Large and folded like a protein - but completely
synthetic.
The physiological functions of proteins depend on
their folding into a particular spatial structure (tertiary structure):
enzymes and their substrates must fit together like the proverbial
lock and key. It has recently been discovered that not only large
biomolecules are capable of stable, defined folding; synthetic
molecules can do it too. Called foldamers, these molecules can even
imitate the biological functions of the proteins they are modeled
after. However, until recently their size and complexity was strictly
limited. French researchers have now produced an intricately folded
molecule exclusively from manmade components. The dimensions of this
foldamer correspond to those of the tertiary structures of smaller
proteins.
The team led by Ivan Huc did not want to base the design of their
foldamer on the structure of proteins, because the synthesis of large
chains from small individual building blocks is difficult. The
alternative was to use branched structures. They did adopt one
important structural element from proteins: the helix. The researchers
hooked eight quinoline units (nitrogen-containing aromatic
six-membered rings with a shared edge) together into a chain. This
type of octamer twists itself into a helix. The researchers then
bridged two such octamers together with a special branching link. This
linker inserts so well into the two octamers that a continuous, stable
helix is formed. The branching linker can then be used to hook two
such helical structures together side by side. Once linked, the two
helices do not lie in parallel, but rather at right angles to each
other.
Helices can be twisted to the left or the right. In peptides, the
direction of the helix is uniquely defined by the spatial structure of
the individual building blocks. In the synthesis of the
quadruple-octamers, however, an equal number of right- and left-handed
helices are formed. The preferences demonstrated by the helices on
pairing are determined by the solvent: In aromatic solvents, pairing
of two helices with the same direction of twist is clearly preferred
(70 %), while in chlorinated hydrocarbons up to 93 % of the pairs are
formed from helices with opposite directions of twist. When the
solvent is changed, the helices change their directionality to match
these preferences. “This proves both helices are involved in strong
interactions with each other, just like a folded protein,” says Huc.
“Our abiotic foldamer is the first of its kind and shows that it is
possible to synthesize folded molecules that imitate the size and
structural complexity of the tertiary structure of proteins, while
consisting entirely of manmade building blocks.” The goal is to
produce artificial structures with defined binding sites and uniquely
positioned catalytic groups for controlled reactions with specific
substrates.
Source / Further
information:
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Publishing date: 27-Oct-2006
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Nicolas Delsuc, Jean-Michel Léger, Prof.,
Stéphane Massip, Dr., Ivan Huc, Dr. -
Proteomorphous Objects from Abiotic Backbones - DOI
10.1002/anie.200603390, Angewandte Chemie International Edition
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Author:
Ivan Huc, Institut Européen de Chimie et Biologie, Pessac
(France)
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