The China-US (Henan) Hormel Cancer Institute, Zhengzhou, 450003, Henan, People's Republic of China.
The Hormel Institute, University of Minnesota, Austin, MN, 55912, USA.
Gastric Cancer. 2022 Jul;25(4):726-740. doi: 10.1007/s10120-022-01297-7. Epub 2022 May 7.
Helicobacter pylori (H. pylori) has been recognized as the class I carcinogen of gastric cancer and several studies have demonstrated that chronic stress may accelerate gastric cancer progression. However, the evidence is not sufficient.
Here, we developed a mouse model that combined H. pylori infection with chronic stress. Gastric inflammation promotes gastric tumor development progression. To evaluate the number of pro-inflammatory cells through observing the numbers of activated macrophages and neutrophils in mice gastric tumors compared with untreated mice or only treated with one factor. ADRα1d /SerpinA1 expression and localization were assessed under stress conditions and H. pylori infection, and evaluated by analyzing IL-1α, CD8, platelet, and RBC status using α- or β- blockers against gastritis to prevent gastric cancer.
Further mechanism study showed that stress hormones increase the number of CD8 lymphocytes by activating ADRβ2 receptors, leading to IL-1α secretion and tumorigenicity. Gastric carcinogenesis also involves gastric muscle contraction mediated through ADRα1d/Serpina1 interaction. Specifically, we showed that the ADRα1d/SerpinA1 complex increases glucose uptake and the development of hypoxia conditions. These responses promote platelet aggregation and muscle contraction. In turn, gastric cancer cells increase lactate production and promote gastric cell proliferation through Muc-13 and IL-1α stimulation.
H. pylori infection in combination with chronic stress can lead to gastric cancer, and the synergistic effects of cytokine production (i.e. IL-1α), T lymphocyte dysfunction contributes to gastric carcinogenesis which will offer treatment opportunities for stress-associated gastric cancer and provide new strategies for the prevention and treatment of gastric cancer in clinics.
幽门螺杆菌(H. pylori)已被确认为胃癌的 I 类致癌物,多项研究表明慢性应激可能加速胃癌进展。然而,证据并不充分。
在这里,我们开发了一种将 H. pylori 感染与慢性应激相结合的小鼠模型。胃炎症促进胃肿瘤发展进展。通过观察与未处理小鼠或仅用一种因素处理的小鼠的胃肿瘤中的活化巨噬细胞和中性粒细胞的数量来评估促炎细胞的数量。在应激条件和 H. pylori 感染下评估 ADRα1d/SerpinA1 的表达和定位,并通过使用针对胃炎的α或β受体阻滞剂分析 IL-1α、CD8、血小板和 RBC 状态来评估预防胃癌的效果。
进一步的机制研究表明,应激激素通过激活 ADRβ2 受体增加 CD8 淋巴细胞的数量,导致 IL-1α 的分泌和肿瘤发生。胃癌发生还涉及通过 ADRα1d/Serpina1 相互作用介导的胃肌肉收缩。具体来说,我们表明 ADRα1d/SerpinA1 复合物增加葡萄糖摄取和缺氧条件的发展。这些反应促进血小板聚集和肌肉收缩。反过来,胃癌细胞通过 Muc-13 和 IL-1α 刺激增加乳酸的产生并促进胃细胞增殖。
H. pylori 感染与慢性应激相结合可导致胃癌,细胞因子产生(即 IL-1α)的协同作用、T 淋巴细胞功能障碍有助于胃发生癌变,这将为应激相关胃癌的治疗提供机会,并为临床预防和治疗胃癌提供新策略。
