C-ansa-zirconocene complexes with O/S donor ligands: Novel homoleptic six coordinate 4-mercaptophenolate complex of Zr(IV)

New C-ansa-zirconocene complexes containing methoxythiophenolate and mercaptophenolate ligands have been synthesized and characterized. The reaction of (HSC₆H₄-n-OMe) (n = 2, 3 or 4) with [Zr{(t-Bu)HC(η⁵-C₅Me₄)(η⁵-C₅H₄)}Me₂] (1) led to the formation of monosubstituted complexes [Zr{(t-Bu)HC(η⁵-C₅Me₄)(η⁵-C₅H₄)}Me(κ,S-SC₆H₄-n-OMe)] (n = 2 (2); n = 3 (3)) and the disubstituted complex [Zr{(t-Bu)HC(η⁵-C₅Me₄)(η⁵-C₅H₄)}(κ,S-SC₆H₄-4-OMe)₂] (4). The complexes [Zr{(R)HC(η⁵-C₅Me₄)(η⁵-C₅H₄)}(κ,O-OC₆H₄-4-SH)₂] (R = t-Bu (6); R = CH₂CHCH₂ (7)) and [Zr(η⁵-C₅H₄)₂(OC₆H₄-n-SH)₂] (n = 3 (9); n = 4 (10)) have been synthesized using the corresponding dimethyl zirconocene and mercaptophenol. However, the reaction of [Zr{(t-Bu)HC(η⁵-C₅Me₄)(η⁵-C₅H₄)}Cl₂] (11) with 4-mercaptophenol in the presence of NEt₃ led to the formation of the first example of a homoleptic six-coordinate mercaptophenolate complex of zirconium, namely [HNEt₃]₂[Zr(κ,O-OC₆H₄-4-SH)₆] (12). Complex 12 can be obtained in higher yield by the reaction of ZrCl₄ with six equivalents of 4-mercaptophenol and NEt_3. The reaction of 12 with [Zr(η⁵-C₅H₄)₂Cl₂] gave the unexpected disubstituted complex [Zr(η⁵-C₅H₄)₂(OC₆H₄-4-SH)₂] (10). The molecular structures of 4 and 12 have been determined by single-crystal X-ray diffraction studies.     

Acid activation of titanium alkoxide systems - Structural characterisation of Ti(IV) sulfonyl-imide complexes

Treatment of [Ti(OⁱPr)₄] with the sulfonyl-imine systems Tos₂NH ([(p-Me-C₆H₄SO₂)₂NH]) and Tf₂NH ([(CF₃SO₂)₂NH]) results in the formation of the new Lewis acidic titanium sulfonyl-imide complexes [Ti(OⁱPr)₂(O,O′-Tos₂N)₂] (1) and [Ti(OⁱPr)₂(HOⁱPr)₂(O-Tf₂N)₂] (2), respectively. The molecular structures of the complexes have been determined by single crystal X-ray diffraction. The reaction of [Ti(OⁱPr)₃(OAr)] (Ar = 2,6-di-tert-butyl-4-methyl phenyl) with Tf₂NH results in the formation of the dimeric complex [Ti(OⁱPr)₃(O,O′-Tf₂N)]₂ (3), which has also been structurally characterised. The ability of the complexes to catalyst the Friedel-Crafts acylation of anisole has also been assessed.     

