Pagano Bruno, Martino Luigi, Randazzo Antonio, Giancola Concetta
Dipartimento di Scienze Farmaceutiche, Università di Salerno, Fisciano, Salerno, Italy.
Biophys J. 2008 Jan 15;94(2):562-9. doi: 10.1529/biophysj.107.117382. Epub 2007 Sep 21.
Aptamer-based drugs represent an attractive approach in pharmacological therapy. The most studied aptamer, thrombin binding aptamer (TBA), folds into a well-defined quadruplex structure and binds to its target with good specificity and affinity. Modified aptamers with improved biophysical properties could constitute a new class of therapeutic aptamers. In this study we show that the modified thrombin binding aptamer (mTBA), (3')GGT(5')-(5')TGGTGTGGTTGG(3'), which also folds into a quadruplex structure, is more stable than its unmodified counterpart and shows a higher thrombin affinity. The stability of the modified aptamer was investigated using differential scanning calorimetry, and the energetics of mTBA and TBA binding to thrombin was characterized by means of isothermal titration calorimetry (ITC). ITC data revealed that TBA/thrombin and mTBA/thrombin binding stoichiometry is 1:2 for both interactions. Structural models of the two complexes of thrombin with TBA and with mTBA were also obtained and subjected to molecular dynamics simulations in explicit water. Analysis of the models led to an improvement of the understanding of the aptamer-thrombin recognition at a molecular level.
基于适配体的药物是药理学治疗中一种有吸引力的方法。研究最多的适配体——凝血酶结合适配体(TBA),折叠成明确的四链体结构,并以良好的特异性和亲和力与其靶标结合。具有改善的生物物理性质的修饰适配体可以构成一类新的治疗性适配体。在本研究中,我们表明修饰的凝血酶结合适配体(mTBA),即(3')GGT(5')-(5')TGGTGTGGTTGG(3'),也折叠成四链体结构,比其未修饰的对应物更稳定,并且显示出更高的凝血酶亲和力。使用差示扫描量热法研究了修饰适配体的稳定性,并通过等温滴定量热法(ITC)表征了mTBA和TBA与凝血酶结合的能量学。ITC数据表明,TBA/凝血酶和mTBA/凝血酶的结合化学计量比对于这两种相互作用均为1:2。还获得了凝血酶与TBA和与mTBA的两种复合物的结构模型,并在显式水中进行了分子动力学模拟。对模型的分析有助于在分子水平上更好地理解适配体 - 凝血酶识别。
