Heide Solveig, Masliah-Planchon Julien, Isidor Bertrand, Guimier Anne, Bodet Damien, Coze Carole, Deville Anne, Thebault Estelle, Pasquier Corinne Jeanne, Cassagnau Elisabeth, Pierron Gaelle, Clément Nathalie, Schleiermacher Gudrun, Amiel Jeanne, Delattre Olivier, Peuchmaur Michel, Bourdeaut Franck
Service de Pathologie, Hôpital Robert Debré, APHP, Paris, France.
INSERM U830, Génétique et Biologie des Cancers, Institut Curie, Paris, France.
Pediatr Blood Cancer. 2016 Jan;63(1):71-7. doi: 10.1002/pbc.25723. Epub 2015 Sep 16.
Germline non-polyalanine repeat expansion mutations in PHOX2B (PHOX2B NPARM) predispose to peripheral neuroblastic tumors (PNT), frequently in association with other neurocristopathies: Hirschsprung disease (HSCR) or congenital central hypoventilation syndrome (CCHS). Although PHOX2B polyalanine repeat expansions predispose to a low incidence of benign PNTs, the oncologic phenotype associated with PHOX2B NPARM is still not known in detail.
We analyzed prognostic factors, treatment toxicity, and outcome of patients with PNT and PHOX2B NPARM.
Thirteen patients were identified, six of whom also had CCHS and/or HSCR, one also had late-onset hypoventilation with hypothalamic dysfunction (LO-CHS/HD), and six had no other neurocristopathy. Four tumours were "poorly differentiated," and nine were differentiated, including five ganglioneuromas, three ganglioneuroblastomas, and one differentiating neuroblastoma, hence illustrating that PHOX2B NPARM are predominantly associated with differentiating tumors. Nevertheless, three patients had stage 4 and one patient had stage 3 disease. Segmental chromosomal alterations, correlating with poor prognosis, were found in all the six tumors analyzed by array-comparative genomic hybridization. One patient died of tumor progression, one is on palliative care, one died of hypoventilation, and 10 patients are still alive, with median follow-up of 5 years.
Based on histological phenotype, our series suggests that heterozygous PHOX2B NPARM do not fully preclude ganglion cell differentiation in tumors. However, this tumor predisposition syndrome may also be associated with poorly differentiated tumors with unfavorable genomic profiles and clinically aggressive behaviors. The intrafamilial variability and the unpredictable tumor prognosis should be considered in genetic counseling.
PHOX2B基因的种系非多聚丙氨酸重复扩增突变(PHOX2B NPARM)易患外周神经母细胞瘤(PNT),常与其他神经嵴病相关:先天性巨结肠症(HSCR)或先天性中枢性低通气综合征(CCHS)。虽然PHOX2B多聚丙氨酸重复扩增易患良性PNT的发生率较低,但与PHOX2B NPARM相关的肿瘤表型仍不清楚。
我们分析了PNT和PHOX2B NPARM患者的预后因素、治疗毒性和结局。
共确定13例患者,其中6例还患有CCHS和/或HSCR,1例还患有迟发性低通气伴下丘脑功能障碍(LO-CHS/HD),6例无其他神经嵴病。4例肿瘤为“低分化”,9例为分化型,包括5例神经节瘤、3例神经节神经母细胞瘤和1例分化型神经母细胞瘤,因此说明PHOX2B NPARM主要与分化型肿瘤相关。然而,3例患者为4期,1例患者为3期疾病。通过阵列比较基因组杂交分析的所有6例肿瘤中均发现与预后不良相关的节段性染色体改变。1例患者死于肿瘤进展,1例接受姑息治疗,1例死于低通气,10例患者仍存活,中位随访时间为5年。
基于组织学表型,我们的系列研究表明,杂合性PHOX2B NPARM不能完全排除肿瘤中的神经节细胞分化。然而,这种肿瘤易患综合征也可能与具有不良基因组特征和临床侵袭性行为的低分化肿瘤相关。在遗传咨询中应考虑家族内变异性和不可预测的肿瘤预后。
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