Characterization of a putative type IV aminophospholipid transporter P-type ATPase

被引:0
|
作者
Stéphane Flamant
Pascale Pescher
Brigitte Lemercier
Mathieu Clément-Ziza
François Képès
Marc Fellous
Geneviève Milon
Gilles Marchal
Claude Besmond
机构
[1] Hôpital Necker-Enfants Malades,
[2] INSERM U393,undefined
[3] Tour Lavoisier,undefined
[4] 2 ème étage,undefined
[5] 149 rue de Sèvres,undefined
[6] 75015 Paris,undefined
[7] France,undefined
[8] Laboratoire de Référence des Mycobactéries,undefined
[9] Institut Pasteur,undefined
[10] 25 rue du Dr. Roux,undefined
[11] 75015 Paris,undefined
[12] France,undefined
[13] Laboratoire d'Immunogénétique Humaine,undefined
[14] Institut Pasteur,undefined
[15] 25 rue du Dr. Roux,undefined
[16] 75015 Paris,undefined
[17] France,undefined
[18] ATelier de Génomique Cognitive,undefined
[19] CNRS ESA 8071/Génopole®,undefined
[20] 523 Terrasses de l'Agora,undefined
[21] 91000 Evry,undefined
[22] France,undefined
[23] Unité d'Immunophysiologie et Parasitisme Intracellulaire,undefined
[24] Institut Pasteur,undefined
[25] 25 rue du Dr. Roux,undefined
[26] 75015 Paris,undefined
[27] France,undefined
来源
Mammalian Genome | 2003年 / 14卷
关键词
Inbred Mouse; Consensus Motif; Inbred Mouse Strain; Trapping Strategy; Charged Substrate;
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学科分类号
摘要
The P-type ATPases comprise a well-studied family of proteins involved in the active transport of charged substrates across biological membranes. Starting from a mouse bone marrow-derived macrophage cDNA library and using a signal peptide trapping strategy, we identified a new P-type ATPase family member. We characterized the genomic structure of this gene, named Atp10d, as well as its human counterpart. The presence of P-type ATPase consensus motifs and phylogenetic analysis showed that this gene is a member of the type IV, putative amphipath transporters subfamily. We showed that this gene is expressed in kidney and placenta. We also found that the C57BL/6 strain carries a constitutive stop codon in the sequence of Atp10d exon 12, whereas 14 other inbred mouse strains show an uninterrupted reading frame at this location. This mutation in C57BL/6 should lead to a non-functional protein, suggesting that this gene may not be essential. We discuss the involvement of the Atp10d gene in the fat-prone phenotype of the C57BL/6 strain and its physical mapping within a QTL associated with HDL-cholesterol levels.
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页码:21 / 30
页数:9
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