Heteroaromatic substituted diimidosulfinates

Coupling of two diimidosulfinate units via a conjugated organic substituent to facilitate electronic communication between the two S(NR)₂-moieties seems advantageous because polyimido sulfur compounds are exposed to SET processes. The coupling might facilitate electron transport. In this paper we present the syntheses and crystal structures of the heteroaromatic S-substituted metal diimidosulfinates [(thf)Li₂{(H₃CNC₄H₃)S(N^tBu)₂}₂] (1), [(tmeda)Li{(SC₈H₅)S(N^tBu)₂}] (2), [Fe{(SC₈H₅)S(N^tBu)₂}₂] (3), and [Cu{(SC₈H₅)S(N^tBu)₂}]₂ (4), as potential starting materials. As the structural investigation shows that electronic communication between the S(NR)₂-moiety and a S-bonded conjugated organic substituent is only feasible when the aromatic perimeter is arranged strictly in-plane to one S-N bond as observed in 1. Here the ring nitrogen atom is blocked against metal coordination. In the other complexes in-plane arrangement of the S-heteroaromatic substituent is precluded even by very weak metal coordination of the ring sulfur atom. The (N,N)-chelating lithium (2) and iron (3) coordination forces the ring in a more or less orthogonal arrangement relative to the SN₂-plane. The ring-S?copper coordination in 4, which could have forced the heteroarene ring into the plane of one S-N bond, apparently is to weak to turn the ring about the S-C(sp²) bond.     

Reactivity of the bridged borylene complex [μ-BCl{η-C5H4Me)Mn(CO)2}2]

The reactivity of the bridged chloro borylene complex [μ-BCl{(η⁵-C₅H₄Me)Mn(CO)₂}₂] (2a) towards various protic reagents was studied. Reaction of 2a with isopropanol yielded the alkoxy borylene complex [μ-BOiPr{(η⁵-C₅H₄Me)Mn(CO)₂}₂] (3d) in very high yield. A further series of protic reagents HX (X=HS⁻, BF₄⁻, Co(CO)₄⁻) gave, in the presence of pyridine, the new amino borylene complex [1-(μ-B)-4-H-(NC₅H₅){(C₅H₄Me)Mn(CO)₂}₂] (5a), which represents the product of an unprecedented 1,4-hydroboration of pyridine. Complex 5a was fully characterised in solution by multinuclear NMR studies, in the solid state by X-ray diffraction, and was also subject to DFT-studies.     

Calix[4]arene supported group 5 imido complexes

The reaction of imidoyl chlorides [V(NR)Cl₃] (R = Ph 1, Tol 2, tBu 3) and calix[4]arene methyl ether H₃Mecalix unexpectedly leads to the formation of the structurally characterized vanadium (IV) complex [VCl(Mecalix)] (4). Calix[4]arene methyl ether stabilized imido complexes of the type [V(NR)(Mecalix)] (R = Ph 7, Tol 8, tBu 9) were afforded from the reaction of [V(NR)Cl₃] (R = Ph 1, Tol 2, tBu 3) and the tris(lithium) or tris(sodium) salt of the calix[4]arene ether. The lithium salt [{Li₃(Mecalix)}₂] (5) is a dimer in the solid state, in which two monomeric trianions are bridged by lithium cations. Imido complexes [M(NR)(Mecalix)] (M = Nb: R = tBu, 12, R = Tol 13, R = Mes 14, R = Dipp 15; M = Ta: R = tBu 16, R = Tol 17) (Tol = 4-C₆H₄Me, Mes = 2,6-C₆H₃Me₂; Dipp = 2,6-C₆H₃iPr₂) have been prepared from structurally characterized [NbCl₂(Mecalix)] (10) and previously known [TaCl₂(Mecalix)] (11) via reaction with two equivalents of the appropriately metallated (Li, K) primary amine. The molecular structures of 13 and 15 confirm the mononuclear nature of these complexes.     

Adduct formation of [(η-C7H7)Zr(η-C5H5)] with phosphines and N-heterocyclic carbenes: An experimental and theoretical study

The reaction of [(η⁷-C₇H₇)Zr(η⁵-C₅H₅)] with two Lewis bases, tetramethylimidazolin-2-ylidene and PMe₃, is reported and their stability probed via spectroscopic and theoretical methods. The strongly σ-basic N-heterocyclic carbene forms a stable adduct which has been structurally characterised, whilst the PMe₃ ligand coordinates weakly to the metal centre. Variable temperature ³¹P NMR spectroscopy has been used to determine the activation energy for this process (ΔG^‡ = 40.5 ± 1.9 kJ mol⁻¹). DFT calculations have been performed on both complexes and the structures discussed. In addition, the enthalpies for the formation of these compounds have been calculated [ΔH⁰(Zr-IMe) = −56.3 kJ mol⁻¹; ΔH⁰(Zr-PMe₃) = −2.3 kJ mol⁻¹] and show that the N-heterocyclic carbene forms a thermodynamically much more stable adduct than that with PMe₃.     

