Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway

<p>Abstract</p> <p>Background</p> <p>Aberrant activation of the Hedgehog (Hh) signaling pathway in different organisms has shown the importance of this family of morphogens during development. Genetic screens in zebrafish have assigned specific roles for Hh in prolifera...

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Main Authors: Groot Evelyn, den Broeder Marjo J, Koudijs Marco J, van Eeden Fredericus JM
Format: Article
Language:English
Published: BMC 2008-02-01
Series:BMC Developmental Biology
Online Access:http://www.biomedcentral.com/1471-213X/8/15
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spelling doaj-415726c6318d42f488189da18b80a9162020-11-25T00:45:01ZengBMCBMC Developmental Biology1471-213X2008-02-01811510.1186/1471-213X-8-15Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathwayGroot Evelynden Broeder Marjo JKoudijs Marco Jvan Eeden Fredericus JM<p>Abstract</p> <p>Background</p> <p>Aberrant activation of the Hedgehog (Hh) signaling pathway in different organisms has shown the importance of this family of morphogens during development. Genetic screens in zebrafish have assigned specific roles for Hh in proliferation, differentiation and patterning, but mainly as a result of a loss of its activity. We attempted to fully activate the Hh pathway by removing both receptors for the Hh proteins, called Patched1 and 2, which are functioning as negative regulators in this pathway.</p> <p>Results</p> <p>Here we describe a splice-donor mutation in Ptc1, called <it>ptc1</it><sup><it>hu1602</it></sup>, which in a homozygous state results in a subtle eye and somite phenotype. Since we recently positionally cloned a <it>ptc2 </it>mutant, a <it>ptc1;ptc2 </it>double mutant was generated, showing severely increased levels of <it>ptc1</it>, <it>gli1 </it>and <it>nkx2.2a</it>, confirming an aberrant activation of Hh signaling. As a consequence, a number of phenotypes were observed that have not been reported previously using <it>Shh </it>mRNA overexpression. Somites of <it>ptc1;ptc2 </it>double mutants do not express anteroposterior polarity markers, however initial segmentation of the somites itself is not affected. This is the first evidence that segmentation and anterior/posterior (A/P) patterning of the somites are genetically uncoupled processes. Furthermore, a novel negative function of Hh signaling is observed in the induction of the fin field, acting well before any of the previously reported function of Shh in fin formation and in a way that is different from the proposed early role of Gli3 in limb/fin bud patterning.</p> <p>Conclusion</p> <p>The generation and characterization of the <it>ptc1;ptc2 </it>double mutant assigned novel and unexpected functions to the Hh signaling pathway. Additionally, these mutants will provide a useful system to further investigate the consequences of constitutively activated Hh signaling during vertebrate development.</p> http://www.biomedcentral.com/1471-213X/8/15
collection DOAJ
language English
format Article
sources DOAJ
author Groot Evelyn
den Broeder Marjo J
Koudijs Marco J
van Eeden Fredericus JM
spellingShingle Groot Evelyn
den Broeder Marjo J
Koudijs Marco J
van Eeden Fredericus JM
Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
BMC Developmental Biology
author_facet Groot Evelyn
den Broeder Marjo J
Koudijs Marco J
van Eeden Fredericus JM
author_sort Groot Evelyn
title Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
title_short Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
title_full Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
title_fullStr Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
title_full_unstemmed Genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
title_sort genetic analysis of the two zebrafish patched homologues identifies novel roles for the hedgehog signaling pathway
publisher BMC
series BMC Developmental Biology
issn 1471-213X
publishDate 2008-02-01
description <p>Abstract</p> <p>Background</p> <p>Aberrant activation of the Hedgehog (Hh) signaling pathway in different organisms has shown the importance of this family of morphogens during development. Genetic screens in zebrafish have assigned specific roles for Hh in proliferation, differentiation and patterning, but mainly as a result of a loss of its activity. We attempted to fully activate the Hh pathway by removing both receptors for the Hh proteins, called Patched1 and 2, which are functioning as negative regulators in this pathway.</p> <p>Results</p> <p>Here we describe a splice-donor mutation in Ptc1, called <it>ptc1</it><sup><it>hu1602</it></sup>, which in a homozygous state results in a subtle eye and somite phenotype. Since we recently positionally cloned a <it>ptc2 </it>mutant, a <it>ptc1;ptc2 </it>double mutant was generated, showing severely increased levels of <it>ptc1</it>, <it>gli1 </it>and <it>nkx2.2a</it>, confirming an aberrant activation of Hh signaling. As a consequence, a number of phenotypes were observed that have not been reported previously using <it>Shh </it>mRNA overexpression. Somites of <it>ptc1;ptc2 </it>double mutants do not express anteroposterior polarity markers, however initial segmentation of the somites itself is not affected. This is the first evidence that segmentation and anterior/posterior (A/P) patterning of the somites are genetically uncoupled processes. Furthermore, a novel negative function of Hh signaling is observed in the induction of the fin field, acting well before any of the previously reported function of Shh in fin formation and in a way that is different from the proposed early role of Gli3 in limb/fin bud patterning.</p> <p>Conclusion</p> <p>The generation and characterization of the <it>ptc1;ptc2 </it>double mutant assigned novel and unexpected functions to the Hh signaling pathway. Additionally, these mutants will provide a useful system to further investigate the consequences of constitutively activated Hh signaling during vertebrate development.</p>
url http://www.biomedcentral.com/1471-213X/8/15
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