Serum proteins associated with acute myocardial infarction (AMI) have been monitored by sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) and high resolution two-dimensional electrophoresis (2-DE) under nonreducing conditions. Proteins a, b, c (Mr 13,000; pI6.2, 6.7 and 7.5, respectively) and e(Mr27,000; pI5.2) appear simultaneously approximately 30 h after infarction, reach maximum intensity after 48 h and progressively decline thereafter. Protein d (Mr15,000; pI7-8.5; identified as hemoglobin) sometimes appears within 18 h of infarction. Proteins a-c are not detected in the 2-DE patterns of healthy myocardium, infarcted myocardium, pectoral muscle or tongue, but e is present in all and tentatively identified as myosin light chain. Other myocardial proteins which are either reduced in amount following infarction or more specifically associated with myocardium than pectoral muscle are not detected in the serum of AMI patients. Analysis of unconcentrated urine by SDS-PAGE and silver staining does not reveal proteins specific to AMI. 相似文献
The clinical significance of the serum enzymes creatine kinase (CK, EC 2.7.3.2), lactate dehydrogenase (LD, EC 1.1.1.27) and aspartate aminotransferase (EC 2.6.1.1), and the isoenzymes CK 1-3 and LD 1-5, in acute myocardial infarction (AMI) is reviewed. Particular attention is given to electrophoretic analysis of the isoenzymes (and the CK isoforms/subforms) following AMI and thrombolytic therapy. Other protein markers for the monitoring of AMI, including myoglobin and muscle contractile proteins, are also discussed and the potential for the detection of new marker proteins using high-resolution two-dimensional electrophoretic methods is demonstrated. Whilst emphasis is placed upon electrophoretic methods the value of complementary immunoassays is acknowledged in order to maintain a balanced perspective. 相似文献
The subforms of MM isozyme of creatine kinase (ATP:creatine N-phosphotransferase, EC 2.7.3.2, CK) in sera obtained from healthy adults and patients were determined by agarose gel isoelectric focusing (IEF). The patients were classified into six groups according to serum CK-MM activities and IEF patterns. The IEF spectra offered useful information on cell hyperplasia, augmented cell membrane permeability, cell destruction and release time of CK-MM in the circulation from the cells for diagnosis, progress observation and prognosis, especially in the cases of chronic hepatic diseases, acute myocardial infarction and muscular dystrophy. Macro CKs were also determined by IEF. Macro CKs could be completely distinguished from each other, and CK isozymes consisting of macro CK type 1 could be presumed by isoelectric points. 相似文献
Two types of mitochondrial creatine kinase (Mi-CK), sarcomeric (sMi-) and ubiquitous (uMi-)CKs, were isolated from normal human cardiac muscle and brain tissue, respectively, and their heterogeneity was characterized by means of isoelectric focusing (IEF). Octameric sMi-CK and uMi-CK were electrophoresed cathodic to cytoplasmic muscle-type creatine kinase isoenzyme (CK-MM) and dimeric Mi-CKs were found at the position of CK-MM on a cellulose acetate membrane. The electrophoretic mobilities of sMi-CK were similar to those of uMi-CK. Octameric sMi-CK was focused at pI 7.1-8.0 and dimeric forms at pI 6.55, 6.75, 6.85, and 6.95. New bands appearing at pI 6.65 and 6.75 after treatment of sMi-CK with carboxypeptidase B were found to be delysined forms. sMi-CK reacted with anti-sMi-CK antibodies, and the immune complexes were focused at pI 5.8. The Km value of sMi-CK for creatine phosphate (PCr) was 1.19 +/-0.20 mmol/L (mean +/- standard error), the activation energy (Ea) was 108.3+/-1.2 kJ/ mol, and the residual enzyme activity after heating at 45 degrees C for 20 min was 79.6+/-1.9%. On the other hand, octameric uMi-CK was focused at pI 7.1-7.9 and the dimeric forms were focused at pI 6.6, 6.7, 6.8, 6.9, and 7.0. Delysined forms were focused around pI 6.3, 6.4, 6.8, and 6.9. uMi-CK reacted with anti-sMi-CK antibodies, and the immune complexes were focused at pI 5.8. The Km value of uMi-CK for PCr was 1.07+/-0.03 mmol/L, Ea of uMi-CK was 110.0+/-0.9 kJ/mol, and the residual enzyme activity after heating at 45 degrees C for 20 min was 90.3+/-0.4%. The sMi-CK and uMi-CK were hybridized and the hybrid Mi-CK appeared at pI 6.78, 6.98, and 7.1-7.95. The pIs of the hybrid Mi-CK were between those of sMi-CK and uMi-CK. As described above, sMi-CK and uMi-CK were slightly different from each other with respect to the pI and some enzyme characteristics. 相似文献
High resolution two-dimensional electrophoresis indicates that serum proteins previously only detected in patients with acute myocardial infarction (AMI) (Gomo et al., Electrophoresis 1983, 4, 298-302) are also present in the serum protein patterns of other patients (AMI negative or demonstrating acute phase response) and are faintly detected even in controls. Thus, these proteins are not specific to AMI and are probably acute phase reactants. However, they do demonstrate a characteristic time course response in sequential samples from AMI patients. 相似文献
