Bacillus subtilis biofilms resemble cross-linked hydrogels in their morphology and swelling properties. All the water in these biofilms is bound water. Water binding is mostly related with accumulated solutes.
Functional amyloid proteins often appear as fibers in extracellular matrices of microbial soft colonies. In contrast to disease-related amyloid structures, they serve a functional goal that benefits the organism that secretes them, which is the reason for the title “functional”. Biofilms are a specific example of a microbial community in which functional amyloid fibers play a role. Functional amyloid proteins contribute to the mechanical stability of biofilms and mediate the adhesion of the cells to themselves as well as to surfaces. Recently, it has been shown that functional amyloid proteins also play a regulatory role in biofilm development. TasA is the major proteinaceous fibrilar component of the extracellular matrix of biofilms made of the soil bacterium and Gram-positive Bacillus subtilis. We have previously shown, as later corroborated by others, that in acidic solutions, TasA forms compact aggregates that are composed of tangled fibers. Here, we show that in a neutral pH and above a certain TasA concentration, the fibers of TasA are elongated and straight and that they bundle up in highly concentrated salt solutions. TasA fibers resemble the canonic amyloid morphology; however, these fibers also bear an interesting nm-scale periodicity along the fiber axis. At the molecular level, TasA fibers contain a twisted β-sheet structure, as indicated by circular dichroism measurements. Our study shows that the morphology of TasA fibers depends on the environmental conditions. Different fibrilar morphologies may be related with different functional roles in biofilms, ranging from granting biofilms with a mechanical support to acting as antibiotic agents.
Biofilms are multicellular communities of microbial cells
that
grow on natural and synthetic surfaces. They have become the major
cause for hospital-acquired infections because once they form, they
are very difficult to eradicate. Nanotechnology offers means to fight
biofilm-associated infections. Here, we report on the synthesis of
silver nanoparticles (AgNPs) with the antibacterial ligand epigallocatechin
gallate (EGCG) and the formation of a lysozyme protein corona on AgNPs,
as shown by UV–vis, dynamic light scattering, and circular
dichroism analyses. We further tested the activity of EGCG-AgNPs and
their lysozyme bioconjugates on the viability of
Bacillus
subtilis
cells and biofilm formation. Our results
showed that, although EGCG-AgNPs presented no antibacterial activity
on planktonic
B. subtilis
cells, they
inhibited
B. subtilis
biofilm formation
at concentrations larger than 40 nM, and EGCG-AgNP-lysozyme bioconjugates
inhibited biofilms at concentrations above 80 nM. Cytotoxicity assays
performed with human cells showed a reverse trend, where EGCG-AgNPs
barely affected human cell viability while EGCG-AgNP-lysozyme bioconjugates
severely hampered viability. Our results therefore demonstrate that
EGCG-AgNPs may be used as noncytotoxic antibiofilm agents.
Biofilms are surface or interface-associated communities of bacterial cells, embedded in a self-secreted extracellular matrix (ECM). Cells in biofilms are 100-1000 times more resistant to antibiotic treatment relative to planktonic...
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