PLoS ONE (Jan 2019)

FBXO7 sensitivity of phenotypic traits elucidated by a hypomorphic allele.

  • Carmen Ballesteros Reviriego,
  • Simon Clare,
  • Mark J Arends,
  • Emma L Cambridge,
  • Agnieszka Swiatkowska,
  • Susana Caetano,
  • Bushra Abu-Helil,
  • Leanne Kane,
  • Katherine Harcourt,
  • David A Goulding,
  • Diane Gleeson,
  • Edward Ryder,
  • Brendan Doe,
  • Jacqueline K White,
  • Louise van der Weyden,
  • Gordon Dougan,
  • David J Adams,
  • Anneliese O Speak

DOI
https://doi.org/10.1371/journal.pone.0212481
Journal volume & issue
Vol. 14, no. 3
p. e0212481

Abstract

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FBXO7 encodes an F box containing protein that interacts with multiple partners to facilitate numerous cellular processes and has a canonical role as part of an SCF E3 ubiquitin ligase complex. Mutation of FBXO7 is responsible for an early onset Parkinsonian pyramidal syndrome and genome-wide association studies have linked variants in FBXO7 to erythroid traits. A putative orthologue in Drosophila, nutcracker, has been shown to regulate the proteasome, and deficiency of nutcracker results in male infertility. Therefore, we reasoned that modulating Fbxo7 levels in a murine model could provide insights into the role of this protein in mammals. We used a targeted gene trap model which retained 4-16% residual gene expression and assessed the sensitivity of phenotypic traits to gene dosage. Fbxo7 hypomorphs showed regenerative anaemia associated with a shorter erythrocyte half-life, and male mice were infertile. Alterations to T cell phenotypes were also observed, which intriguingly were both T cell intrinsic and extrinsic. Hypomorphic mice were also sensitive to infection with Salmonella, succumbing to a normally sublethal challenge. Despite these phenotypes, Fbxo7 hypomorphs were produced at a normal Mendelian ratio with a normal lifespan and no evidence of neurological symptoms. These data suggest that erythrocyte survival, T cell development and spermatogenesis are particularly sensitive to Fbxo7 gene dosage.