Some μ-oxo compounds of iron-hemiporphyrazine. Synthesis and properties

Details of the conditions necessary for preparing the recently reported μ-oxo-ironhemiporphyrazinate compounds (Fe(IV)hpO)_n and [(Fe(III)hp)₂O]H₂O are given. Two further homologous μ-oxo Fe(III)hemiporphyrazinates are described: an amorphous μ-oxo dimer and a μ-oxo dimer HCl adduct. The thermal and spectroscopic (UV-Vis, IR, Mössbauer, XPS) properties and magnetic susceptibilities of these compounds have been investigated. The reducibility of these species in solution, in the presence and absence of O₂, has been monitored. The results do not indicate a change in oxidation state of the iron in (FehpO)_n. Attempts to obtain the hemiporphyrazinato Fe(III) chloride are described.     

Redox potentials of trinuclear μ-oxo ruthenium acetate clusters with N-heterocyclic ligands

The trinuclear clusters of general composition [Ru₃O(OOCCH₃)₆(N-Het)₃], where N-Het=pyridine and pyrazine derivatives, exhibit a series of reversible waves in the range of −1.8 to 2.4 V versus SHE, in acetonitrile, ascribed to the successive [cluster]^{−2/−1/0/+1/+2/+3} redox couples. The redox potentials decrease with the pK_a of the N-heterocyclic ligands according to the equations E°(+3/+2)= 2.24−0.023 pK_a; E°(+2/+1)=1.34−0.029 pK_a; E°(+1/0)=0.36−0.039 pK_a and E°(0/−1)=−0.68− 0.074 pK_a. The dependence is greater at lower oxidation states, reflecting the role of π-backbonding in the complexes.     

A nitric oxide releaser based on the μ-oxo-hexaacetate-bis(4-methylpyridine)triruthenium nitrosyl complex

The properties of the trinuclear cluster [Ru₃OAc₆(pic)₂(NO)]PF₆ (pic = 4-methyl pyridine, Ac = acetate ion) and the photochemical behavior of the corresponding molecular films are reported in this paper. In this compound, the unpaired π* electron from NO and the unpaired electron from the π-orbitals of the Ru₃O unity are strongly coupled; as a consequence, the changes in electronic distribution associated with the several successive redox states promote dramatic effects in the spectroscopic and electrochemical properties of the nitric oxide ligand and the entire complex. NO release has been observed by light irradiation (? = 0.038 at 365 nm and ? = 0.019 at 468 nm, in acetonitrile solution), changing the original violet color into deep blue. The same behavior has been observed in solid state and in PVA films incorporating this compound, revealing its potential usefulness as NO photoreleaser, as well as for the monitoration of light exposure intensities.     

Human kidney anion exchanger 1 interacts with adaptor-related protein complex 1 μ1A (AP-1 mu1A)

Kidney anion exchanger 1 (kAE1) mediates chloride (Cl⁻) and bicarbonate (HCO₃⁻) exchange at the basolateral membrane of kidney α-intercalated cells. Impaired trafficking of kAE1 leads to defect of the Cl⁻/HCO₃⁻ exchange at the basolateral membrane and failure of proton (H⁺) secretion at the apical membrane, causing a kidney disease - distal renal tubular acidosis (dRTA). To gain a better insight into kAE1 trafficking, we searched for proteins physically interacting with the C-terminal region of kAE1 (Ct-kAE1), which contains motifs crucial for intracellular trafficking, by a yeast two-hybrid (Y2H) system. An adaptor-related protein complex 1 μ1A (AP-1 mu1A) subunit was found to interact with Ct-kAE1. The interaction between either Ct-kAE1 or full-length kAE1 and AP-1 mu1A were confirmed in human embryonic kidney (HEK) 293T by co-immunoprecipitation, affinity co-purification, co-localization, yellow fluorescent protein (YFP)-based protein fragment complementation assay (PCA) and GST pull-down assay. The interacting site for AP-1 mu1A on Ct-kAE1 was found to be Y904DEV907, a subset of YXXØ motif. Interestingly, suppression of endogenous AP-1 mu1A in HEK 293T by small interfering RNA (siRNA) decreased membrane localization of kAE1 and increased its intracellular accumulation, suggesting for the first time that AP-1 mu1A is involved in the kAE1 trafficking of kidney α-intercalated cells.     

