npj Parkinson's Disease (Mar 2021)

Il-10 signaling reduces survival in mouse models of synucleinopathy

  • Samuel G. Cockey,
  • Karen N. McFarland,
  • Emily J. Koller,
  • Mieu M. T. Brooks,
  • Elsa Gonzalez De La Cruz,
  • Pedro E. Cruz,
  • Carolina Ceballos-Diaz,
  • Awilda M. Rosario,
  • Yona R. Levites,
  • David R. Borchelt,
  • Todd E. Golde,
  • Benoit I. Giasson,
  • Paramita Chakrabarty

DOI
https://doi.org/10.1038/s41531-021-00169-8
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 14

Abstract

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Abstract Parkinson’s disease (PD) and related synucleinopathies are characterized by chronic neuroinflammation leading to the premise that anti-inflammatory therapies could ameliorate synucleinopathy and associated sequelae. To test this idea, we used recombinant adeno-associated viruses (AAV) to express the anti-inflammatory cytokine, Interleukin (Il)-10, in Line M83 transgenic mice that expresses the PD-associated A53T mutant human α-synuclein (αSyn). Contrary to our expectations, we observed that intraspinal Il-10 expression initiated at birth upregulated microgliosis and led to early death in homozygous M83+/+ mice. We further observed that Il-10 preconditioning led to reduced lifespan in the hemizygous M83+/− mice injected with preformed αSyn aggregates in hindlimb muscles. To determine the mechanistic basis for these adverse effects, we took advantage of the I87A variant Il-10 (vIl-10) that has predominantly immunosuppressive properties. Sustained intraspinal expression of vIl-10 in preformed αSyn-aggregate seeded M83+/− mice resulted in earlier death, accelerated αSyn pathology, pronounced microgliosis, and increased apoptosis compared to control mice. AAV-vIl-10 expression robustly induced p62 and neuronal LC3B accumulation in these mice, indicating that Il-10 signaling mediated preconditioning of the neuraxis can potentially exacerbate αSyn accumulation through autophagy dysfunction in the neurons. Together, our data demonstrate unexpected adverse effects of both Il-10 and its immunosuppressive variant, vIl-10, in a mouse model of PD, highlighting the pleiotropic functions of immune mediators and their complex role in non-cell autonomous signaling in neurodegenerative proteinopathies.