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Mutational landscape and genetic signatures of cell‐free DNA in tumour‐induced osteomalacia

机译:肿瘤诱导的骨科在肿瘤骨癌中无细胞DNA的突变景观和遗传特征

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Tumour‐induced osteomalacia (TIO) is a very rare paraneoplastic syndrome with bone pain, fractures and muscle weakness, which is mostly caused by phosphaturic mesenchymal tumours (PMTs). Cell‐free DNA (cfDNA) has been regarded as a non‐invasive liquid biopsy for many malignant tumours. However, it has not been studied in benign tumours, which prompted us to adopt the targeted next‐generation sequencing approach to compare cfDNAs of 4 TIO patients, four patients with bone metastasis (BM) and 10 healthy controls. The mutational landscapes of cfDNA in TIO and BM groups were similar in the spectrum of allele frequencies and mutation types. Markedly, deleterious missense mutations in FGFR1 and loss‐of‐function mutations in MED12 were found in 3/4 TIO patients but none of BM patients. The gene ontology analysis strongly supported that these mutated genes found in TIOs would play a potential role in PMTs' process. The genetic signatures and corresponding change in expression of FGFR1 and FGF23 were further validated in PMT tissues from a test cohort of another three TIO patients. In summary, we reported the first study of the mutational landscape and genetic signatures of cfDNA in TIO/PMTs.
机译:肿瘤诱导的骨癌(TIO)是一种非常罕见的骨瓣综合征,具有骨疼痛,骨折和肌肉弱点,主要由磷酸性间充质肿瘤(PMTS)引起。对于许多恶性肿瘤,无细胞DNA(CFDNA)被认为是非侵入性液体活组织检查。然而,它尚未在良性肿瘤中进行研究,这促使我们采用目标下一代测序方法来比较4 TIO患者的CFDNA,4例骨转移(BM)和10名健康对照。在等位基因频率和突变类型的频谱中,TiO和BM组中CFDNA的突变景观类似。显着,在3/4 TiO患者中发现了FGFR1中的有害密码突变和Med12中的功能突变,但没有BM患者。基因本体分析强烈支持,在TIOS中发现的这些突变基因将在PMTS过程中发挥潜在作用。 FGFR1和FGF23表达的遗传签名和相应的变化在来自另外三个TiO患者的试验队列的PMT组织中进一步验证。总之,我们报告了TIO / PMTS中CFDNA的突变景观和遗传特征的首次研究。

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