Sponsored Links
-->

Wednesday, July 4, 2018

Exploiting the Oxacalixarene Scaffold: Structural Diversity ...
src: acswebcontent.acs.org

Molecular tweezers, and molecular clips, are host molecules with open cavities capable of binding guest molecules. The open cavity of the molecular tweezers may bind guests using non-covalent bonding which includes hydrogen bonding, metal coordination, hydrophobic forces, van der Waals forces, ?-? interactions, and/or electrostatic effects. These complexes are a subset of macrocyclic molecular receptors and their structure is that the two "arms" that bind the guest molecule between them are only connected at one end leading to a certain flexibility of these receptor molecules (induced fit model).


Video Molecular tweezers



History

The term "molecular tweezers" was first used by Howard J. Whitlock. The class of hosts was developed and popularized by Steven C. Zimmerman in the mid-1980s to early 1990s and later by Frank-Gerrit Klärner and colleagues.


Maps Molecular tweezers



Examples

One example of molecular tweezers has been reported by Jean-Marie Lehn and coworkers. This molecule is capable of binding aromatic guests. These molecular tweezers consist of a pair of anthracene arms held at a distance that allows aromatic guests to gain ?-? interactions from both (see Figure).

Another class of molecular tweezers is composed of two substituted porphyrin macrocycles tethered by an amide linker with a variable length. This example of a molecular tweezer shows the potential mobility of this class of molecules, as the orientation of the porphyrin planes which comprise the tweezer can be altered by the guest which is bound

Yet another structure for molecular tweezers which specifically bind fullerenes is called a buckycatcher and has been reported. This molecular tweezer is composed of two concaved corannulene pincers that complement the surface of the convex fullerene guest (Figure 2). An association constant (Ka) of 8,600 M-1 between the host buckycatcher and a C60 fullerene was calculated using 1H NMR spectroscopy.

Using 1,4-benzoquinone and two equivalents of cyclopentadiene to construct the arms of the tweezers (via formal [4+2] cycloaddition), Stoermer and co-workers succeeded synthesising clefts capable of capturing cyclohexane or chloroform molecules. Intriguingly, pi interactions played key roles in guest capture as well as cleft formation rate.

Water-soluble phosphate-substituted molecular tweezers made of alternating benzene and norbornene rings bind selectively to positively charged aliphatic side chains of basic amino acids, such as lysine and arginine (Figure 3, binding to lysine is stronger than to arginine). Similar compounds called "molecular clips," whose side walls are flat rather than convex, prefer to enclose flat pyridinium rings (for example the nicotinamide ring of NAD(P)+) between their plane naphthalene sidewalls (Figure 4). These mutually exclusive binding modes make these compounds valuable tools for probing critical biological interactions of basic amino acid side chains in peptides and proteins as well as of NAD(P)+ and similar cofactors. For example, both types of compounds inhibit the oxidation reactions of ethanol by alcohol dehydrogenase or of glucose-6-phosphate by glucose-6-phosphate dehydrogenase, respectively.

The molecular tweezers, but not the clips, efficiently inhibit the formation of toxic oligomers and aggregates by amyloidogenic proteins associated with different diseases. Examples include the proteins involved in Alzheimer's disease - amyloid ?-protein (A?) and tau; ?-synuclein, which is thought to cause Parkinson's disease and other synucleinopathies and is involved in spinal-cord injury; mutant huntingtin, which causes Huntington's disease; islet amyloid polypeptide (amylin), which kills pancreatic ?-cells in type-2 diabetes; transthyretin (TTR), which causes familial amyloid polyneuropathy, familial amyloid cardiomyopathy, and senile systemic amyloidosis; aggregation-prone mutants of the tumor-suppressor protein p53; and semen proteins whose aggregation enhances HIV infection. Importantly, the molecular tweezers have been found to be effective and safe not only in the test tube but also in animal models of different diseases, suggesting that they may be developed as drugs against diseases caused by abnormal protein aggregation, all of which currently have no cure. They were also shown to destroy the membranes of enveloped viruses, such as HIV, herpes, and hepatitis C, which makes them good candidates for development of microbicides.

The above examples show the potential reactivity and specificity of these molecules. The binding cavity between the side arms of the tweezer can evolve to bind to an appropriate guest with high specificity, depending on the configuration of the tweezer. That makes this overall class of macromolecule truly synthetic molecular receptors with important application to biology and medicine.


Portable Optical Tweezers Demonstration Kit
src: www.thorlabs.com


See also

  • Clathrate compound
  • Host-guest chemistry

TU München on Twitter:
src: pbs.twimg.com


References


Portable Optical Tweezers Demonstration Kit
src: www.thorlabs.com


External links

  • Journal of Chemical Education Featured Molecules December 2004: Nanoscale Molecular Tweezers and article
  • Crystalmaker molecular tweezers

Source of article : Wikipedia