Cell Reports Medicine (May 2021)

NOTCH3-targeted antibody drug conjugates regress tumors by inducing apoptosis in receptor cells and through transendocytosis into ligand cells

  • Kenneth G. Geles,
  • Yijie Gao,
  • Andreas Giannakou,
  • Latha Sridharan,
  • Ting-Ting Yamin,
  • Jing Zhang,
  • Riyez Karim,
  • Joel Bard,
  • Nicole Piche-Nicholas,
  • Manoj Charati,
  • Andreas Maderna,
  • Judy Lucas,
  • Jonathon Golas,
  • Magali Guffroy,
  • Steven Pirie-Shepherd,
  • Marc Roy,
  • Jessie Qian,
  • Tania Franks,
  • Wenyan Zhong,
  • Christopher J. O’Donnell,
  • Lioudmila Tchistiakova,
  • Hans-Peter Gerber,
  • Puja Sapra

Journal volume & issue
Vol. 2, no. 5
p. 100279

Abstract

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Summary: Aberrant NOTCH3 signaling and overexpression is oncogenic, associated with cancer stem cells and drug resistance, yet therapeutic targeting remains elusive. Here, we develop NOTCH3-targeted antibody drug conjugates (NOTCH3-ADCs) by bioconjugation of an auristatin microtubule inhibitor through a protease cleavable linker to two antibodies with differential abilities to inhibit signaling. The signaling inhibitory antibody rapidly induces ligand-independent receptor clustering and internalization through both caveolin and clathrin-mediated pathways. The non-inhibitory antibody also efficiently endocytoses via clathrin without inducing receptor clustering but with slower lysosomal co-localization kinetics. In addition, DLL4 ligand binding to the NOTCH3 receptor mediates transendocytosis of NOTCH3-ADCs into ligand-expressing cells. NOTCH3-ADCs internalize into receptor and ligand cells independent of signaling and induce cell death in both cell types representing an atypical mechanism of ADC cytotoxicity. Treatment of xenografts with NOTCH3-ADCs leads to sustained tumor regressions, outperforms standard-of-care chemotherapy, and allows targeting of tumors that overexpress NOTCH3 independent of signaling inhibition.

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