Green butyryl-coenzyme A dehydrogenase. An enzyme–acyl-coenzyme A complex

1. Butyryl-CoA dehydrogenase from Peptostreptococcus elsdenii forms very tightly bound complexes with various acyl-CoA compounds. Spectra in some cases merely show resolution of the 450nm band, but those with acetoacetyl-, pent-2-enoyl- and 4-methylpent-2-enoyl-CoA show long-wavelength bands similar to the 710nm band of native enzyme. These complexes are formed instantaneously by the yellow form of the enzyme and much more slowly by the green form. 2. An acid extract of the green enzyme reconverts the yellow into the green form. 3. Hydroxylamine makes irreversible the otherwise reversible conversion of the green enzyme into the yellow form by phenylmercuric acetate. 4. Amino acid analysis for taurine and beta-alanine shows approx. 1mol of CoA/mol of flavin in green enzyme. Anaerobic dialysis of reduced enzyme removes the CoA. On acid precipitation of green enzyme the CoA is found only in the supernatant. 5. It is concluded that native green enzyme is probably complexed with unsaturated acyl-CoA. This is shown to be consistent with findings of other workers. Catalytic activity requires displacement of the acyl-CoA, which is therefore likely to be a potent inhibitor. 6. An explanation is offered for the irreversible conversion of green into yellow enzyme by sodium dithionite. 7. The enzyme displays a feeble, previously undetected, activity towards beta-hydroxybutyryl-CoA. 8. The product of oxidation of pent-4-enoyl-CoA forms a complex with reduced enzyme and strongly inhibits reoxidation of the FAD. This may contribute to inhibition of fatty acid oxidation by pent-4-enoic acid in mammals.     

Kinetics and mechanism of reactions of S-protected dithiol monoaminemonoamide (MAMA) ligands with technetium: Characterization of a technetium—thiolate—thioether—MAMA complex,a kinetic intermediate of the reaction

The exchange reactions of S-protected dithiol monoaminemonoamide (MAMA) ligands with Tc(V)-gluconate were investigated. Protection of the mercaptide sulfur atoms with acid, base and metal labile groups permitted complex formation of the MAMA ligands at a range of pHs. In general, the rate of complex formation was faster with the MAMA ligands than with the corresponding diamide dithiol (DADS) ligands. The rate of Tc complex formation depended on the nature of the sulfur protecting groups and on the position of the amine group with respect to the other donor groups in the ligands. Two isomeric ligands showed different mechanisms of complex formation. The isomer which gave the final Tc-dithiolate-MAMA complex in higher yield was shown to form a Tc-thioether-thiol-MAMA complex as an intermediate prior to metal-assisted S-dealkylation. The formation of the Tc-thioether complex intermediate at a lower temperature may account for the enhanced kinetics of chelation compared to the isomer which did not form the intermediate complex.     

Synthesis, structure and magnetic properties of two μ-oxo and thiocyanato-bridged manganese(II)-mercury(II) coordination polymers

Mixed-metal thiocyanate complexes [MnHg(SCN)₄(NOP)] (1) and [MnHg(SCN)₄(DMSO)] (2) (NOP = 3-methyl-4-nitropyridine-N-oxide, DMSO = dimethylsulfoxide) have been synthesized and structurally characterized by single crystal X-ray analysis. Complex 1 and 2 both contain a [Mn₂(μ₂-O)₂] lozenge, which is bridged to Hg(II) ions by end-to-end thiocyanate groups to form a 2-D and 3-D polymeric network, respectively. Magnetic studies indicate that both complexes are anti-ferromagnets, with 1 showing anti-ferrimagnetic ordering below 8.0 K.     

