Cyclometalated Iridium(III)–Polyamine Complexes with Intense and Long‐Lived Multicolor Phosphorescence: Synthesis,Crystal Structure,Photophysical Behavior,Cellular Uptake,and Transfection Properties

A new class of phosphorescent cyclometalated iridium(III)–polyamine complexes [{Ir(N^C)₂}_n(bPEI)](PF₆)_n (bPEI=branched poly(ethyleneimine), average M_w=25 kDa, n=15.6–27.4; HN^C=2‐phenylpyridine Hppy ( 1 a ), 2‐((1,1′‐biphenyl)‐4‐yl)pyridine Hpppy ( 2 a ), 2‐phenylquinoline Hpq ( 3 a ), 2‐phenylbenzothiazole Hbt ( 4 a ), 2‐(1‐naphthyl)benzothiazole Hbsn ( 5 a )) and [Ir(N^C)₂(en)](PF₆) (en=ethylenediamine; HN^C=Hppy ( 1 b ), Hpppy ( 2 b ), Hpq ( 3 b ), Hbt ( 4 b ), Hbsn ( 5 b )) have been synthesized and characterized. The X‐ray crystal structure of complex 5 b was also determined. All of these complexes showed a reversible iridium(IV/III) oxidation couple at +1.01 to +1.26 V and a quasi‐reversible ligand‐based reduction couple at ?1.54 to ?2.08 V (versus SCE). Upon photoexcitation, the complexes displayed intense and long‐lived green to orange–red emission in fluid solutions at room temperature and in low‐temperature glass. Lipophilicity measurements indicated that bPEI played a dominant role in the polar nature of complexes 1 a – 5 a , thus rendering them very soluble in aqueous solutions. Inductively coupled plasma–mass spectrometry (ICP‐MS) and confocal laser scanning microscopy (CLSM) data indicated that an energy‐requiring process, such as endocytosis, was involved in the cellular uptake of all of the complexes. In addition, the cytotoxicity of the complexes toward human cervix epithelioid carcinoma (HeLa) and human embryonic kidney 293T (HEK293T) cell‐lines has been evaluated by the 3‐(4,5‐dimethyl‐2‐thiazolyl)‐2,5‐diphenyltetrazolium bromide (MTT) assay. The DNA‐binding properties of complex 5 a have been investigated by gel‐retardation assays and the polyplexes that were formed from this complex with plasmid DNA (pDNA) were studied by zeta‐potential measurements and particle‐size estimation. Furthermore, complex 5 a was grafted with poly(ethylene glycol) (PEG, average M_w=2 kDa) to different extents, thereby yielding the phosphorescent copolymers PEG_12.3‐g‐5 a , PEG_25.4‐g‐5 a , and PEG_62.1‐g‐5 a . Interestingly, these copolymers showed enhanced transfection activity, as revealed by in vitro transfection experiments with tissue‐culture‐based luciferase assays.     

Synthesis of thianthrene‐5,5,10,10‐tetraoxide‐containing polyimides via Yamazaki–Higashi phosphorylation method and their pervaporation properties to aromatic/nonaromatic hydrocarbon mixtures

High molecular weight polyimide was successfully prepared from thianthrene‐2,3,7,8‐tetracarboxylic acid‐5,5,10,10‐tetraoxide (TADATO‐4A) and 3,7‐diamino‐2,8(6)‐dimethyldibenzothiophene sulfone (DDBT) via the Yamazaki–Higashi phosphorylation method in the presence of triphenyl phosphite (TPP) and pyridine (Py). The obtained polyimide showed about 3–4 times larger inherent viscosity than that prepared by the conventional two‐step method in which the anhydride form (TADATO) of TADATO‐4A was used. The combination of the conventional two‐step method and Yamazaki–Higashi phosphorylation method, in which a dianhydride monomer [3,3′,4,4′‐diphenylsulfonetetracarboxylic dianhydride (DSDA)] was allowed to react with excessive DDBT to form an amine end‐capped polyamic acid oligomer and subsequently the oligomer was further polymerized with TADATO‐4A in the presence of TPP and Py, succeeded in giving the high molecular weight copolyimide, TADATO/DSDA(1/1)‐DDBT. However, both TADATO‐DDBT and TADATO/DSDA(1/1)‐DDBT showed fairly poor thermal stability due to the highly rigid structures. The pervaporation (PV) properties of the prepared polyimide membranes for benzene/cyclohexane (Bz/Cx) and benzene/n‐hexane (Bz/n‐Hx) mixtures were investigated. TADATO‐DDBT showed similar PV performance to DSDA‐DDBT at 60 °C. The sorption measurement revealed that these two kinds of polyimide membranes had a similar sorption amount, solubility selectivity, and diffusivity selectivity. The PV performance of TADATO/DSDA(1/1)‐DDBT was also found similar to DSDA‐DDBT for Bz/Cx mixture. © 2000 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 38: 895–906, 2000     

