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Engraftment of chronic myelomonocytic leukemia cells in immunocompromised mice supports disease dependency on cytokines

机译:在免疫功能低下的小鼠中植入慢性粒单核细胞白血病细胞支持疾病对细胞因子的依赖性

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摘要

Chronic myelomonocytic leukemia (CMML) is a clonal hematopoietic stem cell disorder that typically associates with mutations in epigenetic, splicing, and signaling genes. Genetically modified mouse models only partially recapitulate the disease phenotype, whereas xenotransplantation of CMML cells in immunocompromised mice has been rarely successful so far. Here, CMML CD34+ cells sorted from patient bone marrow (BM) or peripheral blood (PB) were injected intravenously into NSG (NOD/LtSz-scid IL2rγnull) mice and NSG mice engineered to express human granulo-monocyte colony-stimulating factor, stem cell factor, and interleukin-3 (NSGS mice). Fifteen out of 16 patient samples (94%) successfully engrafted into NSG or NSGS or both mouse strains. The expansion of human cells, predominant in the BM, was also observed in the spleen and the PB and was greatly enhanced in mice producing the 3 human cytokines. Gene mutations identified in engrafted cells were mostly similar to those identified in patient cells before injection. Successful secondary engraftment was obtained in NSGS mice in 3 out of 10 attempts. Thus, primary CMML leukemic cells expand much better in NSGS compared with NSG mice with limited efficacy of secondary transplant.
机译:慢性粒细胞单核细胞白血病(CMML)是一种克隆性造血干细胞疾病,通常与表观遗传,剪接和信号传导基因的突变相关。转基因的小鼠模型仅部分概括了疾病的表型,而迄今为止,在免疫受损的小鼠中CMML细胞的异种移植很少成功。在这里,将从患者骨髓(BM)或外周血(PB)中分选出的CMML CD34 + 细胞静脉内注射到NSG(NOD / LtSz-scidIL2rγnull)小鼠和经过工程改造以表达人颗粒-单核细胞集落刺激因子,干细胞因子和白介素3(NSGS小鼠)。 16个患者样本中有15个(94%)成功植入了NSG或NSGS或两种小鼠品系。在脾脏和PB中也观察到主要在BM中的人细胞的扩增,并且在产生3种人细胞因子的小鼠中大大增强了。在移植细胞中鉴定出的基因突变与注射前在患者细胞中鉴定出的基因突变最为相似。在10次尝试中有3次在NSGS小鼠中获得了成功的二次移植。因此,与二次移植疗效有限的NSG小鼠相比,原代CMML白血病细胞在NSGS中的扩增要好得多。

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