Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin

Drosophila melanogaster has been widely used as a model of human Mendelian disease, but its value in modeling complex disease has received little attention. Fly models of complex disease would enable high-resolution mapping of disease-modifying loci and the identification of novel targets for therap...

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Autores principales: Park, Soo-Young, Ludwig, Michael Z., Tamarina, Natalia A., He, Bin Z., Carl, Sarah H., Dickerson, Desiree A., Barse, Levi, Arun, Bharath, Williams, Calvin L., Miles, Cecelia M., Philipson, Louis H., Steiner, Donald F., Bell, Graeme I., Kreitman, Martin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Genetics Society of America 2014
Materias:
Investigations
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3914625/
https://www.ncbi.nlm.nih.gov/pubmed/24281154
http://dx.doi.org/10.1534/genetics.113.157602
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author Park, Soo-Young
Ludwig, Michael Z.
Tamarina, Natalia A.
He, Bin Z.
Carl, Sarah H.
Dickerson, Desiree A.
Barse, Levi
Arun, Bharath
Williams, Calvin L.
Miles, Cecelia M.
Philipson, Louis H.
Steiner, Donald F.
Bell, Graeme I.
Kreitman, Martin
author_facet Park, Soo-Young
Ludwig, Michael Z.
Tamarina, Natalia A.
He, Bin Z.
Carl, Sarah H.
Dickerson, Desiree A.
Barse, Levi
Arun, Bharath
Williams, Calvin L.
Miles, Cecelia M.
Philipson, Louis H.
Steiner, Donald F.
Bell, Graeme I.
Kreitman, Martin
author_sort Park, Soo-Young
collection PubMed
description Drosophila melanogaster has been widely used as a model of human Mendelian disease, but its value in modeling complex disease has received little attention. Fly models of complex disease would enable high-resolution mapping of disease-modifying loci and the identification of novel targets for therapeutic intervention. Here, we describe a fly model of permanent neonatal diabetes mellitus and explore the complexity of this model. The approach involves the transgenic expression of a misfolded mutant of human preproinsulin, hINS(C96Y), which is a cause of permanent neonatal diabetes. When expressed in fly imaginal discs, hINS(C96Y) causes a reduction of adult structures, including the eye, wing, and notum. Eye imaginal discs exhibit defects in both the structure and the arrangement of ommatidia. In the wing, expression of hINS(C96Y) leads to ectopic expression of veins and mechano-sensory organs, indicating disruption of wild-type signaling processes regulating cell fates. These readily measurable “disease” phenotypes are sensitive to temperature, gene dose, and sex. Mutant (but not wild-type) proinsulin expression in the eye imaginal disc induces IRE1-mediated XBP1 alternative splicing, a signal for endoplasmic reticulum stress response activation, and produces global change in gene expression. Mutant hINS transgene tester strains, when crossed to stocks from the Drosophila Genetic Reference Panel, produce F(1) adults with a continuous range of disease phenotypes and large broad-sense heritability. Surprisingly, the severity of mutant hINS-induced disease in the eye is not correlated with that in the notum in these crosses, nor with eye reduction phenotypes caused by the expression of two dominant eye mutants acting in two different eye development pathways, Drop (Dr) or Lobe (L), when crossed into the same genetic backgrounds. The tissue specificity of genetic variability for mutant hINS-induced disease has, therefore, its own distinct signature. The genetic dominance of disease-specific phenotypic variability in our model of misfolded human proinsulin makes this approach amenable to genome-wide association study in a simple F(1) screen of natural variation.
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spelling pubmed-39146252015-02-01 Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin Park, Soo-Young Ludwig, Michael Z. Tamarina, Natalia A. He, Bin Z. Carl, Sarah H. Dickerson, Desiree A. Barse, Levi Arun, Bharath Williams, Calvin L. Miles, Cecelia M. Philipson, Louis H. Steiner, Donald F. Bell, Graeme I. Kreitman, Martin Genetics Investigations Drosophila melanogaster has been widely used as a model of human Mendelian disease, but its value in modeling complex disease has received little attention. Fly models of complex disease would enable high-resolution mapping of disease-modifying loci and the identification of novel targets for therapeutic intervention. Here, we describe a fly model of permanent neonatal diabetes mellitus and explore the complexity of this model. The approach involves the transgenic expression of a misfolded mutant of human preproinsulin, hINS(C96Y), which is a cause of permanent neonatal diabetes. When expressed in fly imaginal discs, hINS(C96Y) causes a reduction of adult structures, including the eye, wing, and notum. Eye imaginal discs exhibit defects in both the structure and the arrangement of ommatidia. In the wing, expression of hINS(C96Y) leads to ectopic expression of veins and mechano-sensory organs, indicating disruption of wild-type signaling processes regulating cell fates. These readily measurable “disease” phenotypes are sensitive to temperature, gene dose, and sex. Mutant (but not wild-type) proinsulin expression in the eye imaginal disc induces IRE1-mediated XBP1 alternative splicing, a signal for endoplasmic reticulum stress response activation, and produces global change in gene expression. Mutant hINS transgene tester strains, when crossed to stocks from the Drosophila Genetic Reference Panel, produce F(1) adults with a continuous range of disease phenotypes and large broad-sense heritability. Surprisingly, the severity of mutant hINS-induced disease in the eye is not correlated with that in the notum in these crosses, nor with eye reduction phenotypes caused by the expression of two dominant eye mutants acting in two different eye development pathways, Drop (Dr) or Lobe (L), when crossed into the same genetic backgrounds. The tissue specificity of genetic variability for mutant hINS-induced disease has, therefore, its own distinct signature. The genetic dominance of disease-specific phenotypic variability in our model of misfolded human proinsulin makes this approach amenable to genome-wide association study in a simple F(1) screen of natural variation. Genetics Society of America 2014-02 2013-11-26 /pmc/articles/PMC3914625/ /pubmed/24281154 http://dx.doi.org/10.1534/genetics.113.157602 Text en Copyright © 2014 by the Genetics Society of America Available freely online through the author-supported open access option.
spellingShingle Investigations
Park, Soo-Young
Ludwig, Michael Z.
Tamarina, Natalia A.
He, Bin Z.
Carl, Sarah H.
Dickerson, Desiree A.
Barse, Levi
Arun, Bharath
Williams, Calvin L.
Miles, Cecelia M.
Philipson, Louis H.
Steiner, Donald F.
Bell, Graeme I.
Kreitman, Martin
Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin
title Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin
title_full Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin
title_fullStr Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin
title_full_unstemmed Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin
title_short Genetic Complexity in a Drosophila Model of Diabetes-Associated Misfolded Human Proinsulin
title_sort genetic complexity in a drosophila model of diabetes-associated misfolded human proinsulin
topic Investigations
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3914625/
https://www.ncbi.nlm.nih.gov/pubmed/24281154
http://dx.doi.org/10.1534/genetics.113.157602
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