CRISPR gene-drive systems based on Cas9 nickases promote super-Mendelian inheritance in Drosophila

ABSTRACTCRISPR-based gene drive systems can be used to modify entire wild populations due to their ability to bias their own inheritance towards super-Mendelian rates (>100%). Current gene drives contain a Cas9 and a gRNA gene inserted at the location targeted by the gRNA. These gene products are able to cut the opposing wildtype allele, and lead to its replacement with a copy of the gene drive through the homology-directed DNA repair pathway. When this allelic conversion occurs in the germline it leads to the preferential inheritance of the engineered allele — a property that has been proposed to disseminate engineered traits for managing disease-transmitting mosquito populations. Here, we report a novel gene-drive strategy relying on Cas9 nickases which operates by generating staggered paired-nicks in the DNA to promote propagation of the gene drive allele. We show that only when 5’ overhangs are generated, the system efficiently leads to allelic conversion. Further, the nickase gene-drive arrangement produces large stereotyped deletions, providing potential advantages for targeting essential genes. Indeed, the nickase-gene-drive design should expand the options available for gene drive designs aimed at applications in mosquitoes and beyond.

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Evolutionary dynamics of CRISPR gene drives

10.1101/057281 ◽

2016 ◽

Cited By ~ 10

Author(s):

Charleston Noble ◽

Jason Olejarz ◽

Kevin M. Esvelt ◽

George M. Church ◽

Martin A. Nowak

Keyword(s):

Evolutionary Dynamics ◽

Evolutionary Stability ◽

Clear Understanding ◽

Gene Drive ◽

Host Organism ◽

Wild Populations ◽

Selfish Genetic Elements ◽

Real World Applications ◽

Drive Systems ◽

Gene Drives

AbstractThe alteration of wild populations has been discussed as a solution to a number of humanity’s most pressing ecological and public health concerns. Enabled by the recent revolution in genome editing, CRISPR gene drives, selfish genetic elements which can spread through populations even if they confer no advantage to their host organism, are rapidly emerging as the most promising approach. But before real-world applications are considered, it is imperative to develop a clear understanding of the outcomes of drive release in nature. Toward this aim, we mathematically study the evolutionary dynamics of CRISPR gene drives. We demonstrate that the emergence of drive-resistant alleles presents a major challenge to previously reported constructs, and we show that an alternative design which selects against resistant alleles greatly improves evolutionary stability. We discuss all results in the context of CRISPR technology and provide insights which inform the engineering of practical gene drive systems.

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Current CRISPR gene drive systems are likely to be highly invasive in wild populations

10.1101/219022 ◽

2017 ◽

Cited By ~ 10

Author(s):

Charleston Noble ◽

Ben Adlam ◽

George M. Church ◽

Kevin M. Esvelt ◽

Martin A. Nowak

Keyword(s):

Local Population ◽

Gene Drive ◽

Host Organism ◽

Wild Populations ◽

Flow Rates ◽

Standing Variation ◽

Large Populations ◽

Mitigating Factors ◽

Drive Systems ◽

Gene Drives

AbstractRecent reports have suggested that CRISPR-based gene drives are unlikely to invade wild populations due to drive-resistant alleles that prevent cutting. Here we develop mathematical models based on existing empirical data to explicitly test this assumption. We show that although resistance prevents drive systems from spreading to fixation in large populations, even the least effective systems reported to date are highly invasive. Releasing a small number of organisms often causes invasion of the local population, followed by invasion of additional populations connected by very low gene flow rates. Examining the effects of mitigating factors including standing variation, inbreeding, and family size revealed that none of these prevent invasion in realistic scenarios. Highly effective drive systems are predicted to be even more invasive. Contrary to the National Academies report on gene drive, our results suggest that standard drive systems should not be developed nor field-tested in regions harboring the host organism.

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The effect of mating complexity on gene drive dynamics

10.1101/2021.09.16.460618 ◽

2021 ◽

Author(s):

Prateek Verma ◽

R. Guy Reeves ◽

Samson Simon ◽

Mathias Otto ◽

Chaitanya S. Gokhale

Keyword(s):

Mate Choice ◽

Mating Systems ◽

Population Level ◽

Gene Drive ◽

Wild Populations ◽

Transgenic Organisms ◽

Drive Systems ◽

The Impact ◽

Gene Drives ◽

Drive Dynamics

AbstractGene drive technology is being presented as a means to deliver on some of the global challenges humanity faces today in healthcare, agriculture and conservation. However, there is a limited understanding of the consequences of releasing self-perpetuating transgenic organisms into the wild populations under complex ecological conditions. In this study, we analyze the impact of three factors, mate-choice, mating systems and spatial mating network, on the population dynamics for two distinct classes of modification gene drive systems; distortion and viability-based ones. All three factors had a high impact on the modelling outcome. First, we demonstrate that distortion based gene drives appear to be more robust against the mate-choice than viability-based gene drives. Second, we find that gene drive spread is much faster for higher degrees of polygamy. With fitness cost, speed is the highest for intermediate levels of polygamy. Finally, the spread of gene drive is faster and more effective when the individuals have fewer connections in a spatial mating network. Our results highlight the need to include mating complexities while modelling the population-level spread of gene drives. This will enable a more confident prediction of release thresholds, timescales and consequences of gene drive in populations.

