Carboxylic acid

About: Carboxylic acid is a research topic. Over the lifetime, 48544 publications have been published within this topic receiving 605696 citations.

Method for the preparation of relief structures

Abstract: The invention provides a method for the preparation of relief structures of highly heat-resistant polymers, using radiation-sensitive, soluble preliminary polymers in the form of polyaddition or polycondensation products of polyfunctional carbocyclic or heterocyclic compounds containing radiation-sensitive radicals in ester groups bound to said compounds with diamines, diisocyanates, bis-acid chlorides or dicarboxylic acids of cyclic structure. According to the invention, the polyfunctional compounds containing the radiation-sensitive radicals contain, besides carboxyl, carboxylic acid chloride, amino, isocyanate or hydroxyl groups suitable for addition or condensation reactions, partly in ortho or peri-position thereto, radiation-reactive radicals in the ester groups bound to the compounds having an oxyalkylene methacrylate or acrylate structure.

Effect of Carboxylic Acid on Sintering of Inkjet-Printed Copper Nanoparticulate Films

Abstract: The reduction effect of various carboxylic acids on inkjet-printed copper film was investigated. Carboxylic acids were exposed to the film by nitrogen gas that was bubbled through the liquid acids during the annealing process. It was observed that in the case of saturated monocarboxylic acid (formic, acetic, propionic, butyric), the acids with shorter hydrocarbon chains perform better in reducing the surface copper oxides in the printed copper conductive film. The printed films exposed to formic acid vapor exhibited the lowest resistivity (3.10 and 2.30 μΩ cm when annealed at 200 and 250 °C, respectively). In addition, the oxalic acid more effectively reduces copper oxide than formic acid and its usage can shorten the annealing time for highly conductive printed copper film. This reductive annealing process allows fabrication of copper patterns with low resistivity, (3.82 μΩ cm annealed at 250 °C) comparable to the resistivity of bulk copper.

Derivatization of Glucose and 2-Deoxyglucose for Transition Metal Complexation: Substitution Reactions with Organometallic 99mTc and Re Precursors and Fundamental NMR Investigations

Abstract: Synthetic strategies for the bifunctionalization of glucose and 2-deoxyglucose at position C-1 for transition metal coordination are reported. In particular organometallic technetium and rhenium complexes for potential use in diagnostic nuclear medicine were synthesized and investigated. Specifically, a common iminodiacetic acid (IDA) moiety was O-glycosidically connected through an ethylene spacer group to produce the pure alpha- (in case of 2-deoxyglucose) and beta-anomer (in case of glucose). Reaction of the sugar derivatives with the organometallic precursor [M(H2O)3(CO)3]+ (M = 99mTc, Re) produced single products in high yield, which are water-soluble and water-stable. The displacement of the three water molecules of the metal precursor and thus the tridentate coordination of the metal-tricarbonyl core exclusively via the amine and the two carboxylic acid functionalities of the IDA chelate was verified by means of 1D and 2D 1H NMR spectroscopy, mass spectrometry, and IR spectroscopy. The radioactive-labeled products (99mTc) proved their excellent stability in vitro in physiological phosphate buffer (pH = 7.4) and human plasma over a period of 24 h at 37 degrees C.

General and Practical Carboxyl-Group-Directed Remote C–H Oxygenation Reactions of Arenes

