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1 earoyl-2-oleoyl- and sn-1-palmitoyl-2-oleoyl phosphoglycerides.
2 f comparable docosahexaenoic acid-containing phosphoglycerides.
3 sed from 0 to 10 mol % of the total membrane phosphoglycerides.
9 alkenyl chain lowers the molecular area of a phosphoglyceride and, concomitantly, makes it less compr
10 ut bound to membranes that contained anionic phosphoglycerides and could be stabilized by these membr
11 onal regulation of ACD11 and CPTP by anionic phosphoglycerides and found that 1-palmitoyl-2-oleoyl-ph
12 ic and lateral packing properties of related phosphoglycerides and found that: 1), The dipole moment-
13 he molecular packing properties of polyenoic phosphoglycerides and raise important questions about th
15 did bind to vesicles that contained anionic phosphoglycerides, and maximal binding occurred (in the
17 activity of the bound enzyme toward membrane phosphoglycerides, assayed in the presence of albumin, i
18 ahexaenoyl- and sn-1-stearoyl-2-arachidonoyl phosphoglycerides, but the structural significance of th
19 onoyl group increases the molecular areas of phosphoglycerides by 3.8 A(2) (7%) relative to the prese
23 pe 1 diabetes group had lower plasma choline phosphoglyceride DHA (3.7 +/- 0.9%; P < 0.01) than did t
25 s provide the first evidence for a potential phosphoglyceride headgroup-specific regulatory interacti
30 nd time-resolved anisotropy decay induced by phosphoglyceride membranes lacking or containing glycoli
31 P < 0.01) and RBC (type 2: P < 0.05) choline phosphoglycerides of the diabetics than of the control s
32 ess stabilized by the addition of an anionic phosphoglyceride or stearoyl-coenzyme A; and they show s
33 s that contained various mixtures of anionic phosphoglycerides, phosphatidylcholine, phosphatidyletha
34 of homogeneous monolayers of these and other phosphoglyceride species to obtain insights into their p
36 hil membranes consistent with utilization of phosphoglyceride substrate and release of free fatty aci
37 affecting its preference for specific diacyl phosphoglyceride substrates, (b) the activator promoted
38 entration of cellular fatty acids as well as phosphoglycerides, the components of cellular membranes.
39 is transferred from an sn-1-stearoyl-2-acyl phosphoglyceride to coenzyme A, and a relatively non-acy
40 referential transfer of stearoyl groups from phosphoglycerides to sn-2-acyl molecular species of lyso
41 nimals respond to chronic cold by increasing phosphoglyceride unsaturation to restore the fluidity of
42 control subjects, and cord RBC ethanolamine phosphoglycerides were lower in DHA (P < 0.05) in both d
43 d cholesterol provided evidence that anionic phosphoglycerides were positive effectors of binding, ph
45 lipid bilayers allowed us to determine that phosphoglycerides with glycerol or inositol on the extra
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