Acyl- und Alkylidenphosphane. XXIV. (N,N-Dimethylthiocarbamoyl)trimethylsilylphosphane und 1,2-Di(tert-butyl)-3-dimethylamino-1-thio-4-trimethylsilylsulfano-1λ5,2λ3-diphosphet-3-en

Acyl- and Alkylidenephosphines. XXIV. (N,N-Dimethylthiocarbamoyl)trimethylsilyl-phosphines and 1.2-Di(tert-butyl)-3-dimethylamino-1-thio-4-trimethylsilylsulfano-1λ⁵, 2λ³-diphosphet-3-ene In contrast to bis(trimethylsilyl)phosphines R? P[? Si(CH₃)₃]₂ 1 {R ? H₃C a ; (H₃C)₃C b ; H₅H₆ c ; H₁₁C₉ d ; (H₃C)₃Si e }, the more nucleophilic lithium trimethylsilylphosphides 4 react with N,N-dimethylthiocarbamoyl chloride already at ?78°C to give (N,N-dimethylthiocarbamoyl)trimethylsilylphosphines 2 . Working up the reaction, a dismutation of the mesityl derivative 2d is observed, whereas the tert-butyl compound 2b dissolved in toluene, eliminates dimethyl(trimethylsilyl)amine to form 1,2-di(tert-butyl)-3-dimethylamino-1-thio-4-trimethylsilyl-sulfano- 1λ⁵, 2λ³-diphosphet-3-ene 6b , nearly quantitatively within several days at +20°C.     

Element-Element-Bindungen. I. Synthese und Struktur des Tetra(tert-butyl)tetrarsetans und des Tetra(tert-butyl)tetrastibetans

Element-Element Bonds. I. Syntheses and Structure of Tetra(tert-butyl)tetrarsetane and of Tetra(tert-butyl)tetrastibetane Dilithium (tert-butyl)arsenide reacts with (tert-butyl)dichloroarsine to give tetra-(tert-butyl)tetrarsetane 1 ; homologous tetra(tert-butyl)tetrastibetane 2 is formed by reduction of (tert-butyl)dichlorostibane with magnesium. The isotypic compounds 1/2 crystallize in the monoclinic space group P2₁/c with Z = 4. The dimensions of the unit cells determined at ?45 ± 5°C are: a = 957.4(8)/1 000.2(3); b = 1 399.1(14)/1 423.9(4); c = 1 697.4(9)/1 749.8(7) pm; β = 96.02(6)/96.77(3)°. As shown by low temperature X-ray structure determinations (3 531/3 232 symmetry independent reflections; R_g = 4.0/4.6%) the four membered rings E₄ (E = As or Sb) are folded; in all-trans configuration the bulky organic substituents occupy pseudo-equatorial positions. Characteristic averaged bond distances and angles are: E? E 244/282; E? C 202/221 pm; ? E? E? E 86/85° ? E? E? C 101/99°. The dihedral angels of the bisphenoides built up by the atoms of the rings are found to be 139/133°.     

Synthese und Molekülstruktur des (N,N′ -Dimethylpiperazin)lithium-(μ-hydrido)(tert-butyl)bis[bis(trimethylsilyl)methyl]alanats mit intramolekularer Wechselwirkung zwischen Lithium und C?H?σ-Bindungen

Synthesis and Molecular Structure of (N,N′-Dimethyl-piperazine)lithium-(·-hydrido)(tert-butyl)bis[bis(trimethylsilyl)methyl]alanate with an Intramolecular Interaction between Lithium and C? H-σ-Bonds Syntheses and properties of the starting compounds bis[bromo-di(tert-butyl)alane] 3 , bis[dibromo-tert-butyl-alane] 4 , and (tert-butyl)bis[bis(trimethylsilyl)methyl]alane 5 are described. In the presence of 5 and the chelating amine N,N′-dimethylpiperazine lithium tert-butyl gives via μ-elimination isobutene and LiH, which is taken up by the starting alane 5 to give the title compound 6 . No attack of the strong base (lithium alkyl/amine) to the bis(trimethylsilyl) methyl substituent is observed as recently occured for the sterically more crowded tris[bis(trimethylsilyl)methyl]alane. Crystal structure of 6 shows a angled Li? H? Al bridge and a short intramolecular contact between Li and C? H-σ-bonds of a trimethylsilyl group.     

