Synthesis of 1,4‐Cyclohexanedimethanol, 1,4‐Cyclohexanedicarboxylic Acid and 1,2‐Cyclohexanedicarboxylates from Formaldehyde,Crotonaldehyde and Acrylate/Fumarate

Valuable polyester monomers and plasticizers—1,4‐cyclohexanedimethanol (CHDM), 1,4‐cyclohexanedicarboxylic acid (CHDA), and 1,2‐cyclohexanedicarboxylates—have been prepared by a new strategy. The synthetic processes involve a proline‐catalyzed formal [3+1+2] cycloaddition of formaldehyde, crotonaldehyde, and acrylate (or fumarate). CHDM is produced after a subsequent hydrogenation step over a commercially available Cu/Zn/Al catalyst and a one‐pot hydrogenation/oxidation/hydrolysis process yields CHDA, whereas 1,2‐cyclohexanedicarboxylate is obtained by a Pd/C‐catalyzed tandem decarbonylation/hydrogenation step.     

聚合条件对透明聚(1,4-环己烷二甲酸-1,4-环己烷二甲醇酯)分子量的影响

采用1,4-环己烷二甲醇(CHDM)与1,4-环己烷二甲酸(CHDA)合成出了高透明全脂环族聚酯——聚(1,4-环己烷二甲酸-1,4-环己烷二甲醇酯)(PCCD).研究了CHDM和CHDA的顺反异构体含量对PCCD结晶性能和光学性能的影响,结果表明当CHDA顺式异构体含量达到40%以上时,可以获得高透明无定型PCCD.3种钛系化合物包括钛酸四丁酯(TBT)、钛酸四异丙酯(TPT)和二氧化钛与二氧化硅复合物C-94用作反应的催化剂,结果以TBT的催化活性最好.TBT用量的增加可以使PCCD分子量小幅度增长.通过对生成物PCCD的分子量和特性黏数测试,分析了CHDM/CHDA初始摩尔比对PCCD的影响规律,随着CHDM/CHDA初始摩尔比的增加,PCCD的分子量呈现先增加后降低的趋势,NMR分析表明,CHDM的挥发性较低导致其只能稍微过量于CHDA,否则会残留于产物中影响分子量.最后研究了合成工艺包括缩聚时间和缩聚温度对PCCD的影响,其中PCCD分子量达到最大值所需要的缩聚时间随CHDM/CHDA初始摩尔比的增加而增加.当原料CHDM和CHDA的初始摩尔比为1.04∶1,催化剂TBT为30 mg/kg时,在275℃缩聚时间达到120 min后可以获得分子量最大的PCCD.     

Controlled stereochemistry of polyamides derived from cis/trans‐1,4‐cyclohexanedicarboxylic acid

A series of copolyamides 12.y was synthesized either with y = 6, or 1,4‐cyclohexanedicarboxylic acid (1,4‐CHDA) residue, or a mixture of both. The influence of the synthetic route of 1,4‐CHDA containing polyamides on the obtained cis–trans ratio of the incorporated 1,4‐CHDA was investigated. The use of acid chlorides provided a synthetic route with full control of the cis–trans ratio of the 1,4‐CHDA residue during synthesis, whereas synthesis at elevated pressure and temperature caused isomerization. The content and cis–trans ratio of 1,4‐CHDA in the copolyamides were determined by solution ¹³C NMR spectroscopy. Increasing the degree of partial substitution of the adipic acid by 1,4‐CHDA resulted in an increase in T_m, even for low molar precentages of 1,4‐CHDA. This phenomenon points to isomorphous crystallization of both the 12.6 and 12.CHDA repeating units. The mps of the synthesized polyamides were independent of the initial cis–trans ratio of 1,4‐CHDA, provided that the samples were annealed at 300 °C before DSC analysis. The polyamides exhibited a different melting pattern depending on the 1,4‐CHDA content. At a low a 1,4‐CHDA content a net exothermic recrystallization occurred during melting, whereas at higher contents of 1,4‐CHDA this recrystallization occurs to a lesser extent, and two separate melting areas are observed. © 2001 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 39: 833–840, 2001     

