ID | 117617 |
タイトル別表記 | 中央アミノ酸残基はプリオン蛋白質PrPCが病原性アイソフォームに変換するのに重要である
Central residues crucial for prion protein conversion
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著者 |
パシアナ, アグリアニ ディニ
徳島大学大学院医学研究科(医学専攻)
Miyata, Hironori
University of Occupational and Environmental Health
Imamura, Morikazu
University of Miyazaki
Atarashi, Ryuichiro
University of Miyazaki
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キーワード | prion
prion disease
protein misfolding
structure-function
transgenic mice
neurodegenerative disease
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資料タイプ |
学位論文
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抄録 | Conformational conversion of the cellular prion protein, PrPC, into the amyloidogenic isoform, PrPSc, is a key pathogenic event in prion diseases. However, the conversion mechanism remains to be elucidated. Here, we generated Tg(PrPΔ91-106)-8545/Prnp0/0 mice, which overexpress mouse PrP lacking residues 91-106. We showed that none of the mice became sick after intracerebral inoculation with RML, 22L, and FK-1 prion strains nor accumulated PrPScΔ91-106 in their brains except for a small amount of PrPScΔ91-106 detected in one 22L-inoculated mouse. However, they developed disease around 85 days after inoculation with bovine spongiform encephalopathy (BSE) prions with PrPScΔ91-106 in their brains. These results suggest that residues 91-106 are important for PrPC conversion into PrPSc in infection with RML, 22L, and FK-1 prions but not BSE prions. We then narrowed down the residues 91-106 by transducing various PrP deletional mutants into RML- and 22L-infected cells and identified that PrP mutants lacking residues 97-99 failed to convert into PrPSc in these cells. Our in vitro conversion assay also showed that RML, 22L, and FK-1 prions did not convert PrPΔ97-99 into PrPScΔ97-99, but BSE prions did. We further found that PrP mutants with proline residues at positions 97 to 99 or charged residues at positions 97 and 99 completely or almost completely lost their converting activity into PrPSc in RML- and 22L-infected cells. These results suggest that the structurally flexible and noncharged residues 97-99 could be important for PrPC conversion into PrPSc following infection with RML, 22L, and FK-1 prions but not BSE prions.
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掲載誌名 |
Journal of Biological Chemistry
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ISSN | 00219258
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cat書誌ID | AA1202441X
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出版者 | American Society for Biochemistry and Molecular Biology|Elsevier
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巻 | 298
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号 | 9
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開始ページ | 102381
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発行日 | 2022-08-13
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備考 | 内容要旨・審査要旨・論文本文の公開
本論文は,著者Agriani Dini Pasianaの学位論文として提出され,学位審査・授与の対象となっている。 |
権利情報 | This is an open access article under the CCBY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
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出版社版DOI | |
出版社版URL | |
フルテキストファイル | |
言語 |
eng
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著者版フラグ |
博士論文全文を含む
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文科省報告番号 | 甲第3662号
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学位記番号 | 甲医第1544号
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学位授与年月日 | 2022-09-22
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学位名 |
博士(医学)
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学位授与機関 |
徳島大学
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部局 |
先端酵素学研究所
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