4.7 Article

Trp53 deficient mice predisposed to preterm birth display region-specific lipid alterations at the embryo implantation site

Journal

SCIENTIFIC REPORTS
Volume 6, Issue -, Pages -

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/srep33023

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Funding

  1. US Department of Energy (DOE) [DE-AC05-76RL01830]
  2. DOE's Office of Biological and Environmental Research
  3. NIH [HD068524, DA06668]
  4. March of Dimes
  5. NRSA predoctoral fellowship [F30AG040858]
  6. Swedish Research Counsel (VR) [621-2013-4231]
  7. Swedish Foundation for Strategic Research (SSF) at Uppsala University [ICA-6]

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Here we demonstrate that conditional deletion of mouse uterine Trp53 (p53(d/d)), molecularly linked to mTORC1 activation and causally linked to premature uterine senescence and preterm birth, results in aberrant lipid signatures within the heterogeneous cell types of embryo implantation sites on day 8 of pregnancy. In situ nanospray desorption electrospray ionization mass spectrometry imaging (nano-DESI MSI) was used to characterize the molecular speciation of free fatty acids, monoacylglycerol species, unmodified and oxidized phosphatidylcholine (PC/Ox-PC), and diacylglycerol (DG) species within implantation sites of p53(d/d) mice and floxed littermates. Implantation sites from p53(d/d) mice exhibited distinct spatially resolved changes demonstrating accumulation of DG species, depletion of Ox-PC species, and increase in species with more unsaturated acyl chains, including arachidonic and docosahexaenoic acid. Understanding abnormal changes in the abundance and localization of individual lipid species early in the progression to premature birth is an important step toward discovering novel targets for treatments and diagnosis.

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