1. Academic Validation
  2. The nuclear export inhibitor aminoratjadone is a potent effector in extracellular-targeted drug conjugates

The nuclear export inhibitor aminoratjadone is a potent effector in extracellular-targeted drug conjugates

  • Chem Sci. 2019 Apr 15;10(20):5197-5210. doi: 10.1039/c8sc05542d.
Philipp Klahn 1 2 Verena Fetz 1 Antje Ritter 1 Wera Collisi 1 3 Bettina Hinkelmann 1 Tatjana Arnold 1 Werner Tegge 1 Katharina Rox 1 4 Stephan Hüttel 3 Kathrin I Mohr 3 Joachim Wink 3 Marc Stadler 3 Josef Wissing 5 Lothar Jänsch 5 Mark Brönstrup 1 6 4
Affiliations

Affiliations

  • 1 Department of Chemical Biology , Helmholtz Centre for Infection Research , Inhoffenstrasse 7 , 38124 Braunschweig , Germany . Email: mark.broenstrup@helmholtz-hzi.de.
  • 2 Institute of Organic Chemistry , Technische Universität Braunschweig , Hagenring 30 , 38106 Braunschweig , Germany . Email: p.klahn@tu-braunschweig.de.
  • 3 Department of Microbial Drugs , Helmholtz Centre for Infection Research , Inhoffenstrasse 7 , 38124 Braunschweig , Germany.
  • 4 German Centre of Infection Research (DZIF) , Partner Site Hannover-Braunschweig , Germany.
  • 5 Department of Structure and Function of Proteins , Research Group Cellular Proteomic , Helmholtz Centre for Infection Research , Inhoffenstrasse 7 , 38124 Braunschweig , Germany.
  • 6 Biomolecular Drug Research Center (BMWZ) , Schneiderberg 38 , 30167 Hannover , Germany.
Abstract

The concept of targeted drug conjugates has been successfully translated to clinical practice in oncology. Whereas the majority of cytotoxic effectors in drug conjugates are directed against either DNA or tubulin, our study aimed to validate nuclear export inhibition as a novel effector principle in drug conjugates. For this purpose, a semisynthetic route starting from the natural product ratjadone A, a potent nuclear export inhibitor, has been developed. The biological evaluation of ratjadones functionalized at the 16-position revealed that oxo- and amino-analogues had very high potencies against Cancer cell lines (e.g. 16R-aminoratjadone 16 with IC50 = 260 pM against MCF-7 cells, or 19-oxoratjadone 14 with IC50 = 100 pM against A-549 cells). Mechanistically, the conjugates retained a nuclear export inhibitory activity through binding CRM1. To demonstrate a proof-of-principle for cellular targeting, folate- and luteinizing hormone releasing hormone (LHRH)-based carrier molecules were synthesized and coupled to aminoratjadones as well as fluorescein for cellular efficacy and imaging studies, respectively. The Trojan-Horse conjugates selectively addressed receptor-positive cell lines and were highly potent inhibitors of their proliferation. For example, the folate conjugate FA-7-Val-Cit-pABA-16R-aminoratjadone had an IC50 of 34.3 nM, and the LHRH conjugate d-Orn-Gose-Val-Cit-pABA-16R-aminoratjadone had an IC50 of 12.8 nM. The results demonstrate that nuclear export inhibition is a promising mode-of-action for extracellular-targeted drug conjugate payloads.

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