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- W2600306912 abstract "Sphingomyelin (SM) has been proposed to form cholesterol-dependent raft domains and sphingolipid domains in the plasma membrane (PM). How SM contributes to the formation and function of these domains remains unknown, primarily because of the scarcity of suitable fluorescent SM analogs. We developed new fluorescent SM analogs by conjugating a hydrophilic fluorophore to the SM choline headgroup without eliminating its positive charge, via a hydrophilic nonaethylene glycol linker. The new analogs behaved similarly to the native SM in terms of their partitioning behaviors in artificial liquid order-disorder phase-separated membranes and detergent-resistant PM preparations. Single fluorescent molecule tracking in the live-cell PM revealed that they indirectly interact with each other in cholesterol- and sphingosine backbone–dependent manners, and that, for ∼10–50 ms, they undergo transient colocalization-codiffusion with a glycosylphosphatidylinositol (GPI)-anchored protein, CD59 (in monomers, transient-dimer rafts, and clusters), in CD59-oligomer size–, cholesterol-, and GPI anchoring–dependent manners. These results suggest that SM continually and rapidly exchanges between CD59-associated raft domains and the bulk PM." @default.
- W2600306912 created "2017-04-07" @default.
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- W2600306912 date "2017-03-22" @default.
- W2600306912 modified "2023-10-18" @default.
- W2600306912 title "Raft-based sphingomyelin interactions revealed by new fluorescent sphingomyelin analogs" @default.
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- W2600306912 doi "https://doi.org/10.1083/jcb.201607086" @default.
- W2600306912 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5379944" @default.
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