PUBLICATION

CRISPR mutation in lysine (K)-specific demethylase 1a (kdm1a/LSD1) does not produce defects to skeletal development in maternal zygotic mutant zebrafish larvae

Authors: DeLaurier A., Wiggins K.J., Mishoe Hernandez L., Loyo Rosado F., Pugh, K., Shabdue, C.
ID: ZDB-PUB-200515-15
Date: 2020
Source: ZebraShare : (Unpublished)
Registered Authors: DeLaurier, April
Keywords: none
MeSH Terms: none
PubMed: none

Abstract

CRISPR-Cas9 technology was used to generate a mutation in exon 1 of kdm1a (LSD1). A 14 bp deletion was generated, causing missense and a premature stop codon predicted to cause a truncated protein. Mutants are viable and able to reproduce. Maternal zygotic mutants were generated and examined for skeletal phenotypes using Alician Blue and Alizarin Red dyes. No obvious skeletal defects were observed in fish at 4 days post-fertilization.

Genes / Markers

Figures

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Expression

Phenotype

Fish	Conditions	Stage	Phenotype	Figure
kdm1a^aik5/aik5 (AB)	standard conditions	Day 4	cranium morphology, normal	Fig. 1
kdm1a^aik5/aik5 (AB)	standard conditions	Day 4	neurocranium morphology, normal	Fig. 1
kdm1a^aik5/aik5 (AB)	standard conditions	Day 4	splanchnocranium morphology, normal	Fig. 1

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Mutations / Transgenics

Allele	Construct	Type	Affected Genomic Region
aik5		Small Deletion	kdm1a

Human Disease / Model

Sequence Targeting Reagents

Target	Reagent	Reagent Type
kdm1a	CRISPR1-kdm1a	CRISPR

Fish

Fish
kdm1a^aik5/aik5 (AB)

Antibodies

Orthology

Engineered Foreign Genes

Mapping

DeLaurier A. et al., 2020 ZDB-PUB-200515-15

CRISPR mutation in lysine (K)-specific demethylase 1a (kdm1a/LSD1) does not produce defects to skeletal development in maternal zygotic mutant zebrafish larvae

DeLaurier A. et al., 2020

ZDB-PUB-200515-15