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Microenvironment-dependent growth of pre-neoplastic and malignantplasma cells in humanized mice

机译:肿瘤前和恶性肿瘤的微环境依赖性生长人源化小鼠的浆细胞

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摘要

Most human cancers including myeloma are preceded by a precursor state. There is an unmet need for in vivo models to study the interaction of human preneoplastic cells in the bone marrow microenvironment with non-malignant cells. Here, we genetically humanized mice to permit the growth of primary human pre-neoplastic and malignant plasma cells together with non-malignant cells in vivo. Growth was largely restricted to the bone marrow, mirroring the pattern in patients. Xenografts captured the genomic complexity of parental tumors and revealed additional somatic changes. Moreover, xenografts from patients with preneoplastic gammopathy showed progressive growth, suggesting that the clinical stability of these lesions may in part be due to growth controls extrinsic to tumor cells. These data demonstrate a new approach to investigate the entire spectrum of human plasma cell neoplasia and illustrate the utility of humanized models for understanding the functional diversity of human tumors.
机译:大多数人类癌症(包括骨髓瘤)都处于先兆状态。对于研究骨髓微环境中人类肿瘤前细胞与非恶性细胞之间相互作用的体内模型,存在未满足的需求。在这里,我们对小鼠进行了人源化,使其在体内能够生长原发性人类肿瘤前和恶性浆细胞以及非恶性细胞。生长主要局限于骨髓,这反映了患者的模式。异种移植物捕获了亲本肿瘤的基因组复杂性,并揭示了额外的体细胞变化。此外,来自肿瘤前性丙种病患者的异种移植物显示出进行性生长,表明这些病变的临床稳定性可能部分归因于肿瘤细胞外在的生长控制。这些数据证明了一种研究人类浆细胞瘤形成的整个光谱的新方法,并说明了人源化模型对理解人类肿瘤功能多样性的实用性。

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