Functional Expression of TRPM8 and TRPA1 Channels in Rat Odontoblasts

Odontoblasts produce dentin during development, throughout life, and in response to pathological conditions by sensing stimulation of exposed dentin. The functional properties and localization patterns of transient receptor potential (TRP) melastatin subfamily member 8 (TRPM8) and ankyrin subfamily member 1 (TRPA1) channels in odontoblasts remain to be clarified. We investigated the localization and the pharmacological, biophysical, and mechano-sensitive properties of TRPM8 and TRPA1 channels in rat odontoblasts. Menthol and icilin increased the intracellular free Ca²⁺ concentration ([Ca²⁺]_i). Icilin-, WS3-, or WS12-induced [Ca²⁺]_i increases were inhibited by capsazepine or 5-benzyloxytriptamine. The increase in [Ca²⁺]_i elicited by allyl isothiocyanate (AITC) was inhibited by HC030031. WS12 and AITC exerted a desensitizing effect on [Ca²⁺]_i increase. Low-temperature stimuli elicited [Ca²⁺]_i increases that are sensitive to both 5-benzyloxytriptamine and HC030031. Hypotonic stimulation-induced membrane stretch increased [Ca²⁺]_i; HC030031 but not 5-benzyloxytriptamine inhibited the effect. The results suggest that TRPM8 channels in rat odontoblasts play a role in detecting low-temperature stimulation of the dentin surface and that TRPA1 channels are involved in sensing membrane stretching and low-temperature stimulation. The results also indicate that odontoblasts act as mechanical and thermal receptor cells, detecting the stimulation of exposed dentin to drive multiple cellular functions, such as sensory transduction.     

Hydrocortisone inhibits antigen-induced rise in intracellular free calcium concentration and abolishes leukotriene C4 production in leukemic basophils

Antigenic stimulation of rat basophilic leukemia cells (RBL-3H3) elevates intracellular free Ca²⁺ concentration ([Ca²⁺]_i) and induces production of leukotriene C₄ (LTC₄). This model was used to examine the role of Ca²⁺ in LTC₄ formation, and inhibition by hydrocortisone (HC). HC, at a physiological concentration (2×10⁻⁷M), selectively prevented the stimulatory effect of the antigen on LTC₄ production whereas the response to calcium inophore (A23187) remained unimpaired. The inhibition by HC was time-dependent: half maximal response was reached at 2 hour and maximal response at 3 hours. Addition of arachidonic acid (3 μg/ml) did not overcome the inhibitory action of HC. An elevated [Ca²⁺]_i is known to be essential for the activation ob both 5-lipoxygenase and phospholipase A₂. The stimulatory effect of the antigen on LTC₄ production was abolished when the cells were incubated in Ca²⁺-deficient medium. Likewise, calcium ionophore stimulation shows dependence on extracellular Ca²⁺. Half maximal stimulation by the antigen and calcium ionophore was observed at external Ca²⁺ concentration of 150 μM and 40 μM respectively. Treatment with HC largely prevented the antigen-induced rise in [Ca²⁺]_i, measured by Quin 2. In addition, HC reduced by 70% the accumulation of ⁴⁵Ca²⁺ induced by the antigen. Collectively, these results demonstrate for the first time that HC reduces antigen-induced elevation of [Ca²⁺]_i, and this may be associated with the inhibitory action of HC on LTC₄ formation. This property could be partly responsible for the antiallergic and antiinflammatory activities of HC.     

