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      <dc:title>Rapamycin administration is not a valid therapeutic strategy for every case of mitochondrial disease</dc:title>
      <dc:creator>Barriocanal Casado, Eliana</dc:creator>
      <dc:creator>Hidalgo Gutiérrez, Agustín</dc:creator>
      <dc:creator>Raimundo, Nuno</dc:creator>
      <dc:creator>González García, Pilar</dc:creator>
      <dc:creator>Acuña Castroviejo, Darío</dc:creator>
      <dc:creator>Escames Rosa, Germaine</dc:creator>
      <dc:creator>López García, Luis Carlos</dc:creator>
      <dc:subject>CoQ deficiency</dc:subject>
      <dc:subject>Mitochondrial encephalopathy</dc:subject>
      <dc:subject>Mitochondrial diseases</dc:subject>
      <dc:subject>mTORC1</dc:subject>
      <dc:subject>Mouse model</dc:subject>
      <dc:description>Supplementary data to this article can be found online at https://doi.&#xd;
org/10.1016/j.ebiom.2019.03.025.</dc:description>
      <dc:description>Background: The vastmajority ofmitochondrial disorders have limited the clinicalmanagement to palliative care.&#xd;
Rapamycin has emerged as a potential therapeutic drug formitochondrial diseases since it has shown therapeutic&#xd;
benefits in a fewmousemodels ofmitochondrial disorders. However, the underlying therapeutic mechanism&#xd;
is unclear, theminimal effective dose needs to be defined and whether this therapy can be generally used is unknown.&#xd;
Methods: Wehave evaluatedwhether lowand high doses of rapamycin administration may result in therapeutic&#xd;
effects in a mousemodel (Coq9R239X) ofmitochondrial encephalopathy due to CoQ deficiency. The evaluation involved&#xd;
phenotypic, molecular, image (histopathology and MRI),metabolomics, transcriptomics and bioenergetics&#xd;
analyses.&#xd;
Findings: Low dose of rapamycin induces metabolic changes in liver and transcriptomics modifications in midbrain.&#xd;
The high dose of rapamycin induces further changes in the transcriptomics profile in midbrain due to&#xd;
the general inhibition of mTORC1. However, neither low nor high dose of rapamycin were able to improve the&#xd;
mitochondrial bioenergetics, the brain injuries and the phenotypic characteristics of Coq9R239X mice, resulting&#xd;
in the lack of efficacy for increasing the survival.&#xd;
Interpretation: These results may be due to the lack ofmicrogliosis-derived neuroinflammation, the limitation to&#xd;
induce autophagy, or the need of a functional CoQ-junction. Therefore, the translation of rapamycin therapy into&#xd;
the clinic for patients with mitochondrial disorders requires, at least, the consideration of the particularities of&#xd;
each mitochondrial disease.</dc:description>
      <dc:date>2019-07-19T10:53:48Z</dc:date>
      <dc:date>2019-07-19T10:53:48Z</dc:date>
      <dc:date>2019-03-18</dc:date>
      <dc:type>info:eu-repo/semantics/article</dc:type>
      <dc:identifier>E. Barriocanal-Casado et al. Rapamycin administration is not a valid therapeutic strategy for every case of mitochondrial disease. EBioMedicine 42 (2019) 511–523 [https://doi.org/10.1016/j.ebiom.2019.03.025]</dc:identifier>
      <dc:identifier>http://hdl.handle.net/10481/56472</dc:identifier>
      <dc:identifier>https://doi.org/10.1016/j.ebiom.2019.03.025</dc:identifier>
      <dc:language>eng</dc:language>
      <dc:rights>http://creativecommons.org/licenses/by/3.0/es/</dc:rights>
      <dc:rights>info:eu-repo/semantics/openAccess</dc:rights>
      <dc:rights>Atribución 3.0 España</dc:rights>
      <dc:publisher>Elsevier B. V.</dc:publisher>
   </ow:Publication>
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