Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster
About two-thirds of the vital genes in the Drosophila genome are involved in eye development, making the fly eye an excellent genetic system to study cellular function and development, neurodevelopment/degeneration, and complex diseases such as cancer and diabetes. We developed a novel computational...
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2016-05-01
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doaj-72d18acb1b274b0f8846de16bf2ebfcc2021-07-02T09:30:44ZengOxford University PressG3: Genes, Genomes, Genetics2160-18362016-05-01651427143710.1534/g3.116.02706026Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogasterJanani IyerQingyu WangThanh LeLucilla PizzoSebastian GrönkeSurendra S. AmbegaokarYuzuru ImaiAshutosh SrivastavaBeatriz Llamusí TroisíGraeme MardonRuben ArteroGeorge R. JacksonAdrian M. IsaacsLinda PartridgeBingwei LuJustin P. KumarSanthosh GirirajanAbout two-thirds of the vital genes in the Drosophila genome are involved in eye development, making the fly eye an excellent genetic system to study cellular function and development, neurodevelopment/degeneration, and complex diseases such as cancer and diabetes. We developed a novel computational method, implemented as Flynotyper software (http://flynotyper.sourceforge.net), to quantitatively assess the morphological defects in the Drosophila eye resulting from genetic alterations affecting basic cellular and developmental processes. Flynotyper utilizes a series of image processing operations to automatically detect the fly eye and the individual ommatidium, and calculates a phenotypic score as a measure of the disorderliness of ommatidial arrangement in the fly eye. As a proof of principle, we tested our method by analyzing the defects due to eye-specific knockdown of Drosophila orthologs of 12 neurodevelopmental genes to accurately document differential sensitivities of these genes to dosage alteration. We also evaluated eye images from six independent studies assessing the effect of overexpression of repeats, candidates from peptide library screens, and modifiers of neurotoxicity and developmental processes on eye morphology, and show strong concordance with the original assessment. We further demonstrate the utility of this method by analyzing 16 modifiers of sine oculis obtained from two genome-wide deficiency screens of Drosophila and accurately quantifying the effect of its enhancers and suppressors during eye development. Our method will complement existing assays for eye phenotypes, and increase the accuracy of studies that use fly eyes for functional evaluation of genes and genetic interactions.http://g3journal.org/lookup/doi/10.1534/g3.116.027060ommatidiaDrosophila melanogasterneurodevelopmental disordersmodifier screensrough eyehuman disease models |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Janani Iyer Qingyu Wang Thanh Le Lucilla Pizzo Sebastian Grönke Surendra S. Ambegaokar Yuzuru Imai Ashutosh Srivastava Beatriz Llamusí Troisí Graeme Mardon Ruben Artero George R. Jackson Adrian M. Isaacs Linda Partridge Bingwei Lu Justin P. Kumar Santhosh Girirajan |
spellingShingle |
Janani Iyer Qingyu Wang Thanh Le Lucilla Pizzo Sebastian Grönke Surendra S. Ambegaokar Yuzuru Imai Ashutosh Srivastava Beatriz Llamusí Troisí Graeme Mardon Ruben Artero George R. Jackson Adrian M. Isaacs Linda Partridge Bingwei Lu Justin P. Kumar Santhosh Girirajan Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster G3: Genes, Genomes, Genetics ommatidia Drosophila melanogaster neurodevelopmental disorders modifier screens rough eye human disease models |
author_facet |
Janani Iyer Qingyu Wang Thanh Le Lucilla Pizzo Sebastian Grönke Surendra S. Ambegaokar Yuzuru Imai Ashutosh Srivastava Beatriz Llamusí Troisí Graeme Mardon Ruben Artero George R. Jackson Adrian M. Isaacs Linda Partridge Bingwei Lu Justin P. Kumar Santhosh Girirajan |
author_sort |
Janani Iyer |
title |
Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster |
title_short |
Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster |
title_full |
Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster |
title_fullStr |
Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster |
title_full_unstemmed |
Quantitative Assessment of Eye Phenotypes for Functional Genetic Studies Using Drosophila melanogaster |
title_sort |
quantitative assessment of eye phenotypes for functional genetic studies using drosophila melanogaster |
publisher |
Oxford University Press |
series |
G3: Genes, Genomes, Genetics |
issn |
2160-1836 |
publishDate |
2016-05-01 |
description |
About two-thirds of the vital genes in the Drosophila genome are involved in eye development, making the fly eye an excellent genetic system to study cellular function and development, neurodevelopment/degeneration, and complex diseases such as cancer and diabetes. We developed a novel computational method, implemented as Flynotyper software (http://flynotyper.sourceforge.net), to quantitatively assess the morphological defects in the Drosophila eye resulting from genetic alterations affecting basic cellular and developmental processes. Flynotyper utilizes a series of image processing operations to automatically detect the fly eye and the individual ommatidium, and calculates a phenotypic score as a measure of the disorderliness of ommatidial arrangement in the fly eye. As a proof of principle, we tested our method by analyzing the defects due to eye-specific knockdown of Drosophila orthologs of 12 neurodevelopmental genes to accurately document differential sensitivities of these genes to dosage alteration. We also evaluated eye images from six independent studies assessing the effect of overexpression of repeats, candidates from peptide library screens, and modifiers of neurotoxicity and developmental processes on eye morphology, and show strong concordance with the original assessment. We further demonstrate the utility of this method by analyzing 16 modifiers of sine oculis obtained from two genome-wide deficiency screens of Drosophila and accurately quantifying the effect of its enhancers and suppressors during eye development. Our method will complement existing assays for eye phenotypes, and increase the accuracy of studies that use fly eyes for functional evaluation of genes and genetic interactions. |
topic |
ommatidia Drosophila melanogaster neurodevelopmental disorders modifier screens rough eye human disease models |
url |
http://g3journal.org/lookup/doi/10.1534/g3.116.027060 |
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