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Kumar, S.* ; Rathkolb, B.* ; Kemter, E.* ; Sabrautzki, S. ; Michel, D. ; Adler, T. ; Becker, L. ; Beckers, J. ; Busch, D.H.* ; Garrett, L. ; Hans, W. ; Hölter, S.M. ; Horsch, M. ; Klingenspor, M.* ; Klopstock, T.* ; Rácz, I.* ; Rozman, J. ; Vargas Panesso, I.L. ; Vernaleken, A. ; Zimmer, A.* ; Fuchs, H. ; Gailus-Durner, V. ; Hrabě de Angelis, M. ; Wolf, E.* ; Aigner, B.*

Generation and standardized, systemic phenotypic analysis of Pou3f3L423P mutant mice.

PLoS ONE 11:e0150472 (2016)
Publ. Version/Full Text DOI PMC
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Increased levels of blood plasma urea were used as phenotypic parameter for establishing novel mouse models for kidney diseases on the genetic background of C3H inbred mice in the phenotype-driven Munich ENU mouse mutagenesis project. The phenotypically recessive mutant line HST011 was established and further analyzed. The causative mutation was detected in the POU domain, class 3 transcription factor 3 (Pou3f3) gene, which leads to the amino acid exchange Pou3f3L423P thereby affecting the conserved homeobox domain of the protein. Pou3f3 homozygous knockout mice are published and show perinatal death. Line Pou3f3L423P is a viable mouse model harboring a homozygous Pou3f3 mutation. Standardized, systemic phenotypic analysis of homozygous mutants was carried out in the German Mouse Clinic. Main phenotypic changes were low body weight and a state of low energy stores, kidney dysfunction and secondary effects thereof including low bone mineralization, multiple behavioral and neurological defects including locomotor, vestibular, auditory and nociceptive impairments, as well as multiple subtle changes in immunological parameters. Genome-wide transcriptome profiling analysis of kidney and brain of Pou3f3L423P homozygous mutants identified significantly regulated genes as compared to wild-type controls.
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Publication type Article: Journal article
Document type Scientific Article
Keywords Mouse Mutagenesis Project; Kidney-disease; Crucial Roles; Mutation; Genes; Expression; Uromodulin; Models; Brn-1
Language german
Publication Year 2016
HGF-reported in Year 2016
ISSN (print) / ISBN 1932-6203
Journal PLoS ONE
Quellenangaben Volume: 11, Issue: 3, Pages: , Article Number: e0150472 Supplement: ,
Publisher Public Library of Science (PLoS)
Publishing Place Lawrence, Kan.
Reviewing status Peer reviewed
Institute(s) CF Comparative Medicine (AVM)
Institute of Experimental Genetics (IEG)
Institute of Developmental Genetics (IDG)
POF-Topic(s) 30202 - Environmental Health
30201 - Metabolic Health
90000 - German Center for Diabetes Research
30204 - Cell Programming and Repair
Research field(s) Genetics and Epidemiology
PSP Element(s) G-500900-001
G-500600-001
G-501900-063
G-500692-001
G-500600-004
G-500500-001
G-501900-066
DOI 10.1371/journal.pone.0150472
WOS ID WOS:000372697400014
Scopus ID 84962449714
PubMed ID 27003440
Erfassungsdatum 2016-04-13
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