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建立和鉴定 13 个人结直肠癌细胞系:基因突变及药物敏感性基因和肿瘤干细胞标志物的表达。

Establishment and characterization of 13 human colorectal carcinoma cell lines: mutations of genes and expressions of drug-sensitivity genes and cancer stem cell markers.

机构信息

Laboratory of Cell Biology, Cancer Research Institute, Seoul National University College of Medicine, Seoul 110-744, Korea.

出版信息

Carcinogenesis. 2010 Jun;31(6):1003-9. doi: 10.1093/carcin/bgq043. Epub 2010 Feb 22.

Abstract

Thirteen human colorectal cancer (CRC) cell lines were established from 10 primary tumors and 3 metastatic tumors obtained from 13 Korean patients. Characteristics of the cell lines including morphology in vivo and in vitro; mutations of the K-ras, p53, APC and MMR genes and microsatellite instability (MSI) status in vitro were determined. Expression of drug-sensitivity genes including MDR1, MXR, MRP1 and COX2 was also analyzed. The cell lines were unique as judged by DNA fingerprinting using 16 short tandem repeats. Eleven of the cell lines grew as adherent populations and the remaining two as floating aggregates. None of the cell lines were contaminated with Mycoplasma or bacteria. All cell lines showed high viability with relatively long doubling times. Six cell lines contained mutations at K-ras. Seven cell lines displayed p53 gene missense, nonsense and frameshift mutations. MSI was found in three cell lines and two cell lines with an MSI-high phenotype-possessed hMLH1 mutations. Nine cell lines had an APC mutation. MRP1 was highly expressed in all cell lines, and high expression of MDR1, MXR and COX2 evident in eight, six and six cell lines, respectively. Embryonal stem cell markers (MELK, SOX4 and OCT4) were expressed in most of cell lines. The cancer stem cell biomarkers CD133, CD44 and Lgr5 were expressed in 12, 13 and 13 cell lines, respectively. The presently well-characterized CRC cell lines should be useful in investigations of the biological characteristics of CRC, particularly for investigations related to gene alterations associated with CRC and biology of cancer stem cells.

摘要

十三株人类结直肠癌细胞系源自 10 个原发肿瘤和 3 个转移性肿瘤,这些肿瘤均取自 13 位韩国患者。我们对细胞系的特征进行了鉴定,包括体内和体外的形态;体外 K-ras、p53、APC 和 MMR 基因的突变和微卫星不稳定性(MSI)状态;还分析了药物敏感性基因(包括 MDR1、MXR、MRP1 和 COX2)的表达情况。通过使用 16 个短串联重复序列进行 DNA 指纹分析,判断这些细胞系是独特的。11 株细胞系以贴壁细胞群生长,其余 2 株以悬浮聚集体生长。所有细胞系均未被支原体或细菌污染。所有细胞系的活力均较高,倍增时间相对较长。6 株细胞系在 K-ras 中含有突变。7 株细胞系显示 p53 基因突变,包括错义、无义和移码突变。3 株细胞系存在 MSI,2 株具有 MSI 高表型的细胞系存在 hMLH1 突变。9 株细胞系存在 APC 突变。所有细胞系均高度表达 MRP1,8、6 和 6 株细胞系分别高表达 MDR1、MXR 和 COX2。大多数细胞系表达胚胎干细胞标志物(MELK、SOX4 和 OCT4)。12、13 和 13 株细胞系分别表达癌症干细胞标志物 CD133、CD44 和 Lgr5。目前这些特征良好的结直肠癌细胞系应该有助于对结直肠癌生物学特征的研究,特别是对与结直肠癌相关的基因改变和癌症干细胞生物学的研究。

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