姜黄素通过调节肿瘤相关巨噬细胞M2极化和结肠癌转移相关的癌症1(MACC1)表达来抑制结直肠癌癌症细胞的恶性行为。

Shuke Ge, Xu Sun, Limin Sang, Min Zhang, Xubo Yan, Qi Ju, Xuefeng Ma, Meng Xu
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摘要

本研究旨在研究姜黄素对结直肠癌癌症细胞抗肿瘤作用的潜在机制,重点研究肿瘤相关巨噬细胞(TAMs)的M2极化。通过细胞生长的WST测定和细胞迁移/侵袭的Transwell测定,研究了姜黄素对结直肠癌癌症细胞恶性行为的影响。将THP-1细胞分化为巨噬细胞,并与结直肠癌癌症细胞共培养,以研究姜黄素对M2极化的影响,表现为ARG1 mRNA、IL-10和CD163阳性细胞的水平。在GEO数据库中搜索结肠直肠癌细胞和人单核细胞中姜黄素的共享改变基因。使用分子对接来观察姜黄素和MACC1之间的结合。姜黄素抑制HCT 116和SW620细胞的增殖、凋亡和迁移/侵袭。姜黄素降低M2巨噬细胞标志物CD163的水平 + 细胞、IL-10分泌和ARG1 mRNA。MACC1是结直肠癌癌症细胞中姜黄素的靶点,与巨噬细胞有关。拯救实验表明,MACC1过表达可以逆转姜黄素对结直肠癌癌症细胞的抗肿瘤作用和TAM的M2极化。姜黄素在结直肠癌癌症细胞中的抗增殖和抗迁移作用可能是由MACC1和抑制TAM的M2极化介导的。
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Curcumin inhibits malignant behavior of colorectal cancer cells by regulating M2 polarization of tumor-associated macrophages and metastasis associated in colon cancer 1 (MACC1) expression

The present study was to investigate the underlying mechanism of the antitumor effect of curcumin in colorectal cancer cells, focusing on the M2 polarization of tumor-associated macrophages (TAMs). The effect of curcumin on the malignant behavior of colorectal cancer cells was investigated by WST assay for cell growth, and Transwell assay for cell migration/invasion. THP-1 cells were differentiated into macrophages and coculture with colorectal cancer cells to study the influence of curcumin on M2 polarization, presenting as the levels of ARG1 mRNA, IL-10, and CD163-positive cells. GEO database was searched for the shared altered gene of curcumin in colorectal cells and human monocytes. Molecular docking was used to visualize the binding between curcumin and MACC1. Curcumin restricted the proliferation, apoptosis, and migration/invasion of HCT 116 and SW620 cells. Curcumin attenuated levels of the M2 macrophage markers, CD163 + cells, IL-10 secretion, and ARG1 mRNA. MACC1 was a target of curcumin in colorectal cancer cells, relating to macrophage. Rescue experiments showed that MACC1 overexpression can reverse the antitumor effect of curcumin in colorectal cancer cells and M2 polarization of TAMs. Curcumin's antiproliferative and anti-migratory effects in colorectal cancer cells may be mediated by MACC1 and inhibition of M2 polarization of TAMs.

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