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数秒内形成的白细胞介素-1受体相关蛋白(ILPR)G-四链体具有很高的机械稳定性。

ILPR G-quadruplexes formed in seconds demonstrate high mechanical stabilities.

作者信息

Yu Zhongbo, Schonhoft Joseph D, Dhakal Soma, Bajracharya Rabindra, Hegde Ravi, Basu Soumitra, Mao Hanbin

机构信息

Department of Chemistry, Kent State University, Kent, Ohio 44242, USA.

出版信息

J Am Chem Soc. 2009 Feb 11;131(5):1876-82. doi: 10.1021/ja806782s.

DOI:10.1021/ja806782s
PMID:19154151
Abstract

The insulin linked polymorphism region (ILPR) is known to regulate transcription of the gene coding for insulin. The ILPR has guanine rich segments, suggesting that G quadruplexes may be responsible for this regulatory role. Using mechanical unfolding in a laser tweezers instrument and circular dichroism (CD) spectroscopy, we provide compelling evidence that highly stable parallel and antiparallel G quadruplex structures coexist in the predominant ILPR sequence of (ACAGGGGTGTGGGG)(2) at a physiologically relevant concentration of 100 mM KCl. Experiments at the single molecular level have shown that unfolding forces for parallel and antiparallel structures (F(unfold): 22.6 vs 36.9 pN, respectively) are higher than the stall forces of enzymes having helicase activities. From a mechanical perspective alone, these data support the hypothesis that G quadruplexes may cause replication slippage by blocking replication process. Using the unique combination of the rupture force and the contour length measured by laser tweezers, the simultaneous determination of probable parallel and antiparallel G quadruplex structures in a solution mixture has been achieved. Jarzynski's equality analysis has revealed that the antiparallel G quadruplex is thermodynamically more stable than the parallel conformer (DeltaG (unfold): 23 vs 14 kcal/mol, respectively). On the other hand, kinetic measurements have indicated that both parallel and antiparallel structures fold rather rapidly (k(fold): 0.4 vs 0.3 s(-1), respectively), suggesting that they may be kinetically accessible for gene control. This work provides an unprecedented mechanical perspective on G quadruplex stability, presenting a unique opportunity to predict the functional consequence when motor enzymes encounter such structures.

摘要

胰岛素连锁多态性区域(ILPR)已知可调节胰岛素编码基因的转录。ILPR具有富含鸟嘌呤的片段,这表明G-四链体可能负责这种调节作用。通过在激光镊子仪器中进行机械解折叠和圆二色性(CD)光谱分析,我们提供了令人信服的证据,即在100 mM KCl的生理相关浓度下,高度稳定的平行和反平行G-四链体结构共存于(ACAGGGGTGTGGGG)(2)的主要ILPR序列中。单分子水平的实验表明,平行和反平行结构的解折叠力(F(unfold):分别为22.6和36.9 pN)高于具有解旋酶活性的酶的停滞力。仅从力学角度来看,这些数据支持了G-四链体可能通过阻断复制过程导致复制滑移的假说。利用激光镊子测量的断裂力和轮廓长度的独特组合,实现了对溶液混合物中可能的平行和反平行G-四链体结构的同时测定。雅尔津斯基等式分析表明,反平行G-四链体在热力学上比平行构象更稳定(DeltaG (unfold):分别为23和14 kcal/mol)。另一方面,动力学测量表明,平行和反平行结构折叠都相当迅速(k(fold):分别为0.4和0.3 s(-1)),这表明它们在动力学上可能易于进行基因调控。这项工作为G-四链体稳定性提供了前所未有的力学视角,为预测运动酶遇到此类结构时的功能后果提供了独特机会。

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