Mitochondrial Dysfunction in Pten Haplo-Insufficient Mice with Social Deficits and Repetitive Behavior: Interplay between Pten and p53

Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential of being enhanced by defects in bioenergetics. To this end, the occurrence of social deficits and mitochondrial outcomes were evaluated in con...

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Published in	PloS one Vol. 7; no. 8; p. e42504
Main Authors	Napoli, Eleonora, Ross-Inta, Catherine, Wong, Sarah, Hung, Connie, Fujisawa, Yasuko, Sakaguchi, Danielle, Angelastro, James, Omanska-Klusek, Alicja, Schoenfeld, Robert, Giulivi, Cecilia
Format	Journal Article
Language	English
Published	United States Public Library of Science 10.08.2012 Public Library of Science (PLoS)
Subjects	1-Phosphatidylinositol 3-kinase Aberration Abnormalities AKT protein Alzheimer's disease Animal tissues Animals Autism Avoidance behavior Behavior Behavior, Animal Bioenergetics Biology Cerebellar Cortex - metabolism Cerebellum Cerebellum - metabolism Cytochrome Cytochrome-c oxidase Defects Disabilities Electron Transport Complex IV - metabolism Etiology Female Gene dosage Genetic aspects Grooming GTP-binding protein Haploinsufficiency - genetics HCT116 Cells Hippocampus - metabolism Homology Humans Macrocephaly Male Medicine Megalencephaly - genetics Mice Mice, Knockout Mitochondria Mitochondria - genetics Mitochondria - metabolism Mitochondrial DNA Mutation Neostriatum Neurodegenerative diseases Neurons Neurons - metabolism Oxidative stress p53 Protein Phosphatases Proteins PTEN Phosphohydrolase - genetics PTEN Phosphohydrolase - metabolism PTEN protein Rodents Signal transduction Signaling Social aspects Social behavior Social Behavior Disorders - genetics Social Behavior Disorders - metabolism Tensin Tumor proteins Tumor Suppressor Protein p53 - genetics Tumor Suppressor Protein p53 - metabolism Veterinary colleges United States > US California
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Abstract	Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential of being enhanced by defects in bioenergetics. To this end, the occurrence of social deficits and mitochondrial outcomes were evaluated in conditional Pten (Phosphatase and tensin homolog) haplo-insufficient mice, in which only one allele was selectively knocked-out in neural tissues. Pten mutations have been linked to Alzheimer's disease and syndromic autism spectrum disorders, among others. By 4-6 weeks of age, Pten insufficiency resulted in the increase of several mitochondrial Complex activities (II-III, IV and V) not accompanied by increases in mitochondrial mass, consistent with an activation of the PI3K/Akt pathway, of which Pten is a negative modulator. At 8-13 weeks of age, Pten haplo-insufficient mice did not show significant behavioral abnormalities or changes in mitochondrial outcomes, but by 20-29 weeks, they displayed aberrant social behavior (social avoidance, failure to recognize familiar mouse, and repetitive self-grooming), macrocephaly, increased oxidative stress, decreased cytochrome c oxidase (CCO) activity (50%) and increased mtDNA deletions in cerebellum and hippocampus. Mitochondrial dysfunction was the result of a downregulation of p53-signaling pathway evaluated by lower protein expression of p21 (65% of controls) and the CCO chaperone SCO2 (47% of controls), two p53-downstream targets. This mechanism was confirmed in Pten-deficient striatal neurons and, HCT 116 cells with different p53 gene dosage. These results suggest a unique pathogenic mechanism of the Pten-p53 axis in mice with aberrant social behavior: loss of Pten (via p53) impairs mitochondrial function elicited by an early defective assembly of CCO and later enhanced by the accumulation of mtDNA deletions. Consistent with our results, (i) SCO2 deficiency and/or CCO activity defects have been reported in patients with learning disabilities including autism and (ii) mutated proteins in ASD have been found associated with p53-signaling pathways.
