An AAV-CRISPR/Cas9 strategy for gene editing across divergent rodent species: Targeting neural oxytocin receptors as a proof of concept

Arjen J. Boender; Marina Boon; H. Elliott Albers; Samantha R. Eck; Brandon A. Fricker; Aubrey M. Kelly; Joseph E. LeDoux; Simone C. Motta; Prerana Shrestha; Jack H. Taylor; Brian C. Trainor; Rodrigo Triana-Del Rio; Larry J. Young

doi:10.1126/sciadv.adf4950

An AAV-CRISPR/Cas9 strategy for gene editing across divergent rodent species: Targeting neural oxytocin receptors as a proof of concept

Arjen J. Boender, Marina Boon, H. Elliott Albers, Samantha R. Eck, Brandon A. Fricker, Aubrey M. Kelly, Joseph E. LeDoux, Simone C. Motta, Prerana Shrestha, Jack H. Taylor, Brian C. Trainor, Rodrigo Triana-Del Rio, Larry J. Young

Neural Science

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Abstract

A major issue in neuroscience is the poor translatability of research results from preclinical studies in animals to clinical outcomes. Comparative neuroscience can overcome this barrier by studying multiple species to differentiate between species-specific and general mechanisms of neural circuit functioning. Targeted manipulation of neural circuits often depends on genetic dissection, and use of this technique has been restricted to only a few model species, limiting its application in comparative research. However, ongoing advances in genomics make genetic dissection attainable in a growing number of species. To demonstrate the potential of comparative gene editing approaches, we developed a viral-mediated CRISPR/Cas9 strategy that is predicted to target the oxytocin receptor (Oxtr) gene in >80 rodent species. This strategy specifically reduced OXTR levels in all evaluated species (n = 6) without causing gross neuronal toxicity. Thus, we show that CRISPR/Cas9-based tools can function in multiple species simultaneously. Thereby, we hope to encourage comparative gene editing and improve the translatability of neuroscientific research.

Original language	English (US)
Article number	eadf4950
Pages (from-to)	eadf4950
Journal	Science Advances
Volume	9
Issue number	22
DOIs	https://doi.org/10.1126/sciadv.adf4950
State	Published - Jun 2 2023

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Boender, A. J., Boon, M., Albers, H. E., Eck, S. R., Fricker, B. A., Kelly, A. M., LeDoux, J. E., Motta, S. C., Shrestha, P., Taylor, J. H., Trainor, B. C., Triana-Del Rio, R., & Young, L. J. (2023). An AAV-CRISPR/Cas9 strategy for gene editing across divergent rodent species: Targeting neural oxytocin receptors as a proof of concept. Science Advances, 9(22), eadf4950. Article eadf4950. https://doi.org/10.1126/sciadv.adf4950

Boender, AJ, Boon, M, Albers, HE, Eck, SR, Fricker, BA, Kelly, AM, LeDoux, JE, Motta, SC, Shrestha, P, Taylor, JH, Trainor, BC, Triana-Del Rio, R & Young, LJ 2023, 'An AAV-CRISPR/Cas9 strategy for gene editing across divergent rodent species: Targeting neural oxytocin receptors as a proof of concept', Science Advances, vol. 9, no. 22, eadf4950, pp. eadf4950. https://doi.org/10.1126/sciadv.adf4950

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abstract = "A major issue in neuroscience is the poor translatability of research results from preclinical studies in animals to clinical outcomes. Comparative neuroscience can overcome this barrier by studying multiple species to differentiate between species-specific and general mechanisms of neural circuit functioning. Targeted manipulation of neural circuits often depends on genetic dissection, and use of this technique has been restricted to only a few model species, limiting its application in comparative research. However, ongoing advances in genomics make genetic dissection attainable in a growing number of species. To demonstrate the potential of comparative gene editing approaches, we developed a viral-mediated CRISPR/Cas9 strategy that is predicted to target the oxytocin receptor (Oxtr) gene in >80 rodent species. This strategy specifically reduced OXTR levels in all evaluated species (n = 6) without causing gross neuronal toxicity. Thus, we show that CRISPR/Cas9-based tools can function in multiple species simultaneously. Thereby, we hope to encourage comparative gene editing and improve the translatability of neuroscientific research.",

author = "Boender, {Arjen J.} and Marina Boon and Albers, {H. Elliott} and Eck, {Samantha R.} and Fricker, {Brandon A.} and Kelly, {Aubrey M.} and LeDoux, {Joseph E.} and Motta, {Simone C.} and Prerana Shrestha and Taylor, {Jack H.} and Trainor, {Brian C.} and {Triana-Del Rio}, Rodrigo and Young, {Larry J.}",

note = "Funding Information: This work was supported by a 2017 NARSAD Young Investigator Grant (ID 26058) from the Brain & Behavior Research Foundation to A.J.B.; a Klingenstein-Simons Fellowship Award in Neuroscience to A.M.K.; NIH R01MH121829 and NSF IOS1937335 to B.C.T.; OD P51OD011132*%blankline%* Publisher Copyright: Copyright {\textcopyright} 2023 The Authors.",

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An AAV-CRISPR/Cas9 strategy for gene editing across divergent rodent species: Targeting neural oxytocin receptors as a proof of concept

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