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Genomic landscape of high-grade meningiomas

机译:高档脑膜瘤的基因组景观

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摘要

High-grade meningiomas frequently recur and are associated with high rates of morbidity and mortality. To determine the factors that promote the development and evolution of these tumors, we analyzed the genomes of 134 high-grade meningiomas and compared this information with data from 595 previously published meningiomas. High-grade meningiomas had a higher mutation burden than low-grade meningiomas but did not harbor any significantly mutated genes aside from NF2. High-grade meningiomas also possessed significantly elevated rates of chromosomal gains and losses, especially among tumors with monosomy 22. Meningiomas previously treated with adjuvant radiation had significantly more copy number alterations than radiation-induced or radiation-naïve meningiomas. Across serial recurrences, genomic disruption preceded the emergence of nearly all mutations, remained largely uniform across time, and when present in low-grade meningiomas correlated with subsequent progression to a higher grade. In contrast to the largely stable copy number alterations, mutations were strikingly heterogeneous across tumor recurrences, likely due to extensive geographic heterogeneity in the primary tumor. While high-grade meningiomas harbored significantly fewer overtly targetable alterations than low-grade meningiomas, they contained numerous mutations that are predicted to be neoantigens, suggesting that immunologic targeting may be of therapeutic value.
机译:高级别脑膜瘤经常复发,并与高发病率和死亡率相关。为了确定促进这些肿瘤发生和发展的因素,我们分析了134个高级脑膜瘤的基因组,并将此信息与595个先前发表的脑膜瘤的数据进行了比较。高级别脑膜瘤比低级别脑膜瘤具有更高的突变负担,但是除了NF2以外没有任何明显的突变基因。高档脑膜瘤还具有显着提高的染色体得失率,尤其是在患有22号染色体单体性肿瘤的肿瘤中。先前接受辅助放射治疗的脑膜瘤的拷贝数变化明显多于放射诱导或未经放射的脑膜瘤。在一系列复发中,基因组破坏发生在几乎所有突变出现之前,并在整个时间范围内保持基本一致,并且当存在低度脑膜瘤时与随后的更高级别相关。与基本上稳定的拷贝数改变相反,突变在整个肿瘤复发中具有显着异质性,这可能是由于原发性肿瘤中广泛的地理异质性所致。尽管高级脑膜瘤比低级脑膜瘤具有明显更少的明显可靶向改变,但它们包含许多被认为是新抗原的突变,这表明免疫学靶向可能具有治疗价值。

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