Acyl- und Alkylidenphosphane. XXV. Molekül- und Kristallstruktur des 1,2-Di(tert-butyl)-3-dimethylamino-1-thio-4-trimethylsilylsulfano-1λ5,2λ3-diphosphet-3-ens

Acyl- and Alkylidenephosphines. XXV. Molecular and Crystal Structure of 1,2-Di(tert-butyl)-3-dimethylamino-1-thio-4-trimethylsilylsulfano-1λ⁵, 2λ³-diphosphet-3-ene The title compound 1 formed in a nearly quantitative yield by decomposition of tert-butyl(N,N-dimethylthiocarbamoyl)trimethylsilylphosphine, crystallizes in the orthorhombic space group P2₁2₁2₁ with {a = 1067.3(1); b = 1077.1(1); c = 1924.6(5) pm; Z = 4} at +20°C. An X-ray structure determination (R_G = 0.038) shows two tert-butyl groups at a four- (P1) and a three-coordinate phosphorus atom (P2) to be placed on different sides of the four membered ring. Characteristic bond lengths as well as the angles at the atoms P1, P2, C3, and C4 inside the ring have already been given above.     

Synthese und Struktur von Lithium-tris(trimethylsilyl)silanid · 1,5 DME

Synthesis and Structure of Lithium Tris(trimethylsilyl)silanide · 1,5 DME Lithium tris(trimethylsilyl)silanide · 1,5 DME 2a synthesized from tetrakis(trimethylsilyl)silane 1 [6] and methyllithium in 1,2-dimethoxyethane , crystallizes in the monoclinic space group P2₁/c with following dimensions of the unit cell determined at a temperature of measurement of ?120 ± 2°C: a = 1 072.9(3); b = 1 408.3(4); c = 1 775.1(5) pm; β = 107.74(2)°; 4 formula units (Z = 2). An X-ray structure determination (R_w = 0.040) shows the compound to be built up from two [lithium tris(trimethylsilyl)silanide] moieties which are connected via a bridging DME molecule. Two remaining sites of each four-coordinate lithium atom are occupied by a chelating DME ligand. The Li? Si distance of 263 pm is considerably longer than the sum of covalent radii; further characteristic mean bond lengths and angles are: Si? Si 234, Li? O 200, O? C 144, O?O (biß) 264 pm; Si? Si? Si 104°, Li? Si? Si 107° to 126°; O? Li? O (inside the chelate ring) 83°. Unfortunately, di(tert-butyl)bis(trimethylsilyl)silane 17 prepared from di(tert-butyl)dichlorsilane 15 , chlorotrimethylsilane and lithium, does not react with alkyllithium compounds to give the analogous silanide.     

Acyl- und Alkylidenphosphane. XXVI. 2, 4-Bis(phenylimino)-1,3-diphosphetane aus Thiocarbamoyl- und Carbamoyltrimethylsilylphosphanen

Acyl-and Alkylidenephosphines. XXVI. 2, 4-Bis (phenylimino)-1, 3-diphosphetanes from Thiocarbamoyl- and Carbamoyltrimethylsilylphosphines . Bis(trimethylsilyl)phosphines R? P[? Si(CH₃)₃]₂ 1 (R = H₃C a, H₅C₆ b, (H₃C)₃C e, H₁₁C₉ d) and phenyl isothiocyanate give insertion compounds which were identified as [CN-phenyl, N-trimethylsilyl)thiocarbamoyl]trimethylsilylphosphines 3 ? 2 in solution as well as in the solid state [2]. In the presence of small amounts of solid sodium hydroxide the phenyl derivative 3 ? 2b eliminates bis(trimethylsilyl) sulfane, whereas the tert-butyl 3 ? 2c and the mesityl compound 3 ? 2d show the same reaction even without a catalyst. The unstable [(phenylimino)methylidene]phosphines 6 formed first, dimerize rapidly to give 2, 4-bis(phenylimino)-1,3-diphosphetanes 7 which in solution exist as mixtures of the E and Z isomers. Via a NaOH-catalyzed elimination of hexamethyldisiloxane these cyclic phosphines 7 can also be obtained from the adducts of phenyl isocyanate and bis(trimethylsilyl)phosphines 1. Taking the thermally sufficiently stable tert-butyl derivative 7 c as an example, the temperature dependence of n.m.r. spectra is discussed in detail.     

