4.8 Article

Fatty acids homeostasis during fasting predicts protection from chemotherapy toxicity

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NATURE COMMUNICATIONS
卷 13, 期 1, 页码 -

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NATURE PORTFOLIO
DOI: 10.1038/s41467-022-33352-3

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资金

  1. Ramon Areces Foundation [CIVP18A3891]
  2. Asociacion Espanola contra el Cancer-AECC [SIRTBIO-LABAE18008FERN]
  3. Spanish Ministry of Science, Innovation and Universities (MICINN) [RYC-2017-22335]
  4. RETOS projects Program of MICINN [SAF2017-85766-R]
  5. Portuguese Foundation for Science and Technology (FCT-MCTES) [SFRH/BD/124022/2016]
  6. MICINN [PID2019-110183RB-C21, PID-2019-106893RA-100]
  7. Regional Government of Community of Madrid [P2018/BAA-4343-ALIBIRD2020-CM]
  8. Ramon Areces Foundation
  9. Comunidad de Madrid-Talento Grant [2018-T1/BMD-11966]
  10. Health Research Fund [ISCIII FIS PI14/01374, FISPI17/00508]
  11. Manuel de Oya research fellowship from the Beer and Health Foundation
  12. Ramon y Cajal Award from MICINN [RYC-2013-13546]
  13. RETOS projects Program of the MICINN
  14. European Regional Development Fund (ERDF) [SAF2015-67538-R, SAF2013-48256-R]
  15. IRB
  16. Spanish Ministry of Economy
  17. European Research Council [ERC-2014-AdG/669622]
  18. laCaixa Foundation

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The study shows that fasting can provide protection from chemotherapy-associated toxicity. They found that the profile of fatty acids in erythrocyte membranes and gene expression in peripheral blood mononuclear cells are associated with the benefits of fasting during cancer treatment in mice and patients.
Fasting exerts beneficial effects in mice and humans, including protection from chemotherapy toxicity. To explore the involved mechanisms, we collect blood from humans and mice before and after 36 or 24 hours of fasting, respectively, and measure lipid composition of erythrocyte membranes, circulating micro RNAs (miRNAs), and RNA expression at peripheral blood mononuclear cells (PBMCs). Fasting coordinately affects the proportion of polyunsaturated versus saturated and monounsaturated fatty acids at the erythrocyte membrane; and reduces the expression of insulin signaling-related genes in PBMCs. When fasted for 24 hours before and 24 hours after administration of oxaliplatin or doxorubicin, mice show a strong protection from toxicity in several tissues. Erythrocyte membrane lipids and PBMC gene expression define two separate groups of individuals that accurately predict a differential protection from chemotherapy toxicity, with important clinical implications. Our results reveal a mechanism of fasting associated with lipid homeostasis, and provide biomarkers of fasting to predict fasting-mediated protection from chemotherapy toxicity. Fasting has been reported to protect from chemotherapy-associated toxicity. Here, the authors show that fatty acid profiles in erythrocyte membranes and gene expression from peripheral blood mononuclear cells are associated to the fasting-mediated benefits during cancer treatment in mice and patients.

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