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基于荧光寿命信号读出的钙指示剂:结构-功能研究

Calcium Indicators with Fluorescence Lifetime-Based Signal Readout: A Structure-Function Study.

作者信息

Simonyan Tatiana R, Varfolomeeva Larisa A, Mamontova Anastasia V, Kotlobay Alexey A, Gorokhovatsky Andrey Y, Bogdanov Alexey M, Boyko Konstantin M

机构信息

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, Moscow 117997, Russia.

A.N. Bach Institute of Biochemistry, Research Centre of Biotechnology of the Russian Academy of Sciences, Moscow 119071, Russia.

出版信息

Int J Mol Sci. 2024 Nov 21;25(23):12493. doi: 10.3390/ijms252312493.

Abstract

The calcium cation is a crucial signaling molecule involved in numerous cellular pathways. Beyond its role as a messenger or modulator in intracellular cascades, calcium's function in excitable cells, including nerve impulse transmission, is remarkable. The central role of calcium in nervous activity has driven the rapid development of fluorescent techniques for monitoring this cation in living cells. Specifically, genetically encoded calcium indicators (GECIs) are the most in-demand molecular tools in their class. In this work, we address two issues of calcium imaging by designing indicators based on the successful GCaMP6 backbone and the fluorescent protein BrUSLEE. The first indicator variant (GCaMP6s-BrUS), with a reduced, calcium-insensitive fluorescence lifetime, has potential in monitoring calcium dynamics with a high temporal resolution in combination with advanced microscopy techniques, such as light beads microscopy, where the fluorescence lifetime limits acquisition speed. Conversely, the second variant (GCaMP6s-BrUS-145), with a flexible, calcium-sensitive fluorescence lifetime, is relevant for static measurements, particularly for determining absolute calcium concentration values using fluorescence lifetime imaging microscopy (FLIM). To identify the structural determinants of calcium sensitivity in these indicator variants, we determine their spatial structures. A comparative structural analysis allowed the optimization of the GCaMP6s-BrUS construct, resulting in an indicator variant combining calcium-sensitive behavior in the time domain and enhanced molecular brightness. Our data may serve as a starting point for further engineering efforts towards improved GECI variants with fine-tuned fluorescence lifetimes.

摘要

钙离子是一种关键的信号分子,参与众多细胞通路。除了在细胞内级联反应中作为信使或调节剂发挥作用外,钙在可兴奋细胞中的功能,包括神经冲动传递,也十分显著。钙在神经活动中的核心作用推动了用于监测活细胞中这种阳离子的荧光技术的快速发展。具体而言,基因编码钙指示剂(GECIs)是该类别中最受欢迎的分子工具。在这项工作中,我们基于成功的GCaMP6骨架和荧光蛋白BrUSLEE设计指示剂,解决了钙成像的两个问题。第一个指示剂变体(GCaMP6s-BrUS)具有降低的、对钙不敏感的荧光寿命,结合先进的显微镜技术,如光珠显微镜,在荧光寿命限制采集速度的情况下,它在以高时间分辨率监测钙动力学方面具有潜力。相反,第二个变体(GCaMP6s-BrUS-145)具有灵活的、对钙敏感的荧光寿命,适用于静态测量,特别是使用荧光寿命成像显微镜(FLIM)确定绝对钙浓度值。为了确定这些指示剂变体中钙敏感性的结构决定因素,我们确定了它们的空间结构。通过比较结构分析优化了GCaMP6s-BrUS构建体,得到了一种在时域中结合钙敏感行为和增强分子亮度的指示剂变体。我们的数据可以作为进一步工程努力的起点,以开发具有微调荧光寿命的改进型GECI变体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e532/11640911/453b9e6a97fe/ijms-25-12493-g001.jpg

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