A hydrophobic ligand-binding protein of the Taenia solium metacestode mediates uptake of the host lipid: Implication for the maintenance of parasitic cellular homeostasis
- Authors
- Lee, E.-G.; Kim, S.-H.; Bae, Y.-A.; Chung, J.-Y.; Suh, M.; Na, B.-K.; Kim, T.-S.; Kang, I.; Ma, L.; Kong, Y.
- Issue Date
- Nov-2007
- Publisher
- WILEY-V C H VERLAG GMBH
- Keywords
- Cellular homeostasis; Host lipid uptake; Hydrophobic ligand-binding protein; Taenia solium neurocysticercosis; Therapeutic vaccine
- Citation
- Proteomics, v.7, no.21, pp 4016 - 4030
- Pages
- 15
- Indexed
- SCIE
SCOPUS
- Journal Title
- Proteomics
- Volume
- 7
- Number
- 21
- Start Page
- 4016
- End Page
- 4030
- URI
- https://scholarworks.gnu.ac.kr/handle/sw.gnu/29027
- DOI
- 10.1002/pmic.200700332
- ISSN
- 1615-9853
1615-9861
- Abstract
- Parasitic organisms are incapable of de novo fatty acid synthesis due to a down-regulated expression of enzymes involved in the oxygen-dependent pathway. We investigated the uptake of host lipids by a 150-kDa hydrophobic ligand-binding protein (HLBP) of Taenia solium metacestode, an agent causative of neurocysticercosis. The protein was found to be a hetero-oligomeric complex consisting of multiple subunits (M r 7, 10, and 15 kDa within pH 8.0-9.7), which may originate from four unique genes of 7- and 10-kDa gene families with 2-3 polymorphic alleles/paralogs. The 15-kDa protein represented glycosylated forms of the 10-kDa. With high binding affinity to lipid analogs, these subunits evidenced high-level sequence identity with other cestode HLBPs and form a novel clade associated with excretory-secretory type HLBP. In vitro experiments with viable worms suggested that the excreted 150-kDa protein might bind to lipids, and participate in the translocation of host lipids across the syncytial membrane. This process was substantially inhibited by the specific anti-150 kDa antibodies. The protein was localized in the parasite syncytium and in the lipid droplets within host granuloma wall, where significant lipase activity was expressed. HLBP-mediated uptake of the host lipid may be critical for the parasite survival and thus could be targeted by chemotherapeutics and/or vaccine. ? 2007 Wiley-VCH Verlag GmbH & Co. KGaA.
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