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Mathematical modeling of self-contained CRISPR gene drive reversal systems

Scientific Reports ◽

10.1038/s41598-019-54805-8 ◽

2019 ◽

Vol 9 (1) ◽

Cited By ~ 2

Author(s):

Matthew G. Heffel ◽

Gregory C. Finnigan

Keyword(s):

Mendelian Inheritance ◽

Ecological Systems ◽

Mathematical Work ◽

Gene Drive ◽

Key Species ◽

Type Population ◽

Reversal Mechanism ◽

Drive Systems ◽

External Stimuli ◽

Gene Drives

AbstractThere is a critical need for further research into methods to control biological populations. Numerous challenges to agriculture, ecological systems, and human health could be mitigated by the targeted reduction and management of key species (e.g. pests, parasites, and vectors for pathogens). The discovery and adaptation of the CRISPR/Cas editing platform co-opted from bacteria has provided a mechanism for a means to alter an entire population. A CRISPR-based gene drive system can allow for the forced propagation of a genetic element that bypasses Mendelian inheritance which can be used to bias sex determination, install exogenous information, or remove endogenous DNA within an entire species. Laboratory studies have demonstrated the potency by which gene drives can operate within insects and other organisms. However, continued research and eventual application face serious opposition regarding issues of policy, biosafety, effectiveness, and reversal. Previous mathematical work has suggested the use of modified gene drive designs that are limited in spread such as daisy chain or underdominance drives. However, no system has yet been proposed that allows for an inducible reversal mechanism without requiring the introduction of additional individuals. Here, we study gene drive effectiveness, fitness, and inducible drive systems that could respond to external stimuli expanding from a previous frequency-based population model. We find that programmed modification during gene drive propagation could serve as a potent safeguard to either slow or completely reverse drive systems and allow for a return to the original wild-type population.

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Invasion and migration of spatially self-limiting gene drives: a comparative analysis

10.1101/159855 ◽

2017 ◽

Cited By ~ 2

Author(s):

Sumit Dhole ◽

Michael R. Vella ◽

Alun L. Loyd ◽

Fred Gould

Keyword(s):

Target Population ◽

Gene Drive ◽

Fitness Costs ◽

Invasion And Migration ◽

Migration Rates ◽

Chain System ◽

Drive Systems ◽

And Migration ◽

The One ◽

Gene Drives

AbstractRecent advances in research on gene drives have produced genetic constructs that could theoretically spread a desired gene (payload) into all populations of a species, with a single release in one place. This attribute has advantages, but also comes with risks and ethical concerns. There has been a call for research on gene drive systems that are spatially and/or temporally self-limiting. Here we use a population genetics model to compare the expected characteristics of three spatially self-limiting gene drive systems: one-locus underdominance, two-locus underdominance, and daisy-chain drives. We find large differences between these gene drives in the minimum release size required for successfully driving a payload into a population. The daisy-chain system is the most efficient, requiring the smallest release, followed by the two-locus underdominance system, and then the one-locus underdominance system. However, when the target population exchanges migrants with a non-target population, the gene drives requiring smaller releases suffer from higher risks of unintended spread. For payloads that incur relatively low fitness costs (up to 30%), a simple daisy-chain drive is practically incapable of remaining localized, even with migration rates as low as 0.5% per generation. The two-locus underdominance system can achieve localized spread under a broader range of migration rates and of payload fitness costs, while the one-locus underdominance system largely remains localized. We also find differences in the extent of population alteration and in the permanence of the alteration achieved by the three gene drives. The two-locus underdominance system does not always spread the payload to fixation, even after successful drive, while the daisy-chain system can, for a small set of parameter values, achieve a temporally-limited spread of the payload. These differences could affect the suitability of each gene drive for specific applications.Note:This manuscript has been accepted for publication in the journal Evolutionary Applications and is pending publication. We suggest that any reference to or quotation of this article should be made with this recognition.

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Modulating CRISPR gene drive activity through nucleocytoplasmic localization of Cas9 in S. cerevisiae

10.1101/408369 ◽

2018 ◽

Author(s):

Megan E. Goeckel ◽

Erianna M. Basgall ◽

Isabel C. Lewis ◽

Samantha C. Goetting ◽

Yao Yan ◽

...

