Ion-Pair Recognition by Metal - Salophen and Metal - Salen Complexes

Francesco Yafteh Mihan; Silvia Bartocci; Michele Bruschini; Paolo De Bernardin; Gianpiero Forte; Ilaria Giannicchi; Antonella Dalla Cort

doi:10.1071/ch12353

Ion-Pair Recognition by Metal - Salophen and Metal - Salen Complexes

Australian Journal of Chemistry ◽

10.1071/ch12353 ◽

2012 ◽

Vol 65 (12) ◽

pp. 1638 ◽

Cited By ~ 18

Author(s):

Francesco Yafteh Mihan ◽

Silvia Bartocci ◽

Michele Bruschini ◽

Paolo De Bernardin ◽

Gianpiero Forte ◽

...

Keyword(s):

Binding Sites ◽

Ion Pairs ◽

Anion Recognition ◽

Short Review ◽

Ion Pair ◽

Cation Binding ◽

Binding Motifs ◽

Salen Complexes ◽

Challenging Research ◽

Anionic Species

The development of heteroditopic receptor systems that can simultaneously bind cationic and anionic species is one of the most challenging research topics in supramolecular chemistry, attracting the attention of a large number of research groups worldwide. Such an interest is due especially to the fact that the overall receptor–ion-pair complex is neutral and this can be advantageous in many situations, such as salt solubilization and extraction, and membrane-transport applications. Receptors designed for ion-pair complexation are molecules comprising well-known anion-binding motifs and familiar cation-binding sites. An important family of compounds that can use metal Lewis-acidic centres for anion recognition and that can be easily derivatized to introduce an additional binding site for the cation is metal–salophen and metal–salen complexes. This short review shows that the high versatility of salen and salophen ligands and of the corresponding metal complexes allows, through simple modifications of the basic skeleton, the obtention of highly efficient receptors for ion pairs.

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Phosphate binding by a novel Zn(ii) complex featuring a trans-1,2-diaminocyclohexane ligand. Effective anion recognition in water

Organic & Biomolecular Chemistry ◽

10.1039/c4ob02321h ◽

2015 ◽

Vol 13 (6) ◽

pp. 1860-1868 ◽

Cited By ~ 10

Author(s):

Oscar Francesconi ◽

Matteo Gentili ◽

Francesco Bartoli ◽

Andrea Bencini ◽

Luca Conti ◽

...

Keyword(s):

Binding Sites ◽

Metal Ion ◽

Anion Recognition ◽

Cation Binding ◽

Phosphate Binding ◽

Ditopic Receptor ◽

Phosphate Anions

Excellent affinities and selectivities toward triphosphates are achieved through an adaptive ditopic receptor featuring a metal ion and a macrocyclic polyammonium cation binding sites, concertedly bridging phosphate anions.

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Stereospecific 1,3-H Transfer of Indenols Proceeds via Persistent Ion-Pairs Anchored By NH···Pi Interactions

10.26434/chemrxiv.7057892.v1 ◽

2018 ◽

Author(s):

David Ascough ◽

Fernanda Duarte ◽

Robert Paton

Keyword(s):