An integrated procedure of selective injection, sample stacking and fractionation of phosphopeptides for MALDI MS analysis

Protein phosphorylation is one of the most important post-translational modifications (PTM), however, the detection of phosphorylation in proteins using mass spectrometry (MS) remains challenging. This is because many phosphorylated proteins are only present in low abundance, and the ionization of the phosphorylated components in MS is very inefficient compared to the non-phosphorylated counterparts. Recently, we have reported a selective injection technique that can separate phosphopeptides from non-phosphorylated peptides due to the differences in their isoelectric points (pI) [1]. Phosphorylated peptides from α-casein were clearly observed at low femtomole level using MALDI MS. In this work, further developments on selective injection of phosphopeptides are presented to enhance its capability in handling higher sample complexity. The approach is to integrate selective injection with a sample stacking technique used in capillary electrophoresis to enrich the sample concentration, followed by electrophoresis to fractionate the components in preparation for MALDI MS analysis. The effectiveness of the selective injection and stacking was evaluated quantitatively using a synthetic phosphopeptide as sample, with an enrichment factor of up to 600 being recorded. Next, a tryptic digest of α-casein was used to evaluate the separation and fractionation of peptides for MALDI MS analysis. The elution order of phosphopeptides essentially followed the order of decreasing number of phosphates on the peptides. Finally, to illustrate the applicability, the integrated procedure was applied to evaluate the phosphorylation of a highly phosphorylated protein, osteopontin. Up to 41 phosphopeptides were observed, which allowed us to examine the phosphorylation of all 29 possible sites previously reported [2]. A high level of heterogeneity in the phosphorylation of OPN was evident by the multiple-forms of variable phosphorylation detected for a large number of peptides.     

Self-oriented pseudoisocyanine J-aggregates in solution

Highly oriented fiber-shaped J-aggregates of pseudoisocyanine (PIC) molecules were prepared by simply growing the aggregates in a narrow glass cell, which allows evaporation of the solution in one direction.     

Stereocontrol in organic synthesis using silicon-containing compounds. Studies directed towards the synthesis of ebelactone A

Several approaches to the synthesis of ebelactone A 2 are described, culminating in the synthesis of the benzenesulfonate of 2-epi-ebelactone A 161. All the approaches were based on three fragments A, B and C, originally defined in general terms in, but eventually used as the aldehyde 72, the allenylsilane 3 and the aldehyde 139, respectively. They were joined, first B with C, and then B+C with A. In the main routes to fragments A and C, the relative stereochemistry was controlled by highly stereoselective enolate methylations 67-->67, 68-->69, and 135-->136, in each case anti to an adjacent silyl group, and by a highly stereoselective hydroboration of an allylsilane 137-->138, also anti to the silyl group. The hydroxyl groups destined to be on C-3 and C-11 were unmasked by silyl-to-hydroxy conversions 69-->70 and 138-->139 with retention of configuration. The stereochemistry created in the coupling of fragment B to C was controlled by the stereospecifically anti S(E)2' reaction between the enantiomerically enriched allenylsilane 3 and the aldehyde 139. The double bond geometry was controlled by syn stereospecific silylcupration 148-->151, and preserved by iododesilylation 151-->152 of the vinylsilane with retention of configuration, and Nozaki-Hiyama-Kishi coupling with the aldehyde 72 gave the whole carbon skeleton 153 of ebelactone A with the correct relative configuration, all of which had been controlled by organosilicon chemistry. In the steps to remove the superfluous allylic hydroxyl, an intermediate allyllithium species 156 abstracted the proton on C-2, and its reprotonation inverted the configuration at that atom. Other routes to the fragments A and C were also explored, both successful and unsuccessful, both silicon-based and conventional, and a number of unexpected side reactions were investigated.     

Construction of porphyrin-cyclodextrin self-assembly with molecular wedge

A new host porphyrin bearing four permethyl-beta-cyclodextrin moieties for multi-porphyrin assembly forms a unique 2 : 2 assembly with the tetra-anion of tetrakis(p-sulfonylphenyl)porphyrin (TPPS) in aqueous solution.     