A complex equation – adding to Plasmodium falciparum invasion

The Plasmodium falciparum invasion complex – consisting of the prime blood-stage vaccine candidates PfRH5, PfCyRPA and PfRipr – is essential and conserved. New data from Scally et al. reveal that the complex consists of two additional proteins, adding important knowledge to the current understanding of the biology behind the invasion process.     

Speciation and structure of ferriprotoporphyrin IX in aqueous solution: spectroscopic and diffusion measurements demonstrate dimerization,but not μ-oxo dimer formation

Changes in epsilon (393) (the Soret band) of aqueous ferriprotoporphyrin IX [Fe(III)PPIX] with concentration indicate that it dimerizes, but does not form higher aggregates. Diffusion measurements support this observation. The diffusion coefficient of aqueous Fe(III)PPIX is half that of the hydrated monomeric dicyano complex. Much of the apparent instability of aqueous Fe(III)PPIX solutions could be attributed to adsorption onto glass and plastic surfaces. However, epsilon (347) was found to be independent of the aggregation state of the porphyrin and was used to correct for the effects of adsorption. The UV-vis spectrum of the aqueous dimer is not consistent with that expected for a mu-oxo dimer and the (1)H NMR spectrum is characteristic of five-coordinate, high-spin Fe(III)PPIX. Magnetic susceptibility measurements using the Evans method showed that there is no antiferromagnetic coupling in the dimer. By contrast, when the mu-oxo dimer is induced in 10% aqueous pyridine, characteristic UV-vis and (1)H NMR spectra of this species are observed and the magnetic moment is consistent with strong antiferromagnetic coupling. We propose a model in which the spontaneously formed aqueous Fe(III)PPIX dimer involves noncovalent interaction of the unligated faces of two five-coordinate H(2)O/HO-Fe(III)PPIX molecules, with the axial H(2)O/OH(-) ligands directed outwards. This arrangement is consistent with the crystal structures of related five-coordinate iron(III) porphyrins and accounts for the observed pH dependence of the dimerization constant and the spectra of the monomer and dimer. Structures for the aqueous dimer are proposed on the basis of molecular dynamics/simulated annealing calculations using a force field previously developed for modeling metalloporphyrins.     

Electrochemical formation of bi- versus tetranuclear μ-oxo terpyridine manganese complexes in CH3CN. Influence of the terpyridine substituents

To complete the elucidation of the electrochemical properties of Mn^II-bis(terpyridine) complexes in CH₃CN and evaluate the influence of the bulkiness of the terpy substituents, the oxidation processes of [Mn^II(L)₂]²⁺ (L = terpy for 2,2′:6′,2″-terpyridine, pTol-terpy for 4′-(4-methylphenyl)-2,2′:6′,2″-terpyridine and tBu₃-terpy for 4,4′,4″-tri-tert-butyl-2,2′:6′,2″-terpyridine) have been investigated in aqueous (1 M) CH₃CN solution. In this medium, exhaustive oxidations at 1.10-1.20 V versus Ag/Ag⁺ release two electrons per molecule of initial complex and lead to clean dimerization processes with the quantitative formation of the oxo-bridged binuclear [Mn₂^IVO₂(L)₂(H₂O)₂]⁴⁺ complex for L = tBu₃-terpy and of the tetranuclear [Mn₄^IVO₅(L)₄(H₂O)₂]⁶⁺ complexes for L = terpy and pTol-terpy. The formation of the tetranuclear complex with the tBu₃-terpy derivative is prevented by the steric hindrance induced by the bulkiness of the tert-butyl groups, as confirmed by molecular mechanics calculations, as well as by their strong electron-donating properties. All these electrogenerated multinuclear complexes have been fully characterized in solution by UV-vis and electron paramagnetic resonance (EPR) spectroscopy. A markedly improved chemical synthesis of [Mn₄^IVO₅(terpy)₄(H₂O)₂]⁶⁺ is also reported.     

