Your search keyword '"Cheng, Keguang"' showing total 2 results

1. (4-Picolylamino)-17β-Estradiol derivative and analogues induce apoptosis with death receptor trail R2/DR5 in MCF-7.

Author

Yin, Yudong, Sun, Li, Sheng, Lixin, Zhang, Liqiong, Liu, Jingjing, Wen, Xiaoan, Mo, Weibin, Wang, Quande, and Cheng, Keguang

Subjects

*DEATH receptors, *CELL death, *CELL cycle, *APOPTOSIS, *TRAIL protein, *IMMUNOHISTOCHEMISTRY

Abstract

In order to discover more effective and less toxic drugs in the field of anti-tumor, the backbone structure of 17 β -estradiol was modified, and 11 target compounds were synthesized. Compounds 5 and 10 , which exhibited better anti-tumor activity and higher selectivity (more than 10-fold), were chosen for further biological investigation. Flow cytometry results indicated that 5 and 10 could arrest MCF-7 cells in the G2 phase and induce apoptosis. Immunohistochemical analysis revealed that 5 and 10 could bind to the estradiol receptor alpha in MCF-7 cells. Western blotting and real-time PCR assays were performed to detect the effects of compounds on apoptosis-related targets at the protein and gene levels. These results showed that both 5 and 10 could dosed-dependently increase the expression of Apaf-1, Bax, caspase-3,8,9 and reduce the expression levels of the anti-apoptotic factors Bcl-2 and Bcl-xL. Besides, the Human apoptosis array assay demonstrated the expression level of death receptor Trail R2/DR5 was upregulated obviously while the expression of TNF R1, IAPs and Hsp27/60/70 were downregulated. On the whole, 5 induced MCF-7 cell death through the endogenous pathway in mitochondria and the exogenous pathway with death receptor Trail R2/DR5. • Eleven 17 β -estradiol derivatives from modification were synthesized. • 5 and 10 possessed much better antiproliferative activities and higher selectivity than 17 β -estradiol. • 5 and 10 could arrest cell cycle at the G2 phase in MCF-7 cells and partly bind with the estradiol receptor alpha. • 5 induced MCF-7 cells death through both endogenous and exogenous pathways. [ABSTRACT FROM AUTHOR]

Published

2023

2. Synthesis and in vitro/in vivo anticancer evaluation of pentacyclic triterpenoid derivatives linked with l-phenylalanine or l-proline.

Author

Yin, Yudong, Sheng, Lixin, Zhang, Juzheng, Zhang, Liqiong, Liu, Jingjing, Wen, Xiaoan, Liu, Yanghan, Si, Yang, and Cheng, Keguang

Subjects

*WESTERN immunoblotting, *PROTEASOMES, *STRUCTURE-activity relationships, *MEMBRANE potential, *PHENYLALANINE, *MITOCHONDRIAL membranes, *CANCER cells

Abstract

The newly synthesized glycine- l -phenylalanine conjugates 11 and 16 have good anticancer activity. In vivo and in vitro experiments showed that both compounds inhibit the growth of solid tumors by inducing apoptosis of cancer cells. [Display omitted] • 37 triterpenoid acid derivatives linked to l -phenylalanine or l -proline were synthesized. • Glycyrrhetinic acid (GA) derivatives 11 (IC 50 = 0.2 μM) and 16 (IC 50 = 0.7 μM) are much more potent than GA. • 11 and 16 showed significant tumor growth inhibition in A549 and T24 tumor xenograft model, respectively. • 16 showed low toxicity in vitro and in vivo experiments. • The mechanisms of action of compounds 11 and 16 were extensively investigated. Extensive research effort has been put in pentacyclic triterpenoids due to their numerous biological activities. However, their poor water solubility and low oral bioavailability limit their antitumor effects in vivo. To address these issues, 37 triterpenoid acid derivatives linked to l -phenylalanine or l -proline were designed and synthesized in this study. Structure-activity relationship (SAR) studies found two promising glycyrrhetinic acid (GA) derivatives 11 and 16. Compound 11 was obtained by C3-OH esterification and C30-COOH modification with l -phenylalanine while 16 was obtained by attaching C3-OH with l -phenylalanine. Compounds 11 and 16 exhibit up to 48- and 120-fold improvement respectively compared with the IC 50 values of naturally occurring GA in the cellular assay. Fluorescence microscope and flow cytometric analysis suggested that both compounds 11 and 16 increased the content of ROS and Ca2+ in cancer cells, decreased mitochondrial membrane potential (JC-1), and activated the regulator caspase-3/8/9 to trigger cell apoptosis. RNA-seq analysis and western blot analysis indicated that compounds 11 and 16 may promote apoptosis by upregulating the functions of pro-apoptotic factors while inhibiting the proteasome activity. [ABSTRACT FROM AUTHOR]

Published

2022