Organocatalytic Asymmetric Conjugate Addition of 3‐Monosubstituted Oxindoles to (E)‐1,4‐Diaryl‐2‐buten‐1,4‐diones: A Strategy for the Indirect Enantioselective Furanylation and Pyrrolylation of 3‐Alkyloxindoles

An asymmetric conjugate addition of 3‐monosubstituted oxindoles to a range of (E)‐1,4‐diaryl‐2‐buten‐1,4‐diones, catalyzed by commercially available cinchonine, is described. This organocatalytic asymmetric reaction affords a broad range of 3,3′‐disubstituted oxindoles that contain a 1,4‐dicarbonyl moiety and vicinal quaternary and tertiary stereogenic centers in high‐to‐excellent yields (up to 98 %), with excellent diastereomeric and moderate‐to‐high enantiomeric ratios (up to 99:1 and 95:5, respectively). Subsequently, cyclization of the 1,4‐dicarbonyl moiety in the resultant Michael adducts under different Paal–Knorr conditions results in two new kinds of 3,3′‐disubstituted oxindoles—3‐furanyl‐ and 3‐pyrrolyl‐3‐alkyl‐oxindoles—in high yields and good enantioselectivities. Notably, the studies presented here sufficiently confirm that this two‐step strategy of sequential conjugate addition/Paal–Knorr cyclization is not only an attractive method for the indirect enantioselective heteroarylation of 3‐alkyloxindoles, but also opens up new avenues toward asymmetric synthesis of structurally diverse 3,3′‐disubstituted oxindole derivatives.     

Highly Regio‐ and Stereodivergent Access to 1,2‐Amino Alcohols or 1,4‐Fluoro Alcohols by NHC‐Catalyzed Ring Opening of Epoxy enals

Described is an unprecedented NHC‐catalyzed (NHC=N‐heterocyclic carbene), stereoselective ring opening of epoxy and cyclopropyl enals to deliver valuable compounds bearing multiple stereocenters. A straightforward three‐step procedure involving two catalytic enantioselective transformations has been developed and leads to a regio‐ and stereodivergent synthesis of either 1,2‐amino alcohols/diamines or 1,4‐fluoro alcohols with excellent diastereo‐ and enantiopurity.     

Rh‐Catalyzed [5+1] and [4+1] Cycloaddition Reactions of 1,4‐Enyne Esters with CO: A Shortcut to Functionalized Resorcinols and Cyclopentenones

We have developed novel Rh‐catalyzed [n+1]‐type cycloadditions of 1,4‐enyne esters, which involve an acyloxy migration as a key step. The efficient preparation of functionalized resorcinols, including biaryl derivatives, from readily available 1,4‐enyne esters and CO was achieved by Rh‐catalyzed [5+1] cycloaddition accompanied by 1,2‐acyloxy migration. When enyne esters had an internal alkyne moiety, the reaction proceeded by a [4+1]‐type cycloaddition involving 1,3‐acyloxy migration, leading to cyclopentenones.     

Catalytic Enantioselective Synthesis of 1,4‐Keto‐Alkenylboronate Esters and 1,4‐Dicarbonyls

A catalytic enantioselective method for the synthesis of 1,4‐keto‐alkenylboronate esters by a rhodium‐catalyzed conjugate addition pathway is disclosed. A variety of novel, bench‐stable alkenyl gem‐diboronate esters are synthesized. These easily accessible reagents react smoothly with a collection of cyclic α,β‐unsaturated ketones, generating a new C?C bond and stereocenter. Products are isolated in up to 99 % yield with greater than 20:1 E/Z and greater than 99:1 e.r. Mechanistic studies show the site‐selectivity of transmetalation and reactivity is ligand dependent. The utility of the approach is highlighted by gram‐scale synthesis of enantioenriched cyclic 1,4‐diketones, and stereoselective transformations of the products by hydrogenation, allylation, and isomerization.     

