Proteasomes Are Involved in the Constitutive Degradation of Growth Hormone Receptors
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概要
- 論文の詳細を見る
In the mouse Ba/F3-hGHR cell line, which stably expresses human growth hormone receptors(hGHRs), the hGHRs were rapidly degraded in the absence of the ligand. Human growth hormone-binding protein(hGH-BP), a soluble form of hGHR, was released from Ba/F3-hGHR cells, but the hGH-BP release was less than 1% of total hGHRs in the cells. Therefore, the hGH-BP release does not markedly contribute to hGHR degradation in Ba/F3-hGHR cells. The constitutive degradation of hGHRs was inhibited by the proteasome inhibitors MG-132 and clasto-lactacystin β-lactone, or the vacuolar H^+-ATPase inhibitor, bafilomycin A_1.hGH-enhanced degradation of hGHRs was also inhibited by MG-132. Moreover, MG-132 inhibited the internalization of hGHRs as assessed by ^<125>I-hGH binding to the cell surfaces. Ubiquitinated hGHRs were detected in the cell lysate and increased by hGH-treatment. Furthermore, MG-132 accumulated the ubiquitinated hGHRs induced by hGH. However, the ratio of ubiquitinated hGHRs to unubiquitinated hGHRs was very small, even with treatment involving both hGH and MG-132. In the hGH-untreated cells, the ubiquitinated hGHRs were weakly detected. However, the ubiquitination of hGHR was not enhanced by MG-132 as a result of immunoblotting. Thus, the ubiquitination of hGHR is unlikely to be involved, at least in the constitutive degradation. Taken together, both the proteasome pathway and endosome/lysosome pathway are involved in the constitutive degradation of hGHRs. Our results also suggest that ubiquitination of the hGHR itself is unlikely to be the trigger of the proteasome-dependent degradation.
- 社団法人日本薬学会の論文
- 2001-07-01
著者
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Takagi Kayoko
Division of Biochemistry and Immunochemistry, National Institute of Health Sciences
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Takagi Kayoko
Division Of Biochemistry And Immunochemistry National Institute Of Health Sciences (nihs)
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Takagi Kayoko
国立医薬品食品衛生研究所 機能生化学部
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Takagi Kayoko
Division Of Biochemistry And Immunochemistry National Institute Of Health Sciences
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Yoshida Shigeaki
国立がんセンター東病院 消化管内科
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Sawada Jun-ichi
Division Of Functional Biochemistry And Genomics National Institute Of Health Sciences
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Saito Yoshiro
Division Of Gastrointestinal Oncology National Cancer Center Hospital
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Saito Yoshiro
Division Of Biochemistry And Immunochemistry National Institute Of Health Science
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Sawada Jun-ichi
Division Of Biochemistry And Immunochemistry Natinal Institute Of Health Sciences
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Saito Yoshiro
Division Of Biochemistry And Immunochemistry National Institute Of Health Sciences
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Sawada J
Mie Univ. School Of Medicine Mie Jpn
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Takagi K
National Inst. Of Health Sci. Tokyo Jpn
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Saito Y
Division Of Biochemistry And Immunochemistry National Institute Of Health Sciences
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