Computational Analysis ◽

Ion Pairs ◽

Ion Pair ◽

Hydrogen Atom Transfer ◽

Polar Solvents ◽

Chirality Transfer ◽

Activation Barriers ◽

Sense And Avoid ◽

Phase Dynamics ◽

Pi Interactions

The base-catalyzed rearrangement of arylindenols is a rare example of a suprafacial [1,3]-hydrogen atom transfer. The mechanism has been proposed to proceed via sequential [1,5]-sigmatropic shifts, which occur in a selective sense and avoid an achiral intermediate. A computational analysis using quantum chemistry casts serious doubt on these suggestions: these pathways have enormous activation barriers and in constrast to what is observed experimentally, they overwhelmingly favor a racemic product. Instead we propose that a suprafacial [1,3]-prototopic shift occurs in a two-step deprotonation/reprotonation sequence. This mechanism is favored by 15 kcal mol<sup>-1</sup> over that previously proposed. Most importantly, this is also consistent with stereospecificity since reprotonation occurs rapidly on the same p-face. We have used explicitly-solvated molecular dynamics studies to study the persistence and condensed-phase dynamics of the intermediate ion-pair formed in this reaction. Chirality transfer is the result of a particularly resilient contact ion-pair, held together by electrostatic attraction and a critical NH···p interaction which ensures that this species has an appreciable lifetime even in polar solvents such as DMSO and MeOH.

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Tripodal, Squaramide-Based Ion Pair Receptor for Effective Extraction of Sulfate Salt

Molecules ◽

10.3390/molecules26092751 ◽

2021 ◽

Vol 26 (9) ◽

pp. 2751

Author(s):

Damian Jagleniec ◽

Marcin Wilczek ◽

Jan Romański

Keyword(s):

Ion Pairs ◽

Binding Mode ◽

Selective Extraction ◽

Ion Pair ◽

Hofmeister Series ◽

Sulfate Salt ◽

Lower Affinity ◽

High Affinity ◽

Binding Domains ◽

Hydrated Sulfate

Combining three features—the high affinity of squaramides toward anions, cooperation in ion pair binding and preorganization of the binding domains in the tripodal platform—led to the effective receptor 2. The lack of at least one of these key elements in the structures of reference receptors 3 and 4 caused a lower affinity towards ion pairs. Receptor 2 was found to form an intramolecular network in wet chloroform, which changed into inorganic–organic associates after contact with ions and allowed salts to be extracted from an aqueous to an organic phase. The disparity in the binding mode of 2 with sulfates and with other monovalent anions led to the selective extraction of extremely hydrated sulfate anions in the presence of more lipophilic salts, thus overcoming the Hofmeister series.

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Cytological Studies on the Absorptive Surfaces of Cestodes. IV. Localization and Cytochemical Properties of Membrane-Fixed Cation Binding Sites

Journal of Parasitology ◽

10.2307/3277721 ◽

1970 ◽

Vol 56 (4) ◽

pp. 736 ◽

Cited By ~ 26

Author(s):

Richard D. Lumsden ◽

John A. Oaks ◽

William L. Alworth

Keyword(s):

Binding Sites ◽

Cation Binding

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First Characterization of an Archaeal GTP-Dependent Phosphoenolpyruvate Carboxykinase from the Hyperthermophilic Archaeon Thermococcus kodakaraensis KOD1

Journal of Bacteriology ◽

10.1128/jb.186.14.4620-4627.2004 ◽

2004 ◽

Vol 186 (14) ◽

pp. 4620-4627 ◽

Cited By ~ 29

Author(s):

Wakao Fukuda ◽

Toshiaki Fukui ◽

Haruyuki Atomi ◽

Tadayuki Imanaka

Keyword(s):

