Synthesis and Anti-Juvenile Hormone Activity of Ethyl 4-[2-(6-Methyl-3-pyridyloxy)alkyloxy]benzoates

Fujita, Norihiro; Furuta, Kenjiro; Shirahashi, Hiromitsu; Hong, Soonsung; Shiotsuki, Takahiro; Kuwano, Eiichi

doi:10.1584/jpestics.30.192

Cited by 11 publications

(12 citation statements)

References 16 publications

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“…The introduction of an n-propyl group (4) increased the degree of activity in comparison with that of 3. In contrast to the results found in ethyl 4-[2-(6-methyl-3-pyridyloxy)alkyloxy]benzoate series, 7) isobutyl analog 5 showed lower activity than n-propyl analog 4. The n-butyl group (6) gave a remarkable increase in activity at a low dose of 1 mg, but the activity comparatively decreased by increasing the applied doses.…”

Section: Synthesiscontrasting

confidence: 96%

“…Similar results have been obtained in the 4-[2-(6-methyl-3-pyridyloxy)-alkyloxy]benzoate series. 7) As previously described, precocious metamorphosis is well known to be induced by JH deficiency in the larval stage caused by allatectomy or treatment of anti-JH agents 2) ; however, we have found that the precocious metamorphosis-inducing activity of some 1,5-disubstituted imidazoles is completely reversible by the dietary administration of 20-hydroxyecdysone, suggesting that a temporary decline of ecdysteroid titers in the larval hemolymph might also cause precocious metamorphosis. 12) We therefore examined the effects of methoprene, a JH agonist, and 20-hydroxyecdysone on the precocious metamorphosis induced by 6 ( Table 3).…”

Section: Biological Activitiessupporting

confidence: 43%

“…By modifying the structure of ETB, we have recently found that ethyl 4-[4-methyl-2-(6-methyl-3-pyridyloxy)pentyloxy]-benzoate (1) 7) and ethyl 4-(2-phenoxyhexyloxy)benzoate (2) 8) showed stronger precocious metamorphosis-inducing activity than ETB against B. mori larvae (Fig. 1).…”

Section: Introductionmentioning

confidence: 99%

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Synthesis and anti-juvenile hormone activity of ethyl 4-(2-benzylalkyloxy)benzoates and their enantiomers

et al. 2007

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A number of ethyl 4-(2-benzylalkyloxy)benzoates were prepared and their activity to induce precocious metamorphosis was evaluated in larvae of the silkworm, Bombyx mori, which was clearly recognized as a juvenile hormone (JH)-deficiency symptom. Ethyl 4-(2-benzylhexyloxy)benzoate (6) and its 2-benzylheptyloxy analog (7) were found to induce precocious metamorphosis at relatively low doses. Both enantiomers of 6 and 7 were prepared using a chiral auxiliary oxazolidinone. (S)-Enatiomers were more active than (R)-isomers at low doses of 0.1 and 1 mg, but at higher doses their activity was reversed. The activity of compound 6 could be fully counteracted by methoprene, a JH agonist, but not by the dietary administration of 20-hydroxyecdysone. The ester group was important in the ability to induce precocious metamorphosis. The (S)-enatiomer of 6 prolonged the duration of the instar and delayed the onset of cocoon spinning when applied to 5th instar larvae, suggesting that this compound might have JH-like activity as well as anti-JH activity.

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Section: Synthesiscontrasting

confidence: 96%

Section: Biological Activitiessupporting

confidence: 43%

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Synthesis and anti-juvenile hormone activity of ethyl 4-(2-benzylalkyloxy)benzoates and their enantiomers

et al. 2007

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“…Riddiford et al have reported that ETB acted as a partial antagonist in the Manduca epidermis at the target-tissue level. 7) As previously reported, 3,4) in our bioassay using 24-hr-old 3rd instar larvae of B. mori, ETB at 1 mg induced precocious pupation in only 10% and no activity was observed at higher doses of 10 mg and 40 mg, while compounds 1 and 2 induced precocious metamorphosis even at high doses. ETB clearly acts as a JH agonist to counteract the effect of allatectomy, the induction of precocious metamorphosis, in a dose-dependent manner.…”

supporting

confidence: 77%

Juvenile Hormone Activity of Ethyl 4-(2-Aryloxyhexyloxy)benzoates with Precocious Metamorphosis-Inducing Activity