The mononuclear–dinuclear dance: Twisting the backbone in metalloligands operates a coordination switch

The copper(II) complex [Cu{(R,R)-1}] in which (R)-H₂1 is 1,6-bis(3-ethoxy-2-hydroxyphenyl)-(3R,4R)-(?)-cyclohexane-1,2-diyl-2,5-diazahexa-1,5-diene possesses an O₄-donor cavity that can bind Pb²⁺, Cd²⁺ and Eu³⁺. The single crystal structures of [Cu(OH₂){(R,R)-1}Pb(ONO₂)₂], {[Cu{(R,R)-1}Cd(ONO₂)(OH₂)₂][NO₃]^.MeOH}^.[Cu{(R,R)-1}] and [Cu{(R,R)-1}Eu(O₂NO)₃] are presented. The co-crystallization of [Cu{(R,R)-1}Cd(ONO₂)(OH₂)₂][NO₃] and [Cu{(R,R)-1}] appears to be driven by hydrogen-bonded host–guest interactions between each axial water ligand in [Cu{(R,R)-1}Cd(ONO₂)(OH₂)₂]⁺ with the O₄-domain of [Cu{(R,R)-1}]. When the ligand scaffold is changed from cyclohexane-1,2-diyl to 1,1′-binaphthyl to give (R)-H₂2, the N₂O₂-cavity is unable to bind copper(II) in its preferred square planar environment. The single crystal structure of [Zn{(R)-2}] confirms the presence of tetrahedral zinc(II). As a result, the spatial properties of the ethoxy arms in [Zn{(R)-2}] and [Cu{(R)-2}] are not suited to the facile formation of dimetallic complexes.     

Reaction of a rhodium(I) carbonyl complex of a para-dimethylaminophenyl substituted diphosphine with methyl iodide and hydrogen iodide

Reaction of [Rh(CO)₂](μ-Cl)]₂ with bis-1,2-(di{4-dimethylaminophenyl)phosphino-ethane (L) gives the monomeric Rh(I) complex of type cis-[RhCl(L)(CO)] that was separated from a side product of type [Rh(L)₂]Cl, and characterised by X-ray crystallography. This complex reacts with methyl iodide at high temperature to give the Rh(III) acetyl complex, [Rh(I)₂(C(O)Me)(L)], which was also structurally characterised by X-ray crystallography. There is no sign of quaternisation of the dimethylamino groups under these conditions. This complex is soluble in organic solvent and insoluble in the polar media used in methanol carbonylation (AcOH/H₂O/MeOH). However, in the presence of HI, this complex is readily soluble in AcOH/H₂O/MeOH, in contrast to [Rh(I)₂(C(O)Me)(dppe)] and most other Rh-acetyl complexes of diphosphine ligands.     

Synthesis of trifluoroborate functionalised imidazolium salts as precursors to weakly coordinating bidentate NHC ligands

A new class of trifluoroborate functionalised N-heterocyclic carbene precursors have been synthesised, isolated and characterised structurally. The ligands were obtained via a serendipitous one-pot reaction in which deprotection, cyclisation and fluorination of boryl-functionalised diarylethylenediamine derivatives occur concurrently. Deprotonation of the imidazolium salts was found to yield the free carbene, though 18-crown-6 was found necessary to prevent further reactivity of the resulting aryl potassium trifluoroborate salts; in the absence of 18-crown-6, elimination of KF resulted in a cyclic carbene-BF₂ arene adduct. Complexation to rhodium was facile, and yielded four-coordinate complexes in which the Rh-BF₃ interaction was determined by ¹⁹F NMR spectroscopy to be weak.     

Recombinant Human NMDA Homomeric NR1 Receptors Expressed in Mammalian Cells Form a High-Affinity Glycine Antagonist Binding Site

