α-synuclein aggregation inhibitory activity of the bromotyrosine derivatives aerothionin and aerophobin-2 from the subtropical marine sponge Aplysinella sp

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Prebble, DW
Er, S
Xu, M
Hlushchuk, I
Domanskyi, A
Airavaara, M
Ekins, MG
Mellick, GD
Carroll, AR
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2022
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Abstract

The neuronal protein α-synuclein (α-syn) is one of the main constituents of intracellular amyloid aggregations found in the post-mortem brains of Parkinson's disease (PD) patients. Recently, we screened the MeOH extracts obtained from 300 sub-tropical marine invertebrates for α-syn binding activity using affinity MS and this resulted in the extract of the Verongida marine sponge Aplysinella sp. 1194, (QM G339263) displaying molecules that bind to the protein. The subsequent bioassay-guided separation of the Aplysinella sp. extract led to the isolation of the known bromotyrosine derivatives (+)-aerothionin (1) and (+)-aerophobin-2 (2). Both compounds bind to α-syn as detected by a MS affinity assay and inhibit α-syn aggregation in an assay that uses the fluorescence probe, thioflavin T, to detect aggregation. (+)-Aerothionin (1) was toxic to primary dopaminergic neurons at its expected α-syn aggregation inhibitory concentration and so could not be tested for inhibition of pSyn aggregates in this functional assay. (+)-Aerophobin-2 (2) was not toxic and shown to weakly inhibit pSyn aggregation in primary dopaminergic neurons at 10 µM.

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Results in Chemistry

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4

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© 2022 The Author(s). Published by Elsevier B.V. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).

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Natural products and bioactive compounds

Medicinal and biomolecular chemistry

Marine and estuarine ecology (incl. marine ichthyology)

Neurosciences

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Prebble, DW; Er, S; Xu, M; Hlushchuk, I; Domanskyi, A; Airavaara, M; Ekins, MG; Mellick, GD; Carroll, AR, α-synuclein aggregation inhibitory activity of the bromotyrosine derivatives aerothionin and aerophobin-2 from the subtropical marine sponge Aplysinella sp, Results in Chemistry, 2022, 4, pp. 100472

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