Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome

Zebrafish represent a valuable model for investigating the molecular and cellular basis of Fragile X syndrome (FXS). Reduced expression of the zebrafish FMR1 orthologous gene, fmr1, causes developmental and behavioural phenotypes related to FXS. Zebrafish homozygous for the hu2787 non-sense mutation...

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Autores principales: Barthelson, Karissa, Baer, Lachlan, Dong, Yang, Hand, Melanie, Pujic, Zac, Newman, Morgan, Goodhill, Geoffrey J., Richards, Robert I., Pederson, Stephen M., Lardelli, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Genetics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8203322/
https://www.ncbi.nlm.nih.gov/pubmed/34135935
http://dx.doi.org/10.3389/fgene.2021.625466
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author Barthelson, Karissa
Baer, Lachlan
Dong, Yang
Hand, Melanie
Pujic, Zac
Newman, Morgan
Goodhill, Geoffrey J.
Richards, Robert I.
Pederson, Stephen M.
Lardelli, Michael
author_facet Barthelson, Karissa
Baer, Lachlan
Dong, Yang
Hand, Melanie
Pujic, Zac
Newman, Morgan
Goodhill, Geoffrey J.
Richards, Robert I.
Pederson, Stephen M.
Lardelli, Michael
author_sort Barthelson, Karissa
collection PubMed
description Zebrafish represent a valuable model for investigating the molecular and cellular basis of Fragile X syndrome (FXS). Reduced expression of the zebrafish FMR1 orthologous gene, fmr1, causes developmental and behavioural phenotypes related to FXS. Zebrafish homozygous for the hu2787 non-sense mutation allele of fmr1 are widely used to model FXS, although FXS-relevant phenotypes seen from morpholino antisense oligonucleotide (morpholino) suppression of fmr1 transcript translation were not observed when hu2787 was first described. The subsequent discovery of transcriptional adaptation (a form of genetic compensation), whereby mutations causing non-sense-mediated decay of transcripts can drive compensatory upregulation of homologous transcripts independent of protein feedback loops, suggested an explanation for the differences reported. We examined the whole-embryo transcriptome effects of homozygosity for fmr1(hu2787) at 2 days post fertilisation. We observed statistically significant changes in expression of a number of gene transcripts, but none from genes showing sequence homology to fmr1. Enrichment testing of differentially expressed genes implied effects on lysosome function and glycosphingolipid biosynthesis. The majority of the differentially expressed genes are located, like fmr1, on Chromosome 14. Quantitative PCR tests did not support that this was artefactual due to changes in relative chromosome abundance. Enrichment testing of the “leading edge” differentially expressed genes from Chromosome 14 revealed that their co-location on this chromosome may be associated with roles in brain development and function. The differential expression of functionally related genes due to mutation of fmr1, and located on the same chromosome as fmr1, is consistent with R.A. Fisher’s assertion that the selective advantage of co-segregation of particular combinations of alleles of genes will favour, during evolution, chromosomal rearrangements that place them in linkage disequilibrium on the same chromosome. However, we cannot exclude that the apparent differential expression of genes on Chromosome 14 genes was, (if only in part), caused by differences between the expression of alleles of genes unrelated to the effects of the fmr1(hu2787) mutation and made manifest due to the limited, but non-zero, allelic diversity between the genotypes compared.
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spelling pubmed-82033222021-06-15 Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome Barthelson, Karissa Baer, Lachlan Dong, Yang Hand, Melanie Pujic, Zac Newman, Morgan Goodhill, Geoffrey J. Richards, Robert I. Pederson, Stephen M. Lardelli, Michael Front Genet Genetics Zebrafish represent a valuable model for investigating the molecular and cellular basis of Fragile X syndrome (FXS). Reduced expression of the zebrafish FMR1 orthologous gene, fmr1, causes developmental and behavioural phenotypes related to FXS. Zebrafish homozygous for the hu2787 non-sense mutation allele of fmr1 are widely used to model FXS, although FXS-relevant phenotypes seen from morpholino antisense oligonucleotide (morpholino) suppression of fmr1 transcript translation were not observed when hu2787 was first described. The subsequent discovery of transcriptional adaptation (a form of genetic compensation), whereby mutations causing non-sense-mediated decay of transcripts can drive compensatory upregulation of homologous transcripts independent of protein feedback loops, suggested an explanation for the differences reported. We examined the whole-embryo transcriptome effects of homozygosity for fmr1(hu2787) at 2 days post fertilisation. We observed statistically significant changes in expression of a number of gene transcripts, but none from genes showing sequence homology to fmr1. Enrichment testing of differentially expressed genes implied effects on lysosome function and glycosphingolipid biosynthesis. The majority of the differentially expressed genes are located, like fmr1, on Chromosome 14. Quantitative PCR tests did not support that this was artefactual due to changes in relative chromosome abundance. Enrichment testing of the “leading edge” differentially expressed genes from Chromosome 14 revealed that their co-location on this chromosome may be associated with roles in brain development and function. The differential expression of functionally related genes due to mutation of fmr1, and located on the same chromosome as fmr1, is consistent with R.A. Fisher’s assertion that the selective advantage of co-segregation of particular combinations of alleles of genes will favour, during evolution, chromosomal rearrangements that place them in linkage disequilibrium on the same chromosome. However, we cannot exclude that the apparent differential expression of genes on Chromosome 14 genes was, (if only in part), caused by differences between the expression of alleles of genes unrelated to the effects of the fmr1(hu2787) mutation and made manifest due to the limited, but non-zero, allelic diversity between the genotypes compared. Frontiers Media S.A. 2021-05-31 /pmc/articles/PMC8203322/ /pubmed/34135935 http://dx.doi.org/10.3389/fgene.2021.625466 Text en Copyright © 2021 Barthelson, Baer, Dong, Hand, Pujic, Newman, Goodhill, Richards, Pederson and Lardelli. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Genetics
Barthelson, Karissa
Baer, Lachlan
Dong, Yang
Hand, Melanie
Pujic, Zac
Newman, Morgan
Goodhill, Geoffrey J.
Richards, Robert I.
Pederson, Stephen M.
Lardelli, Michael
Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome
title Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome
title_full Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome
title_fullStr Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome
title_full_unstemmed Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome
title_short Zebrafish Chromosome 14 Gene Differential Expression in the fmr1(hu2787) Model of Fragile X Syndrome
title_sort zebrafish chromosome 14 gene differential expression in the fmr1(hu2787) model of fragile x syndrome
topic Genetics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8203322/
https://www.ncbi.nlm.nih.gov/pubmed/34135935
http://dx.doi.org/10.3389/fgene.2021.625466
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