Abstract: The cDNA NMDAR1 (NR1) encodes a single polypeptide that forms a receptor-channel complex with electrophysiological and pharmacological properties characteristic of the N-methyl-d -aspartate receptor. Homomeric NR1 recombinant receptors expressed in Xenopus oocytes show functional responses with low levels of conductance. In this study we have characterized, by radioligand binding techniques, the pharmacological properties of homomeric receptors of two human NR1 isoforms (NR1a and NR1e, which differ in their C-terminal region), transiently expressed in human embryonic kidney 293 cells. The glycine site antagonist (±)-4-(trans)-2-carboxy-5,7-dichloro-4-[³H]phenylaminocarbonylamino-1,2,3,4-tetrahydroquinoline ([³H]L-689,560) bound to NR1a- and NR1e-transfected cells with high affinity (K_D = 3.29 and 1.61 nM, respectively). B_max values for NR1a- and NR1e-transfected cells were 3.82 and 1.69 pmol/mg of protein, respectively, and Hill coefficients were close to unity. K_i values for glycine site antagonists inhibiting [³H]L-689,560 binding to NR1e-transfected cells were similar to those observed with rat brain membranes. Affinity values for agonists and partial agonists were four- to 16-fold weaker, indicating that the glycine site of homomeric NR1 receptors is in an antagonist-preferring state. K_i values obtained with NR1a-transfected cells were approximately twofold lower than those obtained with NR1e-transfected cells. High-affinity binding to NR1-transfected cells was not observed with the transmitter recognition site radioligands l -[³H]glutamate and d,l -(ε)-2-[³H]amino-4-propyl-5-phosphono-3-pentanoic acid ([³H]CGP-39653) or the ion-channel radioligand [³H]dizocilpine ([³H]MK-801). These results indicate that although transfection of mammalian cells with homomeric NR1 recombinant receptors does not appear to result in functional receptors, a glycine binding site is formed that may have a physiological role if present in vivo.     

Imidazolium formation from the reaction of N-heterocyclic carbene stabilised group 13 trihydride complexes with organic acids

The reactions of the N-heterocyclic carbene (NHC) stabilised group 13 trihydride complexes [AlH₃(IMeMe)] (1) (IMeMe = 1,3,4,5-tetramethylimidazol-2-ylidene), [AlH₃(IⁱPrMe)] (2) (IⁱPrMe = 1,3-diisopropyl-4,5-dimethylimidazol-2-ylidene) with three molar equivalents of phenol, and [InH₃(IMes)] (3) (IMes = 1,3-bis(2,4,6-trimethylphenyl)imidazole-2-ylidene) with one molar equivalent of 1,1,1,5,5,5-hexafluoropentan-2,4-dione (F₆acacH) are presented. These render the imidazolium tetraphenoxyaluminate species; [IMeMe · H][Al(OPh)₄] (4) and [IⁱPrMe · H][Al(OPh)₄] (5), and 1,3-bis(2,4,6-trimethylphenyl)imidazolium 1,1,1,5,5,5-hexafluoropentan-2,4-dionate; [IMes · H][CH{C(O)CF₃}₂] (6), the latter leading to metallohydride decomposition. The molecular structures of 4 and 6 are described.     

Imidazole,imidazolate, and hydroxide complexes of (protoporphyrin IX)iron(III) and its dimethyl ester as model systems for ferric hemoproteins: Electron paramagnetic resonance and electronic spectral study

The EPR and electronic spectral changes upon titration of systems consisting of (protoporphyrin IX)iron(III) chloride (Fe(PPIX)Cl) or its dimethyl ester (Fe-(PPIXDME)Cl) and imidazole derivatives with tetrabutylammonium hydroxide solution have been measured at 77 and 298 °K in various solvents. The EPR and electronic spectra of the melt of Fe(PPIXDME)Cl in imidazole derivatives have been also measured. The imidazole derivatives studied here were imidazole and 4-methyl-, 4-phenyl-, 2-methyl-, 2,4-dimethyl-, 1-methyl-, and 1-acetylimidazole. The spectral changes upon addition of hydroxide were markedly different between the systems containing NH imidazoles (BH), with a dissociable proton, and those containing NR imidazoles (BR), without it. In the former systems, five spectral species were successively formed at 77 °K and were assigned to following complexes: [Fe(P)(BH)₂]⁺, Fe(P)(BH)(B), [Fe(P)(B)₂]^?, Fe(P)(BH)(OH), and [Fe(P)(B)(OH)]^?, where P is PPIX or PPIXDME. In the latter systems, initial complex, [Fe(P)(BR)₂]⁺, was found to be changed to final complex, Fe(P)(BR)(OH), through an intermediate at 77 °K. At 298 °K, both systems were found to react with hydroxide to finally form Fe(P)(OH). The crystal field parameters were evaluated using the EPR g values in low-spin complexes studied here and in hemoproteins. The five regions corresponding to five low-spin complexes could be distinguished in crystal field diagrams.     

