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Published April 27, 2024 | Submitted
Discussion Paper Open

Generation of a zebrafish neurofibromatosis model via inducible knockout of nf2

Desingu Rajan, Ayyappa Raja ORCID icon
Huang, Yuanyun
Stundl, Jan ORCID icon
Chu, Katelyn
Irodi, Anushka
Yang, Zihan
Applegate, Brian E. ORCID icon
Bronner, Marianne E.1 ORCID icon
  • 1. ROR icon California Institute of Technology

Abstract

Neurofibromatosis Type 2 (NF-2) is a dominantly inherited genetic disorder that results from mutations in the tumor suppressor gene, neurofibromin 2 (NF2) gene. Here, we report the generation of a conditional zebrafish model of neurofibromatosis established by an inducible genetic knockout of nf2a/b, the zebrafish homolog of human NF2. Analysis of nf2a and nf2b expression reveals ubiquitous expression of nf2b in the early embryo, with overlapping expression in the neural crest and its derivatives and in the cranial mesenchyme. In contrast, nf2a displays lower expression levels. Induction of nf2a/b knockout at early stages increases the proliferation of larval Schwann cells and meningeal fibroblasts. Subsequently, in adult zebrafish, nf2a/b knockout triggers the development of a spectrum of tumors, including vestibular schwannomas, spinal schwannomas, meningiomas, and retinal hamartomas, mirroring the tumor manifestations observed in patients with NF-2. Collectively, these findings highlight the generation of a novel zebrafish model that mimics the complexities of the human NF-2 disorder. Consequently, this model holds significant potential for facilitating therapeutic screening and elucidating key driver genes implicated in NF-2 onset.

Copyright and License

The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license.
 

Acknowledgement

We thank the Beckman Institute Biological Imaging Facility of Caltech for technical assistance with microscopy experiments. We thank the Wenbiao Chen lab for generously supplying transgenic fish Tg(HOTCre:Cas9). We thank Justin Yip, Ryan Fraser, and David Mayorga for their help with fish facility maintenance. We thank Johanna Tan-Cabugao and Constanza Gonzales for their technical assistance. We would also like to thank all our fishes for providing embryonic and adult material for our research.

Funding

This work was supported by the National Institutes of Health (NIH R35NS111564) to M.E.B. and the Alex’s Lemonade Stand Foundation (ALSF) Young Investigator award to D.A.R. (Grant Award # 21-24018). A.I was supported by CamSURF (CALTECH exchange program).

Contributions

Conceptualization—D.A.R. and M.E.B. Methodology—D.A.R. and M.E.B. Investigation—D.A.R, Y.H, J.S, K.C, and A.I; Z.Y, D.A.R, and B.E.A. performed and analyzed OCT data. Data curation—D.A.R. Visualization—D.A.R and M.E.B. Writing—original draft preparation—D.A.R. and M.E.B. Supervision—M.E.B. Funding acquisition—M.E.B.

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Additional details

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Created:
May 6, 2024
Modified:
May 6, 2024