Department of Immunology, Mayo Clinic School of Medicine, 13400 E, Shea Blvd, Scottsdale, Arizona-85259, USA.
Breast Cancer Res. 2009;11(4):R56. doi: 10.1186/bcr2345. Epub 2009 Jul 30.
Sites of chronic inflammation are often associated with the establishment and growth of various malignancies including breast cancer. A common inflammatory condition in humans is autoimmune arthritis (AA) that causes inflammation and deformity of the joints. Other systemic effects associated with arthritis include increased cellular infiltration and inflammation of the lungs. Several studies have reported statistically significant risk ratios between AA and breast cancer. Despite this knowledge, available for a decade, it has never been questioned if the site of chronic inflammation linked to AA creates a milieu that attracts tumor cells to home and grow in the inflamed bones and lungs which are frequent sites of breast cancer metastasis.
To determine if chronic inflammation induced by autoimmune arthritis contributes to increased breast cancer-associated metastasis, we generated mammary gland tumors in SKG mice that were genetically prone to develop AA. Two breast cancer cell lines, one highly metastatic (4T1) and the other non-metastatic (TUBO) were used to generate the tumors in the mammary fat pad. Lung and bone metastasis and the associated inflammatory milieu were evaluated in the arthritic versus the non-arthritic mice.
We report a three-fold increase in lung metastasis and a significant increase in the incidence of bone metastasis in the pro-arthritic and arthritic mice compared to non-arthritic control mice. We also report that the metastatic breast cancer cells augment the severity of arthritis resulting in a vicious cycle that increases both bone destruction and metastasis. Enhanced neutrophilic and granulocytic infiltration in lungs and bone of the pro-arthritic and arthritic mice and subsequent increase in circulating levels of proinflammatory cytokines, such as macrophage colony stimulating factor (M-CSF), interleukin-17 (IL-17), interleukin-6 (IL-6), vascular endothelial growth factor (VEGF), and tumor necrosis factor-alpha (TNF-alpha) may contribute to the increased metastasis. Treatment with anti-IL17 + celecoxib, an anti-inflammatory drug completely abrogated the development of metastasis and significantly reduced the primary tumor burden.
The data clearly has important clinical implications for patients diagnosed with metastatic breast cancer, especially with regards to the prognosis and treatment options.
慢性炎症部位常与各种恶性肿瘤的发生和生长有关,包括乳腺癌。人类常见的炎症性疾病是自身免疫性关节炎(AA),它会导致关节炎症和畸形。关节炎相关的其他全身影响包括肺部细胞浸润和炎症增加。几项研究报告了 AA 与乳腺癌之间存在统计学显著的风险比。尽管这一知识已经存在了十年,但从未有人质疑过与 AA 相关的慢性炎症部位是否会创造一个有利于肿瘤细胞向炎症骨骼和肺部归巢和生长的环境,而这些部位是乳腺癌转移的常见部位。
为了确定自身免疫性关节炎引起的慢性炎症是否会导致乳腺癌相关性转移增加,我们在易患 AA 的 SKG 小鼠中生成了乳腺肿瘤。使用两种乳腺癌细胞系,一种高转移性(4T1)和另一种非转移性(TUBO),在乳腺脂肪垫中生成肿瘤。评估关节炎与非关节炎小鼠中的肺部和骨骼转移以及相关炎症环境。
我们报告称,与非关节炎对照小鼠相比,在亲关节炎和关节炎小鼠中,肺部转移增加了三倍,骨转移的发生率也显著增加。我们还报告说,转移性乳腺癌细胞增强了关节炎的严重程度,导致一个恶性循环,既增加了骨破坏又增加了转移。亲关节炎和关节炎小鼠的肺部和骨骼中中性粒细胞和粒细胞浸润增强,循环中促炎细胞因子(如巨噬细胞集落刺激因子(M-CSF)、白细胞介素-17(IL-17)、白细胞介素-6(IL-6)、血管内皮生长因子(VEGF)和肿瘤坏死因子-α(TNF-α)水平升高,可能导致转移增加。用抗 IL-17+塞来昔布(一种抗炎药物)治疗可完全阻断转移的发展,并显著降低原发性肿瘤负担。
这些数据对诊断为转移性乳腺癌的患者具有重要的临床意义,特别是在预后和治疗选择方面。
