Identification of hookworm DAF-16/FOXO response elements and direct gene targets.
The infective stage of the parasitic nematode hookworm is developmentally arrested in the environment and needs to infect a specific host to complete its life cycle. The canine hookworm (Ancylostoma caninum) is an excellent model for investigating human hookworm infections. The transcription factor...
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doaj-59a74554ce0b4a1ab5b1392a91a621e02020-11-24T21:51:02ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-08-0158e1228910.1371/journal.pone.0012289Identification of hookworm DAF-16/FOXO response elements and direct gene targets.Xin GaoZhengyuan WangJohn MartinSahar AbubuckerXu ZhangMakedonka MitrevaJohn M HawdonThe infective stage of the parasitic nematode hookworm is developmentally arrested in the environment and needs to infect a specific host to complete its life cycle. The canine hookworm (Ancylostoma caninum) is an excellent model for investigating human hookworm infections. The transcription factor of A. caninum, Ac-DAF-16, which has a characteristic fork head or "winged helix" DNA binding domain (DBD), has been implicated in the resumption of hookworm development in the host. However, the precise roles of Ac-DAF-16 in hookworm parasitism and its downstream targets are unknown. In the present study, we combined molecular techniques and bioinformatics to identify a group of Ac-DAF-16 binding sites and target genes.The DNA binding domain of Ac-DAF-16 was used to select genomic fragments by in vitro genomic selection. Twenty four bound genomic fragments were analyzed for the presence of the DAF-16 family binding element (DBE) and possible alternative Ac-DAF-16 bind motifs. The 22 genes linked to these genomic fragments were identified using bioinformatics tools and defined as candidate direct gene targets of Ac-DAF-16. Their developmental stage-specific expression patterns were examined. Also, a new putative DAF-16 binding element was identified.Our results show that Ac-DAF-16 is involved in diverse biological processes throughout hookworm development. Further investigation of these target genes will provide insights into the molecular basis by which Ac-DAF-16 regulates its downstream gene network in hookworm infection.http://europepmc.org/articles/PMC2924398?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Xin Gao Zhengyuan Wang John Martin Sahar Abubucker Xu Zhang Makedonka Mitreva John M Hawdon |
spellingShingle |
Xin Gao Zhengyuan Wang John Martin Sahar Abubucker Xu Zhang Makedonka Mitreva John M Hawdon Identification of hookworm DAF-16/FOXO response elements and direct gene targets. PLoS ONE |
author_facet |
Xin Gao Zhengyuan Wang John Martin Sahar Abubucker Xu Zhang Makedonka Mitreva John M Hawdon |
author_sort |
Xin Gao |
title |
Identification of hookworm DAF-16/FOXO response elements and direct gene targets. |
title_short |
Identification of hookworm DAF-16/FOXO response elements and direct gene targets. |
title_full |
Identification of hookworm DAF-16/FOXO response elements and direct gene targets. |
title_fullStr |
Identification of hookworm DAF-16/FOXO response elements and direct gene targets. |
title_full_unstemmed |
Identification of hookworm DAF-16/FOXO response elements and direct gene targets. |
title_sort |
identification of hookworm daf-16/foxo response elements and direct gene targets. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2010-08-01 |
description |
The infective stage of the parasitic nematode hookworm is developmentally arrested in the environment and needs to infect a specific host to complete its life cycle. The canine hookworm (Ancylostoma caninum) is an excellent model for investigating human hookworm infections. The transcription factor of A. caninum, Ac-DAF-16, which has a characteristic fork head or "winged helix" DNA binding domain (DBD), has been implicated in the resumption of hookworm development in the host. However, the precise roles of Ac-DAF-16 in hookworm parasitism and its downstream targets are unknown. In the present study, we combined molecular techniques and bioinformatics to identify a group of Ac-DAF-16 binding sites and target genes.The DNA binding domain of Ac-DAF-16 was used to select genomic fragments by in vitro genomic selection. Twenty four bound genomic fragments were analyzed for the presence of the DAF-16 family binding element (DBE) and possible alternative Ac-DAF-16 bind motifs. The 22 genes linked to these genomic fragments were identified using bioinformatics tools and defined as candidate direct gene targets of Ac-DAF-16. Their developmental stage-specific expression patterns were examined. Also, a new putative DAF-16 binding element was identified.Our results show that Ac-DAF-16 is involved in diverse biological processes throughout hookworm development. Further investigation of these target genes will provide insights into the molecular basis by which Ac-DAF-16 regulates its downstream gene network in hookworm infection. |
url |
http://europepmc.org/articles/PMC2924398?pdf=render |
work_keys_str_mv |
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