Dithiothreitol-based protein equalisation in the context of multiple myeloma: Enhancing proteomic analysis and therapeutic insights

Ines F. Domingos, Luis B. Carvalho, Carlos Lodeiro, Rita Gerivaz, Gali Prag, Emanuele Micaglio, Eli Muchtar, Hugo M. Santos*, Jose L. Capelo*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract

In this study, we employed the dithiothreitol-based protein equalisation technique and analytical proteomics to better understand myeloma diseases by comparing the proteomes of pellets and supernatants formed upon application of DTT on serum samples. The number of unique proteins found in pellets was 252 for healthy individuals and 223 for multiple myeloma patients. The comparison of these proteomes showed 97 dysregulated proteins. The unique proteins found for supernatants were 264 for healthy individuals and 235 for multiple myeloma patients. The comparison of these proteomes showed 87 dysregulated proteins. The analytical proteomic comparison of both groups of dysregulated proteins is translated into parallel dysregulated pathways, including chaperone-mediated autophagy and protein folding, addressing potential therapeutic interventions. Future research endeavours in personalised medicine should prioritize refining analytical proteomic methodologies using serum dithiothreitol-based protein equalisation to explore innovative therapeutic strategies. We highlight the advanced insights gained from this analytical strategy in studying multiple myeloma, emphasising its complex nature and the critical role of personalised, targeted analytical techniques in enhancing therapeutic efficacy in personalised medicine.

Original languageEnglish
Article number126589
JournalTalanta
Volume279
DOIs
StatePublished - 1 Nov 2024

Keywords

  • Amyloidosis
  • Analytical proteomics
  • DTT equalisation
  • Haematological malignancy
  • Multiple myeloma
  • Neurotoxicity
  • Proteomic profiling
  • Proteostasis modulation

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