A sialidase complex from chicken liver: Characterization of a multienzyme complex with β-galactosidase and carboxypeptidase

Mammalian lysosomal sialidase exists as an enzyme complex with β-galactosidase and carboxypeptidase, so-called “protective protein.” In this article, we report that chicken sialidase also occurs as a complex with β-galactosidase and protective protein. The purified sialidase complex had a molecular weight > 700 kDa on gel filtration and showed four protein components of 76, 65, 54 and 48 kDa on SDS-PAGE under nonreducing conditions. N-Terminal sequences of the 65- and 48-kDa proteins were homologous to human lysosomal β-galactosidase and protective protein precursor, respectively. The purified sialidase complex also had carboxypeptidase activity. Both sialidase and carboxypeptidase activities were precipitated together by an antibody against chicken β-galactosidase. The complex reversibly dissociated into 120-kDa β-galactosidase dimer and 100-kDa carboxypeptidase dimer at pH 7.5, but the sialidase irreversibly inactivated during the depolymerization. These findings indicate that chicken sialidase exists as a multienzyme complex, by which the sialidase activity appears to be stabilized.     

The m6A‑methylase complex and mRNA export

During synthesis, mRNA undergoes a number of modifications such as capping, splicing and polyadenylation. These processes are coupled with the orderly deposition of the TREX complex on the mRNA and subsequent recruitment of the NXF1-P15 heterodimer which stimulates the nuclear export of mature mRNAs. mRNAs also undergo a number of internal modifications, the most common of which is the N⁶?methyladenosine (m⁶A) modification. In this review we discuss the recent evidence of coupling between the m⁶A modification, RNA processing and export.     

Human cochlear hydrodynamics: A high-resolution μCT-based finite element study

Measurements of perilymph hydrodynamics in the human cochlea are scarce, being mostly limited to the fluid pressure at the basal or apical turn of the scalae vestibuli and tympani. Indeed, measurements of fluid pressure or volumetric flow rate have only been reported in animal models. In this study we imaged the human ear at 6.7 and 3-µm resolution using µCT scanning to produce highly accurate 3D models of the entire ear and particularly the cochlea scalae. We used a contrast agent to better distinguish soft from hard tissues, including the auditory canal, tympanic membrane, malleus, incus, stapes, ligaments, oval and round window, scalae vestibule and tympani. Using a Computational Fluid Dynamics (CFD) approach and this anatomically correct 3D model of the human cochlea, we examined the pressure and perilymph flow velocity as a function of location, time and frequency within the auditory range. Perimeter, surface, hydraulic diameter, Womersley and Reynolds numbers were computed every 45° of rotation around the central axis of the cochlear spiral. CFD results showed both spatial and temporal pressure gradients along the cochlea. Small Reynolds number and large Womersley values indicate that the perilymph fluid flow at auditory frequencies is laminar and its velocity profile is plug-like. The pressure was found 102–106° out of phase with the fluid flow velocity at the scalae vestibule and tympani, respectively. The average flow velocity was found in the sub-µm/s to nm/s range at 20–100 Hz, and below the nm/s range at 1–20 kHz.     

Glycoprotein import: A common feature of complex plastids?

Complex plastids evolved by secondary endosymbiosis and are, in contrast to primary plastids, surrounded by 3 or 4 envelope membranes. Recently, we provided evidence that in diatoms proteins exist that get N-glycosylated during transport across the outermost membrane of the complex plastid. This gives rise to unique questions on the transport mechanisms of these bulky proteins, which get transported across up to 3 further membranes into the plastid stroma. Here we discuss our results in an evolutionary context and speculate about the existence of plastidal glycoproteins in other organisms with complex plastids.     

