Dendritic Cell-Based Immunity: Screening of Dendritic Cell Subsets in Breast Cancer-Bearing Mice.

Q3 Medicine

Journal of Microscopy and Ultrastructure Pub Date : 2023-01-19 eCollection Date: 2023-07-01 DOI:10.4103/jmau.jmau_85_22

Alia M Aldahlawi, Kawther Sayed Ali Zaher

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Abstract

Background: Breast cancer (BC) is the most devastating disease, particularly the lethal invasive form. It is the most underlying cause of death among women worldwide. The expansion of BC is controlled by a variety of alterations in the tumor cells themselves, in addition to the state of the immune system, which has a direct influence on the tumor microenvironment. Numerous receptors expressed by T-cells interact with ligands on antigen-presenting cells to provide activation signals results in mounting effector anti-tumor T-cell responses. On the other hand, there is a dearth of information about the actual interactions and reactions of T-cells and dendritic cells (DCs) all through the progression of tumor development.

Aim: Immune system response against BC was investigated through tumor induction in mice. The size and volume of the tumor were calculated. Moreover, the phenotypical profile of T-cells and DCs from lymph nodes (LN) and spleens of BC-bearing mice was investigated. In addition, the levels of Transforming growth factor-β, Interferon-gamma (IFN-γ), Interleukin IL-2, IL-10, IL-4, IL-12, and tumor necrosis factor (TNF)-α were determined.

Materials and methods: MDA231 cells were utilized to induce BC in 30 white BALB/C mice, whereas the other 30 mice acted as healthy controls and were not treated with any cancer-causing agents. The impact of malignancy was evaluated using flow cytometry based on the marking surface molecules, as well as the titer of specific cytokines of the mice's LN culture using the ELISA method. These cytokines included transforming growth factor-β (TGF-β), IFN-γ, IL-2, IL -10, IL -4, IL -12, and TNF-α.

Results: The findings showed that the maturation of DCs was inhibited, followed by an accumulation of immature DCs. These immature DCs increase the release of TGF-β and cytokines like IL-10 and inhibit the release of IFN-γ and IL-12 in the culture supernatant of nodal lymph and spleen suspension of BC-bearing mice compared to control. In addition, there was a low expression of CD80 and CD86 on DCs, which indicates a low maturation process.

Conclusion: According to the findings, the tumor microenvironment may have been responsible for preventing the maturation of DCs. This, in turn, weakened the immune response and facilitated the ability of the tumor to proliferate. Furthermore, the tumor microenvironment increased the number of immature DCs by inhibiting their stimulation by overexpression of TGF-β-produced by regulatory T lymphocytes and stimulation of tumor cells. In addition, the tumor microenvironment stimulated the secretion of cytokines such as IL-10, and CD4 and decreased the secretion of IFN-γ-and IL-12 in tumor-induced mice cultured LN and spleen.

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树突状细胞免疫:乳腺癌小鼠树突状细胞亚群的筛选

背景：癌症（BC）是最具破坏性的疾病，尤其是致命的侵袭性疾病，是全球女性死亡的最根本原因。BC的扩增受肿瘤细胞自身的各种变化以及免疫系统状态的控制，免疫系统状态对肿瘤微环境有直接影响。T细胞表达的许多受体与抗原呈递细胞上的配体相互作用，以提供激活信号，从而产生效应抗肿瘤T细胞反应。另一方面，缺乏关于T细胞和树突状细胞（DC）在肿瘤发展过程中的实际相互作用和反应的信息。目的：通过小鼠肿瘤诱导来研究免疫系统对BC的反应。计算肿瘤的大小和体积。此外，还研究了来自BC荷瘤小鼠淋巴结（LN）和脾脏的T细胞和DC的表型特征。此外，还测定了转化生长因子-β、干扰素-γ、白细胞介素IL-2、IL-10、IL-4、IL-12和肿瘤坏死因子（TNF）-α的水平。材料与方法：用MDA231细胞诱导30只白色BALB/C小鼠的BC，而其他30只小鼠作为健康对照，不使用任何致癌剂。使用基于标记表面分子的流式细胞术以及使用ELISA方法的小鼠LN培养物的特异性细胞因子滴度来评估恶性肿瘤的影响。这些细胞因子包括转化生长因子-β（TGF-β）、IFN-γ、IL-2、IL-10、IL-4、IL-12和TNF-α。结果：DC的成熟受到抑制，随后是未成熟DC的积累。与对照组相比，这些未成熟DC增加了携带BC的小鼠淋巴结和脾脏悬浮液的培养上清液中TGF-β和细胞因子如IL-10的释放，并抑制IFN-γ和IL-12的释放。此外，DC上CD80和CD86的表达较低，这表明成熟过程较低。结论：根据研究结果，肿瘤微环境可能是阻止DC成熟的原因。这反过来削弱了免疫反应，促进了肿瘤的增殖能力。此外，肿瘤微环境通过抑制调节性T淋巴细胞产生的TGF-β-的过度表达和肿瘤细胞的刺激来增加未成熟DC的数量。此外，肿瘤微环境刺激了肿瘤诱导的LN和脾脏中细胞因子如IL-10和CD4的分泌，并降低了IFN-γ和IL-12的分泌。

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来源期刊

Journal of Microscopy and Ultrastructure Medicine-Nephrology

CiteScore

1.90

自引率

0.00%

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