AbstractList	Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential of being enhanced by defects in bioenergetics. To this end, the occurrence of social deficits and mitochondrial outcomes were evaluated in conditional Pten (Phosphatase and tensin homolog) haplo-insufficient mice, in which only one allele was selectively knocked-out in neural tissues. Pten mutations have been linked to Alzheimer's disease and syndromic autism spectrum disorders, among others. By 4-6 weeks of age, Pten insufficiency resulted in the increase of several mitochondrial Complex activities (II-III, IV and V) not accompanied by increases in mitochondrial mass, consistent with an activation of the PI3K/Akt pathway, of which Pten is a negative modulator. At 8-13 weeks of age, Pten haplo-insufficient mice did not show significant behavioral abnormalities or changes in mitochondrial outcomes, but by 20-29 weeks, they displayed aberrant social behavior (social avoidance, failure to recognize familiar mouse, and repetitive self-grooming), macrocephaly, increased oxidative stress, decreased cytochrome c oxidase (CCO) activity (50%) and increased mtDNA deletions in cerebellum and hippocampus. Mitochondrial dysfunction was the result of a downregulation of p53-signaling pathway evaluated by lower protein expression of p21 (65% of controls) and the CCO chaperone SCO2 (47% of controls), two p53-downstream targets. This mechanism was confirmed in Pten-deficient striatal neurons and, HCT 116 cells with different p53 gene dosage. These results suggest a unique pathogenic mechanism of the Pten-p53 axis in mice with aberrant social behavior: loss of Pten (via p53) impairs mitochondrial function elicited by an early defective assembly of CCO and later enhanced by the accumulation of mtDNA deletions. Consistent with our results, (i) SCO2 deficiency and/or CCO activity defects have been reported in patients with learning disabilities including autism and (ii) mutated proteins in ASD have been found associated with p53-signaling pathways. Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential of being enhanced by defects in bioenergetics. To this end, the occurrence of social deficits and mitochondrial outcomes were evaluated in conditional Pten (Phosphatase and tensin homolog) haplo-insufficient mice, in which only one allele was selectively knocked-out in neural tissues. Pten mutations have been linked to Alzheimer's disease and syndromic autism spectrum disorders, among others. By 4-6 weeks of age, Pten insufficiency resulted in the increase of several mitochondrial Complex activities (II-III, IV and V) not accompanied by increases in mitochondrial mass, consistent with an activation of the PI3K/Akt pathway, of which Pten is a negative modulator. At 8-13 weeks of age, Pten haplo-insufficient mice did not show significant behavioral abnormalities or changes in mitochondrial outcomes, but by 20-29 weeks, they displayed aberrant social behavior (social avoidance, failure to recognize familiar mouse, and repetitive self-grooming), macrocephaly, increased oxidative stress, decreased cytochrome c oxidase (CCO) activity (50%) and increased mtDNA deletions in cerebellum and hippocampus. Mitochondrial dysfunction was the result of a downregulation of p53-signaling pathway evaluated by lower protein expression of p21 (65% of controls) and the CCO chaperone SCO2 (47% of controls), two p53-downstream targets. This mechanism was confirmed in Pten-deficient striatal neurons and, HCT 116 cells with different p53 gene dosage. These results suggest a unique pathogenic mechanism of the Pten-p53 axis in mice with aberrant social behavior: loss of Pten (via p53) impairs mitochondrial function elicited by an early defective assembly of CCO and later enhanced by the accumulation of mtDNA deletions. Consistent with our results, (i) SCO2 deficiency and/or CCO activity defects have been reported in patients with learning disabilities including autism and (ii) mutated proteins in ASD have been found associated with p53-signaling pathways.Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential of being enhanced by defects in bioenergetics. To this end, the occurrence of social deficits and mitochondrial outcomes were evaluated in conditional Pten (Phosphatase and tensin homolog) haplo-insufficient mice, in which only one allele was selectively knocked-out in neural tissues. Pten mutations have been linked to Alzheimer's disease and syndromic autism spectrum disorders, among others. By 4-6 weeks of age, Pten insufficiency resulted in the increase of several mitochondrial Complex activities (II-III, IV and V) not accompanied by increases in mitochondrial mass, consistent with an activation of the PI3K/Akt pathway, of which Pten is a negative modulator. At 8-13 weeks of age, Pten haplo-insufficient mice did not show significant behavioral abnormalities or changes in mitochondrial outcomes, but by 20-29 weeks, they displayed aberrant social behavior (social avoidance, failure to recognize familiar mouse, and repetitive self-grooming), macrocephaly, increased oxidative stress, decreased cytochrome c oxidase (CCO) activity (50%) and increased mtDNA deletions in cerebellum and hippocampus. Mitochondrial dysfunction was the result of a downregulation of p53-signaling pathway evaluated by lower protein expression of p21 (65% of controls) and the CCO chaperone SCO2 (47% of controls), two p53-downstream targets. This mechanism was confirmed in Pten-deficient striatal neurons and, HCT 116 cells with different p53 gene dosage. These results suggest a unique pathogenic mechanism of the Pten-p53 axis in mice with aberrant social behavior: loss of Pten (via p53) impairs mitochondrial function elicited by an early defective assembly of CCO and later enhanced by the accumulation of mtDNA deletions. Consistent with our results, (i) SCO2 deficiency and/or CCO activity defects have been reported in patients with learning disabilities including autism and (ii) mutated proteins in ASD have been found associated with p53-signaling pathways. Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential of being enhanced by defects in bioenergetics. To this end, the occurrence of social deficits and mitochondrial outcomes were evaluated in conditional Pten (Phosphatase and tensin homolog) haplo-insufficient mice, in which only one allele was selectively knocked-out in neural tissues. Pten mutations have been linked to Alzheimer's disease and syndromic autism spectrum disorders, among others. By 4–6 weeks of age, Pten insufficiency resulted in the increase of several mitochondrial Complex activities (II–III, IV and V) not accompanied by increases in mitochondrial mass, consistent with an activation of the PI3K/Akt pathway, of which Pten is a negative modulator. At 8–13 weeks of age, Pten haplo-insufficient mice did not show significant behavioral abnormalities or changes in mitochondrial outcomes, but by 20–29 weeks, they displayed aberrant social behavior (social avoidance, failure to recognize familiar mouse, and repetitive self-grooming), macrocephaly, increased oxidative stress, decreased cytochrome c oxidase (CCO) activity (50%) and increased mtDNA deletions in cerebellum and hippocampus. Mitochondrial dysfunction was the result of a downregulation of p53-signaling pathway evaluated by lower protein expression of p21 (65% of controls) and the CCO chaperone SCO2 (47% of controls), two p53-downstream targets. This mechanism was confirmed in Pten-deficient striatal neurons and, HCT 116 cells with different p53 gene dosage. These results suggest a unique pathogenic mechanism of the Pten-p53 axis in mice with aberrant social behavior: loss of Pten (via p53) impairs mitochondrial function elicited by an early defective assembly of CCO and later enhanced by the accumulation of mtDNA deletions. Consistent with our results, (i) SCO2 deficiency and/or CCO activity defects have been reported in patients with learning disabilities including autism and (ii) mutated proteins in ASD have been found associated with p53-signaling pathways.