Keyword(s):

Nuclease Activity ◽

Gene Drive ◽

Wild Populations ◽

Vector Borne Diseases ◽

Vector Borne ◽

Mendelian Laws ◽

Artificial Gene ◽

Nuclear Localization Sequences ◽

Gene Drives

ABSTRACTThe bacterial CRISPR/Cas genome editing system has provided a major breakthrough in molecular biology. One use of this technology is within a nuclease-based gene drive. This type of system can install a genetic element within a population at unnatural rates. Combatting of vector-borne diseases carried by metazoans could benefit from a delivery system that bypasses traditional Mendelian laws of segregation. Recently, laboratory studies in fungi, insects, and even mice, have demonstrated successful propagation of CRISPR gene drives and the potential utility of this type of mechanism. However, current gene drives still face challenges including evolved resistance, containment, and the consequences of application in wild populations. In this study, we use an artificial gene drive system in budding yeast to explore mechanisms to modulate nuclease activity of Cas9 through its nucleocytoplasmic localization. We examine non-native nuclear localization sequences on Cas9 fusion proteins in vivo and demonstrate that appended signals can titrate gene drive activity and serve as a potential molecular safeguard.

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Author response: Current CRISPR gene drive systems are likely to be highly invasive in wild populations

10.7554/elife.33423.021 ◽

2018 ◽

Author(s):

Charleston Noble ◽

Ben Adlam ◽

George M Church ◽

Kevin M Esvelt ◽

Martin A Nowak

Keyword(s):

Author Response ◽

Gene Drive ◽

Wild Populations ◽

Drive Systems ◽

Response Current

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Small-molecule control of super-Mendelian inheritance in gene drives

10.1101/665620 ◽

2019 ◽

Cited By ~ 3

Author(s):

Víctor López Del Amo ◽

Brittany S. Leger ◽

Kurt J. Cox ◽

Shubhroz Gill ◽

Alena L. Bishop ◽

...

Keyword(s):

Small Molecule ◽

Chemical Control ◽

Control Strategies ◽

Mendelian Inheritance ◽

Drive System ◽

Gene Drive ◽

Crop Pests ◽

Vector Borne Diseases ◽

Vector Borne ◽

Gene Drives

ABSTRACTBy surpassing the 50% inheritance limit of Mendel’s law of independent assortment, CRISPR-based gene drives have the potential to fight vector-borne diseases or suppress crop pests. However, contemporary gene drives could spread unchecked, posing safety concerns that limit their use in both laboratory and field settings. Current technologies also lack chemical control strategies, which could be applied in the field for dose, spatial and temporal control of gene drives. We describe in Drosophila the first gene-drive system controlled by an engineered Cas9 and a synthetic, orally-available small molecule.Graphical Abstract

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RNA-guided gene drives can efficiently and reversibly bias inheritance in wild yeast

10.1101/013896 ◽

2015 ◽

Cited By ~ 7

Author(s):

James E DiCarlo ◽

Alejandro Chavez ◽

Sven L Dietz ◽

Kevin M Esvelt ◽

George M Church

Keyword(s):

Saccharomyces Cerevisiae ◽

Gene Drive ◽

Wild Type ◽

Wild Populations ◽

Yeast Saccharomyces Cerevisiae ◽

Wild Yeast ◽

Successive Generations ◽

Gene Drives ◽

General Method ◽

Made In

Inheritance-biasing “gene drives” may be capable of spreading genomic alterations made in laboratory organisms through wild populations. We previously considered the potential for RNA-guided gene drives based on the versatile CRISPR/Cas9 genome editing system to serve as a general method of altering populations. Here we report molecularly contained gene drive constructs in the yeast Saccharomyces cerevisiae that are typically copied at rates above 99% when mated to wild yeast. We successfully targeted both non-essential and essential genes, showed that the inheritance of an unrelated “cargo” gene could be biased by an adjacent drive, and constructed a drive capable of overwriting and reversing changes made by a previous drive. Our results demonstrate that RNA-guided gene drives are capable of efficiently biasing inheritance when mated to wild-type organisms over successive generations.

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Synthetically EngineeredMedeaGene Drive System in the Worldwide Crop Pest,D. suzukii

10.1101/162255 ◽

2017 ◽

Cited By ~ 4

Author(s):

Anna Buchman ◽

John M. Marshall ◽

Dennis Ostrovski ◽

Ting Yang ◽

Omar S. Akbari

Keyword(s):

Wild Population ◽

Mendelian Inheritance ◽

Gene Drive ◽

Fitness Costs ◽

High Frequencies ◽

Toxin Resistance ◽

Crop Pest ◽

Naturally Occurring ◽

Drive Systems ◽

Significant Disease

AbstractSynthetic gene drive systems possess enormous potential to replace, alter, or suppress wild populations of significant disease vectors and crop pests; however, their utility in diverse populations remains to be demonstrated. Here, we report the creation of the first-ever syntheticMedeagene drive element in a major worldwide crop pest,D. suzukii. We demonstrate that this drive element, based on an engineered maternal “toxin” coupled with a linked embryonic “antidote,” is capable of biasing Mendelian inheritance rates with up to 100% efficiency. However, we find that drive resistance, resulting from naturally occurring genetic variation and associated fitness costs, can hinder the spread of such an element. Despite this, our results suggest that this element could maintain itself at high frequencies in a wild population, and spread to fixation, if either its fitness costs or toxin resistance were reduced, providing a clear path forward for developing future such systems.

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