A.C. Camargo Cancer Center, Sao Paulo, Brazil.
Center for Research in Inflammatory Diseases (CRID), University of Sao Paulo, Ribeirao Preto, Brazil.
J Immunother Cancer. 2020 May;8(1). doi: 10.1136/jitc-2019-000129.
Previous data have reported that the growth of established tumors may be facilitated by postsepsis disorder through changes in the microenvironment and immune dysfunction. However, the influence of postsepsis disorder in initial carcinogenesis remains elusive.
In the present work, the effect of postsepsis on inflammation-induced early carcinogenesis was evaluated in an experimental model of colitis-associated colorectal cancer (CAC). We also analyzed the frequency and role of intestinal T regulatory cells (Treg) in CAC carcinogenesis.
The colitis grade and the tumor development rate were evaluated postmortem or in vivo through serial colonoscopies. Sepsis-surviving mice (SSM) presented with a lower colonic DNA damage, polyp incidence, reduced tumor load, and milder colitis than their sham-operated counterparts. Ablating Treg led to restoration of the ability to develop colitis and tumor polyps in the SSM, in a similar fashion to that in the sham-operated mice. On the other hand, the growth of subcutaneously inoculated MC38luc colorectal cancer cells or previously established chemical CAC tumors was increased in SSM.
Our results provide evidence that postsepsis disorder has a dual effect in cancer development, inhibiting inflammation-induced early carcinogenesis in a Treg-dependent manner, while increasing the growth of previously established tumors.
先前的数据表明,通过微环境改变和免疫功能障碍,败血症后紊乱可能促进已建立的肿瘤生长。然而,败血症后紊乱在初始致癌作用中的影响仍不清楚。
在本工作中,我们在结肠炎相关结直肠癌(CAC)的实验模型中评估了败血症后对炎症诱导的早期癌变的影响。我们还分析了肠道 T 调节细胞(Treg)在 CAC 癌变中的频率和作用。
通过死后或体内的系列结肠镜检查评估结肠炎严重程度和肿瘤发展速度。存活于败血症的小鼠(SSM)的结肠 DNA 损伤、息肉发生率、肿瘤负荷降低以及结肠炎严重程度低于假手术对照组。在 SSM 中,Treg 耗竭导致能够恢复发生结肠炎和肿瘤息肉的能力,类似于假手术对照组。另一方面,皮下接种的 MC38luc 结直肠癌细胞或先前建立的化学 CAC 肿瘤的生长在 SSM 中增加。
我们的结果提供了证据表明,败血症后紊乱在癌症发展中有双重作用,以 Treg 依赖性方式抑制炎症诱导的早期癌变,同时增加先前建立的肿瘤的生长。
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