孤立性纤维瘤患者对抗血管生成治疗反应中肿瘤部位的适应性免疫结构及循环髓源性抑制细胞的下调
Adaptive immune contexture at the tumour site and downmodulation of circulating myeloid-derived suppressor cells in the response of solitary fibrous tumour patients to anti-angiogenic therapy.
作者信息
Tazzari M, Negri T, Rini F, Vergani B, Huber V, Villa A, Dagrada P, Colombo C, Fiore M, Gronchi A, Stacchiotti S, Casali P G, Pilotti S, Rivoltini L, Castelli C
机构信息
1] Unit of Immunotherapy of Human Tumours, Department of Experimental Oncology and Molecular Medicine, Via G. Venezian 1, Milan 20133, Italy [2] Fondazione IRCCS Istituto Nazionale dei Tumori, Via G. Venezian 1, Milan 20133, Italy.
1] Fondazione IRCCS Istituto Nazionale dei Tumori, Via G. Venezian 1, Milan 20133, Italy [2] Laboratory of Experimental Molecular Pathology, Department of Diagnostic Pathology and Laboratory, Via G. Venezian 1, Milan 20133, Italy.
出版信息
Br J Cancer. 2014 Sep 23;111(7):1350-62. doi: 10.1038/bjc.2014.437. Epub 2014 Aug 7.
BACKGROUND
Host immunity is emerging as a key player in the prognosis and response to treatment of cancer patients. However, the impact of the immune system and its modulation by therapies are unknown in rare soft tissue sarcomas such as solitary fibrous tumours (SFTs), whose management in the advanced forms includes anti-angiogenic therapy. Here, we studied the in situ and systemic immune status of advanced SFT patients and the effects of sunitinib malate (SM) in association with the clinical efficacy.
METHODS
Immune contexture of SFTs was assessed by immunohistochemistry in lesions from untreated or SM-treated patients. Frequency of circulating myeloid-derived suppressor cells (MDSCs), regulatory T cells (Tregs) and T-cell functions was assessed ex vivo in SFT patients prior and during anti-angiogenic therapy. Patients with long-term tumour control were included to correlate immune profiles and clinical responses.
RESULTS
Anti-angiogenic naïve SFT lesions were heavily infiltrated by CD163(+)CD14(+)CD68(-) and CD163(+)CD14(-)CD68(-) myeloid cells but devoid of T cells. Conversely, post-SM tumours acquired a new subset of CD68(+)CD14(+) myeloid cells and displayed traits of an on-going adaptive immunity, strongly enriched in activated CD8(+) and CD4(+) T cells. These changes at the tumour site paralleled the alleviation of systemic immunosuppression and the drop in the frequency of circulating monocytic MDSCs (mMDSCs) and granulocytic MDSCs (gMDSCs). Rebound in the number of mMDSCs, but not of gMDSCs occurred at disease progression, and a reduced percentages of mMDSCs, comparable to those found in healthy donors (HDs), endured only in the SM-responsive patients.
CONCLUSIONS
The immune contexture of SFT patients is heavily involved in anti-angiogenic therapy and it could be exploited to achieve more durable disease control through immune-based combination strategies.
背景
宿主免疫正成为癌症患者预后和治疗反应的关键因素。然而,在罕见的软组织肉瘤如孤立性纤维瘤(SFT)中,免疫系统的影响及其受治疗的调节尚不清楚,其晚期形式的治疗包括抗血管生成治疗。在此,我们研究了晚期SFT患者的原位和全身免疫状态以及苹果酸舒尼替尼(SM)的作用及其与临床疗效的关系。
方法
通过免疫组织化学评估未治疗或接受SM治疗患者病变中SFT的免疫格局。在抗血管生成治疗前和治疗期间,对SFT患者的循环髓源性抑制细胞(MDSC)、调节性T细胞(Treg)频率和T细胞功能进行体外评估。纳入长期肿瘤控制患者以关联免疫谱和临床反应。
结果
未经抗血管生成治疗的SFT病变中大量浸润CD163(+)CD14(+)CD68(-)和CD163(+)CD14(-)CD68(-)髓样细胞,但缺乏T细胞。相反,接受SM治疗后的肿瘤获得了新的CD68(+)CD14(+)髓样细胞亚群,并表现出持续适应性免疫的特征,强烈富集活化的CD8(+)和CD4(+)T细胞。肿瘤部位的这些变化与全身免疫抑制的缓解以及循环单核细胞MDSC(mMDSC)和粒细胞MDSC(gMDSC)频率的下降相平行。疾病进展时mMDSC数量反弹,但gMDSC未反弹,且仅在对SM有反应的患者中持续存在与健康供体(HD)相当的降低百分比的mMDSC。
结论
SFT患者的免疫格局在抗血管生成治疗中起重要作用,可通过基于免疫的联合策略加以利用以实现更持久的疾病控制。
Zotero 插件