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Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode

BACKGROUND: Fatty acid (FA) binding proteins (FABPs) of helminths are implicated in acquisition and utilization of host-derived hydrophobic substances, as well as in signaling and cellular interactions. We previously demonstrated that secretory hydrophobic ligand binding proteins (HLBPs) of Taenia s...

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Autores principales: Kim, Seon-Hee, Bae, Young-An, Yang, Hyun-Jong, Shin, Joo-Ho, Diaz-Camacho, Sylvia Paz, Nawa, Yukifumi, Kang, Insug, Kong, Yoon
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3493614/
https://www.ncbi.nlm.nih.gov/pubmed/23150743
http://dx.doi.org/10.1371/journal.pntd.0001868
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author Kim, Seon-Hee
Bae, Young-An
Yang, Hyun-Jong
Shin, Joo-Ho
Diaz-Camacho, Sylvia Paz
Nawa, Yukifumi
Kang, Insug
Kong, Yoon
author_facet Kim, Seon-Hee
Bae, Young-An
Yang, Hyun-Jong
Shin, Joo-Ho
Diaz-Camacho, Sylvia Paz
Nawa, Yukifumi
Kang, Insug
Kong, Yoon
author_sort Kim, Seon-Hee
collection PubMed
description BACKGROUND: Fatty acid (FA) binding proteins (FABPs) of helminths are implicated in acquisition and utilization of host-derived hydrophobic substances, as well as in signaling and cellular interactions. We previously demonstrated that secretory hydrophobic ligand binding proteins (HLBPs) of Taenia solium metacestode (TsM), a causative agent of neurocysticercosis (NC), shuttle FAs in the surrounding host tissues and inwardly transport the FAs across the parasite syncytial membrane. However, the protein molecules responsible for the intracellular trafficking and assimilation of FAs have remained elusive. METHODOLOGY/PRINCIPAL FINDINGS: We isolated two novel TsMFABP genes (TsMFABP1 and TsMFABP2), which encoded 133- and 136-amino acid polypeptides with predicted molecular masses of 14.3 and 14.8 kDa, respectively. They shared 45% sequence identity with each other and 15–95% with other related-members. Homology modeling demonstrated a characteristic β-barrel composed of 10 anti-parallel β-strands and two α-helices. TsMFABP2 harbored two additional loops between β-strands two and three, and β-strands six and seven, respectively. TsMFABP1 was secreted into cyst fluid and surrounding environments, whereas TsMFABP2 was intracellularly confined. Partially purified native proteins migrated to 15 kDa with different isoelectric points of 9.2 (TsMFABP1) and 8.4 (TsMFABP2). Both native and recombinant proteins bound to 11-([5-dimethylaminonaphthalene-1-sulfonyl]amino)undecannoic acid, dansyl-DL-α-amino-caprylic acid, cis-parinaric acid and retinol, which were competitively inhibited by oleic acid. TsMFABP1 exhibited high affinity toward FA analogs. TsMFABPs showed weak binding activity to retinol, but TsMFABP2 showed relatively high affinity. Isolation of two distinct genes from an individual genome strongly suggested their paralogous nature. Abundant expression of TsMFABP1 and TsMFABP2 in the canal region of worm matched well with the histological distributions of lipids and retinol. CONCLUSIONS/SIGNIFICANCE: The divergent biochemical properties, physiological roles and cellular distributions of the TsMFABPs might be one of the critical mechanisms compensating for inadequate de novo FA synthesis. These proteins might exert harmonized or independent roles on lipid assimilation and intracellular signaling. The specialized distribution of retinol in the canal region further implies that cells in this region might differentiate into diverse cell types during metamorphosis into an adult worm. Identification of bioactive systems pertinent to parasitic homeostasis may provide a valuable target for function-related drug design.
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spelling pubmed-34936142012-11-13 Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode Kim, Seon-Hee Bae, Young-An Yang, Hyun-Jong Shin, Joo-Ho Diaz-Camacho, Sylvia Paz Nawa, Yukifumi Kang, Insug Kong, Yoon PLoS Negl Trop Dis Research Article BACKGROUND: Fatty acid (FA) binding proteins (FABPs) of helminths are implicated in acquisition and utilization of host-derived hydrophobic substances, as well as in signaling and cellular interactions. We previously demonstrated that secretory hydrophobic ligand binding proteins (HLBPs) of Taenia solium metacestode (TsM), a causative agent of neurocysticercosis (NC), shuttle FAs in the surrounding host tissues and inwardly transport the FAs across the parasite syncytial membrane. However, the protein molecules responsible for the intracellular trafficking and assimilation of FAs have remained elusive. METHODOLOGY/PRINCIPAL FINDINGS: We isolated two novel TsMFABP genes (TsMFABP1 and TsMFABP2), which encoded 133- and 136-amino acid polypeptides with predicted molecular masses of 14.3 and 14.8 kDa, respectively. They shared 45% sequence identity with each other and 15–95% with other related-members. Homology modeling demonstrated a characteristic β-barrel composed of 10 anti-parallel β-strands and two α-helices. TsMFABP2 harbored two additional loops between β-strands two and three, and β-strands six and seven, respectively. TsMFABP1 was secreted into cyst fluid and surrounding environments, whereas TsMFABP2 was intracellularly confined. Partially purified native proteins migrated to 15 kDa with different isoelectric points of 9.2 (TsMFABP1) and 8.4 (TsMFABP2). Both native and recombinant proteins bound to 11-([5-dimethylaminonaphthalene-1-sulfonyl]amino)undecannoic acid, dansyl-DL-α-amino-caprylic acid, cis-parinaric acid and retinol, which were competitively inhibited by oleic acid. TsMFABP1 exhibited high affinity toward FA analogs. TsMFABPs showed weak binding activity to retinol, but TsMFABP2 showed relatively high affinity. Isolation of two distinct genes from an individual genome strongly suggested their paralogous nature. Abundant expression of TsMFABP1 and TsMFABP2 in the canal region of worm matched well with the histological distributions of lipids and retinol. CONCLUSIONS/SIGNIFICANCE: The divergent biochemical properties, physiological roles and cellular distributions of the TsMFABPs might be one of the critical mechanisms compensating for inadequate de novo FA synthesis. These proteins might exert harmonized or independent roles on lipid assimilation and intracellular signaling. The specialized distribution of retinol in the canal region further implies that cells in this region might differentiate into diverse cell types during metamorphosis into an adult worm. Identification of bioactive systems pertinent to parasitic homeostasis may provide a valuable target for function-related drug design. Public Library of Science 2012-10-25 /pmc/articles/PMC3493614/ /pubmed/23150743 http://dx.doi.org/10.1371/journal.pntd.0001868 Text en © 2012 Kim 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Kim, Seon-Hee
Bae, Young-An
Yang, Hyun-Jong
Shin, Joo-Ho
Diaz-Camacho, Sylvia Paz
Nawa, Yukifumi
Kang, Insug
Kong, Yoon
Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode
title Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode
title_full Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode
title_fullStr Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode
title_full_unstemmed Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode
title_short Structural and Binding Properties of Two Paralogous Fatty Acid Binding Proteins of Taenia solium Metacestode
title_sort structural and binding properties of two paralogous fatty acid binding proteins of taenia solium metacestode
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3493614/
https://www.ncbi.nlm.nih.gov/pubmed/23150743
http://dx.doi.org/10.1371/journal.pntd.0001868
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