| Literature DB >> 16531243 |
Renaud Morales1, Anne Berna, Philippe Carpentier, Carlos Contreras-Martel, Frédérique Renault, Murielle Nicodeme, Marie-Laure Chesne-Seck, François Bernier, Jérôme Dupuy, Christine Schaeffer, Hélène Diemer, Alain Van-Dorsselaer, Juan C Fontecilla-Camps, Patrick Masson, Daniel Rochu, Eric Chabriere.
Abstract
We report the serendipitous discovery of a human plasma phosphate binding protein (HPBP). This 38 kDa protein is copurified with the enzyme paraoxonase. Its X-ray structure is similar to the prokaryotic phosphate solute binding proteins (SBPs) associated with ATP binding cassette transmembrane transporters, though phosphate-SBPs have never been characterized or predicted from nucleic acid databases in eukaryotes. However, HPBP belongs to the family of ubiquitous eukaryotic proteins named DING, meaning that phosphate-SBPs are also widespread in eukaryotes. The systematic absence of complete genes for eukaryotic phosphate-SBP from databases is intriguing, but the astonishing 90% sequence conservation between genes belonging to evolutionary distant species suggests that the corresponding proteins play an important function. HPBP is the only known transporter capable of binding phosphate ions in human plasma and may become a new predictor of or a potential therapeutic agent for phosphate-related diseases such as atherosclerosis.Entities:
Mesh:
Substances:
Year: 2006 PMID: 16531243 DOI: 10.1016/j.str.2005.12.012
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006