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Tumor Budding Micropapillary Pattern and Polyploidy Giant Cancer Cells in Colorectal Cancer: Current Status and Future Prospects

机译:大肠癌中的肿瘤萌发微乳头状和多倍体巨癌细胞:现状和未来展望

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摘要

We previously reported that polyploid giant cancer cells (PGCGs) induced by CoCl2 could form through endoreduplication or cell fusion. A single PGCC formed tumors in immunodeficient mice. PGCCs are also the key contributors to the cellular atypia and associate with the malignant grade of tumors. PGCCs have the properties of cancer stem cells and produce daughter cells via asymmetric cell division. Compared with diploid cancer cells, these daughter cells express less epithelial markers and acquire mesenchymal phenotype with importance in cancer development and progression. Tumor budding is generally recognized to correlate with a high recurrence rate, lymph node metastasis, chemoresistance, and poor prognosis of colorectal cancers (CRCs) and is a good indicator to predict the metastasis and aggressiveness in CRCs. Micropapillary pattern is a special morphologic pattern and also associates with tumor metastasis and poor prognosis. There are similar morphologic features and molecular phenotypes among tumor budding, micropapillary carcinoma pattern, and PGCCs with their budding daughter cells and all of them show strong ability of tumor invasion and migration. In this review, we discuss the cancer stem cell properties of PGCCs, the molecular mechanisms of their regulation, and the relationships with tumor budding and micropapillary pattern in CRCs.
机译:我们以前曾报道过CoCl2诱导的多倍体巨癌细胞(PGCG)可以通过核内复制或细胞融合形成。单个PGCC在免疫缺陷小鼠中形成肿瘤。 PGCC也是导致细胞异型性的关键因素,并且与肿瘤的恶性程度相关。 PGCC具有癌症干细胞的特性,并通过不对称细胞分裂产生子代细胞。与二倍体癌细胞相比,这些子细胞表达较少的上皮标记物并获得间充质表型,这对癌症的发展和进展具有重要意义。肿瘤出芽通常被认为与大肠癌(CRC)的高复发率,淋巴结转移,化学耐药性和预后不良有关,并且是预测CRC转移和侵袭性的良好指标。微乳头状形态是一种特殊的形态学形态,也与肿瘤转移和预后不良有关。肿瘤出芽,微乳头状癌和PGCCs的子代细胞具有相似的形态学特征和分子表型,都具有较强的侵袭和迁移能力。在这篇综述中,我们讨论了PGCC的癌干细胞特性,其调控的分子机制,以及与CRC中的肿瘤出芽和微乳头型的关系。

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