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肾细胞癌 CD105-/CD44- 细胞在体外具有干细胞样特性,并在体内形成侵袭性肿瘤。

Renal carcinoma CD105-/CD44- cells display stem-like properties in vitro and form aggressive tumors in vivo.

机构信息

Mossakowski Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland.

Department of Oncology with Laboratory of Molecular Oncology, Military Institute of Medicine, Warsaw, Poland.

出版信息

Sci Rep. 2020 Mar 25;10(1):5379. doi: 10.1038/s41598-020-62205-6.

Abstract

Clear cell renal cell carcinoma (ccRCC) is the most common kidney cancer. Prognosis for ccRCC is generally poor since it is largely resistant to chemo- and radiotherapy. Many studies suggested that cancer stem cells/tumor initiating cells (CSCs/TICs) are responsible for development of tumor, disease progression, aggressiveness, metastasis and drug resistance. However, tumorigenic potential of CSCs/TICs isolated from established RCC cell lines - basic ccRCC research model - has never been investigated in vivo. CD105+, CD105-, CD44+ and CD44- as well as CD44-/CD105- CD44+/CD105+ and CD44-/CD105+ cells were isolated from Caki-1 RCC cell line, confirming coexistence of multiple subpopulations of stem-related phenotype in stable cell line. Sorted cells were injected subcutaneously into NOD SCID mice and tumor growth was monitored with MRI and PET/CT. Tumor growth was observed after implantation of CD105+, CD44+, CD44-, CD44-/CD105+ and CD44-/CD105- but not CD105- or CD44+/CD105+. Implantation of CD44-/CD105- cells induced tumors that were characterized by longer T1 and distinct metabolic pattern than other tumors. All the tumors were characterized by low uptake of [18F]FDG. CD105+ and CD44- tumors expresses Nanog and Oct-4, while CD44- tumors additionally expressed endothelial cell marker - CD31.

摘要

透明细胞肾细胞癌 (ccRCC) 是最常见的肾癌。由于 ccRCC 对化疗和放疗有很大的抵抗力,因此其预后通常较差。许多研究表明,癌症干细胞/肿瘤起始细胞 (CSCs/TICs) 是肿瘤发展、疾病进展、侵袭性、转移和耐药性的原因。然而,从已建立的肾癌细胞系(基本 ccRCC 研究模型)中分离的 CSCs/TICs 的肿瘤发生潜力从未在体内进行过研究。从 Caki-1 RCC 细胞系中分离出 CD105+、CD105-、CD44+和 CD44-以及 CD44-/CD105-、CD44+/CD105+和 CD44-/CD105+细胞,证实了稳定细胞系中多种与干细胞相关表型的亚群共存。对分选细胞进行皮下注射到 NOD SCID 小鼠中,并通过 MRI 和 PET/CT 监测肿瘤生长。在植入 CD105+、CD44+、CD44-、CD44-/CD105+和 CD44-/CD105-后观察到肿瘤生长,但 CD105-或 CD44+/CD105+则不会。植入 CD44-/CD105-细胞会诱导肿瘤,其 T1 较长且代谢模式与其他肿瘤不同。所有肿瘤的 [18F]FDG 摄取均较低。CD105+和 CD44-肿瘤表达 Nanog 和 Oct-4,而 CD44-肿瘤还表达内皮细胞标志物-CD31。

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