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棕褐色基因和乌木基因调控果蝇光感受器末端神经递质代谢的一条新途径。

tan and ebony genes regulate a novel pathway for transmitter metabolism at fly photoreceptor terminals.

作者信息

Borycz Janusz, Borycz Jolanta A, Loubani Mohammed, Meinertzhagen Ian A

机构信息

Neuroscience Institute, Dalhousie University, Halifax, Nova Scotia, Canada B3H 4J1.

出版信息

J Neurosci. 2002 Dec 15;22(24):10549-57. doi: 10.1523/JNEUROSCI.22-24-10549.2002.

Abstract

In Drosophila melanogaster, ebony and tan, two cuticle melanizing mutants, regulate the conjugation (ebony) of beta-alanine to dopamine or hydrolysis (tan) of the beta-alanyl conjugate to liberate dopamine. beta-alanine biosynthesis is regulated by black. ebony and tan also exert unexplained reciprocal defects in the electroretinogram, at ON and OFF transients attributable to impaired transmission at photoreceptor synapses, which liberate histamine. Compatible with this impairment, we show that both mutants have reduced histamine contents in the head, as measured by HPLC, and have correspondingly reduced numbers of synaptic vesicles in their photoreceptor terminals. Thus, the histamine phenotype is associated with sites of synaptic transmission at photoreceptors. We demonstrate that when they receive microinjections into the head, wild-type Sarcophaga bullata (in whose larger head such injections are routinely possible) rapidly (<5 sec) convert exogenous [3H]histamine into its beta-alanine conjugate, carcinine, a novel metabolite. Drosophila tan has an increased quantity of [3H]carcinine, the hydrolysis of which is blocked; ebony lacks [3H]carcinine, which it cannot synthesize. Confirming these actions, carcinine rescues the histamine phenotype of ebony, whereas beta-alanine rescues the carcinine phenotype of black;tan double mutants. The equilibrium ratio between [3H]carcinine and [3H]histamine after microinjecting wild-type Sarcophaga favors carcinine hydrolysis, increasing to only 0.5 after 30 min. Our findings help resolve a longstanding conundrum of the involvement of tan and ebony in photoreceptor function. We suggest that reversible synthesis of carcinine occurs in surrounding glia, serving to trap histamine after its release at photoreceptor synapses; subsequent hydrolysis liberates histamine for reuptake.

摘要

在黑腹果蝇中,两个表皮黑化突变体乌木色(ebony)和棕褐色(tan),分别调节β-丙氨酸与多巴胺的结合(乌木色)或β-丙氨酰共轭物的水解(棕褐色)以释放多巴胺。β-丙氨酸的生物合成受黑色(black)基因调控。乌木色和棕褐色突变体在视网膜电图中还表现出无法解释的相互缺陷,在光感受器突触传递受损导致的开和关瞬变过程中出现这种情况,光感受器突触会释放组胺。与此种损伤相一致的是,我们发现通过高效液相色谱法测量,这两个突变体头部的组胺含量均降低,并且其光感受器终末的突触小泡数量相应减少。因此,组胺表型与光感受器的突触传递部位相关。我们证明,当向野生型肉蝇(Sarcophaga bullata)头部进行显微注射时(其较大的头部通常可以进行此类注射),野生型肉蝇能迅速(<5秒)将外源[3H]组胺转化为其β-丙氨酸共轭物肌肽(carcinine),这是一种新的代谢产物。果蝇棕褐色突变体中[3H]肌肽的量增加,但其水解受阻;乌木色突变体缺乏[3H]肌肽,因为它无法合成。证实了这些作用后,肌肽挽救了乌木色突变体的组胺表型,而β-丙氨酸挽救了黑色;棕褐色双突变体的肌肽表型。对野生型肉蝇进行显微注射后,[3H]肌肽与[3H]组胺之间的平衡比有利于肌肽水解,30分钟后仅增加到0.5。我们的研究结果有助于解决长期以来关于棕褐色和乌木色基因参与光感受器功能的难题。我们认为,肌肽的可逆合成发生在周围的神经胶质细胞中,用于在组胺于光感受器突触释放后将其捕获;随后的水解释放组胺以便重新摄取。

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