Schwertz Geoffrey, Frei Michelle S, Witschel Matthias C, Rottmann Matthias, Leartsakulpanich Ubolsree, Chitnumsub Penchit, Jaruwat Aritsara, Ittarat Wanwipa, Schäfer Anja, Aponte Raphael A, Trapp Nils, Mark Kerstin, Chaiyen Pimchai, Diederich François
Laboratorium für Organische Chemie, ETH Zurich, Vladimir-Prelog-Weg 3, 8093, Zurich, Switzerland.
BASF SE, Carl-Bosch-Strasse 38, 67056, Ludwigshafen, Germany.
Chemistry. 2017 Oct 12;23(57):14345-14357. doi: 10.1002/chem.201703244. Epub 2017 Oct 2.
Malaria remains a major threat to mankind due to the perpetual emergence of resistance against marketed drugs. Twenty-one pyrazolopyran-based inhibitors bearing terminal biphenyl, aryl sulfonamide, or aryl sulfone motifs were synthesized and tested towards serine hydroxymethyltransferase (SHMT), a key enzyme of the folate cycle. The best ligands inhibited Plasmodium falciparum (Pf) and Arabidopsis thaliana (At) SHMT in target, as well as PfNF54 strains in cell-based assays in the low nanomolar range (18-56 nm). Seven co-crystal structures with P. vivax (Pv) SHMT were solved at 2.2-2.6 Å resolution. We observed an unprecedented influence of the torsion angle of ortho-substituted biphenyl moieties on cell-based efficacy. The peculiar lipophilic character of the sulfonyl moiety was highlighted in the complexes with aryl sulfonamide analogues, which bind in their preferred staggered orientation. The results are discussed within the context of conformational preferences in the ligands.
由于市售药物耐药性的不断出现,疟疾仍然是对人类的重大威胁。合成了21种带有末端联苯、芳基磺酰胺或芳基砜基序的吡唑并吡喃类抑制剂,并针对叶酸循环的关键酶丝氨酸羟甲基转移酶(SHMT)进行了测试。最佳配体在基于细胞的试验中,在低纳摩尔范围(18 - 56 nM)内抑制了恶性疟原虫(Pf)和拟南芥(At)的SHMT以及PfNF54菌株。以2.2 - 2.6 Å分辨率解析了7种与间日疟原虫(Pv)SHMT的共晶体结构。我们观察到邻位取代联苯部分的扭转角对基于细胞的疗效有前所未有的影响。磺酰基部分独特的亲脂性在与芳基磺酰胺类似物的复合物中得到突出体现,这些类似物以其优选的交错取向结合。在配体构象偏好的背景下讨论了结果。