Bruno Stefano, Pinto Andrea, Paredi Gianluca, Tamborini Lucia, De Micheli Carlo, La Pietra Valeria, Marinelli Luciana, Novellino Ettore, Conti Paola, Mozzarelli Andrea
Dipartimento di Farmacia and Centro Siteia.Parma, Università di Parma , Parco Area delle Scienze 23/A, 43124 Parma, Italy.
J Med Chem. 2014 Sep 11;57(17):7465-71. doi: 10.1021/jm500747h. Epub 2014 Sep 2.
We developed a new class of covalent inhibitors of Plasmodium falciparum glyceraldehyde-3-phosphate dehydrogenase, a validated target for the treatment of malaria, by screening a small library of 3-bromo-isoxazoline derivatives that inactivate the enzyme through a covalent, selective bond to the catalytic cysteine, as demonstrated by mass spectrometry. Substituents on the isoxazolinic ring modulated the potency up to 20-fold, predominantly due to an electrostatic effect, as assessed by computational analysis.
我们通过筛选一个由3-溴异恶唑啉衍生物组成的小型文库,开发出了一类新型的恶性疟原虫甘油醛-3-磷酸脱氢酶共价抑制剂。该酶是治疗疟疾的一个经过验证的靶点,质谱分析表明,这些衍生物通过与催化性半胱氨酸形成共价、选择性键来使该酶失活。异恶唑啉环上的取代基使效力提高了20倍,主要是由于静电效应,这是通过计算分析评估得出的。