Synthesis and characterization of yttrium complexes bearing a bulky arylamido ancillary ligand

Reaction of anhydrous YCl₃ with 1 equiv. of arylamido lithium 2,6-ⁱPr₂C₆H₃NSiⁱPr₃Li in THF gave an anionic mono-arylamido-ligated yttrium dichloride complex {[2,6-ⁱPr₂C₆H₃NSiⁱPr₃]YCl₂(THF)}₂[LiCl(THF)₂] (1). Alkylation of 1 with 4 equiv. of LiCH₂SiMe₃ afforded an anionic arylamido-ligated yttrium tris(alkyl) complex [2,6-ⁱPr₂C₆H₃NSiⁱPr₃]Y(CH₂SiMe₃)₃Li(THF)₂ (2). Both complexes were characterized by NMR, elementary analysis, and X-ray structural determination.     

Methyl- and propylacetamidinates of lanthanides: Structures, catalytic and some physical properties

The acetamidinates {[MeNC(Me)NMe]₂Ln}₂[μ-η²-η²-MeNC(Me)NMe]₂ (Ln = Y (1), Dy (2)) and {[PrⁿNC(Me)NPrⁿ]₂Y}₂[μ-η²-η²-PrⁿNC(Me)NPrⁿ]₂ (3) have been prepared by the reactions of amides Ln[N(SiMe₃)₂]₃ with respective N,N′-disubstituted amidines MeNC(Me)NHMe or PrⁿNC(Me)NHPrⁿ. The reaction of Er[N(SiMe₃)₂]₃ with excess of monosubstituted amidine HNC(Me)NHPrⁱ or in a ratio of 1:2 resulted in the formation of compound {Er[NC(Me)NHPrⁱ]₃}_x (4). The same reaction with 1:1 ratio yielded heteroleptic complex {Er[N(SiMe₃)₂]₂[NC(Me)NHPrⁱ]}_x (5). The complexes 1, 2 and 3 have similar structures and contain four terminal and two μ-η²:η²-N,N-bridging amidinate groups binding the metal atoms. Volatility of 1, 2 and 3 is comparable to that of known monomeric La[PrⁱNC(R)NPrⁱ]₃. Compound 1 efficiently catalyzes the ring-opening polymerization of rac-lactide to give polylactide with M_n 53 085 and polydispersity 1.84.     

The Polarized Effect of Intracellular Calcium on the Renal Epithelial Sodium Channel Occurs as a Result of Subcellular Calcium Signaling Domains Maintained by Mitochondria

The renal epithelial sodium channel (ENaC) provides regulated sodium transport in the distal nephron. The effects of intracellular calcium ([Ca²⁺]_i) on this channel are only beginning to be elucidated. It appears from previous studies that the [Ca²⁺]_i increases downstream of ATP administration may have a polarized effect on ENaC, where apical application of ATP and the subsequent [Ca²⁺]_i increase have an inhibitory effect on the channel, whereas basolateral ATP and [Ca²⁺]_i have a stimulatory effect. We asked whether this polarized effect of ATP is, in fact, reflective of a polarized effect of increased [Ca²⁺]_i on ENaC and what underlying mechanism is responsible. We began by performing patch clamp experiments in which ENaC activity was measured during apical or basolateral application of ionomycin to increase [Ca²⁺]_i near the apical or basolateral membrane, respectively. We found that ENaC does indeed respond to increased [Ca²⁺]_i in a polarized fashion, with apical increases being inhibitory and basolateral increases stimulating channel activity. In other epithelial cell types, mitochondria sequester [Ca²⁺]_i, creating [Ca²⁺]_i signaling microdomains within the cell that are dependent on mitochondrial localization. We found that mitochondria localize in bands just beneath the apical and basolateral membranes in two different cortical collecting duct principal cell lines and in cortical collecting duct principal cells in mouse kidney tissue. We found that inhibiting mitochondrial [Ca²⁺]_i uptake destroyed the polarized response of ENaC to [Ca²⁺]_i. Overall, our data suggest that ENaC is regulated by [Ca²⁺]_i in a polarized fashion and that this polarization is maintained by mitochondrial [Ca²⁺]_i sequestration.     

