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The influence of albumin on vitamin D metabolism in fetal chick osteoblast-like cells
Authors:Valentine A. Lance  William A. Murphy  Javier Sueiras-Diaz  David H. Coy
Affiliation:Department of Medicine, Section of Endocrinology and Metabolism, Tulane University School of Medicine, New Orleans, LA 70112 USA
Abstract:Human pancreatic growth hormone releasing factor (1-29)-amide [hpGRF (1-29)-NH2] and the following analogs: [D-Tyr-1]-hpGRF(1-29)-NH2, [D-Ala-2]-hpGRF(1-29)-NH2, [D-Asp-3]-hpGRF(1-29)-NH2, and [N-Ac-Tyr-1]-hpGRF (1-29)-NH2 were synthesized using solid phase methodology and tested for their ability to stimulate growth hormone (GH) secretion in the rat and the pig in vivo. [D-Ala-2]-hpGRF (1-29)-NH2 was approximately 50 times more potent than the parent molecule in eliciting GH secretion in the rat. The other analogs were less active, but all were more potent than the 1-29 amide in the rat. [D-Tyr-1]-hpGRF(1-29)-NH2 was 10 times more potent, [D-Asp-3]-hpGRF(1-29)-NH2 7 times more potent, and the acetylated molecule approximately 12 times more potent than hpGRF(1-29)-NH2.
Keywords:the amidated forms of human growth hormone releasing factor containing 24 amino acids  the amidated forms of human growth hormone releasing factor containing 29 amino acids  the amidated forms of human growth hormone releasing factor containing 44 amino acids  hpGRF (1–40)-OH  human growth hormone releasing factor with a free carboxy terminal consisting of 40 amino acids  rhGRF  rat hypothalamic growth hormone releasing factor  GH  growth hormone  GIP  gastric inhibitory polypeptide  VIP  vasoactive intestinal peptide  PHI  porcine intestinal peptide having N-terminal histidine and C-terminal isoleucine
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