Hydrosilylation of BB triple bonds: catalyst- and reductant-free construction of B-Si bonds and B2Si heterocycles.

Hydrosilanes undergo mild, uncatalyzed single and double 1,2-addition across the B-B triple bonds of diborynes, leading to an unsymmetrical silyldiborene and compounds with novel non-cluster three-membered B2Si rings. The reactions are a new addition to the very few catalyst- and alkali-metal-free methods available for the construction of B-Si bonds.

Synthesis and hydrogenation of polycyclic aromatic hydrocarbon-substituted diborenes via uncatalysed hydrogenative B-C bond cleavage.

The classical route to the PMe3-stabilised polycyclic aromatic hydrocarbon (PAH)-substituted diborenes B2Ar2(PMe3)2 (Ar = 9-phenanthryl 7-Phen; Ar = 1-pyrenyl 7-Pyr) via the corresponding 1,2-diaryl-1,2-dimethoxydiborane(4) precursors, B2Ar2(OMe)2, is marred by the systematic decomposition of the latter to BAr(OMe)2 during reaction workup. Calculations suggest this results from the absence of a second ortho-substituent on the boron-bound aryl rings, which enables their free rotation and exposes the B-B bond to nucleophilic attack. 7-Phen and 7-Pyr are obtained by the reduction of the corresponding 1,2-diaryl-1,2-dichlorodiborane precursors, B2Ar2Cl2(PMe3)2, obtained from the SMe2 adducts, which are synthesised by direct NMe2-Cl exchange at B2Ar2(NMe2)2 with (Me2S)BCl3. The low-lying π* molecular orbitals (MOs) located on the PAH substituents of 7-Phen and 7-Pyr intercalate between the B-B-based π and π* MOs, leading to a relatively small HOMO-LUMO gap of 3.20 and 2.72 eV, respectively. Under vacuum or at high temperature 7-Phen and 7-Pyr undergo intramolecular hydroarylation of the B[double bond, length as m-dash]B bond to yield 1,2-dihydronaphtho[1,8-cd][1,2]diborole derivatives. Hydrogenation of 7-Phen, 7-Pyr and their 9-anthryl and mesityl analogues III and II, respectively, results in all cases in splitting of the B-B bond and isolation of the monoboranes (Me3P)BArH2. NMR-spectroscopic monitoring of the reactions, solid-state structures of isolated reaction intermediates and computational mechanistic analyses show that the hydrogenation of the three PAH-substituted diborenes proceeds via a different pathway to that of the dimesityldiborene. Rather than occurring exclusively at the B-B bond, hydrogenation of 7-Ar and III proceeds via a hydroarylated intermediate, which undergoes one B-B bond-centered H2 addition, followed by hydrogenation of the endocyclic B-C bond resulting from hydroarylation, making the latter effectively reversible.

Azide-alkyne cycloadditions with an electronically activated alkyne: indole formation via 1-aryl-1,2,3-triazole-derived imino carbenes.

We report that the use of a diaminoalkyne in the azide-alkyne cycloaddition with aryl azides leads to 3H-indoles under mild, uncatalysed conditions. Computations reveal that N2 extrusion from, in one case, isolable triazoles is facile, generating imino carbenes, which undergo intramolecular aryl C-H bond activation and give 3H-indoles as products.

Rhodium-Mediated Stoichiometric Synthesis of Mono-, Bi-, and Bis-1,2-Azaborinines: 1-Rhoda-3,2-azaboroles as Reactive Precursors.

A series of highly substituted 1,2-azaborinines, including a phenylene-bridged bis-1,2-azaborinine, was synthesized from the reaction of 1,2-azaborete rhodium complexes with variously substituted alkynes. 1-Rhoda-3,2-azaborole complexes, which are accessible by phosphine addition to the corresponding 1,2-azaborete complexes, were also found to be suitable precursors for the synthesis of 1,2-azaborinines and readily reacted with alkynyl-substituted 1,2-azaborinines to generate new regioisomers of bi-1,2-azaborinines, which feature directly connected aromatic rings. Their molecular structures, which can be viewed as boron-nitrogen isosteres of biphenyls, show nearly perpendicular 1,2-azaborinine rings. The new method using rhodacycles instead of 1,2-azaborete complexes as precursors is shown to be more effective, allowing the synthesis of a wider range of 1,2-azaborinines.

