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Distinct types of tumor-initiating cells form human colon cancer tumors and metastases.

机译:不同类型的肿瘤引发细胞形成人结肠癌肿瘤和转移。

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Human colon cancer harbors a small subfraction of tumor-initiating cells (TICs) that is assumed to be a functionally homogeneous stem-cell-like population driving tumor maintenance and metastasis formation. We found unexpected cellular heterogeneity within the TIC compartment, which contains three types of TICs. Extensively self-renewing long-term TICs (LT-TICs) maintained tumor formation in serial xenotransplants. Tumor transient amplifying cells (T-TACs) with limited or no self-renewal capacity contributed to tumor formation only in primary mice. Rare delayed contributing TICs (DC-TICs) were exclusively active in secondary or tertiary mice. Bone marrow was identified as an important reservoir of LT-TICs. Metastasis formation was almost exclusively driven by self-renewing LT-TICs. Our results demonstrate that tumor initiation, self-renewal, and metastasis formation are limited to particular subpopulations of TICs in primary human colon cancer. We identify LT-TICs as a quantifiable target for therapies aimed toward eradication of self-renewing tumorigenic and metastatic colon cancer cells.
机译:人类结肠癌中有一小部分肿瘤起始细胞(TICs),被认为是功能相同的干细胞样种群,可驱动肿瘤维持和转移形成。我们在TIC隔室内发现了意外的细胞异质性,其中包含三种类型的TIC。广泛自我更新的长期TIC(LT-TIC)维持了系列异种移植物中的肿瘤形成。具有有限的自我更新能力或没有自我更新能力的肿瘤瞬时扩增细胞(T-TAC)仅在原代小鼠中有助于肿瘤形成。罕见的延迟贡献TIC(DC-TIC)仅在次级或三级小鼠中具有活性。骨髓被认为是LT-TIC的重要储存库。转移形成几乎完全由自我更新的LT-TIC驱动。我们的结果表明,肿瘤的发生,自我更新和转移形成仅限于原发性人类结肠癌中TICs的特定亚群。我们确定LT-TICs为旨在消除自我更新的致瘤性和转移性结肠癌细胞的治疗的可量化目标。

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