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Structural Basis of Neurohormone Perception by the Receptor Tyrosine Kinase Torso

机译:受体酪氨酸激酶躯干对神经激素知觉的结构基础

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In insects, brain-derived Prothoracicotropic hormone (PTTH) activates the receptor tyrosine kinase (RTK) Torso to initiate metamorphosis through the release of ecdysone. We have determined the crystal structure of silkworm PTTH in complex with the ligand-binding region of Torso. Here we show that ligand-induced Torso dimerization results from the sequential and negatively cooperative formation of asymmetric heterotetramers. Mathematical modeling of receptor activation based upon our biophysical studies shows that ligand pulses are "buffered'' at low receptor levels, leading to a sustained signal. By contrast, high levels of Torso develop the signal intensity and duration of a noncooperative system. We propose that this may allow Torso to coordinate widely different functions from a single ligand by tuning receptor levels. Phylogenic analysis indicates that Torso is found outside arthropods, including human parasitic roundworms. Together, our findings provide mechanistic insight into how this receptor system, with roles in embryonic and adult development, is regulated.
机译:在昆虫中,脑源性促前列腺激素(PTTH)激活受体酪氨酸激酶(RTK)躯干,通过蜕皮激素的释放引发变态。我们已经确定了家蚕PTTH与Torso的配体结合区的晶体结构。在这里,我们表明配体诱导的躯干二聚体是由不对称异四聚体的顺序和负合作形成的结果。基于我们的生物物理研究的受体激活的数学模型表明,配体脉冲在低受体水平上被“缓冲”,从而产生持续的信号,相比之下,高水平的躯干发展了非合作系统的信号强度和持续时间。系统发育分析表明,躯干存在于节肢动物之外,包括人类寄生round虫,我们的发现为这种受体系统如何发挥作用提供了机械上的见解。胚胎和成年发育受到调节。

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