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新生小鼠富含板层小体的组分:制备技术及部分特性分析

Lamellar body-enriched fractions from neonatal mice: preparative techniques and partial characterization.

作者信息

Grayson S, Johnson-Winegar A G, Wintroub B U, Isseroff R R, Epstein E H, Elias P M

出版信息

J Invest Dermatol. 1985 Oct;85(4):289-94. doi: 10.1111/1523-1747.ep12276826.

Abstract

Several problems have frustrated the isolation of lamellar bodies (LB) from mammalian epidermis. We obtained pellets enriched in intact LB by utilizing the staphylococcal epidermolytic toxin to provide intact, outer epidermal sheets, by controlled homogenization in a cell disrupter, and by passage of homogenates through a graded series of nuclepore filters (Science 221:962, 1983). Such preparations contained more intact LB than did fractions prepared by a variety of differential or sucrose/metrizamide discontinuous centrifugation methods. Initial characterization of the enzymatic content of this fraction revealed it to be enriched in certain hydrolytic enzymes (acid phosphatase, carboxypeptidase, cathepsin B, acid lipase, sphingomyelinase, and phospholipase A), but strikingly depleted in all sulfatases, beta-glucuronidase, and the non-lysosomal protease, plasminogen activator. Thus, LB show some properties of lysosomes, although certain characteristic lysosomal enzymes are strikingly absent. Lamellar body fractions contained 2-3 times more lipid per unit weight than did homogenates, and were enriched in phospholipids, free sterols, and glycosphingolipids, but not in other neutral lipids or ceramides. In summary, whereas some of the enzymes in LB could participate in the metabolism of LB lipid precursors to hydrophobic barrier constituents, others may attack intercellular constituents, ultimately resulting in desquamation. The lipid profile of these organelles suggests that they deliver precursors of permeability barrier lipids to intercellular domains.

摘要

从哺乳动物表皮中分离板层小体(LB)存在几个问题。我们通过利用葡萄球菌表皮溶解毒素获得完整的表皮外层,在细胞破碎仪中进行可控匀浆,并使匀浆通过一系列分级的核孔滤器,从而得到富含完整LB的沉淀(《科学》221:962,1983)。与通过各种差速离心或蔗糖/甲泛影酰胺不连续离心方法制备的组分相比,此类制剂含有更多完整的LB。对该组分酶含量的初步表征显示,它富含某些水解酶(酸性磷酸酶、羧肽酶、组织蛋白酶B、酸性脂肪酶、鞘磷脂酶和磷脂酶A),但所有硫酸酯酶、β-葡萄糖醛酸酶和非溶酶体蛋白酶纤溶酶原激活剂显著缺乏。因此,LB显示出一些溶酶体的特性,尽管某些典型的溶酶体酶明显缺失。板层小体组分每单位重量的脂质含量比匀浆多2至3倍,并且富含磷脂、游离固醇和糖鞘脂,但其他中性脂质或神经酰胺含量不高。总之,虽然LB中的一些酶可能参与LB脂质前体向疏水屏障成分的代谢,但其他酶可能攻击细胞间成分,最终导致脱屑。这些细胞器的脂质谱表明它们将通透性屏障脂质的前体输送到细胞间区域。

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