Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy

Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy

Shwachman-Diamond syndrome (SDS) is characterized by exocrine pancreatic insufficiency, neutropenia, and skeletal abnormalities. Biallelic mutations in SBDS, which encodes a ribosome maturation factor, are found in 90% of SDS cases. Sbds–/– mice are embryonic lethal. Using CRISPR/Cas9 editing, we cr...

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Main Authors: Usua Oyarbide, Arish N. Shah, Wilmer Amaya-Mejia, Matthew Snyderman, Margaret J. Kell, Daniela S. Allende, Eliezer Calo, Jacek Topczewski, Seth J. Corey
Format: Article
Language:English
Published: American Society for Clinical investigation 2020-09-01
Series:JCI Insight
Subjects:
Gastroenterology
Hematology
Online Access:https://doi.org/10.1172/jci.insight.134309
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spelling doaj-24c40a85c3af4d0db9e6f4b4e7b875982021-08-02T15:55:57ZengAmerican Society for Clinical investigationJCI Insight2379-37082020-09-01517Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophyUsua OyarbideArish N. ShahWilmer Amaya-MejiaMatthew SnydermanMargaret J. KellDaniela S. AllendeEliezer CaloJacek TopczewskiSeth J. CoreyShwachman-Diamond syndrome (SDS) is characterized by exocrine pancreatic insufficiency, neutropenia, and skeletal abnormalities. Biallelic mutations in SBDS, which encodes a ribosome maturation factor, are found in 90% of SDS cases. Sbds–/– mice are embryonic lethal. Using CRISPR/Cas9 editing, we created sbds-deficient zebrafish strains. Sbds protein levels progressively decreased and became undetectable at 10 days postfertilization (dpf). Polysome analysis revealed decreased 80S ribosomes. Homozygous mutant fish developed normally until 15 dpf. Mutant fish subsequently had stunted growth and showed signs of atrophy in pancreas, liver, and intestine. In addition, neutropenia occurred by 5 dpf. Upregulation of tp53 mRNA did not occur until 10 dpf, and inhibition of proliferation correlated with death by 21 dpf. Transcriptome analysis showed tp53 activation through upregulation of genes involved in cell cycle arrest, cdkn1a and ccng1, and apoptosis, puma and mdm2. However, elimination of Tp53 function did not prevent lethality. Because of growth retardation and atrophy of intestinal epithelia, we studied the effects of starvation on WT fish. Starved WT fish showed intestinal atrophy, zymogen granule loss, and tp53 upregulation — similar to the mutant phenotype. In addition, there was reduction in neutral lipid storage and ribosomal protein amount, similar to the mutant phenotype. Thus, loss of Sbds in zebrafish phenocopies much of the human disease and is associated with growth arrest and tissue atrophy, particularly of the gastrointestinal system, at the larval stage. A variety of stress responses, some associated with Tp53, contribute to pathophysiology of SDS.https://doi.org/10.1172/jci.insight.134309GastroenterologyHematology
collection DOAJ
language English
format Article
sources DOAJ
author Usua Oyarbide
Arish N. Shah
Wilmer Amaya-Mejia
Matthew Snyderman
Margaret J. Kell
Daniela S. Allende
Eliezer Calo
Jacek Topczewski
Seth J. Corey
spellingShingle Usua Oyarbide
Arish N. Shah
Wilmer Amaya-Mejia
Matthew Snyderman
Margaret J. Kell
Daniela S. Allende
Eliezer Calo
Jacek Topczewski
Seth J. Corey
Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
JCI Insight
Gastroenterology
Hematology
author_facet Usua Oyarbide
Arish N. Shah
Wilmer Amaya-Mejia
Matthew Snyderman
Margaret J. Kell
Daniela S. Allende
Eliezer Calo
Jacek Topczewski
Seth J. Corey
author_sort Usua Oyarbide
title Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
title_short Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
title_full Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
title_fullStr Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
title_full_unstemmed Loss of Sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
title_sort loss of sbds in zebrafish leads to neutropenia and pancreas and liver atrophy
publisher American Society for Clinical investigation
series JCI Insight
issn 2379-3708
publishDate 2020-09-01
description Shwachman-Diamond syndrome (SDS) is characterized by exocrine pancreatic insufficiency, neutropenia, and skeletal abnormalities. Biallelic mutations in SBDS, which encodes a ribosome maturation factor, are found in 90% of SDS cases. Sbds–/– mice are embryonic lethal. Using CRISPR/Cas9 editing, we created sbds-deficient zebrafish strains. Sbds protein levels progressively decreased and became undetectable at 10 days postfertilization (dpf). Polysome analysis revealed decreased 80S ribosomes. Homozygous mutant fish developed normally until 15 dpf. Mutant fish subsequently had stunted growth and showed signs of atrophy in pancreas, liver, and intestine. In addition, neutropenia occurred by 5 dpf. Upregulation of tp53 mRNA did not occur until 10 dpf, and inhibition of proliferation correlated with death by 21 dpf. Transcriptome analysis showed tp53 activation through upregulation of genes involved in cell cycle arrest, cdkn1a and ccng1, and apoptosis, puma and mdm2. However, elimination of Tp53 function did not prevent lethality. Because of growth retardation and atrophy of intestinal epithelia, we studied the effects of starvation on WT fish. Starved WT fish showed intestinal atrophy, zymogen granule loss, and tp53 upregulation — similar to the mutant phenotype. In addition, there was reduction in neutral lipid storage and ribosomal protein amount, similar to the mutant phenotype. Thus, loss of Sbds in zebrafish phenocopies much of the human disease and is associated with growth arrest and tissue atrophy, particularly of the gastrointestinal system, at the larval stage. A variety of stress responses, some associated with Tp53, contribute to pathophysiology of SDS.
topic Gastroenterology
Hematology
url https://doi.org/10.1172/jci.insight.134309
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