Impaired synthesis of retinol-binding protein and transthyretin in rat liver with bile duct obstruction |
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Authors: | Toru Imamine MD PhD Masataka Okuno MD PhD Hisataka Moriwaki MD PhD Yoshihiro Shidoji PhD Dr. Yasutoshi Muto MD PhD Mitsuru Seishima MD PhD Akio Noma MD PhD Soichi Kojima PhD |
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Affiliation: | (1) From the First Department of Internal Medicine, and Department of Laboratory Medicine, Gifu University School of Medicine, 40 Tsukasa-machi, 500 Gifu, Japan;(2) Laboratory of Gene Technology and Safety, Tsukuba Life Science Center, The Institute of Physical and Chemical Research (RIKEN), Koyadai, Tsukuba, 305 Ibaraki, Japan |
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Abstract: | To gain further insight into the protein metabolism in bile duct-obstruction, we examined the synthesis of retinol-binding protein (RBP) and transthyretin (TTR) in rats with common bile duct-ligation. In these rats, liver and plasma levels of RBP and TTR decreased markedly, whereas liver retinoid contents remained unchanged. Although there appeared no decrease in the total amount of RBP or TTR mRNA expressed in the liver, the subcellular distribution of these mRNAs changed from the membrane-bound polysome fraction to the membrane-unbound polysome fraction. This abnormal distribution recovered rapidly after biliary drainage, resulting in the subsequent recovery of the plasma RBP and TTR levels. These observations suggest that cholestasis inhibits the synthesis and secretion of RBP and TTR by disrupting the binding of their mRNAs to membrane-bound polysomes. Plasma levels of RBP and TTR might be sensitive indicators of the recovery of protein synthesis after biliary drainage in patients with obstructive biliary disorders.Supported in part by Grant-in-Aids from the Ministry of Education, Science and Culture (05770350 to M.O.; 05670463 to H.M.; 07780553 to S.K.) and by a grant from the Ryoichi Naito Foundation for medical research (to S.K.). |
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Keywords: | cholestasis retinol-binding protein transthyretin mRNA polysome protein synthesis |
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