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功能网络分析揭示了与癌症患者原位淋巴细胞增殖和存活相关的遗传决定因素。

Functional network pipeline reveals genetic determinants associated with in situ lymphocyte proliferation and survival of cancer patients.

机构信息

INSERM UMRS1138, Laboratory of Integrative Cancer Immunology, Paris F-75006, France.

出版信息

Sci Transl Med. 2014 Mar 19;6(228):228ra37. doi: 10.1126/scitranslmed.3007240.

Abstract

The tumor microenvironment is host to a complex network of cytokines that contribute to shaping the intratumoral immune reaction. Chromosomal gains and losses, coupled with expression analysis, of 59 cytokines and receptors and their functional networks were investigated in colorectal cancers. Changes in local expression for 13 cytokines were shown. Metastatic patients exhibited an increased frequency of deletions of cytokines from chromosome 4. Interleukin 15 (IL15) deletion corresponded with decreased IL15 expression, a higher risk of tumor recurrence, and reduced patient survival. Decreased IL15 expression affected the local proliferation of B and T lymphocytes. Patients with proliferating B and T cells at the invasive margin and within the tumor center had significantly prolonged disease-free survival. These results delineate chromosomal instability as a mechanism of modulating local cytokine expression in human tumors and underline the major role of IL15. Our data provide further mechanisms resulting in changes of specific immune cell densities within the tumor, and the importance of local active lymphocyte proliferation for patient survival.

摘要

肿瘤微环境中存在着复杂的细胞因子网络,这些细胞因子有助于塑造肿瘤内的免疫反应。本研究分析了 59 种细胞因子和受体及其功能网络在结直肠癌中的染色体增益和丢失以及表达情况。结果显示,13 种细胞因子的局部表达发生了变化。与无转移的患者相比,发生转移的患者染色体 4 上细胞因子缺失的频率更高。白细胞介素 15(IL15)缺失对应着 IL15 表达降低、肿瘤复发风险增加以及患者生存率降低。IL15 表达的降低影响了 B 和 T 淋巴细胞的局部增殖。在侵袭边缘和肿瘤中心有增殖的 B 和 T 细胞的患者无病生存期显著延长。这些结果描绘了染色体不稳定性作为调节人类肿瘤中局部细胞因子表达的一种机制,并强调了 IL15 的主要作用。我们的数据提供了导致肿瘤内特定免疫细胞密度变化的进一步机制,以及局部活跃的淋巴细胞增殖对患者生存的重要性。

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