Rafat Mosalli, Alfia Fatma, Mohammed A Almatrafi, Mayada Mazroua, Bosco Paes
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引用次数: 0
摘要
Pfeiffer综合征(PS)是一种常染色体显性遗传病,有三种亚型,源于成纤维细胞生长因子FGFR1和FGFR2的杂合突变。这些亚型重叠,具有不同的临床表现和不同的预后,依赖于影响短期和长期预后和生存的神经和呼吸损害。我们报告了一个患有II型PS的男性足月婴儿,根据三维超声检查结果诊断为产前怀疑,并在出生后通过颅面断层扫描和磁共振成像证实。新一代测序小组发现了一种独特的新生FGFR2, c.335 A > G . Tyr112Cys变体,这是同类中的第一个,其特征与II型PS密切相关。最初的分子结果将该突变归类为非致病性,但后来被重新归类为致病性。产前,多学科的父母咨询关于初步诊断和预后促进了产后决定,最终在知情的选择姑息治疗和早期死亡。
De Novo Heterozygous Mutation in FGFR2 Causing Type II Pfeiffer Syndrome.
Pfeiffer syndrome (PS) is an autosomal dominant disorder with three subtypes stemming from heterozygous mutations in the fibroblast growth factors FGFR1 and FGFR2. The subtypes overlap with heterogeneous clinical manifestations and variable prognosis dependent on neurological and respiratory compromise that impact short- and long-term outcomes and survival. We present a male, term infant with type II PS that was diagnostically suspected antenatally based on three-dimensional ultrasonographic findings that were confirmed postnatally by craniofacial tomography and magnetic resonance imaging. A new generation sequencing panel identified a unique de novo FGFR2, c.335 A > G p. Tyr112Cys variant, the first of its kind, and features that closely aligned with subtype II PS. Initial molecular results categorized the mutation as nonpathogenic, but it was later reclassified as pathogenic. Antenatal, multidisciplinary parental counseling about the tentative diagnosis and prognosis facilitated postnatal decisions that culminated in an informed choice for palliative care and early demise.
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