Three closely related thienyl‐substituted 1,4‐epoxynaphtho[1,2‐b]azepines: hydrogen‐bonded assembly in one,two and three dimensions

(2R,4S)‐2‐(3‐Methylthiophen‐2‐yl)‐2,3,4,5‐tetrahydro‐1,4‐epoxynaphtho[1,2‐b]azepine, C₁₉H₁₇NOS, (I), crystallizes with a single enantiomer in each crystal, whereas its geometrical isomer (2RS,4SR)‐2‐(5‐methylthiophen‐2‐yl)‐2,3,4,5‐tetrahydro‐1,4‐epoxy‐naphtho[1,2‐b]azepine, (II), and (2RS,4SR)‐2‐(5‐bromothiophen‐2‐yl)‐2,3,4,5‐tetrahydro‐1,4‐epoxynaphtho[1,2‐b]azepine, C₁₈H₁₄BrNOS, (III), both crystallize as racemic mixtures. A combination of one C—H...O hydrogen bond and two C—H...π(arene) hydrogen bonds links the molecules of (I) into a three‐dimensional framework; the molecules of (II) are linked into a C(4)C(4)[R₂²(7)] chain of rings by a combination of C—H...N and C—H...O hydrogen bonds; and in (III), where Z′ = 2, a combination of four C—H...π(arene) hydrogen bonds and two C—H...π(thienyl) hydrogen bonds links the molecules into complex sheets. Comparisons are made with the assembly patterns in some aryl‐substituted 1,4‐epoxynaphtho[1,2‐b]azepines.     

Switching Regioselectivity of β‐Ketothioamides by Means of Iodine Catalysis: Synthesis of Thiazolylidenes and 1,4‐Dithiines

An efficient I₂‐catalyzed synthesis of thiazolylidenes and 1,4‐dithiines from β‐ketothioamides (KTAs) has been developed by only controlling the amount of I₂ that triggers different cascade reaction sequences by means of [3+2] or [3+3] cyclocondensation in a one‐step process. A possible mechanistic proposal for these transformations is presented.     

Rhodium‐Catalyzed Intramolecular [5+2] Cycloaddition of Inverted 3‐Acyloxy‐1,4‐enyne and Alkyne: Experimental and Theoretical Studies

By switching the position of the alkene and alkyne, a new type of 3‐acyloxy‐1,4‐enyne (ACE) five‐carbon building block was developed for Rh‐catalyzed intramolecular [5+2] cycloaddition. An electron‐withdrawing acyl group on the alkyne termini of the ACE was essential for a regioselective 1,2‐acyloxy migration. This new method provided bicyclic [5.3.0]decatrienes that are different from previous methods because of the positions of the alkenes and the acyloxy group. Multiple mechanistic pathways become possible for this new [5+2] cycloaddition and they are investigated by computational studies.     

B(C6F5)3‐Catalyzed Transfer Hydrogenation of Imines and Related Heteroarenes Using Cyclohexa‐1,4‐dienes as a Dihydrogen Source

The strong boron Lewis acid tris(pentafluorophenyl)borane, B(C₆F₅)₃, is shown to abstract a hydride from suitably donor‐substituted cyclohexa‐1,4‐dienes, eventually releasing dihydrogen. This process is coupled with the FLP‐type (FLP=frustrated Lewis pair) hydrogenation of imines and nitrogen‐containing heteroarenes that are catalyzed by the same Lewis acid. The net reaction is a B(C₆F₅)₃‐catalyzed, i.e., transition‐metal‐free, transfer hydrogenation using easy‐to‐access cyclohexa‐1,4‐dienes as reducing agents. Competing reaction pathways with or without the involvement of free dihydrogen are discussed.     

