Abstract
Summary The neonatal Fc receptor (FcRn) participates in intracellular trafficking of IgG and the m aintenance of circulating IgG. The relationship between the FcRn and IgG may also augment host defense immunosurveillance. The current studies evaluated FcRn mRNA from intestinal tissues in fetal pigs and FcRn mRNA in weaned pigs fed meal or pelleted diets with or without irradiated or nonirradiated spray-dried animal plasma. In Exp. 1, fetal pigs were obtained at d 55 and 70 of gestation (n = 5 fetuses/gestational age) and total RNA was isolated f rom intestinal tissues for quantitative real-time PCR (qPCR) to determine mRNA for FcRn. The FcRn transcripts were observed in all samples, and greater levels of FcRn mRNA were observed in d 55 fetuses compared to d 70 fetuses. In Exp. 2, weaned pigs were used in an 11d growth assay to determine the effects of feeding meal and pelleted diets with irradiated or non-irradiated spray-dried animal plasma (AP 920) on FcRn expression in intestinal tissues. Pigs were blocked by weight and randomly allotted in a 2 × 2 factorial to one of four dietary treatm ents. Main effects were diet form (meal or pellet) and either irradiated or non-irradiated spray-dried animal plasma. Jejunal, ileal, and cecal tissues were collected from 24 pigs at the conclusion of the growth assay. Total RNA was isolated to quantify relative mRNA expression of FcRn. The FcRn mRNA transcripts were observed in all tissues. The FcRn mRNA was more abundant (P<0.02) in pigs fed the non-irradiated plasma compared with the pigs fed irradiated plasma. The FcRn mRNA was more abundant (P<0.05) in pigs fed the meal diets compared with the pigs fed pelleted diets. In conclusion, these data suggest that fetal and weanling pig tissues have FcRn mRNA present in the jejun al, ileal, and cecal sections of the small intestine. These data also indicate that FcRn varies with age in pigs. Diet form (meal or pellet) and irradiation of spray-dried animal plasma affects the expression of FcRn in weanling pigs.
Highlights
The classic role of the neonatal Fc receptor (FcRn) is to transport IgG from milk across intestinal epithelial cells in newborns
The current studies evaluated FcRn mRNA from intestinal tissues in fetal pigs and FcRn mRNA in weaned pigs fed meal or pelleted diets with or without irradiated or non-irradiated spraydried animal plasma
In Exp. 1, fetal pigs were obtained at d 55 and 70 of gestation (n = 5 fetuses/ gestational age) and total RNA was isolated from intestinal tissues for quantitative real-time PCR to determine mRNA for FcRn
Summary
The classic role of the neonatal Fc receptor (FcRn) is to transport IgG from milk across intestinal epithelial cells in newborns. Evidence from the human and murine experiments suggests that the relationship between the FcRn and IgG may augment host defense immunosurveillance. FcRn was detected by immunostaining on the apical surface of human fetal small intestine and was found to be distributed among stomach, ileal, and colonic epithelium. The intestinal expression of FcRn has not been evaluated in domestic pigs. The objective of Exp. 1 was to evaluate the presence and relative abundance of FcRn mRNA from intestinal tissue in fetal pigs. Experiment 2 further evaluated the presence and relative abundance of FcRn mRNA in intestinal tissues of weaned pigs fed meal or pelleted diets with or without irradiated or non-irradiated spray-dried animal plasma
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