Five lignans, five neolignans, two sesquilignans, and a dilignan were identified from a phytotoxic extract of Brassica fruticulosa L. Compounds 8, 9, 12, and 13 have been isolated for the first time. Structures were determined on the basis of their spectroscopic features. Their effects on the germination and growth of two dicotyledons, Lactuca sativa (lettuce) and Lycopersicon esculentum (tomato), and a monocotyledon, Allium cepa (onion), as standard target species have been studied.
Adjuvants are components of vaccine
that enhance the specific immune
response against co-inoculated antigens. Recently, we reported the
characterization of a synthetic sulfolipid named Sulfavant A (
1
) as a promising candidate of a novel class of molecular
adjuvants based on the sulfoquinovosyl-diacylglycerol skeleton. Here,
we report an improved synthesis of the sulfolipid scaffold, as well
as the preparation of two analogs named Sulfavant-S (
2
) and Sulfavant-R (
3
) with enhanced property to modulate
master immune targets such as human dendritic cells (DCs). According
to the present approach, synthesis of
1
is reduced from
14 to 11 steps with nearly triplication of the overall yield (11%).
The new members
2
and
3
elicit DC maturation
at a concentration of 10 nM, which is 1000 times more potent than
the parent molecule
1
. Analysis of dynamic light scattering
indicates self-assembly of Sulfavants and formation of colloidal particles
with a small hydrodynamic radius (50 nm) for the epimers
2
and
3
and a larger radius (150 nm) for
1
. The colloidal aggregates are responsible for the bell-shaped dose–response
curve of these products. We conclude that the particle size also affects
the equilibrium with free monomers, thus determining the effective
concentration of the sulfolipid molecule at the cellular targets and
the different immunological efficacy of
1–3
. Sulfavants
(
1–3
) do not show in vitro cytotoxicity at concentrations
10
5
higher than the dose that triggers maximal immune response,
thus predicting a low level of toxicological risk in their formulation
in vaccines.
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