Molecular Therapy: Nucleic Acids (Dec 2017)

An Albumin-Oligonucleotide Assembly for Potential Combinatorial Drug Delivery and Half-Life Extension Applications

  • Matthias Kuhlmann,
  • Jonas B.R. Hamming,
  • Anders Voldum,
  • Georgia Tsakiridou,
  • Maja T. Larsen,
  • Julie S. Schmøkel,
  • Emil Sohn,
  • Konrad Bienk,
  • David Schaffert,
  • Esben S. Sørensen,
  • Jesper Wengel,
  • Daniel M. Dupont,
  • Kenneth A. Howard

DOI
https://doi.org/10.1016/j.omtn.2017.10.004
Journal volume & issue
Vol. 9, no. C
pp. 284 – 293

Abstract

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The long blood circulatory property of human serum albumin, due to engagement with the cellular recycling neonatal Fc receptor (FcRn), is an attractive drug half-life extension enabling technology. This work describes a novel site-specific albumin double-stranded (ds) DNA assembly approach, in which the 3′ or 5′ end maleimide-derivatized oligodeoxynucleotides are conjugated to albumin cysteine at position 34 (cys34) and annealed with complementary strands to allow single site-specific protein modification with functionalized ds oligodeoxynucleotides. Electrophoretic gel shift assays demonstrated successful annealing of complementary strands bearing Atto488, 6-carboxyfluorescein (6-FAM), or a factor IXa aptamer to the albumin-oligodeoxynucleotide conjugate. A fluorometric factor IXa activity assay showed retained aptamer inhibitory activity upon assembly with the albumin and completely blocked factor IXa at a concentration of 100 nM for 2 hr. The assembled construct exhibited stability in serum-containing buffer and FcRn engagement that could be increased using an albumin variant engineered for higher FcRn affinity. This work presents a novel albumin-oligodeoxynucleotide assembly technology platform that offers potential combinatorial drug delivery and half-life extension applications.

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