Bruce O. Linn scite author profile

The reactions of sulfonate esters of the allylic/homoallylic 13-alcohol of 5-O-(tert-butyldimethylsilyl)-22,23-dihydroavermectin B1a aglycon (1a) were investigated. Nucleophilic substitution gave 13 beta-chloro and 13 beta-iodo derivatives, while solvolytic reaction conditions yielded 13 alpha-methoxy, 13 alpha-fluoro, and 13 alpha-chloro products. A mixture of 13 alpha- and 13 beta-fluorides was obtained upon reaction with DAST. The 13 beta-iodide gave, upon elimination with lutidine, the 8(9),10(11),12(13),14(15)-tetraene. The 13 beta-alcohol and the rearranged 15-ol 13(14)-ene and 15-amino 13(14)-ene derivatives were obtained by substitution via the allylic carbonium ion. MEM ethers 11 and 12 of the two epimeric 13-ols were prepared by alkylation with MEM chloride. In contrast, methylation of 1a with MeI and Ag2O in CH2Cl2 occurred exclusively at the tertiary 7-hydroxy group and not at the secondary 13 alpha-ol. Oxidation of the allylic alcohol 1a proceeded under Swern conditions but not with MnO2 to the 13-oxo aglycon, which was reduced by NaBH4 exclusively to the natural 13 alpha-ol, while reductive amination with NaCNBH3-NH4OAc gave the 13 alpha-amine. The methoxime derivative was obtained in the form of the two geometric isomers. Anthelmintic activities against the sheep nematode Trichostrongylus colubriformis, miticidal activities against the two-spotted spider mite (Tetranychus urticae), and insecticidal activities against the southern armyworm (Spodoptera eridania) as well as the binding constants to a free living nematode (Caenorhabditis elegans) derived receptor assay were obtained and compared to avermectin B1a, 22,23-dihydroavermectin B1a, and the 13-deoxy-22,23-dihydroavermectin B1 aglycon related to the milbemycins. None of the newly prepared derivatives exceeded the potency of the three reference compounds. Lipophilic 13-substituents such as halogen, alkoxy, and methoxime retained high biological activities in all assays, while the more polar substituents hydroxy and amino had weaker activities. Rearranged 15-substituted 13(14)-ene derivatives were completely inactive. The 13-oxo and the 12,13-dehydro analogues were only weakly active in vivo despite having good binding affinity to the receptor, possibly due to instability or poor absorption.

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Rapid loss of ATP by tumor cells deprived of glucose: Contrast to normal cells

Demetrakopoulos

Linn

Amos

1978

Biochemical and Biophysical Research Communications

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Bruce O. Linn

Discovery of novel avermectins with unprecedented insecticidal activity

Coenzyme Q. I. Structure Studies on the Coenzyme Q Group

Coenzyme Q. VII. Isolation and Distribution of Coenzyme Q₁₀ in Animal Tissues

Syntheses and biological activities of 13-substituted avermectin aglycons

Rapid loss of ATP by tumor cells deprived of glucose: Contrast to normal cells

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About

Bruce O. Linn

Discovery of novel avermectins with unprecedented insecticidal activity

Coenzyme Q. I. Structure Studies on the Coenzyme Q Group

Coenzyme Q. VII. Isolation and Distribution of Coenzyme Q10 in Animal Tissues

Syntheses and biological activities of 13-substituted avermectin aglycons

Rapid loss of ATP by tumor cells deprived of glucose: Contrast to normal cells

Contact Info

Product

Resources

About

Coenzyme Q. VII. Isolation and Distribution of Coenzyme Q₁₀ in Animal Tissues