In this paper, an oxygen‐insensitive degradable resist for UV‐nanoimprint is designed, comprising a polycyclic degradable acrylate monomer, 2,10‐diacryloyloxymethyl‐1,4,9,12‐tetraoxaspiro [4.2.4.2] tetradecane (DAMTT), and a multifunctional thiol monomer pentaerythritol tetra(3‐mercaptopropionate) (PETMP). The resist can be quickly UV‐cured in the air atmosphere and achieve a high monomer conversion of over 98%, which greatly reduce the adhesion force between the resist and the soft mold. High conversion, in company with an adequate Young's modulus (about 1 GPa) and an extremely low shrinkage (1.34%), promises high nanoimprint resolution of sub‐50 nm. The cross‐linked resist is able to break into linear molecules in a hot acid solvent. As a result, metallic patterns are fabricated on highly curved surfaces via the lift off process without the assistance of a thermoplastic polymer layer.
In this work, we describe the direct covalent attachment of protein recognition elements (biotin) with the carboxyl groups present on the walls of polyimide nanochannels. Subsequently, these biotinylated channels were used for the bio‐specific sensing of protein analytes. Moreover, surface charge of these asymmetric nanochannels was reversed from negative to positive via the conversion of carboxyl groups into terminated amino groups. The negatively charge (carboxylated) and positively charged (aminated) channels were further used for the electrochemical sensing of bovine serum albumin (BSA, pI = 4.7). These biorecognition events were assessed from the changes in the ionic current flowing through the nanochannel.
The catalytic asymmetric α-benzylation of aldehydes represents a highly valuable reaction for organic synthesis. For example, the generated α-heteroarylmethyl aldehydes, such as (R)-2-methyl-3-(pyridin-4-yl)propanal ((R)-MPP), are an important class of synthons to access bioactive drugs and natural products. We report herein a new and facile synthetic approach for the asymmetric intermolecular α-benzylation of aldehydes with less sterically hindered alkyl halides using a multifunctional chiral covalent framework (CCOF) catalyst in a heterogeneous way. The integration of chiral BINOL-phosphoric acid and Cu(ii)-porphyrin modules into a single COF framework endows the obtained (R)-CuTAPBP-COF with concomitant Brønsted and Lewis acidic sites, robust chiral confinement space, and visible-light induced photothermal conversion. These features allow it to highly promote the intermolecular asymmetric α-benzylation of aldehydes via visible-light induced photothermal conversion. Notably, this light-induced thermally driven reaction can effectively proceed under natural sunlight irradiation. In addition, this reaction can be easily extended to a gram-scale level, and its generality is ascertained by asymmetric α-benzylation reactions on various substituted aldehydes and alkyl bromides.We report a new synthetic approach for the intermolecular α-alkylation of aldehydes with alkyl halides based on a BINOL-phosphate and Cu(ii)-porphyrin derived multifunctional CCOF catalyst via visible-light induced photothermal conversion.相似文献
1‐Allyl‐2,4,7‐trimethyl‐1 H‐indene ( 1 ) and 1‐(3‐buten‐1‐yl)‐4,7‐dimethyl‐1 H‐indene ( 2 ), which are to prepare from (2,4,7‐trimethylindenyl)lithium and allyl chloride or from (4,7‐dimethylindenyl)lithium and 4‐bromo‐1‐butene, react with n‐butyllithium yielding (1‐allyl‐2,4,7‐trimethylindenyl)lithium [LiL ( 1 a )] or [1‐(3‐buten‐1‐yl)‐4,7‐dimethylindenyl]lithium [LiL′ ( 2 a )], respectively. The reactions of the trichlorides of gadolinium, erbium, yttrium, lutetium, and ytterbium with 1 a or 2 a (mole ratio 1 : 2) in THF produce the bis(indenyl)lanthanide chloride complexes L2LnCl(THF) [Ln = Gd ( 1 b ), Er ( 1 c )], LLnCl(THF) [Y ( 2 d ), Lu ( 2 e )], or LYb(μ‐Cl)2Li(THF)2 ( 2 f ), whereas the trichlorides of the comparatively large samarium and lanthanum ions react with different molar amounts of 2 a in THF exclusively with formation of the tris(indenyl) complexes LSm ( 2 g ) or LLa(μ‐Cl)Li(Et2O)3 ( 2 h ), respectively. All new compounds were characterized by elemental analyses, mass spectrometry, and the diamagnetic compounds 2 d , 2 e and 2 h also by 1H and 13C{1H}‐NMR spectroscopy. The single crystal X‐ray structural analyses of 1 c , 2 f , 2 g and 2 h demonstrate that the alkenyl groups of the indenyl side chains are not coordinated to the lanthanide atoms. 相似文献
Chemical modification reactions of alkyne containing polyHEMA‐based macroporous network structures (cryogels) by Cu(I) catalyzed azide‐alkyne ‘click’ cycloaddition reactions and their monitoring and quantification with high‐resolution magic angle spinning (hr‐MAS) NMR spectroscopy are reported. Complete conversion is obtained when benzylazide is reacted with the grafted alkyne function, but only partial conversion is observed when using azide‐modified poly(ethylene glycol) (PEG‐N3). Subsequent addition of benzylazide consumes all remaining alkyne groups. All chemical modifications are easily monitored at each stage using hr‐MAS NMR spectroscopy. The alkyne functionality and the resulting triazole ring provide well resolved 1H resonances to monitor and quantify the progress of such ‘click’ reactions in general.
