AI Article Synopsis

  • Peptides and proteins can adopt various complex structures, which can lead to harmful forms like aggregates and fibrils that affect drug development and disease.
  • Liraglutide, a drug for diabetes, forms oligomers that can be stabilized by factors like pH and solvents, and these oligomers can influence the drug's stability and effectiveness.
  • Our research highlights how Liraglutide's "oligomer memory effect" from its synthesis process is crucial for understanding its behavior, which has implications for the entire drug development process.

Article Abstract

Peptides and proteins commonly have complex structural landscapes allowing for transformation into a wide array of species including oligomers, aggregates, and fibrils. The formation of undesirable forms including aggregates and fibrils poses serious risks from the perspective of drug development and disease. Liraglutide, a GLP-1 agonist for the treatment of diabetes, is a conjugated peptide that forms oligomers that can be stabilized by pH and organic solvents. We have developed an analytical toolkit to overcome challenges inherent to Liraglutide's conjugated acyl chain and probed the impact its oligomers have on its physical stability. Our studies show that Liraglutide's oligomer states have significant and potentially detrimental impacts on its propensity to aggregate and form fibrils as well as its potency. Liraglutide delivered as a synthetic peptide is able to maintain its oligomerization state in dried lyophilized powders, acting as a memory effect from its synthetic process and purification. Through Liraglutide's oligomer memory effect, we demonstrate the importance and impact the process for synthetic peptides can have on drug development spanning from discovery to formulation development.

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Source
http://dx.doi.org/10.1021/acs.molpharmaceut.9b00106DOI Listing

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