Umsetzung von Di(tert-butyl)- und Diphenyldiazomethan mit 1,3-Thiazol-5(4H)-thionen: Isolierung und Kristallstruktur des primären Cycloadduktes

Reaction of Di(tert-butyl)- and Diphenyldiazomethane and 1,3-Thiazole-5(4H)-thiones: Isolation and Crystal Structure of the Primary Cycloadduct Reactions of diazo compounds with C?S bonds proceed via the formation of thiocarbonyl ylides, which, under the reaction conditions, undergo either 1,3-dipolar cycloadditions or electrocyclic ring closer to thiiranes (Scheme 1). With the sterically hindered di(tert-butyl)diazomethane ( 2c ), 1,3-thiazole-5(4H)-thiones 1 react to give spirocyclic 2,5-dihydro-1,3,4-thiadiazoles 3 (Scheme 2). These adducts are stable in solution at ?20°, and they could be isolated in crystalline form. The structure of 3c was established by X-ray crystallography. In CDCl₃ solution at room temperature, a cycloreversion occurs, and the adducts of type 3 are in an equilibrium with 1 and 2c . In contrast, the reaction of 1 with diphenyldiazomethane ( 2d ) gave spirocyclic thiiranes 4 as the only product in high yield (Scheme 3). The crystal structure of 4b was also determined by X-ray analysis. The desulfurization of compounds 4 to 4,5-dihydro-5-(diphenylmethylidene)-1,3-thiazoles 5 was achieved by treating 4 with triphenylphosphine in boiling THF. The crystal structure of 5f is shown.     

Amino‐ und halogenfunktionelle Siloxititane

Amino‐ and halofunctional Siloxititanes Amino‐di‐tert‐butylsilanol reacts with tetrabutoxititane in a molar ratio of 2:1 to give di‐n‐butoxi(bis(di‐tert‐butyl‐n‐butoxi)siloxi)titane, (C₄H₉OSi(CMe₃)₂‐O)₂Ti(OC₄H₉)₂ ( 1 ), and lithium‐di‐tert‐butylchlorosilanolate in a molar ratio of 3:1 to give n‐butoxi(tris(di‐tert‐butyl‐n‐butoxi)siloxi)titane, (H₉C₄OSi(CMe₃)₂‐O)₃TiOC₄H₉ ( 2 ). The amino‐di‐tert‐butylsilanol substitutes the four chloroatoms of TiCl₄ in the presence of triethylamine as HCl‐acceptor. The tetrakis(amino‐di‐tert‐butyl)siloxititane ( 3 ) is formed. The lithium salt of di‐tert‐butylfluorosilanol reacts with TiCl₄ in a molar ratio of 2:1 to give 1, 1, 3, 3‐tetra‐tert‐butyl‐1‐fluoro‐3‐trichlorotitoxi‐1, 3‐disiloxane, FSi(CMe₃)₂‐O‐Si(CMe₃)₂‐O‐TiCl₃ ( 4 ). In the reaction of di‐tert‐butyl‐chlorosilanol and TiCl₄, the anion [chlorosiloxi‐octa(tri‐μ²‐chlorotitanate)]^— ( 5 ) with protonated diethylether as counterion is obtained by using diethylether as HCl‐acceptor. The crystal structure determinations of 3 and 5 are reported.     

Synthesis of salicylaldehydes bearing bulky substituents in the positions 3 and 5

Reaction of 2,4-disubstituted phenols with paraformaldehyde in the presence of SnCl₄ and 2,6-lutidine afforded a number of new salicylaldehydes, containing bulky substituents (tert-butyl, 1-phenylethyl, 1-(4-tert-butylphenyl)ethyl, α-cumyl, and trityl) in the positions 3 and 5. Dedicated to the memory of Academician N. N. Vorozhtsov on the 100th anniversary of his birth. Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 6, pp. 1084–1088, June, 2007.     

