A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.

Synthetic sex distorters have recently been developed in the malaria mosquito, relying on endonucleases that target the X-chromosome during spermatogenesis. Although inspired by naturally-occurring traits, it has remained unclear how they function and, given their potential for genetic control, how...

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Main Authors: Barbara Fasulo, Angela Meccariello, Maya Morgan, Carl Borufka, Philippos Aris Papathanos, Nikolai Windbichler
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-03-01
Series:PLoS Genetics
Online Access:https://doi.org/10.1371/journal.pgen.1008647
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spelling doaj-10871200997f4d769d01af1a7638d5562021-04-21T13:52:06ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042020-03-01163e100864710.1371/journal.pgen.1008647A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.Barbara FasuloAngela MeccarielloMaya MorganCarl BorufkaPhilippos Aris PapathanosNikolai WindbichlerSynthetic sex distorters have recently been developed in the malaria mosquito, relying on endonucleases that target the X-chromosome during spermatogenesis. Although inspired by naturally-occurring traits, it has remained unclear how they function and, given their potential for genetic control, how portable this strategy is across species. We established Drosophila models for two distinct mechanisms for CRISPR/Cas9 sex-ratio distortion-"X-shredding" and "X-poisoning"-and dissected their target-site requirements and repair dynamics. X-shredding resulted in sex distortion when Cas9 endonuclease activity occurred during the meiotic stages of spermatogenesis but not when Cas9 was expressed from the stem cell stages onwards. Our results suggest that X-shredding is counteracted by the NHEJ DNA repair pathway and can operate on a single repeat cluster of non-essential sequences, although the targeting of a number of such repeats had no effect on the sex ratio. X-poisoning by contrast, i.e. targeting putative haplolethal genes on the X chromosome, induced a high bias towards males (>92%) when we directed Cas9 cleavage to the X-linked ribosomal target gene RpS6. In the case of X-poisoning sex distortion was coupled to a loss in reproductive output, although a dominant-negative effect appeared to drive the mechanism of female lethality. These model systems will guide the study and the application of sex distorters to medically or agriculturally important insect target species.https://doi.org/10.1371/journal.pgen.1008647
collection DOAJ
language English
format Article
sources DOAJ
author Barbara Fasulo
Angela Meccariello
Maya Morgan
Carl Borufka
Philippos Aris Papathanos
Nikolai Windbichler
spellingShingle Barbara Fasulo
Angela Meccariello
Maya Morgan
Carl Borufka
Philippos Aris Papathanos
Nikolai Windbichler
A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.
PLoS Genetics
author_facet Barbara Fasulo
Angela Meccariello
Maya Morgan
Carl Borufka
Philippos Aris Papathanos
Nikolai Windbichler
author_sort Barbara Fasulo
title A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.
title_short A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.
title_full A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.
title_fullStr A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.
title_full_unstemmed A fly model establishes distinct mechanisms for synthetic CRISPR/Cas9 sex distorters.
title_sort fly model establishes distinct mechanisms for synthetic crispr/cas9 sex distorters.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2020-03-01
description Synthetic sex distorters have recently been developed in the malaria mosquito, relying on endonucleases that target the X-chromosome during spermatogenesis. Although inspired by naturally-occurring traits, it has remained unclear how they function and, given their potential for genetic control, how portable this strategy is across species. We established Drosophila models for two distinct mechanisms for CRISPR/Cas9 sex-ratio distortion-"X-shredding" and "X-poisoning"-and dissected their target-site requirements and repair dynamics. X-shredding resulted in sex distortion when Cas9 endonuclease activity occurred during the meiotic stages of spermatogenesis but not when Cas9 was expressed from the stem cell stages onwards. Our results suggest that X-shredding is counteracted by the NHEJ DNA repair pathway and can operate on a single repeat cluster of non-essential sequences, although the targeting of a number of such repeats had no effect on the sex ratio. X-poisoning by contrast, i.e. targeting putative haplolethal genes on the X chromosome, induced a high bias towards males (>92%) when we directed Cas9 cleavage to the X-linked ribosomal target gene RpS6. In the case of X-poisoning sex distortion was coupled to a loss in reproductive output, although a dominant-negative effect appeared to drive the mechanism of female lethality. These model systems will guide the study and the application of sex distorters to medically or agriculturally important insect target species.
url https://doi.org/10.1371/journal.pgen.1008647
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