Neurobiology of Disease (Dec 2021)

ABBV-0805, a novel antibody selective for soluble aggregated α-synuclein, prolongs lifespan and prevents buildup of α-synuclein pathology in mouse models of Parkinson's disease

  • Eva Nordström,
  • Fredrik Eriksson,
  • Jessica Sigvardson,
  • Malin Johannesson,
  • Alex Kasrayan,
  • Martina Jones-Kostalla,
  • Paulina Appelkvist,
  • Linda Söderberg,
  • Patrik Nygren,
  • Magdalena Blom,
  • Adeline Rachalski,
  • Karin Nordenankar,
  • Olof Zachrisson,
  • Ebba Amandius,
  • Gunilla Osswald,
  • Mikael Moge,
  • Martin Ingelsson,
  • Joakim Bergström,
  • Lars Lannfelt,
  • Christer Möller,
  • Marco Giorgetti,
  • Johanna Fälting

Journal volume & issue
Vol. 161
p. 105543

Abstract

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A growing body of evidence suggests that aggregated α-synuclein, the major constituent of Lewy bodies, plays a key role in the pathogenesis of Parkinson's disease and related α-synucleinopathies. Immunotherapies, both active and passive, against α-synuclein have been developed and are promising novel treatment strategies for such disorders. Here, we report on the humanization and pharmacological characteristics of ABBV-0805, a monoclonal antibody that exhibits a high selectivity for human aggregated α-synuclein and very low affinity for monomers. ABBV-0805 binds to a broad spectrum of soluble aggregated α-synuclein, including small and large aggregates of different conformations.Binding of ABBV-0805 to pathological α-synuclein was demonstrated in Lewy body-positive post mortem brains of Parkinson's disease patients. The functional potency of ABBV-0805 was demonstrated in several cellular assays, including Fcγ-receptor mediated uptake of soluble aggregated α-synuclein in microglia and inhibition of neurotoxicity in primary neurons. In vivo, the murine version of ABBV-0805 (mAb47) displayed significant dose-dependent decrease of α-synuclein aggregates in brain in several mouse models, both in prophylactic and therapeutic settings. In addition, mAb47 treatment of α-synuclein transgenic mice resulted in a significantly prolonged survival.ABBV-0805 selectively targets soluble toxic α-synuclein aggregates with a picomolar affinity and demonstrates excellent in vivo efficacy. Based on the strong preclinical findings described herein, ABBV-0805 has been progressed into clinical development as a potential disease-modifying treatment for Parkinson's disease.

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