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Salinosporamides A and B inhibit proteasome activity and delay the degradation of N-end rule model substrates

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Authors

Shin, Seung Kyun; Bang, Dae In; Choi, Won Hoon; Kim, Seong-Hwan; Oh, Dong-Chan; Lee, Min Jae

Issue Date
2013-05
Publisher
대한화학회
Citation
Bulletin of the Korean Chemical Society, Vol.34 No.5, pp.1425-1428
Abstract
The proteasome, which is highly evolutionarily conserved, is responsible for the degradation of most short-lived proteins in cells. Small-molecule inhibitors targeting the proteasome's degradative activity have been extensively developed as lead compounds for various human diseases. An exemplified molecule is bortezomib, which was approved by FDA in 2003 for the treatment of multiple myeloma. Here, using transiently and stably expressed N-end rule model substrates in mammalian cells, we evaluated and identified that salinosporamide A and salinosporamide B effectively inhibited the proteasomal degradation. Considering that a variety of proteasome substrates are implicated in the pathogenesis of many diseases, they have the potential to be clinically applicable as therapeutic agents.
ISSN
0253-2964
URI
https://hdl.handle.net/10371/207659
DOI
https://doi.org/10.5012/bkcs.2013.34.5.1425
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  • College of Pharmacy
  • Department of Manufacturing Pharmacy
Research Area Chemical biology of natural products, Drug discovery from microbial natural products, Study of insect-microbial symbiosis, 미생물 유래 생리활성 천연물 발굴, 천연물 구조 분석

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