ratios showed the best overall performance of the ABD-fused construct. In conclusion, PASylation, XTENylation, and the addition of an ABD are viable strategies for half-life extension of affibody-drug conjugates, with the best performance observed for the construct including the ABD.

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Source
http://dx.doi.org/10.1016/j.jconrel.2024.04.051DOI Listing

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