A distal effect of microsomal triglyceride transfer protein deficiency on the lysosomal recycling of CD1d

Sagiv, Yuval; Bai, Li; Wei, Datsen G.; Agami, Reuven; Savage, Paul B.; Teyton, Luc; Bendelac, Albert

doi:10.1083/jcb1771oia1

Cited by 9 publications

(12 citation statements)

References 10 publications

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“…It is conceivable that secCD1d assembles and leaves the ER in a predominantly lipid-free form, but that the ER-retained version accumulates PC during the prolonged period it spends recycling between the ER and cis -Golgi: the half-life of sec CD1d is > 20 hours ((17), data not shown). There are no data to indicate how efficiently MTP catalyzes lipid loading in the ER, and in fact one view is that it catalyzes the binding of the antigenic lipid α-galactosylceramide in the endocytic pathway and not in the ER (32), which is entirely consistent with empty CD1d molecules being assembled and secreted. Alternatively, PC binding in the ER may be efficient but lipid exchange factors present in the secretory pathway after the cis -Golgi preferentially exchange sphingomyelin for PC.…”

Section: Discussionmentioning

confidence: 99%

Natural Lipid Ligands Associated with Human CD1d Targeted to Different Subcellular Compartments

Yuan

Kang

Evans

et al. 2009

The Journal of Immunology

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*CD1d is an MHC class I-like membrane glycoprotein that presents lipid Ags to NKT cells. Despite intensive biochemical, genetic, and structural studies, the endogenous lipids associated with CD1d remain poorly defined because of the biochemical challenges posed by their hydrophobic nature. In this study, we report the generation of a protease-cleavable CD1d variant with a similar trafficking pattern to wild-type CD1d that can be purified in the absence of detergent and allows the characterization of the naturally associated lipids. In addition, we used soluble variants of CD1d that are secreted or retained in the endoplasmic reticulum (ER) to survey their acquired lipids. By using multiple mass spectrometry methods, we found that CD1d retained in the ER is predominantly loaded with the most abundant phospholipid in the cell, phosphatidyl choline, while the protease cleavable version of CD1d contains bound sphingomyelin and lysophospholipids in addition to phosphatidyl choline. The secreted soluble version of CD1d, in contrast, lacks detectable phosphatidyl choline and the only detectable associated lipid is sphingomyelin. The data suggest that, in the absence of infection or stress, CD1d molecules survey the ER, the secretory pathway, and the endocytic pathway, and accumulate the most abundantly available lipids present in these compartments.

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Section: Discussionmentioning

confidence: 99%

Natural Lipid Ligands Associated with Human CD1d Targeted to Different Subcellular Compartments

Yuan

Kang

Evans

et al. 2009

The Journal of Immunology

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“…Furthermore, the mechanisms by which glycolipids are extracted from membranes and loaded onto CD1d molecules remain to be fully understood. Although recent papers have described the role of lipid transfer proteins, such as saposin [74], microsomal lipid transfer protein [70,75] and CD1e [76], the fine details of the mechanisms that control lipid loading and presentation are still obscure.…”

Section: Box 1 Open Questionsmentioning

confidence: 98%

“…By replacing the gene encoding CXCR6 with GFP cDNA, it has been possible to visualize liver iNKT cells and to assess their role in immunosurveillance [68]. Lastly, the use of fluorescently labelled glycolipids is proving to be a useful tool in the tracking of CD1d molecules throughout the endosomal compartments of the cell [69,70].…”

Section: Future Perspectivesmentioning

confidence: 98%

A closer look at CD1d molecules: new horizons in studying NKT cells

Stronge

Salio

Jones

et al. 2007

Trends in Immunology

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“…MTP affects CD1 molecules probably by facilitating their stabilisation with endogenous lipids. The absence of MTP might cause generation of unstable CD1 molecules more susceptible to lysosomal degradation and with reduced recycling capacity, thus explaining the observed effects on CD1d recycling from lysosomes to plasma membrane [69].…”

Section: Box 2 Mtp and Lipid Antigen Presentationmentioning

confidence: 98%