Ghosal Abhisek, Said Hamid M
Department of Medicine, University of California, Irvine, CA 92697, USA.
Biochim Biophys Acta. 2012 Jan;1818(1):97-102. doi: 10.1016/j.bbamem.2011.10.003. Epub 2011 Oct 12.
The sodium-dependent multivitamin transporter (SMVT) plays an important role in biotin uptake in the intestine and other cell types. While significant knowledge has been gained with regard to regulation and cell biology of the SMVT system, there is little known about its structure-function relationships. Here we examined the role of each of the ten conserved (among species) cysteine residues in the function of the human SMVT (hSMVT) using site-directed mutagenesis. Our results showed a significant impairment in biotin uptake only in cells transfected with hSMVT mutated at Cys(294), but not at the other conserved cysteine residues; the impairment in biotin uptake caused by mutating Cys(294) was not related to the polar status of substituting amino acid. The inhibition in hSMVT function upon mutating Cys(294) was mediated via a significant reduction in the V(max), but not the apparent K(m), of the biotin uptake process, suggesting a decrease in the number (and/or activity) of hSMVT but not affinity. Biotinylation assay confirmed this suggestion by showing a marked reduction in the level of expression of the mutated protein at the cell membrane, without affecting total cellular level of induced hSMVT. These results show an important role for Cys(294) in the function and cell biology of hSMVT.
钠依赖性多种维生素转运体(SMVT)在肠道及其他细胞类型的生物素摄取过程中发挥着重要作用。尽管关于SMVT系统的调节和细胞生物学已经取得了大量认识,但对其结构-功能关系却知之甚少。在此,我们利用定点诱变技术研究了人类SMVT(hSMVT)中十个保守(在物种间)半胱氨酸残基各自在其功能中的作用。我们的结果显示,只有在用在Cys(294)处发生突变的hSMVT转染的细胞中,生物素摄取才出现显著受损,而在其他保守半胱氨酸残基处发生突变的情况下则未出现;由Cys(294)突变导致的生物素摄取受损与取代氨基酸的极性状态无关。Cys(294)突变时hSMVT功能的抑制是通过生物素摄取过程的V(max)显著降低介导的,而非表观K(m),这表明hSMVT的数量(和/或活性)减少而非亲和力降低。生物素化分析通过显示突变蛋白在细胞膜上的表达水平显著降低,而不影响诱导的hSMVT的总细胞水平,证实了这一推测。这些结果表明Cys(294)在hSMVT的功能和细胞生物学中起重要作用。