A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density

PURPOSE: Familial exudative vitreoretinopathy (FEVR) is caused by mutations in the genes encoding low-density lipoprotein receptor-related protein (LRP5) or its interacting partners, namely frizzled class receptor 4 (FZD4) and norrin cystine knot growth factor (NDP). Mouse models for Lrp5, Fzd4, and...

Descripción completa

Detalles Bibliográficos
Autores principales: Charette, Jeremy R., Earp, Sarah E., Bell, Brent A., Ackert-Bicknell, Cheryl L., Godfrey, Dana A., Rao, Sujata, Anand-Apte, Bela, Nishina, Patsy M., Peachey, Neal S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Molecular Vision 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5360454/
https://www.ncbi.nlm.nih.gov/pubmed/28356706
_version_ 1782516609261240320
author Charette, Jeremy R.
Earp, Sarah E.
Bell, Brent A.
Ackert-Bicknell, Cheryl L.
Godfrey, Dana A.
Rao, Sujata
Anand-Apte, Bela
Nishina, Patsy M.
Peachey, Neal S.
author_facet Charette, Jeremy R.
Earp, Sarah E.
Bell, Brent A.
Ackert-Bicknell, Cheryl L.
Godfrey, Dana A.
Rao, Sujata
Anand-Apte, Bela
Nishina, Patsy M.
Peachey, Neal S.
author_sort Charette, Jeremy R.
collection PubMed
description PURPOSE: Familial exudative vitreoretinopathy (FEVR) is caused by mutations in the genes encoding low-density lipoprotein receptor-related protein (LRP5) or its interacting partners, namely frizzled class receptor 4 (FZD4) and norrin cystine knot growth factor (NDP). Mouse models for Lrp5, Fzd4, and Ndp have proven to be important for understanding the retinal pathophysiology underlying FEVR and systemic abnormalities related to defective Wnt signaling. Here, we report a new mouse mutant, tvrm111B, which was identified by electroretinogram (ERG) screening of mice generated in the Jackson Laboratory Translational Vision Research Models (TVRM) mutagenesis program. METHODS: ERGs were used to examine outer retinal physiology. The retinal vasculature was examined by in vivo retinal imaging, as well as by histology and immunohistochemistry. The tvrm111B locus was identified by genetic mapping of mice generated in a cross to DBA/2J, and subsequent sequencing analysis. Gene expression was examined by real-time PCR of retinal RNA. Bone mineral density (BMD) was examined by peripheral dual-energy X-ray absorptiometry. RESULTS: The tvrm111B allele is inherited as an autosomal recessive trait. Genetic mapping of the decreased ERG b-wave phenotype of tvrm111B mice localized the mutation to a region on chromosome 19 that included Lrp5. Sequencing of Lrp5 identified the insertion of a cytosine (c.4724_4725insC), which is predicted to cause a frameshift that disrupts the last three of five conserved PPPSPxS motifs in the cytoplasmic domain of LRP5, culminating in a premature termination. In addition to a reduced ERG b-wave, Lrp5(tvrm111B) homozygotes have low BMD and abnormal features of the retinal vasculature that have been reported previously in Lrp5 mutant mice, including persistent hyaloid vessels, leakage on fluorescein angiography, and an absence of the deep retinal capillary bed. CONCLUSIONS: The phenotype of the Lrp5(tvrm111B) mutant includes abnormalities of the retinal vasculature and of BMD. This model may be a useful resource to further our understanding of the biological role of LRP5 and to evaluate experimental therapies for FEVR or other conditions associated with LRP5 dysfunction.
format Online
Article
Text
id pubmed-5360454
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Molecular Vision
record_format MEDLINE/PubMed
spelling pubmed-53604542017-03-29 A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density Charette, Jeremy R. Earp, Sarah E. Bell, Brent A. Ackert-Bicknell, Cheryl L. Godfrey, Dana A. Rao, Sujata Anand-Apte, Bela Nishina, Patsy M. Peachey, Neal S. Mol Vis Research Article PURPOSE: Familial exudative vitreoretinopathy (FEVR) is caused by mutations in the genes encoding low-density lipoprotein receptor-related protein (LRP5) or its interacting partners, namely frizzled class receptor 4 (FZD4) and norrin cystine knot growth factor (NDP). Mouse models for Lrp5, Fzd4, and Ndp have proven to be important for understanding the retinal pathophysiology underlying FEVR and systemic abnormalities related to defective Wnt signaling. Here, we report a new mouse mutant, tvrm111B, which was identified by electroretinogram (ERG) screening of mice generated in the Jackson Laboratory Translational Vision Research Models (TVRM) mutagenesis program. METHODS: ERGs were used to examine outer retinal physiology. The retinal vasculature was examined by in vivo retinal imaging, as well as by histology and immunohistochemistry. The tvrm111B locus was identified by genetic mapping of mice generated in a cross to DBA/2J, and subsequent sequencing analysis. Gene expression was examined by real-time PCR of retinal RNA. Bone mineral density (BMD) was examined by peripheral dual-energy X-ray absorptiometry. RESULTS: The tvrm111B allele is inherited as an autosomal recessive trait. Genetic mapping of the decreased ERG b-wave phenotype of tvrm111B mice localized the mutation to a region on chromosome 19 that included Lrp5. Sequencing of Lrp5 identified the insertion of a cytosine (c.4724_4725insC), which is predicted to cause a frameshift that disrupts the last three of five conserved PPPSPxS motifs in the cytoplasmic domain of LRP5, culminating in a premature termination. In addition to a reduced ERG b-wave, Lrp5(tvrm111B) homozygotes have low BMD and abnormal features of the retinal vasculature that have been reported previously in Lrp5 mutant mice, including persistent hyaloid vessels, leakage on fluorescein angiography, and an absence of the deep retinal capillary bed. CONCLUSIONS: The phenotype of the Lrp5(tvrm111B) mutant includes abnormalities of the retinal vasculature and of BMD. This model may be a useful resource to further our understanding of the biological role of LRP5 and to evaluate experimental therapies for FEVR or other conditions associated with LRP5 dysfunction. Molecular Vision 2017-03-18 /pmc/articles/PMC5360454/ /pubmed/28356706 Text en Copyright © 2017 Molecular Vision. http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited, used for non-commercial purposes, and is not altered or transformed.
spellingShingle Research Article
Charette, Jeremy R.
Earp, Sarah E.
Bell, Brent A.
Ackert-Bicknell, Cheryl L.
Godfrey, Dana A.
Rao, Sujata
Anand-Apte, Bela
Nishina, Patsy M.
Peachey, Neal S.
A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
title A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
title_full A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
title_fullStr A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
title_full_unstemmed A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
title_short A mutagenesis-derived Lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
title_sort mutagenesis-derived lrp5 mouse mutant with abnormal retinal vasculature and low bone mineral density
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5360454/
https://www.ncbi.nlm.nih.gov/pubmed/28356706
work_keys_str_mv AT charettejeremyr amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT earpsarahe amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT bellbrenta amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT ackertbicknellcheryll amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT godfreydanaa amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT raosujata amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT anandaptebela amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT nishinapatsym amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT peacheyneals amutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT charettejeremyr mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT earpsarahe mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT bellbrenta mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT ackertbicknellcheryll mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT godfreydanaa mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT raosujata mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT anandaptebela mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT nishinapatsym mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity
AT peacheyneals mutagenesisderivedlrp5mousemutantwithabnormalretinalvasculatureandlowbonemineraldensity

Ejemplares similares