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荧光相关光谱法研究分子拥挤剂对与 G-四链体 DNA 结合的配体结合动力学的影响。

Effect of molecular crowders on ligand binding kinetics with G-quadruplex DNA probed by fluorescence correlation spectroscopy.

机构信息

Spectroscopy Laboratory, School of Physical Sciences, Jawaharlal Nehru University, New Delhi 110067, India.

出版信息

Methods Appl Fluoresc. 2024 Jul 26;12(4). doi: 10.1088/2050-6120/ad63f5.

DOI:10.1088/2050-6120/ad63f5
PMID:39013401
Abstract

Guanine-rich single-stranded DNA folds into G-quadruplex DNA (GqDNA) structures, which play crucial roles in various biological processes. These structures are also promising targets for ligands, potentially inducing antitumor effects. While thermodynamic parameters of ligand/DNA interactions are well-studied, the kinetics of ligand interaction with GqDNA, particularly in cell-like crowded environments, remain less explored. In this study, we investigate the impact of molecular crowding agents (glucose, sucrose, and ficoll 70) at physiologically relevant concentrations (20% w/v) on the association and dissociation rates of the benzophenoxazine-core based ligand, cresyl violet (CV), with human telomeric antiparallel-GqDNA. We utilized fluorescence correlation spectroscopy (FCS) along with other techniques. Our findings reveal that crowding agents decrease the binding affinity of CV to GqDNA, with the most significant effect-a nearly three-fold decrease-observed with ficoll 70. FCS measurements indicate that this decrease is primarily due to a viscosity-induced slowdown of ligand association in the crowded environment. Interestingly, dissociation rates remain largely unaffected by smaller crowders, with only small effect observed in presence of ficoll 70 due to direct but weak interaction between the ligand and ficoll. These results along with previously reported data provide valuable insights into ligand/GqDNA interactions in cellular contexts, suggesting a conserved mechanism of saccharide crowder influence, regardless of variations in GqDNA structure and ligand binding mode. This underscores the importance of considering crowding effects in the design and development of GqDNA-targeted drugs for potential cancer treatment.

摘要

鸟嘌呤丰富的单链 DNA 折叠成 G-四链体 DNA(GqDNA)结构,在各种生物过程中发挥着关键作用。这些结构也是配体的有前途的靶点,可能诱导抗肿瘤作用。虽然配体/DNA 相互作用的热力学参数得到了很好的研究,但配体与 GqDNA 的相互作用动力学,特别是在类似细胞的拥挤环境中,仍然研究较少。在这项研究中,我们研究了生理相关浓度(20%w/v)下的分子拥挤剂(葡萄糖、蔗糖和 ficoll 70)对苯并恶嗪核为基础的配体 Cresyl Violet(CV)与人端粒反平行-GqDNA 结合和解离速率的影响。我们利用荧光相关光谱(FCS)和其他技术。我们的研究结果表明,拥挤剂降低了 CV 与 GqDNA 的结合亲和力,其中 ficoll 70 的影响最大,降低了近三倍。FCS 测量表明,这种降低主要是由于在拥挤环境中配体结合的粘度诱导的减慢。有趣的是,较小的拥挤剂对解离速率的影响不大,只有在 ficoll 70 存在的情况下才会观察到较小的影响,这是由于配体和 ficoll 之间的直接但较弱的相互作用。这些结果以及以前报道的数据提供了有关配体/GqDNA 相互作用在细胞环境中的有价值的见解,表明了糖拥挤剂影响的保守机制,而与 GqDNA 结构和配体结合模式的变化无关。这凸显了在设计和开发用于潜在癌症治疗的 GqDNA 靶向药物时考虑拥挤效应的重要性。

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