Desplat Vanessa, Vincenzi Marian, Lucas Romain, Moreau Stéphane, Savrimoutou Solène, Pinaud Noël, Lesbordes Jordi, Peyrilles Elodie, Marchivie Mathieu, Routier Sylvain, Sonnet Pascal, Rossi Filomena, Ronga Luisa, Guillon Jean
Univ. Bordeaux, UFR des Sciences Pharmaceutiques, Cellules souches hématopoïétiques normales et leucémiques, F-33076 Bordeaux cedex, France; INSERM U1035, Cellules souches hématopoïétiques normales et leucémiques, F-33000 Bordeaux, France.
Univ. Bordeaux, UFR des Sciences Pharmaceutiques, ARNA Laboratory, F-33076 Bordeaux cedex, France; INSERM U1212, UMR CNRS 5320, ARNA Laboratory, F-33000 Bordeaux, France; Department of Pharmacy and CIRPeB, University of Naples "Federico II", Via Mezzocannone, 16 80134 Naples, Italy.
Eur J Med Chem. 2016 May 4;113:214-27. doi: 10.1016/j.ejmech.2016.02.047. Epub 2016 Feb 20.
Leukemia is the most common blood cancer, and its development starts at diverse points, leading to distinct subtypes that respond differently to therapy. This heterogeneity is rarely taken into account in therapies, so it is still essential to look for new specific drugs for leukemia subtypes or even for therapy-resistant cases. Among heterocyclic compounds that attracted a lot of attention because of its wide spread biological activities, the pyrrolo[1,2-a]quinoxaline heterocyclic framework has been identified as interesting scaffolds for antiproliferative activity against various human cancer cell lines. In the present study, novel ethyl 4-[4-(4-substitutedpiperidin-1-yl)]benzyl-phenylpyrrolo[1,2-a]quinoxaline-carboxylate derivatives 1a-l have been designed and synthesized. Their cytotoxicities were evaluated against five different leukemia cell lines, including Jurkat and U266 (lymphoid cell lines), and K562, U937, HL60 (myeloid cell lines), as well as normal human peripheral blood mononuclear cells (PBMNCs). Then, apoptosis study was performed with the more interesting compounds. The new pyrrolo[1,2-a]quinoxaline series showed promising cytotoxic potential against all leukemia cell lines tested, and some compounds showed better results than the reference compound A6730. Some compounds, such as 1a, 1e, 1g and 1h are promising because of their high activity against leukemia and their low activity against normal hematopoietic cells. Structure-activity relationships of these new synthetic compounds 1a-l are here also discussed.
白血病是最常见的血液癌症,其发展起始于不同阶段,导致出现对治疗反应各异的不同亚型。治疗中很少考虑到这种异质性,因此寻找针对白血病亚型甚至治疗耐药病例的新型特效药物仍然至关重要。在因其广泛的生物活性而备受关注的杂环化合物中,吡咯并[1,2 - a]喹喔啉杂环骨架已被确定为对多种人类癌细胞系具有抗增殖活性的有趣支架。在本研究中,设计并合成了新型的4 - [4 - (4 - 取代哌啶 - 1 - 基)]苄基 - 苯基吡咯并[1,2 - a]喹喔啉 - 羧酸乙酯衍生物1a - l。评估了它们对五种不同白血病细胞系的细胞毒性,包括Jurkat和U266(淋巴细胞系),以及K562、U937、HL60(髓细胞系),还有正常人外周血单个核细胞(PBMNCs)。然后,对更具研究价值的化合物进行了凋亡研究。新的吡咯并[1,2 - a]喹喔啉系列对所有测试的白血病细胞系均显示出有前景的细胞毒性潜力,一些化合物的结果优于参考化合物A6730。一些化合物,如1a、1e、1g和1h因其对白血病的高活性以及对正常造血细胞的低活性而颇具前景。本文还讨论了这些新合成化合物1a - l的构效关系。