A novel series of poly(p‐phenylene)s (PPPs) with polyhedral oligomeric silsesquioxanes (POSSs) on their side chains was prepared. The obtained POSS‐modified PPPs are as follows: 25POSS‐PPP ( 2b , containing 25 mol‐% of POSS units in all side chains), 50POSS‐PPP ( 2c , containing 50 mol‐% of POSS units in all side chains), 100POSS‐PPP ( 2d , containing 100 mol‐% of POSS units in all side chains), and 0POSS‐PPP ( 2a , as a blank polymer). Films polymer 2d showed the same absorption and photoluminescence (PL) spectra as those in CHCl3 solution, indicating that bulky POSS units strongly suppressed intermolecular aggregation of the PPP backbone. Polymer 2d showed the same PL spectra even after thermal annealing at 150 °C for 6 h. This enhancement of PL stability is due to the significant effect of the bulky POSS units.
The unusual formation of 1‐acyl‐1,2‐dihydro‐3H‐pyrazol‐3‐ones starting from 3‐acyloxypyrazoles by Fries‐type rearrangement is described. Under normal conditions, acylation of 2,4‐dihydro‐3H‐pyrazol‐3‐ones 1 and 2 with acid chlorides or anhydrides in the presence of triethylamine gave the corresponding 3‐acyloxypyrazoles 3a‐f and 4a‐f . Treatment of 3a‐c and 4a‐f with Lewis acid, e.g. titanium(IV) chloride and tin(IV) chloride, caused migration of acyl groups to afford the corresponding 1‐acyl‐1,2‐dihydro‐3H‐pyrazol‐3‐ones 5a‐c and 6a‐f . Interestingly, the reactions of 3‐acyloxypyrazoles 3e and 3f with tin(IV) chloride provided the corresponding tin(IV) complexes 8e and 8f . 相似文献
Ring closure of 2‐N‐benzylamino‐3‐aroylpropionic acids ( 3 ) with acetic anhydride afforded 3‐N‐benzylamino‐5‐aryl‐2(3H)‐furanones ( 4 ). The reaction of the furanones ( 4 ) with benzylamine in benzene was found to be time dependent. Thus refluxing the reaction mixture for 1 h only afforded the open‐chain amides ( 5a‐c ). When the reaction was conducted for 3 h the 2(3H)‐pyrrolones ( 6 ) were obtained. Hydrazine hydrate affected ring opening of the furanones to give the hydrazides ( 5d‐f ). Also, semicarbazide converted ( 4 ) into the corresponding semicarbazide derivatives ( 5g‐i ). The hydrazides ( 5d‐f ) were reacted with benzoyl chloride to give the corresponding diaroylhydrazines ( 5j‐l ). The open‐chain derivatives ( 5 ) were converted into a variety of heterocycles: isothiazolones ( 7 ), dihydropyridazinones ( 8 ), 1,3,4‐oxadiazoles ( 9 ) and 1,2,4‐triazole derivatives ( 10 ) via cyclization reactions. 相似文献
Simulations of polymerization rate, molecular weight development and evolution of the concentrations of species participating in the reaction mechanism over a range of operating conditions, and a parameter sensitivity analysis showing the effects of temperature, activation/deactivation equilibrium constant and initial concentrations of controller and initiator (if present) on these variables are presented for the nitroxide‐mediated radical polymerization of styrene. The simulations were performed with a computer program based on a detailed reaction mechanism. The simulated profiles of conversion, number average molecular weight ( ), and polydispersity agree well with experimental data. Previously unknown activation energies for reactions involved in the mechanism are estimated. The temperature dependence of the kinetic rate constants obtained in this study will be useful for future modeling and optimization studies.
