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首页> 外文期刊>Journal of Neuropathology and Experimental Neurology: Official Journal of the American Association of Neuropathologists, Inc >Development of a Novel Orthotopic Primary Human Chordoma Xenograft Model: A Relevant Support for Future Research on Chordoma
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Development of a Novel Orthotopic Primary Human Chordoma Xenograft Model: A Relevant Support for Future Research on Chordoma

机译:新型原位原发性人脊索瘤异种移植模型的发展:关于脊索瘤的未来研究的相关支持

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摘要

Chordomas are slow-growing rare malignant neoplasms. The aim of this study was to establish a primary model of chordoma in the lumbosacral orthotopic area, to compare the growth rate to the subcutaneous site, and to show that this new graft site optimizes tumor growth and bony invasion. Eleven chordoma samples were transplanted subcutaneously in the flank and/or in contact with the lumbosacral region and grown into nude mice. Engraftment rate was significantly more successful in the lumbosacral environment compared with the flank at P0. Two xenografts from 2 patients showed bone invasion. One tumor was maintained through multiple rounds of serial transplantation, creating a model for study. Histological and immunostaining analysis confirmed that tumor grafts recapitulated the primary tumor from which they were derived, consisting of a myxoid chordoma expressing brachyury, cytokeratin AE1, EMA, and VEGF. Clear destruction of the bone by the tumor cells could be demonstrated. Molecular studies revealed PIK3CA and PTEN mutations involved in PI3K signaling pathway and most of the frequently reported chromosomal alterations. We present a novel orthotopic primary xenograft model of chordoma implanted for the first time in the lumbosacral area showing bone invasion, PIK3CA, and PTEN mutations that will facilitate preclinical studies.
机译:Chordomas是生长缓慢的罕见恶性肿瘤。本研究的目的是在腰骶部地区建立脊架瘤的主要模型,将生长速率与皮下遗址进行比较,并表明该新的移植遗址优化了肿瘤生长和骨侵袭。将11个脊索瘤样品皮下切除在侧面和/或与腰骶部接触并达到裸鼠。与P0的侧面相比,腰骶环境中的植入率明显更成功。来自2名患者的两种异种移植物显示骨侵袭。通过多轮连续移植保持一种肿瘤,从而产生研究模型。组织学和免疫染色分析证实,肿瘤移植物重新覆盖了它们来源的原发性肿瘤,由表达Brachyury,细胞角蛋白AE1,EMA和VEGF的肌瘤脊髓瘤组成。可以证明通过肿瘤细胞清除骨骼破坏骨骼。分子研究揭示了PIK3CA和PTEN突变,参与了PI3K信号通路和大多数经常报告的染色体改变。我们在显示骨侵袭,PIK3CA和PTEN突变的腰骶部第一次植入的新型原发性原发性异种移植模型,其患者将促进临床前研究。

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