Synthesis and characterisation of boranediyl- and diboranediyl-bridged diplatinum A-frame complexes.

A series of boranediyl-bridged diplatinum A-frame complexes, [Pt2X2(µ-BY)(µ-dmpm)2] (X = Cl, Br, I; Y = aryl, alkyl, amino, halo; dmpm = bis(dimethylphosphino)methane), were synthesised by the twofold oxidative addition of BX2Y to [Pt2(nbe)2(µ-dmpm)2] (nbe = norbornene) or to the paddlewheel complex [Pt2(µ-dmpm)3]. Similarly, the addition of B2X2(NMe2)2 (X = Cl, Br) to [Pt2(nbe)2(µ-dmpm)2] provided access to the diborane-1,2-diyl-bridged A-frame complexes [Pt2X2(µ-1,2-B2(NMe2)2)(µ-dmpm)2]. X-ray crystallographic studies of these (BY)n-bridged complexes show structural trends depending on the steric demands of Y and the nature of X. Analysis of higher-order 31P NMR satellites provided information on JP-Pt and JPt-Pt coupling constants, the latter correlating with the PtPt distance. All (di)boranediyl complexes also proved unstable towards (successive) loss of the bridging "BY" unit(s), resulting in the formation of [Pt2X2(µ-dmpm)2].

Synthesis of Boron Analogues of Enamines via Hydroamination of a Boron-Boron Triple Bond.

An N-heterocyclic-carbene-stabilized diboryne undergoes rapid, high-yielding and catalyst-free hydroamination reactions with primary amines, yielding 1-amino-2-hydrodiborenes, which can be considered boron analogues of enamines. The electronics of the organic substituent at nitrogen influence the structure and further reactivity of the diborene product. With electron-rich anilines, a second hydroamination can occur at the diborene to generate 1,1-diamino-2,2-dihydrodiboranes. With isopropylamine, the electronic influence of the alkyl substituent upon the diborene leads to an unprecedented boron-mediated intramolecular N-dearylation reaction of an N-heterocyclic carbene unit.

Distribution and Cytokine Profile of Peripheral B Cell Subsets Is Perturbed in Pediatric IBD and Partially Restored During a Successful IFX Therapy.

BACKGROUND: The role of B cells in inflammatory bowel disease (IBD) is ambiguous, as B cells may have both pathogenic and protective functions in IBD. We studied B cell subsets before and after initiation of an anti-tumor necrosis factor alpha (anti-TNFα) therapy in pediatric IBD. The aim of the study was to examine the behavior of B cells in pediatric IBD patients undergoing an anti-TNFα therapy and, more specifically, to clarify their association with a successful or an unsuccessful infliximab (IFX) treatment. METHODS: A total of N = 42 pediatric IBD patients (Crohn disease, n = 30; ulcerative colitis, n = 12) for whom an anti-TNFα therapy with and without a concomitant azathioprine (AZA) medication was administered were recruited. Fourteen healthy age-matched children served as control patients. Blood samples were collected before initiation of the anti-TNFα therapy, before the fourth infusion at the end of the induction phase, and after 6 and 12 months under therapy maintenance. Flow cytometry (CD20, CD27, CD38, CD138) and intracellular staining (interleukin 10 [IL10], TNFα, granzyme B) were performed. Responders to successful IFX therapy were classified exhibiting a fecal calprotectin level of below 100 µg/g or achieving levels of <10% of the baseline value at initiation than at the end of the 12-month follow-up period. RESULTS: Before initiation of anti-TNFα therapy, flow cytometry revealed increased percentages of naïve B cells whereas transitional B cells were reduced compared with those in the healthy control patients. The IL10-producing B cells of both ulcerative colitis and Crohn disease patients were reduced at the initiation of IFX therapy, whereas TNFα-producing transitional CD24hiCD38hi B cells in ulcerative colitis patients were increased compared with those in healthy control patients. After 12 months of therapy, we detected a significant increase of IL10-producing transitional B cells in responding patients.The IFX trough levels in the responding patients showed a significant increase until 6 months after IFX initiation, attaining mean values of 9.9 µg/mL, whereas the IFX dosage was significantly lower than that in the nonresponding patients. The IFX trough levels in AZA-treated patients reached earlier therapeutic levels than in patients without AZA comedication, whereas during the course of the IFX therapy, comedication with AZA had no significant effect on the outcome. CONCLUSIONS: Attaining a normalization of IL10 production among CD24hiCD38hi B cells after 12 months of therapy may represent additional information about the reconstitution of a patient's immune system in responding patients. The achievement of an IFX trough level of ~10 µg/mL at 6 months of treatment is associated with a successful anti-TNFα therapy. In addition, AZA comedication supports an earlier achievement of therapeutic IFX trough levels.

