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Extended Abstract

Can Short Peptides Be Inhibitors of Serum Amyloid a Protein Aggregation? †

by
Sandra Skibiszewska
* and
Elzbieta Jankowska
Department of Biomedical Chemistry, Faculty of Chemistry, University of Gdansk, 80-309 Gdansk, Poland
*
Author to whom correspondence should be addressed.
Presented at the 2nd Molecules Medicinal Chemistry Symposium (MMCS): Facing Novel Challenges in Drug Discovery, Barcelona, Spain, 15–17 May 2019.
Proceedings 2019, 22(1), 38; https://doi.org/10.3390/proceedings2019022038
Published: 7 August 2019
One of the approaches in the design of anti-amyloid drugs is to find compounds that are able to hamper self-association of amyloidogenic protein molecules. There is an idea that aggregation inhibitors can be sought in the amyloidogenic sequence itself and prevent protein oligomerization due to shielding the interaction site [1,2]. We have focused our studies on inhibitors of the aggregation of serum amyloid A protein (SAA). SAA is an acute phase protein whose increased production occurs in response to injury, inflammation or infection [3]. Prolonged high concentration of circulating SAA may lead to its aggregation and accumulation of deposits of the protein in the cellular matrix of various organs and finally cause a death of the affected tissues and organs [4]. In our research, we used the 1–5 fragment of SAA as a lead compound to design aggregation inhibitors. We modified the sequence of this fragment by introducing various natural and unnatural aromatic residues. The inhibitory capacity of the saa1-5 analogs was studied using two fragments of the most amyloidogenic N-terminal region of the SAA protein, SAA1-12 and SAA1-27. In order to determine the impact of the inhibitor on the model peptide structure and the type and morphology of aggregates, circular dichroism spectroscopy, quantitative chromatographic analysis of the soluble fraction, and transmission electron microscopy were employed, respectively.

Acknowledgments

This scientific work was financed under the program “Diamond Grant”, as a research project DI2015 022445.

References

  1. Austen, B.M.; Paleologou, K.E.; Ali, S.A.; Qureshi, M.M.; Allsop, D.; El-Agnaf, O.M. Designing peptide inhibitors for oligomerization and toxicity of Alzheimer’s beta-amyloid peptide. Biochemistry 2008, 47, 1984–1992. [Google Scholar] [CrossRef] [PubMed]
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  3. Husby, G.; Marhaug, G.; Dowton, B.; Sletten, K.; Sipe, J.D. Serum amyloid A (SAA): biochemistry, genetics and the pathogenesis of AA amyloidosis. Amyloid Int. J. Exp. Clin. Investig. 1994, 1, 119–137. [Google Scholar] [CrossRef]
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MDPI and ACS Style

Skibiszewska, S.; Jankowska, E. Can Short Peptides Be Inhibitors of Serum Amyloid a Protein Aggregation? Proceedings 2019, 22, 38. https://doi.org/10.3390/proceedings2019022038

AMA Style

Skibiszewska S, Jankowska E. Can Short Peptides Be Inhibitors of Serum Amyloid a Protein Aggregation? Proceedings. 2019; 22(1):38. https://doi.org/10.3390/proceedings2019022038

Chicago/Turabian Style

Skibiszewska, Sandra, and Elzbieta Jankowska. 2019. "Can Short Peptides Be Inhibitors of Serum Amyloid a Protein Aggregation?" Proceedings 22, no. 1: 38. https://doi.org/10.3390/proceedings2019022038

APA Style

Skibiszewska, S., & Jankowska, E. (2019). Can Short Peptides Be Inhibitors of Serum Amyloid a Protein Aggregation? Proceedings, 22(1), 38. https://doi.org/10.3390/proceedings2019022038

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