Bouillomides A (1) and B (2) are two depsipeptide analogues of dolastatin 13. Isolated from a Guamanian sample of Lyngbya bouillonii, the planar structures were elucidated on the basis of HR-ESI-MS and NMR data, while the absolute configurations were determined by employing functional group conversions, modified Marfey’s analysis, and detailed analyses of ROESY correlations. Compounds 1 and 2 selectively inhibited serine proteases elastase (IC50 = 1.9 μM for both) and chymotrypsin (IC50 = 0.17 and 9.3 μM, respectively) while showing no inhibition of trypsin (IC50 > 100 μM).
Seven new bromotyrosine-derived metabolites, purpuramine M-N (1-2), araplysillin VII-XI (3-7) and six known compounds (8-13) were isolated from an Indonesian sponge belonging to the family Aplysinellidae (Order Verongiida). The structures of the new compounds were determined by extensive NMR experiments and mass spectrometric measurements. These compounds were screened against BACE1 and five cancer cell lines.
Three new ulapualides (3–5) were isolated from egg masses of the nudibranch Hexabranchus sanguineus. The structures of 3–5 were deduced by analyses of physical and spectroscopic data in comparisons with ulapualides A (1) and B (2). Ulapualide C demonstrated submicromolar cytotoxicity against select NCI cell lines (768-0, DU-145, MDA-MB-231, and A549) with the most potent activity against MDA-MB-231 (IC50 0.58 μM). Ulapualides A (1) and B (2) were two to four-fold more potent than 3.
Examination of an active extract of the fruit of Ficus benjamina var. nuda (Miq.) Barrett (Moraceae) has led to the isolation of six new isoflavones and two coumarano-chroman-4-one, along with fifteen known compounds. The structures of the eight new compounds were elucidated on the basis of extensive NMR experiments and mass spectrometric measurements. The inhibitory activity of the compounds on the proteolytic cleavage of amyloid precursor protein by the aspartic protease BACE1 was evaluated. Both coumarano-chroma-4-ones and some isoflavones showed moderate activity in this assay.
Several known sesquiterpenoid quinones and quinols (1–9), and kauamide (10), a new polyketide-peptide containing an 11-membered heterocycle, were isolated from the extracts of the Hawaiian marine sponge Dactylospongia elegans. The planar structure of 10 was determined from spectroscopic analyses, and its relative and absolute configurations were established from density functional theory (DFT) calculations of the GIAO NMR shielding tensors, and advanced Marfey’s analysis of the N-MeLeu residue, respectively. Compounds 1 and 3 showed moderate inhibition of β-secretase 1 (BACE1), whereas 1–9 exhibited moderate to potent inhibition of growth of human glioma (U251) cells. Compounds 1–2 and 4–7 were also active against human pancreatic carcinoma (Panc-1) cells.
New compounds 18-nor-3,17-dihydroxyspongia-3,13(16),14-trien-2-one
(1), 18-nor-3,5,17-trihydroxyspongia-3,13(16),14-trien-2-one
(2), and spongiapyridine (3) and the known
compound 17-hydroxy-4-epi-spongialactone A (4) were isolated from an Indonesian sponge of the genus Spongia. The structures of 1–3 were deduced by analyses of physical and spectroscopic data. Diterpene 3 is unusual, as the D-ring is a pyridyl ring system rather
than the standard δ-lactone. The structure elucidation of this
compound was complicated by facile exchange of the axial proton at
the C-11 methylene with deuterium from methanol-d4. The isolated compounds were tested for biological activity
in a battery of in vitro assays (TNF-α-induced NFκB, LPS-induced
iNOS, RXR stimulation, quinone reductase 1 induction, aromatase inhibition,
TRPM7 ion channels, and aspartic protease BACE1 inhibition). Norditerpene 2 modestly inhibited aromatase with an IC50 of
34 μM and induced quinone reductase 1 activity with a CD (the
concentration needed to double the enzymatic response) of 11.2 μM.
The remaining isolates were inactive.
Four compounds (1–4) were isolated
from a Hawaiian sponge of the genus Myrmekioderma. Myrmenaphthol A (1) incorporates two unusual elements
into an oxidized steroidal core: a naphthyl AB-ring system and a hydroxy
group at C-2. A comparison of the experimental and predicted electronic
circular dichroism (ECD) spectra of 1 assigned an S configuration to the lone stereocenter (ΔESI = 0.75; similarity factor 0.8137). Known compounds, cinanthrenol
A (2), 3,4-dihydroxypregna-5,17-diene-10,2-carbolactone
(3), and 3,4-dihydroxypregna-5,20-diene-10,2-carbolactone
(4), were also isolated. Despite literature reports of
competitive inhibition at nanomolar levels for 2, neither 2 nor the structurally related 1 showed any activity
against estrogen receptors at the concentrations tested.
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