Literature DB >> 29187504

Tissue-Specific Gene Inactivation in Xenopus laevis: Knockout of lhx1 in the Kidney with CRISPR/Cas9.

Bridget D DeLay1, Mark E Corkins1, Hannah L Hanania1,2, Matthew Salanga3, Jian Min Deng4, Norihiro Sudou5, Masanori Taira6, Marko E Horb3, Rachel K Miller7,4,8,9.   

Abstract

Studying genes involved in organogenesis is often difficult because many of these genes are also essential for early development. The allotetraploid frog, Xenopus laevis, is commonly used to study developmental processes, but because of the presence of two homeologs for many genes, it has been difficult to use as a genetic model. Few studies have successfully used CRISPR in amphibians, and currently there is no tissue-targeted knockout strategy described in Xenopus The goal of this study is to determine whether CRISPR/Cas9-mediated gene knockout can be targeted to the Xenopus kidney without perturbing essential early gene function. We demonstrate that targeting CRISPR gene editing to the kidney and the eye of F0 embryos is feasible. Our study shows that knockout of both homeologs of lhx1 results in the disruption of kidney development and function but does not lead to early developmental defects. Therefore, targeting of CRISPR to the kidney may not be necessary to bypass the early developmental defects reported upon disruption of Lhx1 protein expression or function by morpholinos, antisense RNA, or dominant negative constructs. We also establish a control for CRISPR in Xenopus by editing a gene (slc45a2) that when knocked out results in albinism without altering kidney development. This study establishes the feasibility of tissue-specific gene knockout in Xenopus, providing a cost-effective and efficient method for assessing the roles of genes implicated in developmental abnormalities that is amenable to high-throughput gene or drug screening techniques.
Copyright © 2018 by the Genetics Society of America.

Entities:  

Keywords:  CRISPR; Xenopus laevis; kidney; lhx1; targeted injection

Mesh:

Substances:

Year:  2017        PMID: 29187504      PMCID: PMC5788530          DOI: 10.1534/genetics.117.300468

Source DB:  PubMed          Journal:  Genetics        ISSN: 0016-6731            Impact factor:   4.562


  56 in total

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Authors:  Panna Tandon; Frank Conlon; J David Furlow; Marko E Horb
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4.  Technique to Target Microinjection to the Developing Xenopus Kidney.

Authors:  Bridget D DeLay; Vanja Krneta-Stankic; Rachel K Miller
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5.  Conservatism and variability of gene expression profiles among homeologous transcription factors in Xenopus laevis.

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Journal:  Dev Biol       Date:  2016-10-31       Impact factor: 3.582

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Authors:  S A Moody; M J Kline
Journal:  Anat Embryol (Berl)       Date:  1990

7.  Enzymatically Generated CRISPR Libraries for Genome Labeling and Screening.

Authors:  Andrew B Lane; Magdalena Strzelecka; Andreas Ettinger; Andrew W Grenfell; Torsten Wittmann; Rebecca Heald
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Authors:  Jon P Lyons; Rachel K Miller; Xiaolan Zhou; Gilbert Weidinger; Tom Deroo; Tinneke Denayer; Jae-Il Park; Hong Ji; Ji Yeon Hong; Annette Li; Randall T Moon; Elizabeth A Jones; Kris Vleminckx; Peter D Vize; Pierre D McCrea
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Authors:  M Taira; M Jamrich; P J Good; I B Dawid
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2.  A convergent molecular network underlying autism and congenital heart disease.

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Review 4.  Aquatic models of human ciliary diseases.

Authors:  Mark E Corkins; Vanja Krneta-Stankic; Malgorzata Kloc; Rachel K Miller
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5.  Parallel in vivo analysis of large-effect autism genes implicates cortical neurogenesis and estrogen in risk and resilience.

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Journal:  Neuron       Date:  2021-01-25       Impact factor: 18.688

6.  Dynamin Binding Protein Is Required for Xenopus laevis Kidney Development.

Authors:  Bridget D DeLay; Tanya A Baldwin; Rachel K Miller
Journal:  Front Physiol       Date:  2019-02-26       Impact factor: 4.566

Review 7.  Xenopus leads the way: Frogs as a pioneering model to understand the human brain.

Authors:  Cameron R T Exner; Helen Rankin Willsey
Journal:  Genesis       Date:  2020-12-27       Impact factor: 2.487

8.  SLC45A2 protein stability and regulation of melanosome pH determine melanocyte pigmentation.

Authors:  Linh Le; Iliana E Escobar; Tina Ho; Ariel J Lefkovith; Emily Latteri; Kirk D Haltaufderhyde; Megan K Dennis; Lynn Plowright; Elena V Sviderskaya; Dorothy C Bennett; Elena Oancea; Michael S Marks
Journal:  Mol Biol Cell       Date:  2020-09-23       Impact factor: 4.138

9.  Transgenic Xenopus laevis Line for In Vivo Labeling of Nephrons within the Kidney.

Authors:  Mark E Corkins; Hannah L Hanania; Vanja Krneta-Stankic; Bridget D DeLay; Esther J Pearl; Moonsup Lee; Hong Ji; Alan J Davidson; Marko E Horb; Rachel K Miller
Journal:  Genes (Basel)       Date:  2018-04-06       Impact factor: 4.096

10.  The Lhx1-Ldb1 complex interacts with Furry to regulate microRNA expression during pronephric kidney development.

Authors:  Eugenel B Espiritu; Amanda E Crunk; Abha Bais; Daniel Hochbaum; Ailen S Cervino; Yu Leng Phua; Michael B Butterworth; Toshiyasu Goto; Jacqueline Ho; Neil A Hukriede; M Cecilia Cirio
Journal:  Sci Rep       Date:  2018-10-30       Impact factor: 4.379

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