Diverse ring-opening reactions of rhodium η4-azaborete complexes.

Sequential treatment of [Rh(COE)2Cl]2 (COE = cyclooctene) with PiPr3, alkyne derivatives and t BuN[triple bond, length as m-dash]BMes (Mes = 2,4,6-trimethylphenyl) provided functionalized rhodium η4-1,2-azaborete complexes of the form (η4-azaborete)RhCl(PiPr3). The scope of this reaction was expanded to encompass alkynes with hydrogen, alkyl, aryl, ferrocenyl, alkynyl, azaborinyl and boronate ester substituents. Treatment of these complexes with PMe3 led to insertion of the rhodium atom into the B-C bond of the BNC2 ring, forming 1-rhoda-3,2-azaboroles. Addition of N-heterocyclic carbenes to azaborete complexes led to highly unusual rearrangements to rhodium η2,κ1-allenylborylamino complexes via deprotonation and C-N bond cleavage. Heating and photolysis of an azaborete complex also led to rupture of the C-N bond followed by subsequent rearrangements, yielding an η4-aminoborylallene complex and two isomeric η4-butadiene complexes.

Single and Double Hydroboration of B-B Triple Bonds and Convergent Routes to a Cationic Tetraborane.

A compound with a boron-boron triple bond is shown to undergo stepwise hydroboration reactions with catecholborane to yield an unsymmetrical hydro(boryl)diborene and a 2,3-dihydrotetraborane. Abstraction of H- from the latter compound produces an unusual cationic, planar tetraborane with a hydrogen atom bridging the central B2 moiety. Spectroscopic and crystallographic data and DFT calculations support a "protonated diborene" structure for this compound, which can also be accessed via direct protonation of the corresponding diborene.

Synthesis of fused B,N-heterocycles by alkyne cleavage, NHC ring-expansion and C-H activation at a diboryne.

The addition of alkynes to a saturated N-heterocyclic carbene (NHC)-supported diboryne results in spontaneous cycloaddition, with complete B[triple bond, length as m-dash]B and C[triple bond, length as m-dash]C triple bond cleavage, NHC ring-expansion and activation of a variety of C-H bonds, leading to the formation of complex mixtures of fused B,N-heterocycles.

Isolation of diborenes and their 90°-twisted diradical congeners.

Molecules containing multiple bonds between atoms-most often in the form of olefins-are ubiquitous in nature, commerce, and science, and as such have a huge impact on everyday life. Given their prominence, over the last few decades, frequent attempts have been made to perturb the structure and reactivity of multiply-bound species through bending and twisting. However, only modest success has been achieved in the quest to completely twist double bonds in order to homolytically cleave the associated π bond. Here, we present the isolation of double-bond-containing species based on boron, as well as their fully twisted diradical congeners, by the incorporation of attached groups with different electronic properties. The compounds comprise a structurally authenticated set of diamagnetic multiply-bound and diradical singly-bound congeners of the same class of compound.

Highly Strained Heterocycles Constructed from Boron-Boron Multiple Bonds and Heavy Chalcogens.

The reactions of a diborene with elemental selenium or tellurium are shown to afford a diboraselenirane or diboratellurirane, respectively. These reactions are reminiscent of the sequestration of subvalent oxygen and nitrogen in the formation of oxiranes and aziridines; however, such reactivity is not known between alkenes and the heavy chalcogens. Although carbon is too electronegative to affect the reduction of elements with lower relative electronegativity, the highly reducing nature of the B-B double bond enables reactions with Se(0) and Te(0) . The capacity of multiple bonds between boron atoms to donate electron density is highlighted in reactions where diborynes behave as nucleophiles, attacking one of the two Te atoms of diaryltellurides, forming salts consisting of diboratellurenium cations and aryltelluride anions.