Synthesis of some insect juvenile hormone analogues from thujone

Leyten, Wayne J.

January 1984

Treatment of cedar leaf oil with aqueous potassium permanganate resulted in the oxidative ring opening of thujone (XXIV) to yield the crystalline α-thujaketonic acid (XXV).⁷⁰ This material, because of its availability and interesting structure, represented an attractive starting material for the synthesis of analogues of insect juvenile hormone. Therefore, to achieve this aim, α-thujaketonic acid (XXV) was converted to form two products (or 'half-molecules') which were then coupled together and transformed to the analogues. In the initial study Grignard treatment of (XXV) produced an intermediate tertiary alcohol (LVIII) which cyclized spontaneously to a lactone (XXVI). The latter compound resisted further transformation and this approach was abandoned. On the other hand, (XXV) was refluxed in water to give β-thujaketonic acid (XXIX). This ring-opened acid was hydrogenated to give the ketoacid (XXX) which reacted with excess methylmagnesiurn iodide to yield the alcohol acid (XXXI). In the last reaction of this sequence some carboxylic acid was found to be converted to an alcohol ketone. This product (XXXII) was apparently formed via attack of the excess Grignard reagent (on to the salt of the acid) to yield the ketone from the acid. This alcohol ketone (XXXII) was reduced to a diol (XXXIII) and the latter converted to an acetate derivative (XXIV) 1n order to investigate its structure. Next, the desired alcohol acid (XXXI) was pyrolyzed to give the olefin acids (XXVII) and (XXVIII) which were separated via silver nitrate impregnated silica gel column chromatography. The required intermediate (XXVII) afforded one of the necessary products or 'half molecules'. In order to improve the overall yield of the required synthon (XXVII), α-thujaketonic acid was quantitatively converted to the methylene derivative (LIX) via reaction with two equivalents of methyl triphenyphosphorane.⁵⁹ Pyrolytic ring opening of the cyclopropane ring system in (LIX) afforded a good yield of the dienoic acid (XXXV). Reduction of the desired acid (XXXV) with potassium in liquid ammonia gave an 85% yield of the key intermediate (XXVII). The second required intermediate was synthesized via the esterification of β-thujaketonic acid (XXIX) with diazomethane in ether. This yielded the ketoester (XXXVII) which was used in the following coupling reaction sequence. Thus the key intermediate (XXVII) was treated with lithium diisopropylamide (LDA) in tetrahydrofuran (THF) to form the carboxylic acid dianion which was reacted with the keto ester (XXXVII) in THF to give a mixture of β-hydroxy carboxylic acids (XXXIX) and (XL). This product mixture was dissolved in dry pyridine and excess benzene-sulfonyl chloride was added 1n order to achieve the required cyclization to the expected olefinic β-lactones (XLI) and (XLII). Epoxidation of this mixture with metachloroperbenzoic acid (MCPBA) in methylene chloride yielded the corresponding epoxy β-lactones (XLIII) and (XLIV). The final step in the synthetic strategy was to utilize the pyrolytic decomposition of the intermediate β-lactone function to the central double bond inherent in the juvenile hormone systems. Therefore, the epoxy lactones (XLIII) and (XLIV) were subjected to such pyrolytic conditions but only decomposition products resulted. For this reason further studies with (XLIII) and (XLIV) were abandoned. The olefin acid (XXVII) was reacted with mercuric acetate in dry alcohol and the mercury intermediate thus derived was converted with sodium borohydride in methanol or ethanol to yield respectively the methoxy (IL) or the ethoxy acids (XLVIII). The ethoxy acid (XLVIII) was reacted with LDA in THF to give the expected carboxylic acid dianion, the latter upon addition of the ketoester (XXXVII) yielded a mixture of the β-hydroxycarboxylic acids (L) and (LI). This mixture was lactonized with benzenesulfonyl chloride in pyridine as described above to yield the ethoxy β-lactones (L11) and (LI 11). These were pyrolyzed and separated to give the juvenile hormone analogues (LIV) and (LV). Analogous investigations on the methoxy acid (IL) yielded the analogous β-hydroxy carboxylic acids (LVI) and (LVII). Time constraints precluded the conversion of these to the hormone analogues. / Science, Faculty of / Chemistry, Department of / Graduate

Thujone

Insect hormones

Kinetics of Atmospheric Reactions of Biogenic Volatile Organic Compounds: Measurement of the Rate Constant ofThujone + Cl· at 296 K and Calculation ofthe Equilibrium Constant for the HO2CH2CH2O2· H2O Complex

Killian, Marie Coy

19 April 2013

Biogenic volatile organic compounds (VOCs) react with Cl and OH radicals and the resulting radicals combine with oxygen to form peroxy radicals RO2. Organic peroxy radicals can then react with NO to form NO2, a precursor of tropospheric ozone. The work presented here explored the initial reaction between Cl and thujone, a VOC emitted by Great Basin sagebrush. The rate constant for the reaction of thujone + Cl at 296 K was measured with the method of relative rates with FTIR for detection of reactants. LEDs were used to photolyze Cl2 to generate Cl in the reaction cell. Thujone was also photolyzed by the LEDs and therefore the relative rates model was revised to account for this photolysis. With toluene as the reference compound, the rate constant for thujone + Cl at 296 K is 2.62 ± 1.90 × 10-12 molecules-1 s-1, giving an atmospheric lifetime of 0.5--2.6 minutes for thujone. Cline et al. showed that the rate of the self-reaction of HO2CH2CH2O2 (β-HEP) increases in the presence of water vapor. This enhancement has a strong temperature dependence with a greater enhancement observed at colder temperatures. The observed rate enhancement has been attributed to the formation of a β-HEP--H2O complex. In this work, the equilibrium constant for the formation of the β-HEP--H2O complex was calculated by ab initio calculations. Given the energy available at room temperature, the complex will populate three local minimum geometries and β-HEP will populate two local minimum geometries. The partition function for each of these geometries was calculated and used to calculate the equilibrium constant for complex formation as a function of temperature. Based on these computational results, the observed temperature dependence for the rate enhancement can be attributed to the strong temperature dependence for the rate constant of the reaction of β-HEP--H2O + β-HEP rather than the temperature dependence of complex formation.

biogenic volatile organic compounds

thujone

Cl atom

relative rates

peroxy radical-water complex

HOCH2CH2O2

β-HEP

water vapor

Biochemistry

Chemistry