Is2Si(Li)?P(Li)SiR3 (Is = 2,4,6-iPr3C6H2): die ersten Lithiumsilanidyl-lithiumphosphanide und ihre Umwandlung in Disilaphosphirane und neuartige Mercuriophosphane

Is₂Si(Li)? P(Li)SiR₃ (Is = 2,4,6-ⁱPr₃C₆H₂): The First Lithiumsilanidyl-lithiumphosphanides and their Transformation into Disilaphosphiranes and Novel Mercuriophosphanes Upon addition of two mol equivalents lithium metal to the Si?P bond of the silylidenephosphanes (“phosphasilenes”) Is₂Si?P(SiⁱPr₃) and Is₂Si?P(SiPh₂Me) (Is = 2,4,6-ⁱPr₃C₆H₂) in tetrahydrofurane, the corresponding lithiumsilanidyl-lithiumsilylphosphanides are formed, which have been isolated as pale yellow solids; each Li center is solvated by two tetrahydrofurane molecules. The constitution of these compounds is established by multi nuclei NMR spectroscopy and derivatization reactions with water, deuteriumoxide, dichlorodimethylsilane, and tert-butylmercuriochloride, respectively. The reaction with dichlorodimethylsilane yields, via cyclocondensation reaction and elimination of lithiumchloride, the first disilaphosphacyclopropane derivatives, and the reaction with tert-butylmercuriochloride gives, under loss of the triorganosilyl group at phosphorus and via rearrangement processes, an unusual P, P-dimercuriosilylphosphane; the latter reacts with tert-butylmercuriochloride and mercuriodichloride in the molar ratio of 2 : 1 : 1 to give an molecular aggregate bearing a P₂Hg₆Cl₃ framework, which can be regared as an Lewis-acid base complex of a mercuriophosphane chelate ligand and mercuriodichloride.     

Interactions intramoléculaires. XXVI—Constantes de couplage et hétérogénéités conformationnelles dans une série de R-3 et R-5 cyano-4 cyclohexènes deutériés (R=méthyl ou t-butyl)

For trans-3-R- and 5-R-1-acetoxy-4-cyanocyclohexene-6,6-d₂ the molar fractions of diequatorial conformers are 0.83 (3-methyl), 0.68 (5-methyl), 0.57 (3-tert-butyl) and 0.55–0.69 (5-tert-butyl). For the last two compounds the values of the coupling constants are in agreement with the hypothesis of an ee?aa equilibrium. For the cis isomers, the molar fractions of equatorial alkyl conformers are 0.76 (3-methyl and 5-methyl) and 1.0 (3-tert-butyl and 5-tert-butyl). The cis-1-acetoxy-3-tert-butyl-4-methoxycarbonyl-cyclohexene presents a conformational heterogeneity. The conformational free energy of the methyl group in position 4 has been evaluated as ?0.6 kcal mol^?1 (2.5 kJ mol^?1).     

Beiträge zur Chemie des Phosphors. 224. Zur Thermolyse von 1,2-Di-tert-butyldiphosphan, 1,2,3-Tri-tert-butyltriphosphan und Tetra-tert-butylcyclotetraphosphan

Contributions to the Chemistry of Phosphorus. 224. On the Thermolysis of 1,2-Di-tert-butyldiphosphane, 1,2,3-Tri-tert-butyltriphosphane, and Tetra-tert-butylcyclotetraphosphane On disproportionation of 1,2-di-tert-butyldiphosphane, H(t-Bu)P? P(t-Bu)H (1) , 1,2,3-tri-tert-butyltriphosphane, H₂(t-BuP)₃ (2) , is formed which reacts further at temperatures above 100°C to give 1-(tert-butylphosphino)-2,3,4-tri-tert-butylcyclotetraphosphan, P₅(t-Bu)₄H (4) . Compound 4 reacts with 1 or 2 with lengthening of the P-sidechain to furnish the corresponding 1-(1,2-di-tert-butyldiphosphino)-2,3,4-tri-tert-butylcyclotetraphosphane, P₆(t-Bu)₅H (5) . At temperatures above 170°C, 5 disproportionates into the tetra-tert-butylcyclotetraphosphane, (t-BuP)₄ (3) which is stable up to about 200°C, and the bicyclo[3.1.0]hexaphosphane P₆(t-Bu)₄ from which the polycyclophosphanes P₉(t-Bu)₃ and P₈(t-Bu)₆ arise during the further course of the thermolysis. These products are finally converted through even more phosphorus-rich and more highly condensed t-butylcyclophosphanes into elemental phosphorus. In each reaction step, varying amounts of the monophosphane derivatives t-BuPH₂, (t-Bu)₂PH, and (t-Bu)₃P are formed. The proposed course of the reaction is further substantiated by the pyrolysis products of pure 2 and 3 .     

