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Enantioselective Synthesis, DFT Calculations, and Preliminary Antineoplastic Activity of Dibenzo 1-Azaspiro[4.5]decanes on Drug-Resistant Leukemias

机译:抗毒性白血病二苯并苯并1-Azaspiro [4.5]癸烯的映选择性合成,DFT计算和初步抗肿瘤活性

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摘要

The addition of 2-bromobenzylmagnesium bromide to chiral N-tert-butanesulfinyl imines derived from tetralone-type ketones proceeds with high levels of diastereocontrol. The resulting sulfinamide derivatives were transformed into dibenzoazaspiro compounds after a palladium catalyzed intramolecular N-arylation. DFT calculations have been performed to rationalize the stereochemical course of the reaction. Similar results have been obtained considering either diethyl ether or toluene as a solvent, in both cases in an excellent agreement with experimental findings. NCI topological calculations have also been used to evidence crucial noncovalent interactions. In addition, the azaspiro compounds reduced the viability of chronic myeloid leukemia cells in the micromolar ;range. Notably, both the halogen-substituted (R)- and (S)-8g and -8h as well as (R)-8j were at least two times more effective on a multidrug-resistant derivative than on the parental cell line, exerting a collateral sensitivity effect.
机译:将2-溴苄基溴化镁加入到衍生自向retralone酮的手性N-叔丁沙磺酰基亚胺的溴化物与高水平的非对乳核细胞进行。将得到的磺胺胺衍生物在钯催化的分子内N-芳基后转化成二苯脲氮杂物化合物。已经进行了DFT计算以合理化反应的立体化学过程。在两种情况下,在与实验结果的良好协议中,考虑到乙醚或甲苯作为溶剂,已经获得了类似的结果。 NCI拓扑计算也已用于证明关键的非共价相互作用。此外,阿扎希罗化合物降低了微摩尔中慢性骨髓性白血病细胞的活力;范围。值得注意的是,卤素取代的(R) - 和(s)-8g和-8h以及(r)-8j均在多药衍生物上的至少两倍,而不是父母细胞系,施加a侧支敏感效应。

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  • 来源
    《The Journal of Organic Chemistry》 |2019年第4期|共15页
  • 作者单位

    Pontifical Catholic Univ Rio de Janeiro Puc Rio Dept Chem BR-22435900 Rio De Janeiro Brazil;

    Univ Zaragoza Fac Ciencias Inst Biocomp &

    Fis Sistemas Complejos BIFI Campus San Francisco E-50009 Zaragoza Spain;

    Univ Alicante Serv Tecn Invest Apdo 99 E-03080 Alicante Spain;

    Fed Univ Rio de Janeiro UFRJ Hlth Sci Ctr Carlos Chagas Filho Inst Biophys Lab Glycobiol BR-21941590 Rio De Janeiro Brazil;

    Fed Univ Rio de Janeiro UFRJ Hlth Sci Ctr Nucleus Res Nat Prod Lab Bioorgan Chem BR-21941590 Rio De Janeiro Brazil;

    Univ Alicante Ctr Innovac Quim Avanzada ORFEO CINQA Apdo 99 E-03080 Alicante Spain;

    Univ Alicante Ctr Innovac Quim Avanzada ORFEO CINQA Apdo 99 E-03080 Alicante Spain;

    Pontifical Catholic Univ Rio de Janeiro Puc Rio Dept Chem BR-22435900 Rio De Janeiro Brazil;

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  • 正文语种 eng
  • 中图分类 有机化学;
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