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GROWTH AND METABOLISM OF GASTROINTESTINAL AND SKELETAL-MUSCLE TISSUES IN PROTEIN-MALNOURISHED NEONATAL PIGS

被引:50
作者
EBNER, S
SCHOKNECHT, P
REEDS, P
BURRIN, D
机构
[1] BAYLOR COLL MED, USDA ARS, CHILDRENS NUTR RES CTR, HOUSTON, TX 77030 USA
[2] BAYLOR COLL MED, DEPT PEDIAT, HOUSTON, TX 77030 USA
[3] INRA, RECH PORCINES STN, F-35590 HERMITAGE, FRANCE
来源
AMERICAN JOURNAL OF PHYSIOLOGY | 1994年 / 266卷 / 06期
关键词
INSULIN; AMINO ACIDS; BLOOD FLOW;
D O I
10.1152/ajpregu.1994.266.6.R1736
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
Our objective was to, determine whether neonates adapt to protein malnutrition by preserving the relative growth and metabolism of gastrointestinal tissue at the expense of skeletal muscle. We measured gastrointestinal, liver, and carcass tissue masses and blood flow, oxygen consumption, and net glucose and amino acid fluxes in vivo of the portal-drained visceral tissues (PDV) in neonatal pigs fed isocaloric diets containing either 30% protein [control (C)] or 15% [low protein (LP)] for 14 days. Relative protein mass and fasting blood flow and oxygen consumption of PDV tissue in either group were not different. Relative protein mass; of liver and carcass was lower in LP pigs. Net essential amino acid absorption; and insulin concentration after feeding were lower in LP pigs. Results demonstrate that protein malnutrition in neonatal pigs differentially altered rates of tissue growth, such that the proportion of body protein partitioned into gastrointestinal tissue was preserved, while that of skeletal muscle was reduced. Chronic reduction in amino acid absorption in protein-malnourished pigs resulted in a reduced insulin response to feeding, which presumably limited substrate availability and the anabolic stimulus for skeletal muscle protein accretion.
引用
收藏
页码:R1736 / R1743
页数:8
相关论文
共 30 条
[21]   EFFECT OF DIETARY PROTEINS ON INSULIN-LIKE GROWTH FACTOR-I (IGF-1) MESSENGER-RIBONUCLEIC-ACID CONTENT IN RAT-LIVER [J].
MIURA, Y ;
KATO, H ;
NOGUCHI, T .
BRITISH JOURNAL OF NUTRITION, 1992, 67 (02) :257-265
[22]   DIETARY-PROTEIN RESTRICTION IN ARTIFICIALLY REARED NEONATAL RATS CAUSES A REDUCTION OF INSULIN-LIKE GROWTH FACTOR-I GENE-EXPRESSION [J].
MOATSSTAATS, BM ;
BRADY, JL ;
UNDERWOOD, LE ;
DERCOLE, AJ .
ENDOCRINOLOGY, 1989, 125 (05) :2368-2374
[23]   EFFECT OF INSULIN ON HINDLIMB AND WHOLE-BODY LEUCINE AND PROTEIN-METABOLISM IN FED AND FASTED LAMBS [J].
ODDY, VH ;
LINDSAY, DB ;
BARKER, PJ ;
NORTHROP, AJ .
BRITISH JOURNAL OF NUTRITION, 1987, 58 (03) :437-452
[24]   THE EFFECTS OF ALTERED NUTRITIONAL-STATUS UPON INSULIN-LIKE GROWTH-FACTORS AND THEIR BINDING-PROTEINS IN NEONATAL RATS [J].
PHILIPPS, A ;
DRAKENBERG, K ;
PERSSON, B ;
SJOGREN, B ;
EKLOF, C ;
HALL, K ;
SARA, V .
PEDIATRIC RESEARCH, 1989, 26 (02) :128-134
[25]   NUTRITION AND SOMATOMEDIN .26. MOLECULAR REGULATION OF IGF-I BY INSULIN IN CULTURED RAT HEPATOCYTES [J].
PHILLIPS, LS ;
GOLDSTEIN, S ;
PAO, CI .
DIABETES, 1991, 40 (11) :1525-1530
[26]   RELATIONSHIP OF SERUM IMMUNOREACTIVE SOMATOMEDIN-C TO DIETARY-PROTEIN AND ENERGY IN GROWING-RATS [J].
PREWITT, TE ;
DERCOLE, AJ ;
SWITZER, BR ;
VANWYK, JJ .
JOURNAL OF NUTRITION, 1982, 112 (01) :144-150
[27]   DIFFERENCES IN INSULIN, GROWTH-HORMONE AND PANCREATIC ENZYME SECRETION AFTER INTRAVENOUS AND INTRADUODENAL ADMINISTRATION OF MIXED AMINO-ACIDS IN MAN [J].
RAPTIS, S ;
DOLLINGER, HC ;
SCHRODER, KE ;
SCHLEYER, M ;
ROTHENBUCHNER, G ;
PFEIFFER, EF .
NEW ENGLAND JOURNAL OF MEDICINE, 1973, 288 (23) :1199-1202
[28]   PROTEIN-SYNTHESIS AND RETENTION IN SOME TISSUES OF THE YOUNG-PIG AS INFLUENCED BY DIETARY-PROTEIN INTAKE AFTER EARLY-WEANING - POSSIBLE CONNECTION TO THE ENERGY-METABOLISM [J].
SEVE, B ;
REEDS, PJ ;
FULLER, MF ;
CADENHEAD, A ;
HAY, SM .
REPRODUCTION NUTRITION DEVELOPMENT, 1986, 26 (03) :849-861
[29]   CHANGES IN SWINE BODY-COMPOSITION FROM BIRTH TO 145 KG [J].
SHIELDS, RG ;
MAHAN, DC ;
GRAHAM, PL .
JOURNAL OF ANIMAL SCIENCE, 1983, 57 (01) :43-54
[30]   PERSISTENT REDUCTION OF PANCREATIC BETA-CELL MASS AFTER A LIMITED PERIOD OF PROTEIN-ENERGY MALNUTRITION IN THE YOUNG-RAT [J].
SWENNE, I ;
BORG, LAH ;
CRACE, CJ ;
LANDSTROM, AS .
DIABETOLOGIA, 1992, 35 (10) :939-945
123