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果蝇(黑腹果蝇)中一种假定的法尼酸O-甲基转移酶(FAMeT)同源物(CG10527):与保幼激素生物合成的关系?

A putative farnesoic acid O-methyltransferase (FAMeT) orthologue in Drosophila melanogaster (CG10527): relationship to juvenile hormone biosynthesis?

作者信息

Burtenshaw S M, Su P P, Zhang J R, Tobe S S, Dayton L, Bendena W G

机构信息

Department of Biology, Queen's University, Kingston, Ont. K7L 3N6, Canada.

出版信息

Peptides. 2008 Feb;29(2):242-51. doi: 10.1016/j.peptides.2007.10.030. Epub 2007 Dec 7.

Abstract

Juvenile hormones (JHs) are key regulators of both metamorphosis and adult reproductive processes. Farnesoic acid O-methyltransferase (FAMeT) is thought to be an important enzyme in the JH biosynthetic pathway, catalyzing methylation of farnesoic acid (FA) to methyl farnesoate (MF). Previous evidence in other insects suggested that FAMeT is rate limiting and regulated by a neuropeptide family, the allatostatins. A full-length cDNA encoding a 296 amino acid putative FAMeT has been isolated. A recombinant (r)FAMeT was cloned, expressed and a specific antiserum generated. rFAMeT was assayed for enzymatic activity using a radiochemical assay. In this assay, no activity was detected either with rFAMeT alone or when added to a corpus allatum CA extract. Immunohistochemical analysis was used to confirm the presence of FAMeT in the CA of Drosophila melanogaster ring gland. Analysis of MF, JHIII and JHB3 release in wild type and mutant stocks in the presence and absence of Drome AST (PISCF-type) suggest that Drosophila FAMeT has little if any effect on sesquiterpenoid biosynthesis. Drome AST appears to have a select effect on JH bisepoxide biosynthesis and not MF or JHIII. Additional analysis of MF, JHIII and JHB3 release in strains with a deficiency or decrease of FAMeT compared to wild type shows no significant decrease in MF, JHIII or JH bisepoxide synthesis. Deficiency strains that reduce the level of FAMeT showed reduced longevity relative to wildtype but this result may be due to other genetic influences.

摘要

保幼激素(JHs)是变态发育和成虫生殖过程的关键调节因子。法尼酸O - 甲基转移酶(FAMeT)被认为是保幼激素生物合成途径中的一种重要酶,它催化法尼酸(FA)甲基化生成甲基法尼酯(MF)。此前在其他昆虫中的证据表明,FAMeT是限速酶,并受一种神经肽家族——咽侧体抑制素调控。现已分离出一个编码296个氨基酸的假定FAMeT的全长cDNA。克隆并表达了重组(r)FAMeT,并制备了特异性抗血清。使用放射性化学分析法测定rFAMeT的酶活性。在该分析中,单独的rFAMeT或添加到咽侧体(CA)提取物中时均未检测到活性。免疫组织化学分析用于确认FAMeT在黑腹果蝇环腺CA中的存在。在有和没有果蝇咽侧体抑制素(PISCF型)的情况下,对野生型和突变品系中MF、保幼激素III(JHIII)和保幼激素酸甲酯(JHB3)释放的分析表明,果蝇FAMeT对倍半萜生物合成几乎没有影响。果蝇咽侧体抑制素似乎对保幼激素双环氧物的生物合成有选择性作用,而对MF或JHIII没有作用。与野生型相比,对FAMeT缺乏或减少的品系中MF、JHIII和JHB3释放的进一步分析表明,MF、JHIII或保幼激素双环氧物的合成没有显著减少。相对于野生型,降低FAMeT水平的缺陷品系寿命缩短,但这一结果可能是由于其他基因影响。

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