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Microenvironmental control of malignancy exerted by RNASET2 a widely conserved extracellular RNase

机译:RNASET2(一种广泛保存的细胞外RNase)对恶性肿瘤的微环境控制

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摘要

A recent body of evidence indicates an active role for stromal (mis)-regulation in the progression of neoplasias. Within this conceptual framework, genes belonging to the growing but still poorly characterized class of tumor antagonizing/malignancy suppressor genes (TAG/MSG) seem to play a crucial role in the regulation of the cross-talk between stromal and epithelial cells by controlling malignant growth in vivo without affecting any cancer-related phenotype in vitro. Here, we have functionally characterized the human RNASET2 gene, which encodes the first human member of the widespread Rh/T2/S family of extracellular RNases and was recently found to be down-regulated at the transcript level in several primary ovarian tumors or cell lines and in melanoma cell lines. Although we could not detect any activity for RNASET2 in several functional in vitro assays, a remarkable control of ovarian tumorigenesis could be detected in vivo. Moreover, the control of ovarian tumorigenesis mediated by this unique tumor suppressor gene occurs through modification of the cellular microenvironment and the induction of immunocompetent cells of the monocyte/macrophage lineage. Taken together, the data presented in this work strongly indicate RNASET2 as a previously unexplored member of the growing family of tumor-antagonizing genes.
机译:最近的证据表明,基质(mis)调节在肿瘤形成过程中起积极作用。在这一概念框架内,属于正在生长但仍缺乏特征的肿瘤拮抗/恶性肿瘤抑制基因(TAG / MSG)的基因似乎在通过控制恶性肿瘤的生长而调控基质细胞与上皮细胞之间的相互作用中起着至关重要的作用。在体内不影响任何与癌症相关的表型。在这里,我们已经在功能上表征了人类RNASET2基因,该基因编码广泛的细胞外RNase Rh / T2 / S家族的第一个人类成员,并且最近发现在一些原发性卵巢肿瘤或细胞系中其转录水平下调和黑色素瘤细胞系中尽管我们无法在几种功能性体外测定中检测到RNASET2的任何活性,但可以在体内检测到对卵巢肿瘤发生的显着控制。而且,由这种独特的抑癌基因介导的卵巢肿瘤发生的控制通过细胞微环境的修饰和单核细胞/巨噬细胞谱系的免疫活性细胞的诱导而发生。两者合计,这项工作中提供的数据强烈表明RNASET2是肿瘤拮抗基因不断增长的家族中一个尚未探索的成员。

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