International Journal of Molecular Sciences (Dec 2022)

Anti-SOD1 Nanobodies That Stabilize Misfolded SOD1 Proteins Also Promote Neurite Outgrowth in Mutant SOD1 Human Neurons

  • Meenakshi Sundaram Kumar,
  • Megan E. Fowler-Magaw,
  • Daniel Kulick,
  • Sivakumar Boopathy,
  • Del Hayden Gadd,
  • Melissa Rotunno,
  • Catherine Douthwright,
  • Diane Golebiowski,
  • Issa Yusuf,
  • Zuoshang Xu,
  • Robert H. Brown,
  • Miguel Sena-Esteves,
  • Alison L. O'Neil,
  • Daryl A. Bosco

DOI
https://doi.org/10.3390/ijms232416013
Journal volume & issue
Vol. 23, no. 24
p. 16013

Abstract

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ALS-linked mutations induce aberrant conformations within the SOD1 protein that are thought to underlie the pathogenic mechanism of SOD1-mediated ALS. Although clinical trials are underway for gene silencing of SOD1, these approaches reduce both wild-type and mutated forms of SOD1. Here, we sought to develop anti-SOD1 nanobodies with selectivity for mutant and misfolded forms of human SOD1 over wild-type SOD1. Characterization of two anti-SOD1 nanobodies revealed that these biologics stabilize mutant SOD1 in vitro. Further, SOD1 expression levels were enhanced and the physiological subcellular localization of mutant SOD1 was restored upon co-expression of anti-SOD1 nanobodies in immortalized cells. In human motor neurons harboring the SOD1 A4V mutation, anti-SOD1 nanobody expression promoted neurite outgrowth, demonstrating a protective effect of anti-SOD1 nanobodies in otherwise unhealthy cells. In vitro assays revealed that an anti-SOD1 nanobody exhibited selectivity for human mutant SOD1 over endogenous murine SOD1, thus supporting the preclinical utility of anti-SOD1 nanobodies for testing in animal models of ALS. In sum, the anti-SOD1 nanobodies developed and presented herein represent viable biologics for further preclinical testing in human and mouse models of ALS.

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