Literature DB >> 32631902

Impact of Losing hRpn13 Pru or UCHL5 on Proteasome Clearance of Ubiquitinated Proteins and RA190 Cytotoxicity.

Vasty Osei-Amponsa1, Vinidhra Sridharan1, Mayank Tandon2,3, Christine N Evans4, Kimberly Klarmann5, Kwong Tai Cheng6, Justin Lack3,7, Raj Chari4, Kylie J Walters8.   

Abstract

hRpn13/ADRM1 links substrate recruitment with deubiquitination at the proteasome through its proteasome- and ubiquitin-binding Pru domain and DEUBAD domain, which binds and activates deubiquitinating enzyme (DUB) UCHL5/Uch37. Here, we edit the HCT116 colorectal cancer cell line to delete part of the hRpn13 Pru, producing cells that express truncated hRpn13 (trRpn13), which is competent for UCHL5 binding but defective for proteasome interaction. trRpn13 cells demonstrate reduced levels of proteasome-bound ubiquitinated proteins, indicating that the loss of hRpn13 function at proteasomes cannot be fully compensated for by the two other dedicated substrate receptors (hRpn1 and hRpn10). Previous studies indicated that the loss of full-length hRpn13 causes a corresponding reduction of UCHL5. We find UCHL5 levels unaltered in trRpn13 cells, but hRpn11 is elevated in ΔhRpn13 and trRpn13 cells, perhaps from cell stress. Despite the ∼90 DUBs in human cells, including two others in addition to UCHL5 at the proteasome, we found deletion of UCHL5 from HCT116 cells to cause increased levels of ubiquitinated proteins in whole-cell extract and at proteasomes, suggesting that UCHL5 activity cannot be fully assumed by other DUBs. We also report anticancer molecule RA190, which binds covalently to hRpn13 and UCHL5, to require hRpn13 Pru and not UCHL5 for cytotoxicity.

Entities:  

Keywords:  ADRM1; Adrm1; RA190; Rpn13; UCHL5; Uch37; apoptosis; cell cycle progression; cell viability; proteasome; ubiquitin

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Year:  2020        PMID: 32631902      PMCID: PMC7459265          DOI: 10.1128/MCB.00122-20

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  87 in total

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Authors:  A B Niculescu; X Chen; M Smeets; L Hengst; C Prives; S I Reed
Journal:  Mol Cell Biol       Date:  1998-01       Impact factor: 4.272

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Authors:  Ravi K Anchoori; Rosie Jiang; Shiwen Peng; Ruey-Shyang Soong; Aliyah Algethami; Michelle A Rudek; Nicole Anders; Chien-Fu Hung; Xiang Chen; Xiuxiu Lu; Olumide Kayode; Marzena Dyba; Kylie J Walters; Richard B S Roden
Journal:  ACS Omega       Date:  2018-09-27
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2.  Proteasome-Bound UCH37/UCHL5 Debranches Ubiquitin Chains to Promote Degradation.

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Review 3.  Proteasome interaction with ubiquitinated substrates: from mechanisms to therapies.

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4.  Structure-guided bifunctional molecules hit a DEUBAD-lacking hRpn13 species upregulated in multiple myeloma.

Authors:  Xiuxiu Lu; Venkata R Sabbasani; Vasty Osei-Amponsa; Christine N Evans; Julianna C King; Sergey G Tarasov; Marzena Dyba; Sudipto Das; King C Chan; Charles D Schwieters; Sulbha Choudhari; Caroline Fromont; Yongmei Zhao; Bao Tran; Xiang Chen; Hiroshi Matsuo; Thorkell Andresson; Raj Chari; Rolf E Swenson; Nadya I Tarasova; Kylie J Walters
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5.  Branched ubiquitin chain binding and deubiquitination by UCH37 facilitate proteasome clearance of stress-induced inclusions.

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7.  Sensitivity of Acute Myelocytic Leukemia Cells to the Dienone Compound VLX1570 Is Associated with Inhibition of the Ubiquitin-Proteasome System.

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8.  Chirality and asymmetry increase the potency of candidate ADRM1/RPN13 inhibitors.

Authors:  Ravi K Anchoori; Logan George; Ssu-Hsueh Tseng; Brandon Lam; Srinidhi Polkampally; Anjali D Amiano; Palmer Foran; Hannah Tsingine; Harideep Samanapally; Fernanda Carrizo Velasquez; Samarjit Das; Deyin Xing; Ahmad Bin Salam; Balasubramanyam Karanam; Chien-Fu Hung; Richard B S Roden
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  8 in total

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