PXD041167 is an
original dataset announced via ProteomeXchange.
Dataset Summary
| Title | Proteasome beta2 and beta5 subunit inhibition by carfilzomib causes acute contractility impairment due to dysbalance of calcium homeostasis |
| Description | Treatment of multiple myeloma (MM) with the second-generation proteasome inhibitor (PI) carfilzomib (CFZ) is associated with higher incidence of cardiovascular adverse events compared to first-generation PI bortezomib (BTZ). CFZ and BTZ inhibit at lower doses only the β5 proteasome subunit, whereas they differ in co-inhibition of other proteasome subunits at the higher doses: BTZ co-inhibits β1 subunit, whereas CFZ co- inhibits β2 subunit. This different pattern of inhibition affects differently the degree of functional proteasome inhibition with β5+β2 showing more effective functional proteasome inhibition. It is unclear, whether CFZ-induced cardiotoxicity is the result of proteasome inhibition, or an off-target effect. With an unbiased multi-omics approach in conjunction with proteasome subunit-specific inhibitors, we show that CFZ-type β5+β2 proteasome subunit inhibition, in contrast to the BTZ-type β5+β1 inhibition, directly interferes with cardiomyocyte contractility in vitro and in vivo. For the in vivo analysis, we used 6-8 weeks old Balb/c mice that were exposed to the drugs for 1h and subsequently euthanized. The hearts were processed for LC/MS-MS analysis. The hearts from CFZ-treated mice for 1h show showed impaired accumulation of proteins related to calcium handling (Atp2a2) and retinoid pathway (Aldh1a1), which is prevented by atRA (1 mg/kg) co-treatment. Our data suggests a novel mechanism for PI-induced cardiotoxicity that reflects clinical findings in which CFZ-type β5+β2 proteasome inhibition, in contrast to β5+β1 co-inhibition of BTZ, directly interferes with the contractile activity of cardiomyocytes. |
| HostingRepository | PRIDE |
| AnnounceDate | 2025-08-12 |
| AnnouncementXML | Submission_2025-08-12_09:53:27.588.xml |
| DigitalObjectIdentifier | |
| ReviewLevel | Peer-reviewed dataset |
| DatasetOrigin | Original dataset |
| RepositorySupport | Unsupported dataset by repository |
| PrimarySubmitter | Lenka Besse |
| SpeciesList | scientific name: Mus musculus (Mouse); NCBI TaxID: 10090; |
| ModificationList | No PTMs are included in the dataset |
| Instrument | Q Exactive |
Dataset History
| Revision | Datetime | Status | ChangeLog Entry |
|---|
| 0 | 2023-03-28 06:48:43 | ID requested | |
| ⏵ 1 | 2025-08-12 09:53:27 | announced | |
Publication List
Keyword List
| submitter keyword: mouse, heart, atRA, carfilzomib, proteasome |
Contact List
| Lenka Besse |
|---|
| contact affiliation | Cantonal Hospital St. Gallen, Switzerland |
| contact email | lenka.besse@kssg.ch |
| lab head | |
| Lenka Besse |
|---|
| contact affiliation | Cantonal Hospital St. Gallen |
| contact email | lenka.besse@kssg.ch |
| dataset submitter | |
Full Dataset Link List
Dataset FTP location
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| PRIDE project URI |
Repository Record List
[ + ]
[ - ]
- PRIDE
- PXD041167
- Label: PRIDE project
- Name: Proteasome beta2 and beta5 subunit inhibition by carfilzomib causes acute contractility impairment due to dysbalance of calcium homeostasis
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