Graduate Program in Areas of Basic and Applied Biology (GABBA) PhD Program, ICBAS-Instituto de Ciências Biomédicas Abel Salazar, Universidade do Porto, Porto, Portugal.
Gene Regulation - Instituto de Investigação e Inovação em Saúde, Universidade do Porto, Porto, Portugal.
Front Immunol. 2023 Jun 8;14:1182525. doi: 10.3389/fimmu.2023.1182525. eCollection 2023.
Macrophages are essential cells of the immune system that alter their inflammatory profile depending on their microenvironment. Alternative polyadenylation in the 3'UTR (3'UTR-APA) and intronic polyadenylation (IPA) are mechanisms that modulate gene expression, particularly in cancer and activated immune cells. Yet, how polarization and colorectal cancer (CRC) cells affect 3'UTR-APA and IPA in primary human macrophages was unclear.
In this study, we isolated primary human monocytes from healthy donors, differentiated and polarized them into a pro-inflammatory state and performed indirect co-cultures with CRC cells. ChrRNA-Seq and 3'RNA-Seq was performed to quantify gene expression and characterize new 3'UTR-APA and IPA mRNA isoforms.
Our results show that polarization of human macrophages from naïve to a pro-inflammatory state causes a marked increase of proximal polyA site selection in the 3'UTR and IPA events in genes relevant to macrophage functions. Additionally, we found a negative correlation between differential gene expression and IPA during pro-inflammatory polarization of primary human macrophages. As macrophages are abundant immune cells in the CRC microenvironment that either promote or abrogate cancer progression, we investigated how indirect exposure to CRC cells affects macrophage gene expression and 3'UTR-APA and IPA events. Co-culture with CRC cells alters the inflammatory phenotype of macrophages, increases the expression of pro-tumoral genes and induces 3'UTR-APA alterations. Notably, some of these gene expression differences were also found in tumor-associated macrophages of CRC patients, indicating that they are physiologically relevant. Upon macrophage pro-inflammatory polarization, is the pre-mRNA processing gene that is most upregulated. After knockdown in M1 macrophages there is a global downregulation of gene expression, in particular in genes involved in gene expression regulation and in immune responses.
Our results reveal new 3'UTR-APA and IPA mRNA isoforms produced during pro-inflammatory polarization of primary human macrophages and CRC co-culture that may be used in the future as diagnostic or therapeutic tools. Furthermore, our results highlight a function for in pro-inflammatory macrophages, key cells in the tumor response.
巨噬细胞是免疫系统的重要细胞,它们根据微环境改变其炎症特征。3'UTR(3'UTR-APA)和内含子多聚腺苷酸化(IPA)的可变多聚腺苷酸化是调节基因表达的机制,特别是在癌症和激活的免疫细胞中。然而,极化和结直肠癌(CRC)细胞如何影响原代人巨噬细胞中的 3'UTR-APA 和 IPA 尚不清楚。
在这项研究中,我们从健康供体中分离原代人单核细胞,将其分化并极化到促炎状态,并与 CRC 细胞进行间接共培养。进行 ChrRNA-Seq 和 3'RNA-Seq 以定量基因表达并表征新的 3'UTR-APA 和 IPA mRNA 异构体。
我们的结果表明,从幼稚状态到促炎状态的人巨噬细胞的极化导致 3'UTR 中近端 polyA 位点选择和与巨噬细胞功能相关基因的 IPA 事件显著增加。此外,我们发现在原代人巨噬细胞促炎极化过程中,差异基因表达与 IPA 之间呈负相关。由于巨噬细胞是 CRC 微环境中丰富的免疫细胞,它们既促进也阻止癌症进展,因此我们研究了间接暴露于 CRC 细胞如何影响巨噬细胞基因表达和 3'UTR-APA 和 IPA 事件。与 CRC 细胞共培养改变了巨噬细胞的炎症表型,增加了促肿瘤基因的表达,并诱导了 3'UTR-APA 改变。值得注意的是,CRC 患者肿瘤相关巨噬细胞中也发现了其中一些基因表达差异,表明它们具有生理相关性。在巨噬细胞促炎极化后, 是上调最多的前体 mRNA 加工基因。在 M1 巨噬细胞中敲低 后,基因表达会全面下调,特别是在参与基因表达调控和免疫反应的基因中。
我们的结果揭示了在原代人巨噬细胞促炎极化和 CRC 共培养过程中产生的新的 3'UTR-APA 和 IPA mRNA 异构体,这些异构体可能在未来用作诊断或治疗工具。此外,我们的结果强调了 在促炎巨噬细胞中的功能,促炎巨噬细胞是肿瘤反应中的关键细胞。
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