Dioxovanadium(V) and μ-oxo bis[oxovanadium(V)] complexes containing thiosemicarbazone based ONS donor set and their antiamoebic activity

Neutral dioxovanadium (V) complexes [VO₂(HL)] (H₂L = I: 1, H₂L = II: 2 and H₂L = III: 3; H₂L are the thiosemicarbazones H₂pydx-tsc (I), H₂pydx-chtsc (II) and H₂pydx-clbtsc (III); pydx = pyridoxal, tsc = thiosemicarbazide, chtsc = N₄-cyclohexylthiosemicarbazide, clbtsc = N₄-(2-chloro)benzylthiosemicarbazide) have been isolated and characterised on the basis of elemental and electrochemical analyses, spectroscopic (IR, UV-Vis, ¹H and ⁵¹V NMR) data, thermogravimetric studies and reactivity patterns. These complexes are stable in solution at ambient temperature but heating of the methanolic solutions yields the μ-oxo binuclear complexes [(VOL)₂μ-O] (H₂L = I: 4, H₂L = II: 5, H₂L = III: 6). Treatments of dioxo species with H₂O₂ yield oxoperoxo species, the formations of which have been established spectrophotometrically. Similarly, the formations of oxohydroxo species, an intermediate proposed during the catalytic action of haloperoxidases, have also been established in solution by treating 1, 2 and 3 with a methanolic solution of HCl. The antiamoebic activities were carried out to ascertain the effectiveness of dioxovanadium(V) and μ-oxobis(oxovanadium(V)) complexes in comparison to their corresponding thiosemicarbazones. These complexes possess noteworthy potencies against HM1:1MSS strain of Entamoeba histolytica. Complexes 2, 3, 5 and 6 showed less IC₅₀ values than metronidazole, indicating that these metal thiosemicarbazones may be the lead molecules to inhibit the growth of E. histolytica. Within the series, complex 5 showed the most promising amoebicidal activity (IC₅₀ = 0.5 μM versus IC₅₀ = 1.8 of metronidazole).     

Studies on metal-drug complexes. Crystal structure and characterization of μ-sulfato bromazepam copper(II) complex

The compound Cu(Bromazepam) SO₄ having been synthesized, its crystal structure shows distorted octahedral environment for the Copper(II) ion. Because of the long Cu-O(4) length (2.90 Å), we can consider that there is a semicoordinative interaction with the sulfate group acting as tridentate bridging ligand. The structure is a polymeric chain where dimeric units are linked by the oxygen (C-O(5)) atom of the Bromazepam carbonyl group. The drug consequently acts as a tridentate ligand in this compound. The magnetic results show a very weak antiferromagnetic interaction.     

What is complex about complex disorders?

Rather than being polygenic, complex disorders probably represent umbrella terms for collections of conditions caused by rare, recent mutations in any of a large number of different genes.     

Synthesis and structure of an oxidation product of hemiporphyrazinatoiron(II): Monoaquo-μ-oxo-bis(hemiporphyrazinato)iron(III). A linear μ-oxo dimer containing six- and five-coordinated iron atoms

The interaction between dioxygen and wer N-base solutions of Fe(II) hemiporphyrazine (Fehp) leads to the title compound, which is a high-spin antiferromagnetically coupled iron(III) complex. The crystal and molecular structure has been determined by X-rays. The unit cell is the tetragonal space group P4/ncc, with a=b=19.083(5) and c=23.509(5) Å. 2141 unique observed reflections were used in the analysis, and the final conventional R is 0.059. The structure consists of Fe(III)hp μ-oxo dimers having strictly linear FeOFe units and a nearly eclipsed internal configuration. This is the first observation of the formation of a mono-adduct in μ-oxo dimer via axial coordination of a H₂O molecule. The resulting asymmetric dimer, H₂OFeAhpOFeBhp contains a six-coordinated Fe atom (FeA) lying in the plane of the four Ns of the macrocycle. The second Fe atom (FeB) is five-coordinated and lies outside of the coordination plane by 0.45 Å. The FeO distances are: FeAO=1.782(7) Å and FeBO=1.739(7) Å. The axial coordination of the water (FeAO_w=2.210(9) Å) seems weak, probably due to the labilising trans influence of the μ-oxo ligand. The dimers are paired coaxially to form tetramers, which are in turn connected via a two- dimensional net of hydrogen bonds. The structural results are correlated with spectroscopic, thermogravimetric and magnetic properties.