Deregulated expression of polycomb repressive complex 2 target genes in a NF1 patient with microdeletion generating the RNF135-SUZ12 chimeric gene.

IF 1.6 4区 医学 Q3 CLINICAL NEUROLOGY
Neurogenetics Pub Date : 2023-07-01 Epub Date: 2023-05-05 DOI:10.1007/s10048-023-00718-8
Viviana Tritto, Federico Grilli, Donatella Milani, Paola Riva
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引用次数: 0

Abstract

Neurofibromatosis type I (NF1) microdeletion syndrome, accounting for 5-11% of NF1 patients, is caused by the heterozygous deletion of NF1 and a variable number of flanking genes in the 17q11.2 region. This syndrome is characterized by more severe symptoms than those shown by patients with intragenic NF1 mutation and by variable expressivity, which is not fully explained by the haploinsufficiency of the genes included in the deletions. We here reevaluate an 8-year-old NF1 patient, who carries an atypical deletion generating the RNF135-SUZ12 chimeric gene, previously described when he was 3 years old. As the patient has developed multiple cutaneous/subcutaneous neurofibromas over the past 5 years, we hypothesized a role of RNF135-SUZ12 chimeric gene in the onset of the patient's tumor phenotype. Interestingly, SUZ12 is generally lost or disrupted in NF1 microdeletion syndrome and frequently associated to cancer as RNF135. Expression analysis confirmed the presence of the chimeric gene transcript and revealed hypo-expression of five out of the seven analyzed target genes of the polycomb repressive complex 2 (PRC2), to which SUZ12 belongs, in the patient's peripheral blood, indicating a higher transcriptional repression activity mediated by PRC2. Furthermore, decreased expression of tumor suppressor gene TP53, which is targeted by RNF135, was detected. These results suggest that RNF135-SUZ12 chimera may acquire a gain of function, compared with SUZ12 wild type in the PRC2 complex, and a loss of function relative to RNF135 wild type. Both events may have a role in the early onset of the patient's neurofibromas.

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多梳抑制复合物2靶基因在产生RNF135-SUZ12嵌合基因的微缺失的NF1患者中的表达下调。
I型神经纤维瘤病(NF1)微缺失综合征占NF1患者的5-11%,是由NF1和17q11.2区域可变数量的侧翼基因的杂合缺失引起的。该综合征的特征是比基因内NF1突变患者表现出的症状更严重,并且表现力可变,这并不能完全用缺失中包含的基因的单倍性来解释。我们在这里重新评估了一名8岁的NF1患者,他携带产生RNF135-SUZ12嵌合基因的非典型缺失,之前在他3岁时描述过。由于患者在过去5年中发生了多发性皮肤/皮下神经纤维瘤,我们假设RNF135-SUZ12嵌合基因在患者肿瘤表型发生中的作用。有趣的是,SUZ12通常在NF1微缺失综合征中缺失或破坏,并经常与癌症RNF135相关。表达分析证实了嵌合基因转录物的存在,并揭示了SUZ12所属的多梳抑制复合物2(PRC2)的七个分析靶基因中的五个在患者外周血中的低表达,表明PRC2介导的转录抑制活性更高。此外,检测到RNF135靶向的肿瘤抑制基因TP53的表达降低。这些结果表明,与PRC2复合物中的SUZ12野生型相比,RNF135-SUZ12嵌合体可以获得功能增益,并且相对于RNF135野生型可以获得功能损失。这两个事件都可能在患者神经纤维瘤的早期发病中发挥作用。
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来源期刊
Neurogenetics
Neurogenetics 医学-临床神经学
CiteScore
3.90
自引率
0.00%
发文量
24
审稿时长
6 months
期刊介绍: Neurogenetics publishes findings that contribute to a better understanding of the genetic basis of normal and abnormal function of the nervous system. Neurogenetic disorders are the main focus of the journal. Neurogenetics therefore includes findings in humans and other organisms that help understand neurological disease mechanisms and publishes papers from many different fields such as biophysics, cell biology, human genetics, neuroanatomy, neurochemistry, neurology, neuropathology, neurosurgery and psychiatry. All papers submitted to Neurogenetics should be of sufficient immediate importance to justify urgent publication. They should present new scientific results. Data merely confirming previously published findings are not acceptable.
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