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Projects / Programmes
Understanding the mechanisms and prevention of aggregation of biopharmaceutic proteins
Research activity
| Code | Science | Field | Subfield |
|---|---|---|---|
| 4.06.00 | Biotechnical sciences | Biotechnology |
| Code | Science | Field |
|---|---|---|
| 2.09 | Engineering and Technology | Industrial biotechnology |
Keywords
biopharmaceutic proteins, monoclonal antibodies, high-throughput screening, peptide library, protein formulation, protein aggregation and self-association, protein stability and solubility, nuclear magnetic resonance, biomolecular simulations, dynamic light scattering
Evaluation
(metodology)
Points
7,714.86
A''
2,185.89
A'
5,623.76
A1/2
6,508.71
CI10
18,764
CImax
3,292
h10
49
A1
27.94
A3
5.32
Data for the last 5 years (citations for the last 10 years) on
October 15, 2025;
Data for score A3 calculation refer to period
2020-2024
Data for ARIS tenders (
04.04.2019 – Programme tender,
archive
)
Citations
Citations for bibliographic records in COBIB.SI that are linked to records in citation databases
| Database | Linked records | Citations | Pure citations | Average pure citations |
|---|---|---|---|---|
| WoS | 314 | 16,982 | 15,956 | 50.82 |
| Scopus | 308 | 18,504 | 17,434 | 56.6 |
Organisations (1) , Researchers (17)
0794 University of Maribor, Faculty of Chemistry and Chemical Engineering
| no. | Code | Name and surname | Research area | Role | Period | No. of publicationsNo. of publications |
|---|---|---|---|---|---|---|
| 1. | 25434 | Chemistry | Researcher | 2023 - 2025 | 411 | |
| 2. | 53575 | Chemistry | Young researcher | 2023 | 8 | |
| 3. | 50420 | Chemistry | Researcher | 2023 | 44 | |
| 4. | 57143 | Chemistry | Researcher | 2023 - 2025 | 14 | |
| 5. | 50635 | Chemistry | Researcher | 2023 - 2025 | 43 | |
| 6. | 34351 | Chemistry | Researcher | 2023 | 74 | |
| 7. | 32587 | Pharmacy | Researcher | 2023 - 2025 | 193 | |
| 8. | 38261 | Pharmacy | Researcher | 2023 | 34 | |
| 9. | 25435 | Computer intensive methods and applications | Researcher | 2023 - 2025 | 241 | |
| 10. | 55088 | Biotechnology | Researcher | 2023 | 15 | |
| 11. | 37452 | Pharmacy | Researcher | 2023 - 2025 | 64 | |
| 12. | 30953 | Microbiology and immunology | Researcher | 2023 | 57 | |
| 13. | 55902 | Chemistry | Young researcher | 2023 - 2025 | 20 | |
| 14. | 55319 | Chemistry | Researcher | 2023 - 2025 | 12 | |
| 15. | 52708 | Chemistry | Researcher | 2023 | 21 | |
| 16. | 52709 | Chemistry | Researcher | 2023 | 60 | |
| 17. | 56212 | Biotechnology | Head | 2023 - 2025 | 57 |
Abstract
Biopharmaceutic proteins, especially monoclonal antibodies, are the fastest growing class of pharmaceutics globally, due to their high affinity, specificity and non-toxicity. Despite their versatility and wide applicability, their production is costly and poses unique challenges due to their high molecular weight and structural complexity as well as from instabilities like aggregation that lead to loss of quality and efficacy, limit their shelf life and can induce life-threatening immunogenic response. Protein aggregation is thus considered one of the major challenges in biopharmaceutic protein formulation with various strategies being employed to characterise protein aggregation and prevent it.
Protein aggregation occurs through association of aggregation prone regions (APR) which can be located on protein surface or that get exposed upon partial unfolding of the proteins. These regions are experimentally difficult to detect and isolate due to their transient nature therefore high-resolution structural insight into APR composition remains elusive. Motivated by recent advances showing that these APRs can be detected by peptide array screening and that results of such screening correlate with aggregation propensity of proteins, we propose to develop a peptide library that will be used for a high-throughput nuclear magnetic resonance (NMR) screening that will provide structural insight into aggregation prone regions of native as well as partially unfolded protein species. NMR screening will be complemented with biomolecular simulations and traditional biophysical methods for characterisation of protein aggregation. We will also assess how small molecule excipients that bind to APRs influence the protein-protein interactions and mitigate protein aggregation.
This project will contribute to understanding of molecular basis of protein self-association and aggregation which is crucial for rational design of more stable biopharmaceutic proteins in the future, that will reduce waste and significantly lower their production cost making them more accessible to all patients.