Cell Reports (May 2023)

Fanconi anemia-associated chromosomal radial formation is dependent on POLθ-mediated alternative end joining

  • Colette B. Rogers,
  • Rachel E. Kram,
  • Kevin Lin,
  • Chad L. Myers,
  • Alexandra Sobeck,
  • Eric A. Hendrickson,
  • Anja-Katrin Bielinsky

Journal volume & issue
Vol. 42, no. 5
p. 112428

Abstract

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Summary: Activation of the Fanconi anemia (FA) pathway after treatment with mitomycin C (MMC) is essential for preventing chromosome translocations termed “radials.” When replication forks stall at MMC-induced interstrand crosslinks (ICLs), the FA pathway is activated to orchestrate ICL unhooking and repair of the DNA break intermediates. However, in FA-deficient cells, how ICL-associated breaks are resolved in a manner that leads to radials is unclear. Here, we demonstrate that MMC-induced radials are dependent on DNA polymerase theta (POLθ)-mediated alternative end joining (A-EJ). Specifically, we show that radials observed in FANCD2−/− cells are dependent on POLθ and DNA ligase III and occur independently of classical non-homologous end joining. Furthermore, treatment of FANCD2−/− cells with POLθ inhibitors abolishes radials and leads to the accumulation of breaks co-localizing with common fragile sites. Uniformly, these observations implicate A-EJ in radial formation and provide mechanistic insights into the treatment of FA pathway-deficient cancers with POLθ inhibitors.

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