Abstract: Transition-metal-catalyzed aromatic C–H oxygenation reaction[1] is a very powerful tool for straightforward synthesis of valuable oxygen-containing products from abundant arenes.[2] Of these reactions, intramolecular C–H/O–H oxidative coupling of carboxylic acid with unactivated sp2 C–H bond is an important transformation, because it gives an access to a variety of valuable lactone-containing molecules.[3] Thus, 3,4-benzocoumarin fragment 2, containing six-membered lactone moiety, is widely found in natural and bioactive molecules, as well as in useful materials.[4] Expectedly, 2 can be accessed through cyclization of nonpre-functionalized 2-arylbenzoic acids 1; however, the existing methods require either employment of stoichiometric amounts of toxic oxidants[5] or UV irradiation,[6] which substantially limits applicability of these methods (Scheme 1). We hypothesized that it should be possible to develop a general, practical, and environmentally benign dehydrogenative C–H/O–H lactonization reaction of 2-arylbenzoic acids 1 into 3,4-benzocoumarins 2 en route to oxygenated biaryls 3. We envisioned that C–H oxygenation could potentially be performed by formation of carboxyl O-centered radical A, which would undergo a subsequent C–O bond formation.[7] Scheme 1 Carboxyl-group-directed C–H oxygenation reactions. Herein, we report two complimentary methods for this transformation. Method 1, the Cu-catalyzed oxygenation reaction of 2-arylbenzoic acids, which is efficient for electron-neutral and electron-rich substrates. During preparation of this manuscript, a similar to Method 1 Cu-catalyzed transformation was disclosed by Gallardo-Donaire and Martin.[8] Most importantly, we also developed a more general and practical Method 2, the K2S2O8-mediated oxygenation reaction, which is widely applicable for cyclization of electron-neutral, electron-rich, as well as electron-deficient substrates. To develop mild and environmentally benign intramolecular lactonization reaction of 2-arylbenzoic acids, we performed extensive screening of transition-metal catalysts and oxidants.[9] It was found that this reaction can efficiently be accomplished by using CuII catalyst. Thus, 2-phenylbenzoic acid 1a was converted into the desired benzocoumarin product 2a in 88% yield in the presence of Cu(OAc)2·H2O (5 mol%) and tert-butyl peroxybenzoate (TBPB, Luperox P) in dichloroethane (Method 1). We found that substrates with electron-neutral and electron-donating substituents, as well as aryl halide fragments (Hal=F, Cl, Br) and cyanogroup on the “guest” aryl ring, produced the desired products in good to excellent yield (Table 1, entries 2a–j). In general, benzoic acids substituted with arene ring containing meta-substituents (F, Cl, OMe, tBu) preferentially underwent cyclization at the less hindered site (Table 1, entries 2k–n). In contrast, meta-Me substituted substrate 1o cyclized at the more hindered site producing 2o as a major regioisomer (4:1).[10] In addition, 2-naphthyl substituted benzoic acid 1p gave the product of cyclization at the more electron-rich 1-position, exclusively (2p). Likewise, substrates containing 3,5-disubstituted arene ring also underwent efficient cyclization into benzocoumarin products 2q and r. 2-Phenylbenzoic acids containing substituents at 1-, 2-, and 3-positions also underwent smooth C–H oxygenation reaction producing products 2s–v. Although electron-neutral and electron-rich substrates under these reaction conditions (Method 1) gave the corresponding benzocoumarins in good to excellent yields, cyclization reaction of electron-deficient substrates was less efficient. Hence, 2-arylbenzoic acids with important electron-withdrawing functional groups, such as CF3 (1w), COMe (1x), and CONMe2 (1y) provided the corresponding products in diminished yields, whereas substrates possessing CHO (1z), CF3 (1aa, ab), and NO2 groups (1ac–ae) produced trace to no product at all (Table 1). Table 1 CuII-catalyzed C–H oxygenation reaction. To overcome this limitation of the Cu-catalyzed oxygenation reaction (Method 1, Table 1), we aimed at the development of a complementary method for cyclization of electron deficient 2-arylbenzoic acids. Delightfully, we found that this transformation can be performed in the presence of K2S2O8 oxidant in aqueous acetonitrile.[11] Thus, benzocoumarin 2a was formed in 93% yield from 2-phenylbenzoic acid 1a in gram-scale manner by using this convenient and environmentally benign protocol (Table 2). We found that Method 2 works efficiently for electron-neutral and electron-deficient substrates under these conditions (entries 2a, i,p, r, t,u). Notably, in the presence of K2S2O8, benzoic acids substituted with arene ring containing meta-substituents produced the corresponding products in higher selectivity compared to that of Method 1 (Table 2, entries 2k–o′). Most importantly, the developed protocol can be successfully applied to a variety of electron-deficient substrates. Accordingly, 2-arylbenzoic acids with CF3 (2w, 2aa), COMe (2x), CONMe2 (2y), and CHO (2z) groups underwent cyclization producing the corresponding products in good to excellent yields. Moreover, previously incompetent substrates with highly electron- withdrawing NO2 group (2ac, 2ad, 2ae) and even two CF3 groups (2ab) now were smoothly transformed into the corresponding benzocoumarin products (Method 1, Table 1). It should be mentioned that in some cases, addition of a catalytic amount of AgNO3 (10 mol%) led to substantial increases of reaction rates.[12, 13] Table 2 K2S2O8-mediated C–H oxygenation reaction. Naturally, the developed methods open access to a variety of densely functionalized benzocoumarin molecules.[4] In addition, considering the importance of aryl ether moiety, we have shown that the obtained 3,4-benzocoumarins could be nearly quantitatively converted into the corresponding biaryl ethers 3 (Scheme 2). Scheme 2 Conversion of lactones into aryl ethers. It is likely that the CuII-catalyzed oxygenation reaction (Method 1) proceeds through an active CuIII intermediate A (Scheme 3), which may abstract the adjacent hydrogen atom to form aryl radical B (Path A). The latter, upon oxidative ring closure, would produce B′, followed by a reductive elimination to form 2.[14, 15] Alternatively, a single-electron transfer (SET) process in A would give radical–cation specie C (Path B), which would be transformed into 2 by a subsequent C–O bond-forming reaction.[16] Scheme 3 Proposed mechanism for Method 1. The K2S2O8-mediated oxygenation reaction (Method 2) most likely proceeds by oxidation of benzoic acid 1 into an O-centered carboxylic radical D, which undergoes addition to the arene ring to form an aryl radical intermediate E (Scheme 4, [Eq. (1)], Path A). The latter converts into the benzocoumarin product 2a upon loss of a hydrogen radical. This homolytic aromatic substitution mechanism is supported by our experiments on cyclization of substrates containing 2-haloaryl substituents 4a–c (G= F, Cl, Br). It was found that these reactions exclusively produce substitution products 2a instead of possible C–H coupling products 5 (Scheme 4, [Eq. (2)]).[17] Alternative mechanism involving an abstraction of hydrogen radical from the aromatic ring in the intermediate D to form the aromatic radical F cannot be ruled out at this stage (Scheme 4, [Eq. (1)], Path B). Scheme 4 Proposed mechanism for Method 2. In conclusion, two complimentary methods for carboxyl-group- directed remote C–H oxygenation reaction of arenes were developed. Method 1, the Cu-catalyzed reaction, produces a variety of 3,4-benzocoumarins containing electron-neutral and electron-releasing substituents. In addition, a more general Method 2, the K2S2O8-mediated transformation, which is widely applicable to various electron-rich and electron-deficient 2-arylbenzoic acids, was developed. This protocol features a broad scope, a good functional group tolerance, and good selectivity. It is also benign, operationally simple, easily scalable, and proceeds under mild conditions.