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Epithelial sphingolipid sorting allows for extensive variation of the fatty acyl chain and the sphingosine backbone

机译:上皮鞘糖脂分选允许脂肪酰基链和鞘氨醇主链的广泛变化

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pIn kidney MDCK and intestinal Caco-2 epithelial cells, glucosylceramide (GlcCer) and sphingomyelin (SPH) synthesized from the short-chain sphingolipid analogue N-6-[7-nitro-2,1,3-benzoxadiazol-4-yl]aminodecanoyl (C6-NBD)-ceramide are delivered to the cell surface with apical/basolateral polarities of 2-4 and 0.6-0.9 respectively. We have tested how variations in the lipid backbone affect these polarities. First, the C6-NBD moiety was replaced by a bare [14C]octanoyl chain or by the even more bulky fluorophores 8-bimanoylthio-octanoyl (C8-bimane) and 8-diethylaminocoumarin-octanoyl (C8-DECA). In addition, the sphingosine in C6-NBD-ceramide was changed in stereoconfiguration (L-threo) or saturation (dihydro). In all cases, GlcCer and SPH were produced and appeared on the cell surface at 37 degrees C, as assayed by back-exchange. The apical/basolateral polarity of the delivery of GlcCer was variable, but always exceeded 1. GlcCer was apically enriched over SPH (2-6 times for MDCK and 3-9 times for Caco-2). Even GlcCer synthesized from a highly water-soluble truncated ceramide (octanoyl-D-erythro-sphingosine analogue with C8 backbone) was enriched apically by a factor of greater than or equal to 2 both in absolute polarity and compared with SPH. Sphingolipid sorting was quantitatively but not qualitatively affected by dramatic changes in the lipid backbone./p
机译:>在肾脏MDCK和肠Caco-2上皮细胞中,由短链鞘脂类似物N-6- [7-硝基-2,1,3-苯并恶二唑-4-]合成的糖基神经酰胺(GlcCer)和鞘磷脂(SPH) y]氨基癸酰基(C6-NBD)-神经酰胺以分别为2-4和0.6-0.9的顶/基侧极性递送到细胞表面。我们已经测试了脂质骨架的变化如何影响这些极性。首先,C6-NBD部分被一条[14C]辛酰基裸链或什至是更大的荧光团8-二manoylthio-octanoyl(C8-bimane)和8-二乙基氨基香豆素-辛酰基(C8-DECA)取代。另外,C6-NBD-神经酰胺中的鞘氨醇改变了立体构型(L-苏氨酸)或饱和度(二氢)。在所有情况下,通过反向交换分析,都产生了GlcCer和SPH,并在37摄氏度下出现在细胞表面。 GlcCer的顶端/基底外侧极性可变,但始终超过1。GlcCer在SPH上顶端富集(MDCK为2-6倍,Caco-2为3-9倍)。甚至由高度水溶性的截短型神经酰胺(具有C8骨架的辛酰基-D-赤型-神经鞘氨醇类似物)合成的GlcCer的绝对极性和与SPH的比值均增加至大于2。鞘脂的分选受脂质主链急剧变化的定量影响,但没有定性影响。

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