A tetrabromo‐1,4‐ethanonaphthalene and related dibromo‐1,4‐ethenonaphthalene

(1RS,3RS,4RS,10SR)‐2,2,3,10‐Tetrabromo‐1,2,3,4‐tetrahydro‐1,4‐ethanonaphthalene, C₁₂H₁₀Br₄, (I), is the first structure to be reported with four Br atoms bound to a 1,4‐ethanonaphthalene framework and also the first which possesses three Br atoms in exo positions. Interactions between the Br atoms [three short intramolecular Br...Br distances of 3.1094 (4), 3.2669 (4) and 3.4415 (5) Å] have little effect on the C—C bond lengths but lead to significant twisting of the cage structure compared with the parent hydrocarbon, which is expected to be fully eclipsed at the two saturated C₂H₄ bridge positions. Chemically related (1SR,4RS)‐2,3‐dibromo‐1,4‐ethenonaphthalene, C₁₂H₈Br₂, (II), obtained by double dehydrobromination of (I), represents the first structure of any halogen‐substituted benzobarrelene. This cis‐dibromide shows little evidence of steric congestion at the double bond [Br...Br = 3.5276 (8) Å] as a consequence of the large C—C—Br angles [average C=C—Br angle = 126.15 (10)°].     

The low‐melting compounds 1,4‐diethyl‐, 1,2‐diethyl‐ and ethylbenzene

Crystals of 1,4‐diethyl‐ and 1,2‐diethylbenzene, both C₁₀H₁₄, and ethylbenzene, C₈H₉, have been grown in situ. The molecules of 1,4‐diethyl‐ and 1,2‐diethylbenzene are located about a centre of inversion and across a twofold axis, respectively. In both molecules, the terminal methyl groups are located on opposite sides of the plane of the aromatic ring. In the crystal structures of all three compounds, molecules are linked together by (Ar)C—H...π and CH₂...π contacts. The methyl H atoms do not form close contacts with any of the aromatic π systems.     

Non‐isothermal crystallization kinetics and spherulitic morphology of nucleated poly(lactic acid): effect of dilithium cis‐4‐cyclohexene‐1,2‐dicarboxylate as a novel and efficient nucleating agent

The effect of dilithium cis‐4‐cyclohexene‐1,2‐dicarboxylate (CHDA‐Li) as a novel and efficient nucleating agent on the crystallization behaviors and spherulitic morphology of poly(lactic acid) (PLA) as well as non‐isothermal crystallization kinetics of the nucleated PLA was studied by means of differential scanning calorimetry and polarized light microscopy. The results show that CHDA‐Li serves as a good nucleating agent to accelerate the crystallization rate of PLA. The nucleation ability of CHDA‐Li is superior to octamethylenedicarboxylic dibenzoylhydrazide. With the incorporation of CHDA‐Li, the number of the spherulites increases, and the size decreases significantly. The non‐isothermal crystallization kinetics of the nucleated PLA can be well described by Jeziorny's and Mo's models. The activation energies (ΔE) of non‐isothermal crystallization were calculated by Kissinger's and Friedman's methods. The crystallization rate of PLA/0.5 wt% CHDA‐Li sample is faster than that of PLA/0.2 wt% CHDA‐Li sample, while the ΔE of the former is lower than that of the latter. Copyright © 2015 John Wiley & Sons, Ltd.     

Dehydrogenation of poly(1,3‐cyclohexadiene)–polystyrene binary block copolymers

The dehydrogenation of poly(1,3‐cyclohexadiene)–polystyrene binary block copolymers obtained by anionic copolymerization with alkyllithium/amine systems was investigated for the first time. The dehydrogenation of the poly(1,3‐cyclohexadiene) block, which was composed of 1,2‐cyclohexadiene (1,2‐CHD) and 1,4‐cyclohexadiene (1,4‐CHD) units, was strongly affected by the polymer chain structure. The existence of 1,2‐CHD units prevented the dehydrogenation of the poly(1,3‐cyclohexadiene) block in the binary block copolymer. The rate of dehydrogenation was fast on a long sequence of 1,4‐CHD units, whereas it was relatively slow for 1,2‐CHD/1,4‐CHD (≈1/1) unit sequences. The bonding of the polystyrene block to the polymer chain effectively improved not only the rate of dehydrogenation of a long sequence of 1,4‐CHD units but also that of the polymer chain with a high content of 1,2‐CHD units. The dehydrogenation of a poly(1,3‐cyclohexadiene) block containing a small number of 1,2‐CHD units progressed via step‐by‐step reactions. The dehydrogenation of a long sequence of 1,4‐CHD units proceeded as the first step. Subsequently, in the second step, the 1,2‐CHD/1,4‐CHD (≈1/1) unit sequences remaining in the polymer chain were dehydrogenated. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 44: 3526–3537, 2006     