Audience	Academic
Author	Napoli, Eleonora Giulivi, Cecilia Hung, Connie Fujisawa, Yasuko Omanska-Klusek, Alicja Sakaguchi, Danielle Schoenfeld, Robert Wong, Sarah Angelastro, James Ross-Inta, Catherine
AuthorAffiliation	1 Department of Molecular Biosciences, School of Veterinary Medicine, University of California Davis, Davis, California, United States of America University of Texas Health Science Center at San Antonio, United States of America 2 Medical Investigations of Neurodevelopmental Disorders Institute, School of Medicine, University of California Davis, Davis, California, United States of America
AuthorAffiliation_xml	– name: 1 Department of Molecular Biosciences, School of Veterinary Medicine, University of California Davis, Davis, California, United States of America – name: 2 Medical Investigations of Neurodevelopmental Disorders Institute, School of Medicine, University of California Davis, Davis, California, United States of America – name: University of Texas Health Science Center at San Antonio, United States of America
Author_xml	– sequence: 1 givenname: Eleonora surname: Napoli fullname: Napoli, Eleonora – sequence: 2 givenname: Catherine surname: Ross-Inta fullname: Ross-Inta, Catherine – sequence: 3 givenname: Sarah surname: Wong fullname: Wong, Sarah – sequence: 4 givenname: Connie surname: Hung fullname: Hung, Connie – sequence: 5 givenname: Yasuko surname: Fujisawa fullname: Fujisawa, Yasuko – sequence: 6 givenname: Danielle surname: Sakaguchi fullname: Sakaguchi, Danielle – sequence: 7 givenname: James surname: Angelastro fullname: Angelastro, James – sequence: 8 givenname: Alicja surname: Omanska-Klusek fullname: Omanska-Klusek, Alicja – sequence: 9 givenname: Robert surname: Schoenfeld fullname: Schoenfeld, Robert – sequence: 10 givenname: Cecilia surname: Giulivi fullname: Giulivi, Cecilia
BackLink	https://www.ncbi.nlm.nih.gov/pubmed/22900024$$D View this record in MEDLINE/PubMed
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Copyright	COPYRIGHT 2012 Public Library of Science Napoli et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License. 2012 Napoli et al 2012 Napoli et al
Copyright_xml	– notice: COPYRIGHT 2012 Public Library of Science – notice: Napoli et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License. – notice: 2012 Napoli et al 2012 Napoli et al
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Notes	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 14 content type line 23 Conceived and designed the experiments: EN YF CG. Performed the experiments: EN CRI DS SW CH RS YF AOK. Analyzed the data: EN CRI SW CH YF CG. Wrote the paper: EN CRI SW JA CG. Obtained permission to use cell line: CG. Competing Interests: The authors have declared that no competing interests exist.
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Snippet	Etiology of aberrant social behavior consistently points to a strong polygenetic component involved in fundamental developmental pathways, with the potential...
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SubjectTerms	1-Phosphatidylinositol 3-kinase Aberration Abnormalities AKT protein Alzheimer's disease Animal tissues Animals Autism Avoidance behavior Behavior Behavior, Animal Bioenergetics Biology Cerebellar Cortex - metabolism Cerebellum Cerebellum - metabolism Cytochrome Cytochrome-c oxidase Defects Disabilities Electron Transport Complex IV - metabolism Etiology Female Gene dosage Genetic aspects Grooming GTP-binding protein Haploinsufficiency - genetics HCT116 Cells Hippocampus - metabolism Homology Humans Macrocephaly Male Medicine Megalencephaly - genetics Mice Mice, Knockout Mitochondria Mitochondria - genetics Mitochondria - metabolism Mitochondrial DNA Mutation Neostriatum Neurodegenerative diseases Neurons Neurons - metabolism Oxidative stress p53 Protein Phosphatases Proteins PTEN Phosphohydrolase - genetics PTEN Phosphohydrolase - metabolism PTEN protein Rodents Signal transduction Signaling Social aspects Social behavior Social Behavior Disorders - genetics Social Behavior Disorders - metabolism Tensin Tumor proteins Tumor Suppressor Protein p53 - genetics Tumor Suppressor Protein p53 - metabolism Veterinary colleges
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Title	Mitochondrial Dysfunction in Pten Haplo-Insufficient Mice with Social Deficits and Repetitive Behavior: Interplay between Pten and p53
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