Nature Communications (Jan 2025)

The widely used Ucp1-Cre transgene elicits complex developmental and metabolic phenotypes

  • Manasi Suchit Halurkar,
  • Oto Inoue,
  • Archana Singh,
  • Rajib Mukherjee,
  • Meghana Ginugu,
  • Christopher Ahn,
  • Christian Louis Bonatto Paese,
  • Molly Duszynski,
  • Samantha A. Brugmann,
  • Hee-Woong Lim,
  • Joan Sanchez-Gurmaches

DOI
https://doi.org/10.1038/s41467-024-54763-4
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 16

Abstract

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Abstract Bacterial artificial chromosome transgenic models, including most Cre-recombinases, enable potent interrogation of gene function in vivo but require rigorous validation as limitations emerge. Due to its high relevance to metabolic studies, we perform comprehensive analysis of the Ucp1-Cre Evdr line which is widely used for brown fat research. Hemizygotes exhibit major brown and white fat transcriptomic dysregulation, indicating potential altered tissue function. Ucp1-Cre Evdr homozygotes also show high mortality, tissue specific growth defects, and craniofacial abnormalities. Mapping the transgene insertion site reveals insertion in chromosome 1 accompanied by large genomic alterations disrupting several genes expressed in a range of tissues. Notably, Ucp1-Cre Evdr transgene retains an extra Ucp1 gene copy that may be highly expressed under high thermogenic burden. Our multi-faceted analysis highlights a complex phenotype arising from the presence of the Ucp1-Cre Evdr transgene independently of intended genetic manipulations. Overall, comprehensive validation of transgenic mice is imperative to maximize discovery while mitigating unexpected, off-target effects.