Changes in calmodulin immunocytochemical localization associated with capacitation and acrosomal exocytosis of ram spermatozoa

The aim of this study was to determine the localization of calmodulin (CaM) in ram sperm and the possible changes during in vitro capacitation (CA) and the ionophore-induced acrosome reaction (AR). Likewise, changes in intracellular calcium levels ([Ca²⁺]_i) were also analysed by using flow cytometry. CA was induced in vitro in a medium containing BSA, CaCl₂, NaHCO₃, and AR by the addition of the calcium ionophore A23187. The acrosomal status was assessed by the chlortetracycline-fluorescence (CTC) assay. Flow cytometry (FC) analyses were performed by loading samples with Fluo-3 AM, that emits fluorescence at a high [Ca²⁺]_i, combined with propidium iodide (PI) that allowed us to discriminate sperm with/without an integral plasma membrane both with high/low [Ca²⁺]_i. Immunocytochemistry localized CaM to the flagellum, and some sperm also contained CaM in the head (equatorial and post-acrosomal regions). CA and AR resulted in a slight increase in the post-acrosomal labelling. The treatment of sperm with increasing concentrations of two CaM antagonists, W7 and calmidazolium (CZ), accounted for an increase in capacitated and acrosome-reacted CTC-sperm patterns. CZ induced a significant reduction in the content of three protein tyrosine-phosphorylated bands of approximately of 30, 40 and 45 kDa. However, W7 showed no significant effect at any of the studied concentrations. Neither of them significantly influenced protein serine and threonine phosphorylation. FC analysis revealed that the main subpopulation in the control samples contained 70% of the total sperm with integral plasma membrane and a medium [Ca²⁺]_i. After CA, 67.1% of the sperm preserved an integral membrane with a higher [Ca²⁺]_i. After AR, only 7.2% of the total sperm preserved intact membranes with a very high [Ca²⁺]_i. These results imply that CaM appears to be involved in ram sperm capacitation, and both treatments increased its localization in the post-acrosomal region.     

Synthesis and spectroscopic investigations of four-coordinate nickel complexes supported by a strongly donating scorpionate ligand

Two four-coordinate nickel complexes, HB(^tBuIm)₃NiBr and HB(^tBuIm)₃NiNO, were prepared by reaction of a bulky tris(carbene)borate ligand with NiBr₂(PPh₃)₂ and NiBr(NO)(PPh₃)₂, respectively, and structurally and spectroscopically characterized. In addition to standard techniques, high-frequency and -field electron paramagnetic resonance (HFEPR) was employed to understand the spin triplet (S = 1) ground state of the bromo complex. HFEPR, combined with electronic absorption spectroscopy allows comparison of this novel complex with other paramagnetic four-coordinate Ni(II) species. The tris(carbene)borate ligand is a stronger σ-donor than corresponding tris(pyrazolyl)borates (traditional “scorpionate” ligands). The tris(carbene)borate ligand may also act as a π-acceptor, in contrast to tris(pyrazolyl)borates, which show relatively little π-bonding interactions. The influence of tris(carbene)borate substituents on the donor strength of the ligand have been elucidated from IR spectroscopic investigations of {NiNO}¹⁰ derivatives. HFEPR spectra of HB(^tBuIm)₃NiBr exhibit hyperfine coupling from Br, which indicates the strong electronic interaction between Ni(II) and this halide ligand, consistent with studies on tris(pyrazolyl)borate Ni(II) complexes.