Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors.

Bardsley MR; Horvath VJ; Asuzu DT; Lorincz A; Redelman D; Hayashi Y; Popko LN; Young DL; Lomberk GA; Urrutia RA; Farrugia G; Rubin BP; Ordog T

首页> 外文期刊>Gastroenterology >Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors.

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Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors.

机译：Kitlow干细胞在鼠胃肠道间质瘤中引起对Kit /血小板衍生的生长因子α抑制剂的耐药性。

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BACKGROUND & AIMS: Gastrointestinal stromal tumors (GIST) are related to interstitial cells of Cajal (ICC) and often contain activating stem cell factor receptor (Kit) or platelet-derived growth factor receptor alpha (Pdgfra) mutations. Kit/Pdgfra inhibitors such as imatinib mesylate have increased progression-free survival in metastatic GIST but are not curative. In mouse models we investigated whether Kit(low) ICC progenitors could represent an inherently Kit/Pdgfra inhibitor-resistant reservoir for GIST. METHODS: Isolated Kit(low)Cd44(+)Cd34(+) cells were characterized after serial cloning. The tumorigenic potential of spontaneously transformed cells was investigated in nude mice. The Kit(low)Cd44(+)Cd34(+) cells' responsiveness to Kit activation and blockade was studied by enumerating them in Kit(K641E) mice (a GIST model), in mice with defective Kit signaling, and pharmacologically. RESULTS: Single isolated Kit(low)Cd44(+)Cd34(+) cells were clonogenic and capable of self-renewal and differentiation into ICC. In nude mice, spontaneously transformed cells formed malignant tumors expressing GIST markers. The Kit(low)Cd44(+)Cd34(+) cells were resistant to in vitro Kit blockade, including by imatinib, and occurred in normal numbers in mice with reduced Kit signaling. In Kit(K641E) mice, the mutant ICC stem cells were grossly hyperplastic but remained imatinib-resistant. In contrast, the cancer stem, cell-targeting drug salinomycin blocked the proliferation of Kit(low)Cd44(+)Cd34(+) cells and increased their sensitivity to imatinib. CONCLUSIONS: Kit(low)Cd44(+)Cd34(+) progenitors are true stem cells for normal and hyperplastic ICC and give rise to GIST. Resistance to Kit/Pdgfra inhibitors is inherent in GIST and is caused by the native ICC stem cells' lack of dependence on Kit for survival, which is maintained after the acquisition of oncogenic Kit mutation. Cancer stem cell drugs may target these cells.

机译：背景与目的：胃肠道间质瘤（GIST）与Cajal间质细胞（ICC）有关，并且通常包含活化的干细胞因子受体（Kit）或血小板衍生的生长因子受体α（Pdgfra）突变。甲磺酸伊马替尼等Kit / Pdgfra抑制剂在转移性GIST中的无进展生存期增加，但并非治愈性药物。在小鼠模型中，我们研究了Kit（低）ICC祖细胞是否可以代表GIST固有的Kit / Pdgfra抑制剂抗性储库。方法：连续克隆后鉴定分离的Kit（低）Cd44（+）Cd34（+）细胞。在裸鼠中研究了自发转化细胞的致瘤潜力。通过枚举Kit（K641E）小鼠（GIST模型），Kit信号传导缺陷的小鼠以及药理作用，研究了Kit（low）Cd44（+）Cd34（+）细胞对Kit激活和阻断的反应。结果：单个分离的Kit（low）Cd44（+）Cd34（+）细胞具有克隆性，能够自我更新并分化为ICC。在裸鼠中，自发转化的细胞形成表达GIST标志物的恶性肿瘤。 Kit（low）Cd44（+）Cd34（+）细胞对体外Kit阻滞具有抵抗力，包括伊马替尼，并且在Kit信号减少的小鼠中以正常数量发生。在Kit（K641E）小鼠中，突变的ICC干细胞明显增生，但仍然对伊马替尼具有抗性。相比之下，癌症干细胞，靶向细胞的药物salinomycin阻止了Kit（low）Cd44（+）Cd34（+）细胞的增殖，并增加了它们对伊马替尼的敏感性。结论：Kit（low）Cd44（+）Cd34（+）祖细胞是正常和增生ICC的真正干细胞，并产生GIST。对Kit / Pdgfra抑制剂的抗药性是GIST固有的，是由于天然ICC干细胞对Kit生存的依赖性不足而引起的，这种依赖在获得致癌Kit突变后得以维持。癌症干细胞药物可能靶向这些细胞。

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《Gastroenterology》 |2010年第3期|共11页
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Bardsley MR; Horvath VJ; Asuzu DT; Lorincz A; Redelman D; Hayashi Y; Popko LN; Young DL; Lomberk GA; Urrutia RA; Farrugia G; Rubin BP; Ordog T;
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1. Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors. [J] . Bardsley MR, Horvath VJ, Asuzu DT, Gastroenterology . 2010,第3期

机译：Kitlow干细胞在鼠胃肠道间质瘤中引起对Kit /血小板衍生的生长因子α抑制剂的耐药性。
2. Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors. [J] . Bardsley MR, Horvath VJ, Asuzu DT, Gastroenterology . 2010,第3期

机译：KITLOW干细胞导致鼠胃肠间质谱中的试剂盒/血小板衍生的生长因子α抑制剂。
3. Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors. [J] . Bardsley MR, Horvath VJ, Asuzu DT, Gastroenterology . 2010,第3期

机译：KITLOW干细胞导致鼠胃肠间质谱中的试剂盒/血小板衍生的生长因子α抑制剂。
4. Delivery of Platelet-Derived Growth Factor from Bone-Mimetic Electrospun Matrices as a Chemotactic Factor for Mesenchymal Stem Cells [C] . Matthew Phipps, Yuanvuan Xu, Susan L. Bellis Society for Biomaterials fall symposium 2012.;vol. 34. . 2012

机译：从骨模拟电纺丝基质中递送血小板衍生的生长因子作为间充质干细胞的趋化因子
5. Roles of insulin-like growth factor binding protein-3 in gastrointestinal stromal tumors. [D] . Dupart, Jheri J. 2009

机译：胰岛素样生长因子结合蛋白3在胃肠道间质瘤中的作用。
6. Kitlow stem cells cause resistance to Kit/Pdgfra inhibitors in murine gastrointestinal stromal tumors [O] . Michael R. Bardsley, Viktor J. Horváth, David T. Asuzu, -1

机译：KITLOW干细胞导致鼠胃肠间质谱中的试剂盒/ PDGFRA抑制剂耐受性
7. Kitlow Stem Cells Cause Resistance to Kit/Platelet-Derived Growth Factor α Inhibitors in Murine Gastrointestinal Stromal Tumors [O] . Michael R. Bardsley, Viktor J. Horváth, David T. Asuzu, 2010

机译：KITLOW干细胞导致鼠胃肠间质谱中的试剂盒/血小板衍生生长因子α抑制剂

Kitlow stem cells cause resistance to Kit/platelet-derived growth factor alpha inhibitors in murine gastrointestinal stromal tumors.

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