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1 ssively receiving intra-gastric infusions of fat emulsions.
2 eral, the peptide efficacy was higher in low-fat emulsions.
3 ric feeding and increased oral intake of low-fat emulsions.
4 interactions with phospholipid monolayers of fat emulsions are known to regulate the actions of gastr
7 ton relaxation were studied in water-in-milk fat emulsions during in situ cooling from 40 degrees C t
12 the consumption of the following 4 different fat emulsions: lipid emulsion 1 (LE1; acid stable, 0.33
13 faster than long chain fatty acids from milk fat emulsions; long chain polyunsaturated fatty acids, s
14 rder to receive intra-gastric infusions of a fat emulsion maintained constant hourly caloric intake b
15 e influence of the intragastric stability of fat emulsions on their dynamics of gastric processing an
16 whether intragastric self-administration of fat emulsions, that is, bypassing the oral cavity, recap
17 cifically, on the lipid/aqueous interface of fat emulsions, the anionic portions of amphipathic bile
18 an or equal to 5 days, and did not change IV fat emulsion type during the data collection period.