Gold‐Catalyzed Sequential Cyclization of 1‐En‐3,9‐Diyne Esters to Partially Hydrogenated 3H‐Dicyclopenta[a,b]naphthalenes

A synthetic method that relies on a gold(I)‐catalyzed cycloisomerization of 1‐en‐3,9‐diyne esters to spiro[4.4]non‐2‐ene‐substituted 1,2‐dihydronaphthalenes is described. Robust with a wide variety of substitution patterns tolerated, the reaction provides the first example of a one‐step strategy to construct such novel and architecturally challenging members of the carbocycle family in good to excellent yields. A mechanism is proposed in which the sequential cycloisomerization pathway was thought to involve a gold‐catalyzed 1,3‐acyloxy migration/Nazarov cyclization followed by a formal [4+2] cycloaddition to give the tetracarbocyclic product.     

Conformational analysis of cycloheptane,oxacycloheptane, 1,2‐dioxacycloheptane, 1,3‐dioxacycloheptane,and 1,4‐dioxacycloheptane

The conformational analysis of cycloheptane (1), oxacycloheptane (2), 1,2‐dioxacycloheptane (3), 1,3‐dioxacycloheptane (4), and 1,4‐dioxacycloheptane (5) has been carried out using B3LYP, CCD, CCSD, and QCISD with the 6‐311+G(d,p) and cc‐pVDZ basis sets. The twist chair conformers are predicted to be lower in energy than their corresponding boat and chair conformations. All levels of theory predict (4) to be lower in energy than (3) and (5). CCSD predicts remarkably similar activation barriers for the conformational interconversion of the twist chair conformers to their corresponding boat conformers. Small barriers to pseudorotation are also predicted. © 2007 Wiley Periodicals, Inc. Int J Quantum Chem, 2008     

Theoretical study of enantiomeric and geometric control in chiral guanidine‐catalyzed asymmetric 1,4‐addition of 5H‐oxazol‐4‐ones

Density functional theory calculations are used to study the reaction mechanism and origins of high stereoselectivity in chiral guanidine‐catalyzed asymmetric 1,4‐addition of 5H‐oxazol‐4‐ones. The reaction involves proton abstraction of 5H‐oxazol‐4‐one, C—C bond formation, and proton transfer. N1 atom of chiral guanidine exchanges its character as base and acid to activate 5H‐oxazol‐4‐one and to facilitate the product formation. The role of N2—H2 is not only H‐bond donor for 5H‐oxazol‐4‐one but also electron accepter for N1. The enantioselectivity related with rate‐limiting step 1 and Z/E selectivity determined in step 2 are primarily influenced by a five to six‐membered ring link in the backbone of chiral guanidine. The reaction proceeds along the favorable path with smaller rotations of the linked bonds. The enantioselectivity is improved with guanidine involving an electron‐deficient and bulky substituent. With methyl ether‐protected hydroxy in structure, the catalytic ability and enantioselective control of guanidine are extraordinarily low, affording the opposite enantiomer as major product. Z‐isomers are preferred in all cases. © 2013 Wiley Periodicals, Inc.     

Novel and Stereospecific Synthesis of (2S)‐3‐(2,4,5‐Trifluorophenyl)propane‐1,2‐diol from D‐Mannitol

A stereospecific synthesis of (2S)‐3‐(2,4,5‐trifluorophenyl)propane‐1,2‐diol from D ‐mannitol has been developed. The reaction of 2,3‐O‐isopropylidene‐D ‐glyceraldehyde with 2,4,5‐trifluorophenylmagnesium bromide gave [(4R)‐2,2‐dimethyl‐1,3‐dioxolan‐4‐yl](2,4,5‐trifluorophenyl)methanol in 65% yield as a mixture of diastereoisomers (1 : 1). The Ph₃P catalyzed reaction of the latter with C₂Cl₆ followed by reduction with Pd/C‐catalyzed hydrogenation gave (2S)‐3‐(2,4,5‐trifluorophenyl)propane‐1,2‐diol with >99% ee and 65% yield.