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抗肿瘤Heck偶联香紫苏醇类似物的设计与合成:SS - 12对自噬和凋亡性细胞死亡中BH3家族成员的调控

Design and Synthesis of Antitumor Heck-Coupled Sclareol Analogues: Modulation of BH3 Family Members by SS-12 in Autophagy and Apoptotic Cell Death.

作者信息

Rah Bilal, Lone Shabir H, Rasool Reyaz Ur, Farooq Saleem, Nayak Debasis, Chikan Naveed Anjum, Chakraborty Souneek, Behl Akanksha, Mondhe Dilip Manikaro, Goswami Anindya, Bhat Khursheed Ahmad

机构信息

⊥School of Bioscience and Technology, Division of Medical Biotechnology, VIT University, Vellore, Tamilnadu-632014, India.

出版信息

J Med Chem. 2015 Apr 23;58(8):3432-44. doi: 10.1021/jm501942m. Epub 2015 Apr 9.

Abstract

Sclareol, a promising anticancer labdane diterpene, was isolated from Salvia sclarea. Keeping the basic stereochemistry-rich framework of the molecule intact, a method for the synthesis of novel sclareol analogues was designed using palladium(II)-catalyzed oxidative Heck coupling reaction in order to study their structure-activity relationship. Both sclareol and its derivatives showed an interesting cytotoxicity profile, with 15-(4-fluorophenyl)sclareol (SS-12) as the most potent analogue, having IC50 = 0.082 μM against PC-3 cells. It was found that SS-12 commonly interacts with Bcl-2 and Beclin 1 BH3 domain proteins and enhances autophagic flux by modulating autophagy-related proteins. Moreover, inhibition of autophagy by autophagy inhibitors protected against SS-12-induced apoptosis. Finally, SS-12 effectively suppressed tumor growth in vivo in Ehrlich's ascitic and solid Sarcoma-180 mouse models.

摘要

香紫苏醇是一种很有前景的抗癌半日花烷二萜,从南欧丹参中分离得到。为了研究其构效关系,在保持该分子基本富含立体化学结构框架不变的情况下,设计了一种利用钯(II)催化的氧化Heck偶联反应合成新型香紫苏醇类似物的方法。香紫苏醇及其衍生物均表现出有趣的细胞毒性特征,其中15-(4-氟苯基)香紫苏醇(SS-12)是最具活性的类似物,对PC-3细胞的IC50 = 0.082 μM。研究发现,SS-12通常与Bcl-2和Beclin 1 BH3结构域蛋白相互作用,并通过调节自噬相关蛋白来增强自噬通量。此外,自噬抑制剂对自噬的抑制可保护细胞免受SS-12诱导的凋亡。最后,在艾氏腹水癌和实体肉瘤-180小鼠模型中,SS-12在体内有效抑制了肿瘤生长。

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