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タイトル: pSNAP: Proteome-wide analysis of elongating nascent polypeptide chains
著者: Uchiyama, Junki
Roy, Rohini
Wang, Dan Ohtan
Morikawa, Kazuya
Kawahara, Yuka
Iwasaki, Mio  kyouindb  KAKEN_id  orcid https://orcid.org/0000-0003-2085-732X (unconfirmed)
Yoshino, Chiaki
Mishima, Yuichiro
Ishihama, Yasushi
Imami, Koshi
著者名の別形: 内山, 純貴
王, 丹
森川, 和哉
川原, 優香
岩崎, 未央
吉野, 千明
石濱, 泰
今見, 考志
キーワード: biological sciences
biochemistry
biochemistry methods
cell biology
methodology in biological sciences
発行日: 15-Jul-2022
出版者: Elsevier BV
誌名: iScience
巻: 25
号: 7
論文番号: 104516
抄録: Cellular global translation is often measured using ribosome profiling or quantitative mass spectrometry, but these methods do not provide direct information at the level of elongating nascent polypeptide chains (NPCs) and associated co-translational events. Here, we describe pSNAP, a method for proteome-wide profiling of NPCs by affinity enrichment of puromycin- and stable isotope-labeled polypeptides. pSNAP does not require ribosome purification and/or chemical labeling, and captures bona fide NPCs that characteristically exhibit protein N-terminus-biased positions. We applied pSNAP to evaluate the effect of silmitasertib, a potential molecular therapy for cancer, and revealed acute translational repression through casein kinase II and mTOR pathways. We also characterized modifications on NPCs and demonstrated that the combination of different types of modifications, such as acetylation and phosphorylation in the N-terminal region of histone H1.5, can modulate interactions with ribosome-associated factors. Thus, pSNAP provides a framework for dissecting co-translational regulations on a proteome-wide scale.
著作権等: © 2022 The Author(s).
This is an open access article under the CC BY-NC-ND license.
URI: http://hdl.handle.net/2433/283250
DOI(出版社版): 10.1016/j.isci.2022.104516
PubMed ID: 35754732
出現コレクション:学術雑誌掲載論文等

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