Enantioselektive α-Alkylierung von Asparagin- und Glutaminsäure über die Dilithium-enolatocarboxylate von 2-[3-Benzoyl-2-(tert-butyl)-1-methyl-5-oxoimidazolidin-4-yl]essigsäure und 3-[3-Benzoyl-2-(tert-butyl)-1-methyl-5-oxoimidazolidin-4-yl]propionsäure

Overall Enantioselective α-Alkylation of Aspartic and Glutamic Acid through Dilithium Enolatocarboxylates of 2- [3-Benzoyl-2-(tert-butyl)-1-methyl-5-oxoimidazolidin-4-yl]acetic and 3-[3-Benzoyl-2-(tert-butyl)-1-methyl-5-oxoimidazolidin-4-yl]propionic Acid, respectively The pure methyl esters 10 of the heterocyclic carboxylic acids specified in the title were prepared in several steps by known methods from aspartic and glutamic acid, with overall yields of ca. 20%. The corresponding heterocyclic acids 11 were doubly deprotonated by LiNEt₂/BuLi or LiN(i-Pr)₂/BuLi to give enolatocarboxylates ( 3 ). The latter were reacted with electrophiles (MeOD, Mel, C₆H₅CH₂Br) to give the crystalline products 14 – 21 diastereoselectively. Hydrolysis of the imidazolidinone ring of three such products gave the corresponding α-branched aspartic and glutamic acids 22 – 24 of known absolute configuration, thus establishing the stereochemical course of the overall enantioselective alkylations.     

2,2‐Difluor‐1,3‐diaza‐2‐sila‐cyclopenten – Synthese und Reaktionen

2,2‐Difluor‐1,3‐diaza‐2‐sila‐cyclopentene – Synthesis and Reactions N,N′‐Di‐tert‐butyl‐1,4‐diaza‐1,3‐butadiene reacts with elemental lithium under reduction to give a dilithium salt, which forms with fluorosilanes the diazasilacyclopentenes 1 – 4 ; (HCNCMe₃)₂SiFR, R = F ( 1 ), Me ( 2 ), Me₃C ( 3 ), N(CMe₃)SiMe₃ ( 4 ). As by‐product in the synthesis of 1 , the tert‐butyl‐amino‐methylene‐tert‐butyliminomethine substituted compound 5 was isolated, R = N(CMe₃)‐CH₂‐CH = NCMe₃. 5 is formed in the reaction of 1 with the monolithium salt of the 1,4‐diaza‐1,3‐butadiene in an enamine‐imine‐tautomerism. 1 reacts with lithium amides to give (HCNCMe₃)₂SiFNHR, 6 – 12 , R = H ( 6 ), Me ( 7 ), Me₂CH ( 8 ), Me₃C ( 9 ), H₅C₆ ( 10 ), 2,6‐Me₂C₆H₃ ( 11 ), 2,6‐(Me₂CH)₂C₆H₃ ( 12 ). The reaction of 12 with LiNH‐2.6‐(Me₂CH)₂C₆H₃ leads to the formation of (HCNCMe₃)₂Si(NHR)₂, ( 13 ). In the presence of n‐BuLi, 12 forms a lithium salt which looses LiF in boiling toluene. Lithiated 12 adds this LiF and generates a spirocyclic tetramer with a central eight‐membered LiF‐ring ( 14 ), [(HCNCMe₃)₂Si(FLiFLiNR)]₄, R = 2,6‐(Me₂CH)₂C₆H₃. ClSiMe₃ reacts with lithiated 12 to yield the substitution product (HCNCMe₃)₂SiFN(SiMe₃) R, ( 15 ). The crystal structures of 1 , 5 , 6 , 9 , 11 , 13 , 14 are reported.     