The 2‐bromomethyl‐3,5,6,7‐tetrahydrobenzofuranones 1a‐d were subjected to triazidochlorosilanesodium azide‐mediated Schmidt rearrangement to afford the corresponding tetrazolofuroazepine derivatives 2a‐d via methylene shift. Under similar reaction conditions, the 2‐iodomethyl‐3,5,6,7‐tetrahydrobenzofuranones 1e‐h afford mixtures of the corresponding tetrazolofuroazepines 2e‐h and the 4‐azido‐2‐iodomethyl‐2,3‐dihydrobenzofuran derivatives 3a‐c . A mechanism is proposed to account for the divergence in the reactivity of these 2‐halogenomethyltetrahydrobenzofuranones (X = Br versus I). In turn, the 2‐halogenomethyltetrazolofuroazepines 2a,b,d‐h and the 4‐azido‐2‐iodomethyl‐2,3‐dihydrobenzofurans 3a,b underwent nucleophilic substitution with triethyl phosphite and dehydrohalogenation using DBU in refluxing toluene to give the corresponding tetrazolofuroazepines 4a‐d and 5a‐c and benzofurans 6a,b . 相似文献
Novel quinazoline non‐nucleosides analogues of Emivirine were described. Compounds 1a‐c were silylated and reacted with the appropriate chloroethers ( 2a‐c ) in the presence of CsI to give the corresponding non‐nucleosides 3a‐h and 4a‐h . Silylation of 1a‐c and treatment with bis(allyloxy)methanes ( 5a,b ) afforded the corresponding 1‐(allyloxymethyl)quinazolines 6a‐f. 1‐(Propargyloxymethyl)‐quinazolines 8a,b were obtained by treatment of the silylated 1a,b with bis(propargyloxy)methane ( 7 ) in the presence of TMS triflate. 相似文献
Summary: The fabrication of polymer diodes on a glass substrate by an ink‐jet printing technique is reported. Both an n‐type semiconductive polymer, poly[2‐methoxy‐5‐(2‐ethylhexyloxy)‐1,4‐(1‐cyanovinylene)phenylene] (CN‐PPV), and a p‐type semiconductive polymer, polypyrrole (PPy) or poly(3,4‐ethylenedioxythiophene) (PEDOT), were printed through a piezoelectric ink‐jet printer. The printed CN‐PPV/PPy and CN‐PPV/PEDOT diodes showed good rectifying characteristics. These results indicate the potential of the low‐cost ink‐jet printing technique to produce polymer microelectronic devices and circuits.
Schematic diagram of the printed polymer diode 相似文献
Summary: Plasma‐initiated controlled/living radical polymerization of methyl methacrylate (MMA) was carried out in the presence of 2‐cyanoprop‐2‐yl 1‐dithionaphthalate. Well‐defined poly(methyl methacrylate) (PMMA), with a narrow polydispersity, could be synthesized. The polymerization is proposed to occur via a RAFT mechanism. Chain‐extension reactions were also successfully carried out to obtain higher molecular weight PMMA and PMMA‐block‐PSt copolymer.
Dependence of ln([M]0/[M]) on post‐polymerization time (above), and \overline M _{\rm n} and PDI against conversion (below) for plasma initiated RAFT polymerization of MMA at 25 °C. 相似文献
Summary: The recently developed initiation system, activators generated by electron transfer (AGET), is used in atom transfer radical polymerization (ATRP) in the presence of a limited amount of air. Ascorbic acid and tin(II ) 2‐ethylhexanoate are used as reducing agents in miniemulsion and bulk, respectively. An excess of reducing agent consumes the oxygen present in the system and, therefore, provides a deoxygenated environment for ATRP. ATRP of butyl acrylate is successfully carried out in miniemulsion and in the presence of air. During polymerization the radical concentration remains constant. The polymerization reaches over 60% monomer conversion after 6 h, which results in polymers with a predetermined molecular weight = 14 000 g · mol−1 and a low polydispersity ( = 1.23). AGET ATRP of styrene is also successful in bulk in the presence of air, as evidenced by linear semi‐logarithmic kinetics, which leads to polystyrene with an of 13 400 g · mol−1 and a low polydispersity index ( = 1.14).
Appearance of miniemulsion before and after the reducing agent ascorbic acid was added (left); and GPC traces representing molecular weights during the AGET ATRP of BA in miniemulsion in the presence of air (right). 相似文献
