The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia

The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia

Fanconi anemia (FA) is a human genetic disease characterized by congenital defects, bone marrow failure, and increased cancer risk. FA is associated with mutation in one of 24 genes. The protein products of these genes function cooperatively in the FA pathway to orchestrate the repair of DNA interst...

Full description

Bibliographic Details
Main Authors: Edward C. Stanley, Paul A. Azzinaro, David A. Vierra, Niall G. Howlett, Steven Q. Irvine
Format: Article
Language:English
Published: SAGE Publishing 2016-01-01
Series:Evolutionary Bioinformatics
Online Access:https://doi.org/10.4137/EBO.S37920
id doaj-b32dee06a7874c0d8ab1b1f1309d7dc0
record_format Article
spelling doaj-b32dee06a7874c0d8ab1b1f1309d7dc02020-11-25T03:17:51ZengSAGE PublishingEvolutionary Bioinformatics1176-93432016-01-011210.4137/EBO.S37920The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi AnemiaEdward C. Stanley0Paul A. Azzinaro1David A. Vierra2Niall G. Howlett3Steven Q. Irvine4Integrative and Evolutionary Biology Graduate SpecializationCell and Molecular Biology Graduate SpecializationCell and Molecular Biology Graduate SpecializationDepartment of Cell and Molecular BiologyDepartment of Biological Sciences, University of Rhode Island, Kingston, RI, USA.Fanconi anemia (FA) is a human genetic disease characterized by congenital defects, bone marrow failure, and increased cancer risk. FA is associated with mutation in one of 24 genes. The protein products of these genes function cooperatively in the FA pathway to orchestrate the repair of DNA interstrand cross-links. Few model organisms exist for the study of FA. Seeking a model organism with a simpler version of the FA pathway, we searched the genome of the simple chordate Ciona intestinalis for homologs of the human FA-associated proteins. BLAST searches, sequence alignments, hydropathy comparisons, maximum likelihood phylogenetic analysis, and structural modeling were used to infer the likelihood of homology between C. intestinalis and human FA proteins. Our analysis indicates that C. intestinalis indeed has a simpler and potentially functional FA pathway. The C. intestinalis genome was searched for candidates for homology to 24 human FA and FA-associated proteins. Support was found for the existence of homologs for 13 of these 24 human genes in C. intestinalis. Members of each of the three commonly recognized FA gene functional groups were found. In group I, we identified homologs of FANCE, FANCL, FANCM, and UBE2T/FANCT. Both members of group II, FANCD2 and FANCI, have homologs in C. intestinalis. In group III, we found evidence for homologs of FANCJ, FANCO, FANCQ/ERCC4, FANCR/RAD51, and FANCS/BRCA1, as well as the FA-associated proteins ERCC1 and FAN1. Evidence was very weak for the existence of homologs in C. intestinalis for any other recognized FA genes. This work supports the notion that C. intestinalis , as a close relative of vertebrates, but having a much reduced complement of FA genes, offers a means of studying the function of certain FA proteins in a simpler pathway than that of vertebrate cells.https://doi.org/10.4137/EBO.S37920
collection DOAJ
language English
format Article
sources DOAJ
author Edward C. Stanley
Paul A. Azzinaro
David A. Vierra
Niall G. Howlett
Steven Q. Irvine
spellingShingle Edward C. Stanley
Paul A. Azzinaro
David A. Vierra
Niall G. Howlett
Steven Q. Irvine
The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia
Evolutionary Bioinformatics
author_facet Edward C. Stanley
Paul A. Azzinaro
David A. Vierra
Niall G. Howlett
Steven Q. Irvine
author_sort Edward C. Stanley
title The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia
title_short The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia
title_full The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia
title_fullStr The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia
title_full_unstemmed The Simple Chordate Has a Reduced Complement of Genes Associated with Fanconi Anemia
title_sort simple chordate has a reduced complement of genes associated with fanconi anemia
publisher SAGE Publishing
series Evolutionary Bioinformatics
issn 1176-9343
publishDate 2016-01-01
description Fanconi anemia (FA) is a human genetic disease characterized by congenital defects, bone marrow failure, and increased cancer risk. FA is associated with mutation in one of 24 genes. The protein products of these genes function cooperatively in the FA pathway to orchestrate the repair of DNA interstrand cross-links. Few model organisms exist for the study of FA. Seeking a model organism with a simpler version of the FA pathway, we searched the genome of the simple chordate Ciona intestinalis for homologs of the human FA-associated proteins. BLAST searches, sequence alignments, hydropathy comparisons, maximum likelihood phylogenetic analysis, and structural modeling were used to infer the likelihood of homology between C. intestinalis and human FA proteins. Our analysis indicates that C. intestinalis indeed has a simpler and potentially functional FA pathway. The C. intestinalis genome was searched for candidates for homology to 24 human FA and FA-associated proteins. Support was found for the existence of homologs for 13 of these 24 human genes in C. intestinalis. Members of each of the three commonly recognized FA gene functional groups were found. In group I, we identified homologs of FANCE, FANCL, FANCM, and UBE2T/FANCT. Both members of group II, FANCD2 and FANCI, have homologs in C. intestinalis. In group III, we found evidence for homologs of FANCJ, FANCO, FANCQ/ERCC4, FANCR/RAD51, and FANCS/BRCA1, as well as the FA-associated proteins ERCC1 and FAN1. Evidence was very weak for the existence of homologs in C. intestinalis for any other recognized FA genes. This work supports the notion that C. intestinalis , as a close relative of vertebrates, but having a much reduced complement of FA genes, offers a means of studying the function of certain FA proteins in a simpler pathway than that of vertebrate cells.
url https://doi.org/10.4137/EBO.S37920
work_keys_str_mv AT edwardcstanley thesimplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT paulaazzinaro thesimplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT davidavierra thesimplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT niallghowlett thesimplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT stevenqirvine thesimplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT edwardcstanley simplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT paulaazzinaro simplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT davidavierra simplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT niallghowlett simplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
AT stevenqirvine simplechordatehasareducedcomplementofgenesassociatedwithfanconianemia
_version_ 1724629475852812288

Similar Items