2,4‐Disila‐1,3,5‐oxadiazin,Cyclodisilazan‐Carbonsäure‐silylamid und ‐silylester

The lithium salts of the Me₃Si‐ as well as Me₃Si‐ and Me₂SiF‐substituted Cyclotrisilazanes I and II react with tert‐butylacylchloride under ring contraction and formation of the cyclodisilazane‐silylester, Me₃SiN(SiMe₂–N)₂SiMe₂–O–CO–CMe₃ ( 1 ). The lithium salt of the fluorodi‐methylsilyl‐substituted cyclotrisilazan III forms with benzoylchloride primarily in the analogous reaction the carboxy‐silyl‐amide, Me₂SiF(N–SiMe₂)₂SiMe₂–NH–CO–C₆H₅⁺ ( 2 ), which can be converted with III and benzoylchloride into the cyclodisilazane‐silylester, Me₂SiF(NSiMe₂)₂SiMe₂–O–CO–C₆H₅, ( 3 ). A silylester substituted six‐membered disila‐oxadiazine ( 4 ) is the result of the reaction of the lithiated cyclotrisilazane, (Me₂SiNH)₂, (Me₂SiNLi) with tert‐butyl‐acylchloride. The reaction includes anionic ring contraction and can be rationilized by a process analogous to keto‐enol‐tautomerism. Dilithiated octamethyl‐cyclotetrasilazane, (Me₂SiNHMe₂SiNLi)₂, reacts with tert‐butyl‐acylchloride or benzoylchloride in a molar ratio 1:2 to yield symmetrically acylestersubstituted cyclodisilazanes, (RCO–O–SiMe₂–NSiMe₂)₂, R = C₆H₅ ( 5 ), CMe₃ ( 6 ). The reaction mechanisms are discussed and the crystal structures of 2 and 6 are reported.     

Organomagnesium Synthesis of <Emphasis Type="Italic">sec</Emphasis>-Butyl- and <Emphasis Type="Italic">tert</Emphasis>-Alkylchlorogermanes and Their Reaction with Ethynylmagnesium Bromide

The limits of application of organomagnesium synthesis to the substitution of chlorine atoms in tetrachlorogermane with bulky alkyl groups are established. The reaction of tetrachlorogermane with 2-butylmagnesium chloride leads to the substitution of one, two, or three chlorine atoms, yielding the corresponding alkylchlorogermanes (MeEtCH)_nGeCl_4-n . The reaction of GeCl₄ with tert-alkylmagnesium halides leads to the substitution of only one chlorine atom, yielding tert-alkyltrichlorogermanes RMe₂CGeCl₃ (R = Me, Et, Bu). tert-Butyltrichlorogermane reacts with ethylmagnesium bromide to give ethyl(tert-butyl)dichlorogermane. Isopropyltrichlorogermane reacts with tert-butylmagnesium chloride to give isopropyl(tert-butyl)dichlorogermane. This shows that the organomagnesium synthesis does allow linking of two bulky substituents to the germanium atom. The reaction of tert-alkyltrichlorogermanes and 2-butyltrichlorogermane in THF with ethynylmagnesium bromide, in which the hydrocarbon group is the most sterically accessible, allows substitution of all the three chlorine atoms, yielding the corresponding alkyl(triethynyl)germanes. The latter compounds react with the Grignard reagent and trimethylchlorosilane to give the corresponding alkyl(trimethylsilylethynyl)germanes.__________Translated from Zhurnal Obshchei Khimii, Vol. 75, No. 5, 2005, pp. 757–761.Original Russian Text Copyright © 2005 by O. Yarosh, Voronkov, Zhilitskaya, N. Yarosh, Albanov, Korotaeva.     