Binding Sites ◽

Phosphoenolpyruvate Carboxykinase ◽

Cation Binding ◽

Activity Levels ◽

Binding Region ◽

Hyperthermophilic Archaeon ◽

Dependent Activity ◽

Additional Role

ABSTRACT Phosphoenolpyruvate carboxykinase (PCK), which catalyzes the nucleotide-dependent, reversible decarboxylation of oxaloacetate to yield phosphoenolpyruvate and CO2, is one of the important enzymes in the interconversion between C3 and C4 metabolites. This study focused on the first characterization of the enzymatic properties and expression profile of an archaeal PCK from the hyperthermophilic archaeon Thermococcus kodakaraensis (Pck Tk ). Pck Tk showed 30 to 35% identities to GTP-dependent PCKs from mammals and bacteria but was located in a branch distinct from that of the classical enzymes in the phylogenetic tree, together with other archaeal homologs from Pyrococcus and Sulfolobus spp. Several catalytically important regions and residues, found in all known PCKs irrespective of their nucleotide specificities, were conserved in Pck Tk . However, the predicted GTP-binding region was unique compared to those in other GTP-dependent PCKs. The recombinant Pck Tk actually exhibited GTP-dependent activity and was suggested to possess dual cation-binding sites specific for Mn2+ and Mg2+. The enzyme preferred phosphoenolpyruvate formation from oxaloacetate, since the Km value for oxaloacetate was much lower than that for phosphoenolpyruvate. The transcription and activity levels in T. kodakaraensis were higher under gluconeogenic conditions than under glycolytic conditions. These results agreed with the role of Pck Tk in providing phosphoenolpyruvate from oxaloacetate as the first step of gluconeogenesis in this hyperthermophilic archaeon. Additionally, under gluconeogenic conditions, we observed higher expression levels of Pck Tk on pyruvate than on amino acids, implying that it plays an additional role in the recycling of excess phosphoenolpyruvate produced from pyruvate, replacing the function of the anaplerotic phosphoenolpyruvate carboxylase that is missing from this archaeon.

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Ion pair binding by an l-tyrosine-based polymerizable molecular receptor

New Journal of Chemistry ◽

10.1039/c5nj01063b ◽

2015 ◽

Vol 39 (8) ◽

pp. 6216-6222 ◽

Cited By ~ 13

Author(s):

Szymon Zdanowski ◽

Jan Romański

Keyword(s):

Ion Pairs ◽

Functional Polymers ◽

Ion Pair

A polymerizable molecular receptor able to bind ion pairs and new functional polymers containing the receptor units were synthesized and characterized.

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Evolution of mouse circadian enhancers from transposable elements

Genome Biology ◽

10.1186/s13059-021-02409-9 ◽

2021 ◽

Vol 22 (1) ◽

Author(s):

Julius Judd ◽

Hayley Sanderson ◽

Cédric Feschotte

Keyword(s):

Gene Expression ◽

Transposable Elements ◽

Binding Sites ◽

Mouse Liver ◽

Integration Site ◽

Point Mutations ◽

Regulatory Elements ◽

Circadian Gene ◽

Binding Motifs ◽

Reporter Assays

Abstract Background Transposable elements are increasingly recognized as a source of cis-regulatory variation. Previous studies have revealed that transposons are often bound by transcription factors and some have been co-opted into functional enhancers regulating host gene expression. However, the process by which transposons mature into complex regulatory elements, like enhancers, remains poorly understood. To investigate this process, we examined the contribution of transposons to the cis-regulatory network controlling circadian gene expression in the mouse liver, a well-characterized network serving an important physiological function. Results ChIP-seq analyses reveal that transposons and other repeats contribute ~ 14% of the binding sites for core circadian regulators (CRs) including BMAL1, CLOCK, PER1/2, and CRY1/2, in the mouse liver. RSINE1, an abundant murine-specific SINE, is the only transposon family enriched for CR binding sites across all datasets. Sequence analyses and reporter assays reveal that the circadian regulatory activity of RSINE1 stems from the presence of imperfect CR binding motifs in the ancestral RSINE1 sequence. These motifs matured into canonical motifs through point mutations after transposition. Furthermore, maturation occurred preferentially within elements inserted in the proximity of ancestral CR binding sites. RSINE1 also acquired motifs that recruit nuclear receptors known to cooperate with CRs to regulate circadian gene expression specifically in the liver. Conclusions Our results suggest that the birth of enhancers from transposons is predicated both by the sequence of the transposon and by the cis-regulatory landscape surrounding their genomic integration site.

