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成纤维细胞检测可在遗传性癌症panel 检测到嵌合体变异的个体中为医疗管理提供信息。

Fibroblast testing can inform medical management in individuals with mosaic variants detected on hereditary cancer panels.

机构信息

GeneDx, Gaithersburg, MD, United States.

GeneDx, Gaithersburg, MD, United States.

出版信息

Cancer Genet. 2022 Aug;266-267:86-89. doi: 10.1016/j.cancergen.2022.07.004. Epub 2022 Jul 28.

Abstract

Mosaic variants are regularly detected on hereditary cancer genetic tests. While some of these variants may be constitutional, the majority are likely limited to blood lineages. In the present study, we correlate clinical histories from individuals with mosaic findings identified on hereditary cancer testing and the outcomes of follow-up fibroblast (FB) testing. We observed 620 mosaic variants, including 339 pathogenic or likely pathogenic variants (PVs) occurring most often in TP53, CHEK2, ATM, and NF1. About half of individuals with NF1 mosaic PVs did not report any clinical features of NF1 and were older at testing (p<0.0001) compared to those with an NF1-related phenotype. Among 42 mosaic PVs evaluated by FB testing, 17 (40.5%) were confirmed in FB and were mostly identified in individuals with phenotypes consistent with the gene disease spectrum. Our data show that FB testing is helpful for identifying those with likely constitutional mosaicism benefitting from increased screening and follow-up vs. those with blood-limited variants potentially not requiring intense surveillance but warranting further hematologic work-up.

摘要

遗传性癌症基因检测中经常会发现镶嵌变体。虽然其中一些变体可能是构成性的,但大多数可能仅限于血液谱系。在本研究中,我们将遗传性癌症检测中发现的镶嵌发现个体的临床病史与后续成纤维细胞 (FB) 检测的结果进行了关联。我们观察到 620 个镶嵌变体,包括 339 个致病性或可能致病性变体 (PVs),这些变体最常发生在 TP53、CHEK2、ATM 和 NF1 中。大约一半 NF1 镶嵌 PVs 的个体没有报告任何 NF1 的临床特征,并且在检测时年龄更大 (p<0.0001),与具有 NF1 相关表型的个体相比。在 42 个经 FB 检测评估的镶嵌 PVs 中,有 17 个 (40.5%) 在 FB 中得到了确认,并且主要在与基因疾病谱一致的表型个体中发现。我们的数据表明,FB 检测有助于识别那些可能受益于增加筛查和随访的构成性镶嵌体,而不是那些血液受限变体可能不需要强烈监测但需要进一步血液学检查的个体。

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