Fujita

Ashibe

Yamada

et al. 2007

Bioscience, Biotechnology, and Biochemistry

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Ethyl 4-[2-(6-methyl-3-pyridyloxy)hexyloxy]benzoate (1) and ethyl 4-(2-phenoxyhexyloxy)benzoate (2), which induce precocious metamorphosis in larvae of Bombyx mori, a clear sign of juvenile hormone (JH) deficiency, showed JH activity when topically applied to allatectomized 4th instar larvae of B. mori. Compounds 1 and 2 induced precocious metamorphosis with doses at which they were effective as JH agonists.Key words: juvenile hormone; precocious metamorphosis; anti-juvenile hormone; silkwormSince the juvenile hormone (JH) is involved in a wide range of physiological processes in both developing and mature insects, 1) an anti-JH agent, which chemically blocks the functioning of the JH control system, could be an effective probe for studies on insect endocrinology as well as a potential insect growth regulator.2) We have recently reported ethyl 4-[2-(6-methyl-3-pyridyloxy)-hexyloxy]benzoate (1) 3) and ethyl 4-(2-phenoxyhexyloxy)benzoate (2) 4) as novel anti-JH agents (Fig. 1). These compounds induced precocious metamorphosis in larvae of the silkworm, Bombyx mori, a clear sign of JH deficiency, and their activity could be completely counteracted by the simultaneous application of methoprene, a JH agonist. Compounds 1 and 2 were found by modifying the structure of ethyl 4-[2-(tert-butylcarbonyloxy)butyloxy]benzoate (ETB). ETB is known to show anti-JH activity as well as JH activity toward the tobacco hornworm, Manduca sexta, 5) and B. mori,depending on the dose applied; low doses of ETB induced precocious metamorphosis, but at higher doses, this precocious metamorphosis-inducing activity disappeared and instead, JH activity was observed. Riddiford et al. have reported that ETB acted as a partial antagonist in the Manduca epidermis at the target-tissue level. 7) As previously reported, 3,4) in our bioassay using 24-hr-old 3rd instar larvae of B. mori, ETB at 1 mg induced precocious pupation in only 10% and no activity was observed at higher doses of 10 mg and 40 mg, while compounds 1 and 2 induced precocious metamorphosis even at high doses. ETB clearly acts as a JH agonist to counteract the effect of allatectomy, the induction of precocious metamorphosis, in a dose-dependent manner.6) To determine whether compounds 1 and 2 as well as ETB had JH activity, we tested these compounds on allatectomized 4th instar larvae of B. mori.B. mori (Shunrei x Shougetsu strain) larvae were reared on an artificial diet as previously described. 8)Twenty-four hours after the 3rd molt, the corpora allata were extirpated with fine forceps under a binocular microscope as described by Ohtaki et al.9) Test compounds in an acetone solution (14 ml/larva) were each applied topically to the dorsal abdomen of the larvae within 1 hour after the allatectomy. JH activity was evaluated by the molting into normal 5th instar larvae. Table 1 shows the effects of methoprene, ETB, 1 and 2 against the allatectomized 4th instar larvae. All of the allatectomized and acetone-treated control larvae underwent precocious metamorphosis. ETB as well as methopr...

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“…14) In the silkworm, JHE activity in the hemolymph is quite low in 4th-instar larvae and increases in 5th-instar larvae, thereby decreasing the JH titer and inducing metamorphosis. 15) We have found that compound 2 9) and KF-13 16) induce hemolymph JH esterase activity during the 4th instar when applied to 3rd-instar larvae of B. mori. This result supports the concept that the appearance of JHE activity in the hemolymph is indispensable for the initiation of pupation.…”

Section: )mentioning

confidence: 92%

Synthesis and biological activity of novel anti-juvenile hormone agents

et al. 2008

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Ethyl 4-[2-(tert-butylcarbonyloxy)butoxy]benzoate (ETB) is a partial juvenile hormone (JH) antagonist which targets larval epidermis. We converted ETB to ethyl 4-(2-substituted alkyloxy)benzoates. These compounds induced precocious metamorphosis in the silkworm, Bombyx mori, which is a clear sign of JH deficiency, and their activity was completely counteracted by the simultaneous application of a JH agonist, methoprene. Among these novel compounds, ethyl 4-(2-benzylhexyloxy)benzoate (KF-13) showed high precocious metamorphosis-inducing activity at low doses, but its activity decreased with increasing dose, probably due to their JH-like activity. KF-13 is an enantiomeric compound. The (S)-enatiomer of KF-13 was more active than the (R)-enantiomer at low doses, but at high doses the activity was reversed (RϾS). Hemolymph JH esterase activity, which is indispensable for the initiation of pupation in normal last-instar larvae, was induced in 4th-instar larvae by treatment with KF-13. 2-(6-Methyl-3-pyridyloxy)hexyl and 2-phenoxyhexyl analogs showed JH activity when topically applied to allatechtomized 4th-instar larvae.

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Synthesis and Anti-Juvenile Hormone Activity of Ethyl 4-[2-(6-Methyl-3-pyridyloxy)alkyloxy]benzoates

Cited by 11 publications

References 16 publications

Synthesis and anti-juvenile hormone activity of ethyl 4-(2-benzylalkyloxy)benzoates and their enantiomers

Synthesis and anti-juvenile hormone activity of ethyl 4-(2-benzylalkyloxy)benzoates and their enantiomers

Juvenile Hormone Activity of Ethyl 4-(2-Aryloxyhexyloxy)benzoates with Precocious Metamorphosis-Inducing Activity

Synthesis and biological activity of novel anti-juvenile hormone agents

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