Alkylation of pyridine-3,5-dicarboxamide and pyridine-3,5-dicarbonitriles by radical substitution

Structural modification of NAD(P) model compounds, N,N,N',N'-tetramethylpyridine-3,5-dicarboxamide ( 1 ), pyridine-3,5-dicarbonitrile ( 2 ), and 4-methylpyridine-3,5-dicarbonitrile ( 3 ), have been explored by the reaction with alkyl radicals such as the 1-adamantyl, tert-butyl, and isopropyl radicals. The alkyl substitutions of compounds 1 , 2 , and 3 with the 1-adamantyl and the tert-butyl radical gave both 2-mono and 2,6-disubstitution products, whereas the reaction of compound 2 with the isopropyl radical gave 2-mono 6c , 2,4-di 7c, 2,6-di 8c , and 2,4,6-trisubstitution 9c products.     

Mechanism of initiation of methyl methacrylate with lithium tert-alkoxides

An investigation of the solution polymerization of methyl, butyl, isobutyl, sec-butyl, and tert-butyl methacrylates and the polymerization of methyl and butyl methacrylates in the presence of methyl, butyl, and tert-butyl isobutyrate and methyl pivalate showed that the complex order of the initiation reaction with respect to the monomer (about 2) has its cause in the ability of the ester group in the monomer and of methyl or butyl isobutyrate to activate lithium tert-alkoxide. Owing to conjugation, the ester group in the monomer is less active than the ester group in isobutyrate. Steric hindrances of the formation of a complex between lithium tert-alkoxide and ester were also investigated, because this complex is intermediate product necessary for the formation of an activated lithium tert-alkoxide, capable of initiating the polymerization of alkyl methacrylates of the type CH₂?(CH₃)COOCH₂R.     

1,4-Diazobicyclo[2.2.2]octane-catalyzed coupling of aldehydes and activated double bonds. Part 3. A short ans practical synthesis of mikanecic acid (4-vinyl-1-cyclohexene-1,4-dicarboxylic acid)

The title dicarboxylic acid 1d has been prepared in 24% overall yield via, 1,4-diazabicyclo[2.2.2]octane (DABCO)-catalyzed coupling of ethanal and tert-butyl propenoate ( 3 ) to 4 , S_N2′-reaction to tert-butyl (Z)-2-romomethyl-2-butenoate ( 5a ), dehydrobrominatin to tert-butyl 2-methylidene-3-butenoate ( 2c ), dimerizatoin to di-tert-butyl 4-vinyl-1-cyclohexene-1,4-dicarboxylate ( 1c ) and acidic ester cleavage. Acidic cleavage of easily obtainable 5a affords (Z)-2-bromomethyl-2-butenoic acid ( 5a ) in 68% yield with respect to ethanal.     

The Synthesis of tert‐Butyl(dichloromethyl)bis(trimethylsilyl)silane and (Dibromomethyl)ditert‐butyl(trimethylsilyl)silane and their Reactions with Organolithium Derivatives

tert‐Butyl(dichloromethyl)bis(trimethylsilyl)silane ( 4 ), prepared by the reaction of tert‐butylbis(trimethylsilyl)silane with trichloromethane and potassium tert‐butoxide, reacted with 2,4,6‐triisopropylphenyllithium (TipLi) (molar ratio 1 : 2) at room temperature to give (after hydrolytic workup) the silanol tBu(2,4,6‐iPr₃C₆H₂)Si(OH)–CH(SiMe₃)₂ ( 15 ). The formation of 15 is discussed as proceeding through the indefinitely stable silene tBu(2,4,6‐iPr₃C₆H₂)Si=C(SiMe₃)₂ ( 13 ), but attempts to isolate the compound failed. Treatment of (dibromomethyl)ditert‐butyl(trimethylsilyl)silane ( 7 ), made from tBu₂(Me₃Si)SiH, HCBr₃ and KOtBu, with methyllithium (1 : 3) at –78 °C afforded tBu₂MeSi–CHMeSiMe₃ ( 19 ); 7 and phenyllithium (1 : 3) under similar conditions gave tBu₂PhSi–CH₂SiMe₃ ( 20 ). The reaction paths leading to 15 , 19 and 20 are discussed. Reduction of 7 with lithium in THF produced the substituted ethylene tBu₂(Me₃Si)SiCH=CHSitBu₂SiMe₃ ( 21 ). For 21 the results of an X‐ray structural analysis are given.