(Open access funding provided by Eötvös Loránd University)
(VEKOP-2.3.2-16-2017-00014)
(VEKOP-2.3.3-15-2017-00018)
(2018-1.2.1-NKP-2018-00005) Támogató: NKFIH
(FK 142754)
(RRF-2.3.1-21-2022-00015)
Nemzeti Gyógyszerkutatási és Fejlesztési Laboratórium (PharmaLab)(RRF-2.3.1-21-2022-00015)
Támogató: NKFIH
A large group of hormones are stored as amyloid fibrils in acidic secretion vesicles
before they are released into the bloodstream and readopt their functional state.
Here, we identify an evolutionarily conserved hexapeptide sequence as the major aggregation-prone
region (APR) of gastrointestinal peptides of the glucagon family: xFxxWL. We determine
nine polymorphic crystal structures of the APR segments of glucagon-like peptides
1 and 2, and exendin and its derivatives. We follow amyloid formation by CD, FTIR,
ThT assays, and AFM. We propose that the pH-dependent changes of the protonation states
of glutamate/aspartate residues of APRs initiate switching between the amyloid and
the folded, monomeric forms of the hormones. We find that pH sensitivity diminishes
in the absence of acidic gatekeepers and amyloid formation progresses over a broad
pH range. Our results highlight the dual role of short aggregation core motifs in
reversible amyloid formation and receptor binding.
