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Identification and characterization of cancer initiating cells from BRCA1 related mammary tumors using markers for normal mammary stem cells

机译:使用正常乳腺干细胞标记物鉴定和鉴定BRCA1相关乳腺肿瘤中的癌症起始细胞

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摘要

It is hypothesized that cancer stem cells arise either from normal stem cells or from progenitor cells that have gained the ability to self-renew. Here we determine whether mammary cancer stem cells can be isolated by using antibodies that have been used for the isolation of normal mammary stem cells. We show that BRCA1 mutant cancer cell lines contained a subpopulation of CD24+CD29+ or CD24+CD49f+ cells that exhibited increased proliferation and colony forming ability in vitro, and enhanced tumor-forming ability in vivo. The purified CD24+CD29+ cells could differentiate and reconstitute the heterogeneity found in parental cells when plated as a monolayer. Under low-attachment conditions, we detected “tumorspheres” only in the presence of double positive cells, which maintained their ability to self-renew. Furthermore, CD24+CD29+ cells could form tubular structures reminiscent of the mammary ductal tree when grown in three-dimensional cultures, implying that these cancer cells maintain some of the characteristics of the normal stem cells. Nevertheless, they could still drive tumor formation since as low as 500 double positive cells immediately after sorting from BRCA1 mutant primary tumors were able to form tumors with the same heterogeneity found in the original tumors. These data provide evidence that breast cancer stem cells originate from normal stem cells and advance our understanding of BRCA1-associated tumorigenesis with possible implications for future cancer treatment.
机译:假设癌症干细胞来自正常干细胞或已获得自我更新能力的祖细胞。在这里,我们确定是否可以通过使用已用于分离正常乳腺干细胞的抗体来分离乳癌干细胞。我们显示BRCA1突变癌细胞系包含CD24 + CD29 +或CD24 + CD49f +细胞亚群,在体外表现出增加的增殖和集落形成能力,以及在体内增强的肿瘤形成能力。纯化的CD24 + CD29 +细胞可以铺板成单层时,可以分化和重建亲本细胞中发现的异质性。在低附着条件下,我们仅在双阳性细胞存在的情况下才检测到“肿瘤圈”,从而维持了它们的自我更新能力。此外,CD24 + CD29 +细胞在三维培养物中生长时可能会形成管状结构,让人联想到乳腺导管树,这意味着这些癌细胞保持了正常干细胞的某些特性。然而,它们仍然可以驱动肿瘤的形成,因为从BRCA1突变原发肿瘤中分选出的低至500个双重阳性细胞能够立即形成具有与原始肿瘤相同异质性的肿瘤。这些数据提供了证据,表明乳腺癌干细胞源自正常干细胞,并加深了我们对BRCA1相关肿瘤发生的理解,可能对未来的癌症治疗产生影响。

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