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Axle component separated ion-pair recognition by a neutral heteroditopic [2]rotaxane

Chemical Communications ◽

10.1039/c3cc48905a ◽

2014 ◽

Vol 50 (13) ◽

pp. 1540-1542 ◽

Cited By ~ 24

Author(s):

Richard C. Knighton ◽

Paul D. Beer

Keyword(s):

Alkali Metal ◽

Metal Cation ◽

Alkali Metal Cation ◽

Ion Pairs ◽

Ion Pair ◽

Sodium Cation ◽

Halide Anion ◽

Cooperative Recognition

A neutral heteroditopic pyridine N-oxide axle containing [2]rotaxane, synthesised via sodium cation templation, displays cooperative recognition of alkali metal cation-halide anion ion-pairs in an unprecedented axle component separated ion-pair binding fashion.

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Chromatin extrusion explains key features of loop and domain formation in wild-type and engineered genomes

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1518552112 ◽

2015 ◽

Vol 112 (47) ◽

pp. E6456-E6465 ◽

Cited By ~ 857

Author(s):

Adrian L. Sanborn ◽

Suhas S. P. Rao ◽

Su-Chen Huang ◽

Neva C. Durand ◽

Miriam H. Huntley ◽

...

Keyword(s):

Genome Editing ◽

Binding Sites ◽

Physical Structure ◽

Ctcf Binding ◽

Binding Motifs ◽

Physical Simulations ◽

Chromatin Folding ◽

Mammalian Genomes ◽

Single Base Pair ◽

Fractal Globule

We recently used in situ Hi-C to create kilobase-resolution 3D maps of mammalian genomes. Here, we combine these maps with new Hi-C, microscopy, and genome-editing experiments to study the physical structure of chromatin fibers, domains, and loops. We find that the observed contact domains are inconsistent with the equilibrium state for an ordinary condensed polymer. Combining Hi-C data and novel mathematical theorems, we show that contact domains are also not consistent with a fractal globule. Instead, we use physical simulations to study two models of genome folding. In one, intermonomer attraction during polymer condensation leads to formation of an anisotropic “tension globule.” In the other, CCCTC-binding factor (CTCF) and cohesin act together to extrude unknotted loops during interphase. Both models are consistent with the observed contact domains and with the observation that contact domains tend to form inside loops. However, the extrusion model explains a far wider array of observations, such as why loops tend not to overlap and why the CTCF-binding motifs at pairs of loop anchors lie in the convergent orientation. Finally, we perform 13 genome-editing experiments examining the effect of altering CTCF-binding sites on chromatin folding. The convergent rule correctly predicts the affected loops in every case. Moreover, the extrusion model accurately predicts in silico the 3D maps resulting from each experiment using only the location of CTCF-binding sites in the WT. Thus, we show that it is possible to disrupt, restore, and move loops and domains using targeted mutations as small as a single base pair.

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The fluoride permeation pathway and anion recognition in Fluc family fluoride channels

eLife ◽

10.7554/elife.69482 ◽

2021 ◽

Vol 10 ◽

Author(s):

Benjamin C McIlwain ◽

Roja Gundepudi ◽

B Ben Koff ◽

Randy B Stockbridge

Keyword(s):

Binding Sites ◽

Anion Recognition ◽

Anion Binding ◽

Structural Studies ◽

Planar Bilayer ◽

X Ray ◽

X Ray Crystallography ◽

Molecular Determinants ◽

Cytoplasmic Accumulation ◽

Oriented System

Fluc family fluoride channels protect microbes against ambient environmental fluoride by undermining the cytoplasmic accumulation of this toxic halide. These proteins are structurally idiosyncratic, and thus the permeation pathway and mechanism have no analogy in other known ion channels. Although fluoride binding sites were identified in previous structural studies, it was not evident how these ions access aqueous solution, and the molecular determinants of anion recognition and selectivity have not been elucidated. Using x-ray crystallography, planar bilayer electrophysiology and liposome-based assays, we identify additional binding sites along the permeation pathway. We use this information to develop an oriented system for planar lipid bilayer electrophysiology and observe anion block at one of these sites, revealing insights into the mechanism of anion recognition. We propose a permeation mechanism involving alternating occupancy of anion binding sites that are fully assembled only as the substrate approaches.

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