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Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands

The human complement system is composed of more than 30 proteins and many of these have conserved domains that allow tracing the phylogenetic evolution. The complement system seems to be initiated with the appearance of C3 and factor B (FB), the only components found in some protostomes and cnidaria...

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Autores principales: Myamoto, Daniela Tiemi, Pidde-Queiroz, Giselle, Gonçalves-de-Andrade, Rute Maria, Pedroso, Aurélio, van den Berg, Carmen W., Tambourgi, Denise V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4714745/
https://www.ncbi.nlm.nih.gov/pubmed/26771533
http://dx.doi.org/10.1371/journal.pone.0146992
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author Myamoto, Daniela Tiemi
Pidde-Queiroz, Giselle
Gonçalves-de-Andrade, Rute Maria
Pedroso, Aurélio
van den Berg, Carmen W.
Tambourgi, Denise V.
author_facet Myamoto, Daniela Tiemi
Pidde-Queiroz, Giselle
Gonçalves-de-Andrade, Rute Maria
Pedroso, Aurélio
van den Berg, Carmen W.
Tambourgi, Denise V.
author_sort Myamoto, Daniela Tiemi
collection PubMed
description The human complement system is composed of more than 30 proteins and many of these have conserved domains that allow tracing the phylogenetic evolution. The complement system seems to be initiated with the appearance of C3 and factor B (FB), the only components found in some protostomes and cnidarians, suggesting that the alternative pathway is the most ancient. Here, we present the characterization of an arachnid homologue of the human complement component FB from the spider Loxosceles laeta. This homologue, named Lox-FB, was identified from a total RNA L. laeta spider venom gland library and was amplified using RACE-PCR techniques and specific primers. Analysis of the deduced amino acid sequence and the domain structure showed significant similarity to the vertebrate and invertebrate FB/C2 family proteins. Lox-FB has a classical domain organization composed of a control complement protein domain (CCP), a von Willebrand Factor domain (vWFA), and a serine protease domain (SP). The amino acids involved in Mg(2+) metal ion dependent adhesion site (MIDAS) found in the vWFA domain in the vertebrate C2/FB proteins are well conserved; however, the classic catalytic triad present in the serine protease domain is not conserved in Lox-FB. Similarity and phylogenetic analyses indicated that Lox-FB shares a major identity (43%) and has a close evolutionary relationship with the third isoform of FB-like protein (FB-3) from the jumping spider Hasarius adansoni belonging to the Family Salcitidae.
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spelling pubmed-47147452016-01-30 Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands Myamoto, Daniela Tiemi Pidde-Queiroz, Giselle Gonçalves-de-Andrade, Rute Maria Pedroso, Aurélio van den Berg, Carmen W. Tambourgi, Denise V. PLoS One Research Article The human complement system is composed of more than 30 proteins and many of these have conserved domains that allow tracing the phylogenetic evolution. The complement system seems to be initiated with the appearance of C3 and factor B (FB), the only components found in some protostomes and cnidarians, suggesting that the alternative pathway is the most ancient. Here, we present the characterization of an arachnid homologue of the human complement component FB from the spider Loxosceles laeta. This homologue, named Lox-FB, was identified from a total RNA L. laeta spider venom gland library and was amplified using RACE-PCR techniques and specific primers. Analysis of the deduced amino acid sequence and the domain structure showed significant similarity to the vertebrate and invertebrate FB/C2 family proteins. Lox-FB has a classical domain organization composed of a control complement protein domain (CCP), a von Willebrand Factor domain (vWFA), and a serine protease domain (SP). The amino acids involved in Mg(2+) metal ion dependent adhesion site (MIDAS) found in the vWFA domain in the vertebrate C2/FB proteins are well conserved; however, the classic catalytic triad present in the serine protease domain is not conserved in Lox-FB. Similarity and phylogenetic analyses indicated that Lox-FB shares a major identity (43%) and has a close evolutionary relationship with the third isoform of FB-like protein (FB-3) from the jumping spider Hasarius adansoni belonging to the Family Salcitidae. Public Library of Science 2016-01-15 /pmc/articles/PMC4714745/ /pubmed/26771533 http://dx.doi.org/10.1371/journal.pone.0146992 Text en © 2016 Myamoto et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Myamoto, Daniela Tiemi
Pidde-Queiroz, Giselle
Gonçalves-de-Andrade, Rute Maria
Pedroso, Aurélio
van den Berg, Carmen W.
Tambourgi, Denise V.
Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands
title Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands
title_full Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands
title_fullStr Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands
title_full_unstemmed Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands
title_short Characterization of a Gene Coding for the Complement System Component FB from Loxosceles laeta Spider Venom Glands
title_sort characterization of a gene coding for the complement system component fb from loxosceles laeta spider venom glands
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4714745/
https://www.ncbi.nlm.nih.gov/pubmed/26771533
http://dx.doi.org/10.1371/journal.pone.0146992
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