In mammalian cells, adaptation to hypertonic conditions leads to the activation of an array of early (cell shrinkage, regulatory volume increase) and late (accumulation of compatible osmolytes) responses and increased level of HSPs (heat shock proteins). Protein synthesis is strongly inhibited few minutes after the hypertonic challenge as demonstrated in whole cells and as reproduced under controlled conditions in cell-free systems. Different mechanisms known to mediate the accumulation of HSP70, such as mRNA transcription and stabilization, require fully active protein synthesis. We show that the 5'-untranslated region of HSP70 messenger drives a hypertonicity-resistant translation (up to 0.425 osmol/kg of water), whereas cap-dependent protein synthesis is almost totally blocked under the same conditions. The results, obtained in cell-free systems and in whole cells, might help to explain why HSP70 is accumulated in cells when total protein synthesis is impaired. We also observed that translation initiated by viral IRES (from Cricket paralysis virus) is highly efficient in cells exposed to hyperosmolarity, suggesting that the resistance to hypertonic conditions is a more general feature of cap-independent translation. The described mechanism may also play a role in the control of translation of other messengers encoding for proteins involved in the adaptation to hypertonicity. (C) 2012 Elsevier Inc. All rights reserved.
机构:
Nagoya Univ, Ctr Gene Res, Chikusa Ku, Nagoya, Aichi 4648602, Japan
Leica Microsyst KK, Minato Ku, Shirokane Takanawa Stn Bldg,1-27-6 Shirokane, Tokyo 1080072, JapanNagoya Univ, Ctr Gene Res, Chikusa Ku, Nagoya, Aichi 4648602, Japan
Hayashi, Rie
Sugita, Chieko
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Nagoya Univ, Ctr Gene Res, Chikusa Ku, Nagoya, Aichi 4648602, JapanNagoya Univ, Ctr Gene Res, Chikusa Ku, Nagoya, Aichi 4648602, Japan
Sugita, Chieko
Sugita, Mamoru
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Nagoya Univ, Ctr Gene Res, Chikusa Ku, Nagoya, Aichi 4648602, JapanNagoya Univ, Ctr Gene Res, Chikusa Ku, Nagoya, Aichi 4648602, Japan
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UFRJ, IBCCF, BR-21949900 Rio De Janeiro, BrazilUFRJ, IBCCF, BR-21949900 Rio De Janeiro, Brazil
Rodrigues, Deivid C.
Silva, Rosane
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UFRJ, IBCCF, BR-21949900 Rio De Janeiro, BrazilUFRJ, IBCCF, BR-21949900 Rio De Janeiro, Brazil
Silva, Rosane
Rondinelli, Edson
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UFRJ, IBCCF, BR-21949900 Rio De Janeiro, Brazil
UFRJ, Dept Clin Med, Fac Med, BR-21949900 Rio De Janeiro, BrazilUFRJ, IBCCF, BR-21949900 Rio De Janeiro, Brazil
Rondinelli, Edson
Urmenyi, Turan P.
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UFRJ, IBCCF, BR-21949900 Rio De Janeiro, BrazilUFRJ, IBCCF, BR-21949900 Rio De Janeiro, Brazil