Simultaneous determination of bisphenol A and its halogenated derivatives in river water by combination of isotope imprinting and liquid chromatography-mass spectrometry

A restricted access media-molecularly imprinted polymer (RAM-MIP) for [2H16]bisphenol A (BPA-d16) was prepared by a multi-step swelling and polymerization method using 4-vinylpyridine as a functional monomer and ethylene glycol dimethacrylate as a cross-linker, followed by hydrophilic surface modification using glycerol dimethacrylate and glycerol monomethacrylate as hydrophilic monomers. The obtained RAM-MIP showed excellent molecular recognition abilities for BPA and BPA-d6 as well as BPA-d16 used as the template molecule, and good ones for tetrachlorobisphenol A (Cl4-BPA) and tetrabromobisphenol A (Br4-BPA). Next, the RAM-MIP was utilized for selective on-line pretreatment and enrichment of BPA, Cl4-BPA and Br4-BPA in a river water sample, followed by their separation and determination by LC-MS. The calibration graphs of BPA, Cl4-BPA and Br4-BPA, constructed using BPA-d6 as an internal standard, showed good linearity in the range of 12.5-200 pg/mL (r > 0.999) with a 2-mL injection of a river water sample. The inter-day precision data for the assay of BPA, Cl4-BPA and Br4-BPA at 25 pg/mL were 1.08, 3.67 and 1.58%, respectively. Furthermore, this method was successfully applied for the simultaneous determination of BPA and its halogenated derivatives in river water.     

Reaction of α,β-unsaturated Fischer carbene complexes with allyl alkoxide

Optically enriched homo-binuclear Fischer chromium carbene complexes with planar chiral arene chromium complexes gave α-allyl β-arylpropionates up to 97% ee by reaction with allyl alkoxide and subsequent photo-oxidative demetalation. The chiral hetero-binuclear tungsten carbene complexes afforded anti α-allyl β-hydroxy β-arylpropionates as a major product up to 92/8 dr by the same reaction sequence. High diastereoselectivity in these reactions is contributed to the planar chirality of the arene chromium complex, even though the reaction was carried out under vigorous basic media. The reaction products, α-allyl β-arylpropionates were derived by 1,3-M(CO)₅ shift and subsequent [3,3]-sigmatropic rearrangement. Also, the corresponding chromium-uncomplexed α,β-unsaturated Fischer carbene complexes afforded α-allyl β-arylpropionates under the same conditions. Formation of β-allyl β-arylpropionates via 1,2-M(CO)₅ shift followed by [3,4]-sigmatropic rearrangement was not observed in both reactions of chromium-coordinated and the corresponding chromium-uncoordinated α,β-unsaturated Fischer carbene complexes with allyl alkoxide in the presence of base.     

Two-dimensional reversed-phase liquid chromatography using two monolithic silica C18 columns and different mobile phase modifiers in the two dimensions

Comprehensive two-dimensional (2D) HPLC in the reversed-phase liquid chromatography (RPLC) mode using C18 silica monolith columns at first dimension (1st-D) (10 cm x 4.6mm I.D.) and second dimension (2nd-D) (5 cm x 4.6mm I.D.) was carried out successfully. A mixture of water and tetrahydrofuran (THF) was used as a mobile phase in the 1st-D separation, and a mixture of water and methanol (CH3OH) in the 2nd-D separation. Sample fractions from 1st-D column were directly loaded into an injection loop of the 2nd-D HPLC equipped with two injector valves for one column. The fractionation time at the 1st-D that was equal to the separation time at the 2nd-D was 45 or 60s. Total peak capacity up to 900 was obtained in about 60 min for the isocratic mode separation of aromatic compounds in this system. Gradient elution mode applied to both 1st-D and 2nd-D separations resulted in shorter separation time and better separation efficiencies than the isocratic mode. It was demonstrated that 2D-HPLC systems employing popular C18 stationary phases with different organic modifiers in mobile phases for each dimension could produce large peak capacity. The different selectivities were provided by the difference in polar interactions between a solute and the organic modifier existing in the stationary phase.     

Simultaneous construction of the polymer backbone and side chains by three‐component polycondensation: The synthesis of polyurethanes with allyl side chains from dialdehydes,alkylene N,N′‐bis(trimethylsilyl) carbamates,and allyltrimethylsilane

Polyurethanes with allyl side chains were synthesized by the simultaneous acid‐catalyzed reaction of dialdehydes ( 1 ), alkylene N,N′‐bis(trimethylsilyl) carbamates ( 4 ), and allyltrimethylsilane ( 5 ). When 5 was added to a mixture of 1 , 4 , and the catalyst, a low molecular weight polymer was formed, as well as a large amount of an insoluble gel. However, when a mixture of 1 , 4 , and 5 was added to the catalyst, the formation of gel was depressed, and the desired polyurethanes, consisting of 1 , 4 , and 5 in a molar ratio of 1/1/2, were obtained in good yields. This polyurethane synthesis is unusual in that it concurrently constructs both the polymer backbone and the functional side chains from three starting compounds. © 2002 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 40: 1236–1242, 2002