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两种进化保守的昆虫神经激肽样受体的功能比较

Functional comparison of two evolutionary conserved insect neurokinin-like receptors.

作者信息

Poels Jeroen, Verlinden Heleen, Fichna Jakub, Van Loy Tom, Franssens Vanessa, Studzian Kazimierz, Janecka Anna, Nachman Ronald J, Vanden Broeck Jozef

机构信息

Laboratory for Developmental Physiology, Genomics and Proteomics, Catholic University Leuven, Naamsestraat 59, B-3000 Leuven, Belgium.

出版信息

Peptides. 2007 Jan;28(1):103-8. doi: 10.1016/j.peptides.2006.06.014. Epub 2006 Dec 4.

Abstract

Tachykinins are multifunctional neuropeptides that have been identified in vertebrates as well as invertebrates. The C-terminal FXGXRa-motif constitutes the consensus active core region of invertebrate tachykinins. In Drosophila, two putative G protein-coupled tachykinin receptors have been cloned: DTKR and NKD. This study focuses on the functional characterization of DTKR, the Drosophila ortholog of the stable fly's tachykinin receptor (STKR). Tachykinins containing an alanine residue instead of the highly conserved glycine (FXAXRa) display partial agonism on STKR-mediated Ca(2+)-responses, but not on cAMP-responses. STKR therefore seems to differentiate between a number of tachykinins. Gly- and Ala-containing tachykinins are both encoded in the Drosophila tachykinin precursor, thus raising the question of whether DTKR can also distinguish between these two tachykinin types. DTKR was activated by all Drosophila tachykinins and inhibited by tachykinin antagonists. Ala-containing analogs did not produce the remarkable activation behavior previously observed with STKR, suggesting different mechanisms of discerning ligands and/or activating effector pathways for STKR and DTKR.

摘要

速激肽是一类多功能神经肽,已在脊椎动物和无脊椎动物中被鉴定出来。C末端FXGXRa基序构成了无脊椎动物速激肽的共有活性核心区域。在果蝇中,已克隆出两种假定的G蛋白偶联速激肽受体:DTKR和NKD。本研究聚焦于DTKR的功能特性,DTKR是厩螫蝇速激肽受体(STKR)在果蝇中的直系同源物。含有丙氨酸残基而非高度保守的甘氨酸的速激肽(FXAXRa)对STKR介导的Ca(2+)反应表现出部分激动作用,但对cAMP反应则无此作用。因此,STKR似乎能够区分多种速激肽。含甘氨酸和丙氨酸的速激肽均由果蝇速激肽前体编码,这就引发了一个问题,即DTKR是否也能区分这两种速激肽类型。DTKR可被所有果蝇速激肽激活,并被速激肽拮抗剂抑制。含丙氨酸的类似物并未产生先前在STKR中观察到的显著激活行为,这表明STKR和DTKR识别配体和/或激活效应器途径的机制不同。

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