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1 Intralipid also promotes the polarization of macrophages
2 Intralipid and glucosamine infusions decreased insulin-s
3 Intralipid elicited mild inflammation in both perirenal
4 Intralipid enhanced pyruvate dehydrogenase (PDH) phospho
5 Intralipid has been shown to reduce nano-oxaliplatin-med
6 Intralipid increased perirenal fat weight, adipocyte siz
7 Intralipid infusion did not alter the time profiles of p
8 Intralipid infusion reduced insulin-stimulated glucose u
9 Intralipid is a lipid emulsion used for preterm infants,
10 Intralipid/heparin or saline infusion was initiated 2 h
16 mM oleic acid (OA) bound to albumin, 0.5-20% Intralipid, or saline for 3 or 6 h into male C57BL/6J mi
18 levels increased similarly after either 20% Intralipid or 6 mM OA, TG secretion increased only after
21 els were unaffected by either 6 mM OA or 20% Intralipid, but microsomal triglyceride transfer protein
27 examined how endogenous GDF15 responds to an Intralipid infusion in different organs to regulate food
28 ported that a 72-h coinfusion of glucose and Intralipid (GLU+IL) induces insulin resistance and a mar
29 in LPL release after intravenous heparin and Intralipid strongly suggest that GPIHBP1 represents an i
31 eral nutrition containing soybean oil-based (Intralipid) or olive oil-based (ClinOleic) lipid emulsio
33 ing free fatty acid levels in fed animals by Intralipid plus heparin infusion caused significant incr
37 liquid diet plus intravenous lipid emulsion (Intralipid, 4 g fat/kg/d) or intravenous saline for 19 d
38 triphosphate production versus 17+/-16% for Intralipid; P=0.002); however, no change in cardiac func
41 FFAs were increased in seven women by an 8-h Intralipid/heparin (IL/hep) infusion, and the results we
42 subjects to approximately 1 mmol/l by an 8-h Intralipid/heparin (IL/Hep) infusion, whereas they fell
43 sulin clamp period before glucose ingestion, Intralipid/heparin infusion reduced R(d) (4.4 +/- 0.3 vs
44 se 9.3 +/- 0.7 mmol/l) during an intravenous Intralipid/heparin infusion and 7-10 days later during a
45 We investigated the effects of intravenous Intralipid on the adipose tissue development of midgesta
46 stulas during intestinal perfusion of lipid (Intralipid, 170 micromol h(-1), chylous lymph) or a dext
48 te administration of 25 mg ILE/kg body mass (Intralipid(R) 20%) at 1 mL/min using infusion pumps.
49 separate study, short-term (50 and 180 min) Intralipid infusion also failed to increase muscle HBP p
52 sma FFA concentration by coadministration of Intralipid plus heparin to nicotinic acid-treated rats (
53 ocedure with the addition of a coinfusion of Intralipid plus heparin (together with NA) to maintain a
56 which negated the feeding-lowering effect of Intralipid despite a rise in plasma GDF15 levels in chow
57 -fasted rats received a constant infusion of Intralipid or lactate for 5 h, while a control group rec
58 genously via a low- or high-dose infusion of Intralipid plus heparin or endogenously by an infusion o
61 mental conditions, intraduodenal infusion of Intralipid, compared with saline, did not affect plasma
64 Our findings suggest that pre-treatment of Intralipid has the potential to be a powerful agent to e
65 roM C-SNAFL-1 containing 2.0% (by volume) of Intralipid as a scatterer, the values of the average lif
66 underwent cyclic infusions of glucose and/or Intralipid prior to islet isolation and analysis by quan
68 usion of saline, Intralipid, glucosamine, or Intralipid and glucosamine (n = 8 or 9 for each) for 330
69 hicle; Intralipid (30 mL/h) plus vehicle; or Intralipid (30 mL/h) plus eritoran (12 mg i.v. every 12
72 s received an additional infusion of saline, Intralipid, glucosamine, or Intralipid and glucosamine (
76 reast cancer mouse model, we have found that Intralipid pre-treatment significantly increases the amo
83 sover design: saline (30 mL/h) plus vehicle; Intralipid (30 mL/h) plus vehicle; or Intralipid (30 mL/
86 on of free fatty acids during the clamp with Intralipid infusion reduced PAHSAs' effects on EGP in HF
89 A level was impaired in skeletal muscle with Intralipid and lactate infusions, resulting in two- to t
92 uxes could be mimicked by infusing rats with Intralipid or corticosterone and were corrected by lepti