Apratoxin A Reversibly Inhibits the Secretory Pathway by Preventing Cotranslational Translocation

Liu, Yanxia; Law, Brian K.; Luesch, Hendrik

doi:10.1124/mol.109.056085

Cited by 132 publications

(114 citation statements)

References 42 publications

Supporting

Mentioning

105

Contrasting

Order By: Relevance

“…The Sec61 complex is also responsible for export of mis-folded proteins from the ER lumen to the cytosol for further degradation (27). It has been demonstrated previously that apratoxin A can block cotranslational translocation (9). Downregulation of several membrane-associated receptors, such as gp130, c-MET, HER-2, PDGFR-b, and IGF1R-b, was also reported following apratoxin A exposure.…”

Section: Discussionmentioning

confidence: 91%

“…It has also been suggested that apratoxin A can stabilize Hsc70/Hsp70 interaction with Hsp90 client proteins to prevent their binding to Hsp90; such stabilization results in degradation of EGFR and ErbB2 through chaperone-mediated autophagy (8). In a cell-free in vitro system, apratoxin A was also shown to inhibit the secretory pathway by preventing cotranslational translocation of newly synthesized proteins (9).…”

Section: Introductionmentioning

confidence: 97%

See 1 more Smart Citation

Apratoxin A Shows Novel Pancreas-Targeting Activity through the Binding of Sec 61

Huang

Chen

Jiang

et al. 2016

Molecular Cancer Therapeutics

View full text Add to dashboard Cite

Apratoxin A is a natural product with potent antiproliferative activity against many human cancer cell lines. However, we and other investigators observed that it has a narrow therapeutic window in vivo. Previous mechanistic studies have suggested its involvement in the secretory pathway as well as the process of chaperone-mediated autophagy. Still the link between the biologic activities of apratoxin A and its in vivo toxicity has remained largely unknown. A better understanding of this relationship is critically important for any further development of apratoxin A as an anticancer drug. Here, we describe a detailed pathologic analysis that revealed a specific pancreas-targeting activity of apratoxin A, such that severe pancreatic atrophy was observed in apratoxin A-treated animals. Follow-up tissue distribution studies further uncovered a unique drug distribution profile for apratoxin A, showing high drug exposure in pancreas and salivary gland. It has been shown previously that apratoxin A inhibits the protein secretory pathway by preventing cotranslational translocation. However, the molecule targeted by apratoxin A in this pathway has not been well defined. By using a 3 H-labeled apratoxin A probe and specific Sec 61a/b antibodies, we identified that the Sec 61 complex is the molecular target of apratoxin A. We conclude that apratoxin A in vivo toxicity is likely caused by pancreas atrophy due to high apratoxin A exposure.

show abstract

Section: Discussionmentioning

confidence: 91%

Section: Introductionmentioning

confidence: 97%

Apratoxin A Shows Novel Pancreas-Targeting Activity through the Binding of Sec 61

Huang

Chen

Jiang

et al. 2016

Molecular Cancer Therapeutics

View full text Add to dashboard Cite

show abstract

“…Most of these inhibitors interfere with a specific step in the translocation process and thus affect a wide spectrum of translocon substrates, often associated with cellular toxicity (35,36). The fungal cyclic heptadepsipeptide HUN-7293 was originally identified as an inhibitor of vascular cell adhesion molecule 1 (VCAM-1) expression in endothelial cells (37,38).…”

Section: Discussionmentioning

confidence: 99%

A Proteomic Survey Indicates Sortilin as a Secondary Substrate of the ER Translocation Inhibitor Cyclotriazadisulfonamide (CADA)

Puyenbroeck

Claeys

Schols

et al. 2017

Molecular & Cellular Proteomics

View full text Add to dashboard Cite

The small molecule CADA was shown to down-modulate the expression of human CD4 in a signal peptide-dependent way through inhibition of its cotranslational translocation across the ER membrane. Previous studies characterizing general glycoprotein levels and the expression of 14 different cell surface receptors showed selectivity of CADA for human CD4. Here, a PowerBlot Western Array was used as a screen to analyze the proteome of CADAtreated SUP-T1 human CD4؉ T lymphocytes. This highthroughput monoclonal antibody panel-based immunoblotting assay of cellular signaling proteins revealed that only a small subset of the 444 detected proteins was differentially expressed after treatment with CADA. Validation of these proteomic data with optimized immunoblot analysis confirmed the CADA-induced change in expression of the cell cycle progression regulator pRb2 and the transcription factor c-Jun. However, the up-regulation of pRb2 or down-modulation of c-Jun by CADA had no impact on cell cycle transition. Also, the reduced protein level of human CD4 did not inhibit T cell receptor signaling. Interestingly, the signal peptide-containing membrane protein sortilin was identified as a new substrate for CADA. Both cellular expression and in vitro cotranslational translocation of sortilin were significantly reduced by CADA, although to a lesser extent as compared with human CD4. Our data demonstrate that a small signal peptide-binding drug is able to down-modulate the expression of human CD4 and sortilin, apparently with low impact on the cellular proteome. Molecular & Cellular

show abstract

“…Furthermore, the accumulation of cytosolic proteins that would result from an inhibition of ER translocation might also contribute to the cytotoxicity of ES I and its potential anticancer properties (Rane et al, 2008;Wang et al, 2009). The inhibition of ER translocation by the cyclodepsipeptide apratoxinA has also been linked to an anticancer effect, in this case by preventing the biosynthesis of cancer-associated receptor tyrosine kinases (Liu et al, 2009). Thus, modulation of protein homeostasis by targeting fundamental cellular components such as the Sec61 complex appears to be a valid target for therapeutic intervention.…”

Section: Discussionmentioning

confidence: 99%

Eeyarestatin I inhibits Sec61-mediated protein translocation at the endoplasmic reticulum

Cross

McKibbin

Callan

et al. 2009

Journal of Cell Science

143

View full text Add to dashboard Cite

show abstract

Apratoxin A Reversibly Inhibits the Secretory Pathway by Preventing Cotranslational Translocation

Cited by 132 publications

References 42 publications

Apratoxin A Shows Novel Pancreas-Targeting Activity through the Binding of Sec 61

Apratoxin A Shows Novel Pancreas-Targeting Activity through the Binding of Sec 61

A Proteomic Survey Indicates Sortilin as a Secondary Substrate of the ER Translocation Inhibitor Cyclotriazadisulfonamide (CADA)

Eeyarestatin I inhibits Sec61-mediated protein translocation at the endoplasmic reticulum

Contact Info

Product

Resources

About