透明纤维瘤病综合征:一种罕见但可识别的综合征

Tuğba Daşar, Hasibe Nesligül Gönen, K. Kösemehmetoğlu, Ö. Tekşam, K. Boduroğlu, G. Utine, P. Ö. Şimşek Kiper
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摘要

背景。透明纤维瘤病综合征是一种罕见的常染色体隐性遗传疾病,由 ANTXR2 致病变体引起。该病的特征是结缔组织中无定形透明物质的沉积。该病的特征是关节挛缩、全身皮肤僵硬、关节伸展面色素沉着性丘疹、肛周肉质肿块、严重腹泻和牙龈肥大。病情轻重不一,预后不良。目前尚无特效治疗方法。大多数重症患者在 2 岁前死亡。在本研究中,我们描述了土耳其一家三级参考中心诊断和随访的七名透明纤维瘤病综合征患者的临床和分子研究结果。采用标准盐析法从三名患者的外周血样本中提取基因组 DNA。由于无法获得外周血 DNA,因此对一名患者的病理切片进行了 DNA 提取。在 ABI Prism 3500 基因分析仪上对 ANTXR2 的所有编码外显子进行扩增和测序。对 3 名患者进行了 Sanger 测序,在 ANTXR2 中发现了同源 c.945T>G p.(Cys315Trp)、c.1073dup p.(Ala359CysfsTer13)和 c.1074del p.(Ala359HisfsTer50)变异。所有患者均在五岁前去世。HFS是一种罕见的进行性疾病,具有广泛的表型谱。HFS具有独特的临床特征,很容易识别。尽管如此,该病的预后较差,严重的临床失代偿会增加死亡率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hyaline fibromatosis syndrome: a rare, yet recognizable syndrome
Background. Hyaline fibromatosis syndrome is a rare autosomal recessive disorder caused by ANTXR2 pathogenic variants. The disorder is characterized by the deposition of amorphous hyaline material in connective tissues. The hallmarks of the disease are joint contractures, generalized skin stiffness, hyperpigmented papules over extensor surfaces of joints, fleshy perianal masses, severe diarrhea, and gingival hypertrophy. The severity of the disease varies and prognosis is poor. No specific treatment is yet available. Most patients with the severe form of the condition pass away before the second year of age. In this study, we describe the clinical and molecular findings of a cohort of seven hyaline fibromatosis syndrome patients who were diagnosed and followed up at a single tertiary reference center in Turkey. Methods. Genomic DNA was extracted by standard salting out method from peripheric blood samples of three patients. In one patient DNA extraction was performed on pathology slides since peripheric blood DNA was not available. All coding exons of the ANTXR2 were amplified and sequenced on ABI Prism 3500 Genetic Analyser. Results. Sanger sequencing was performed in 3 patients and homozygous c.945T>G p.(Cys315Trp), c.1073dup p.(Ala359CysfsTer13), and c.1074del p.(Ala359HisfsTer50) variants were identified in ANTXR2. All patients passed away before the age of five years. Conclusions. HFS is a rare, progressive disorder with a broad phenotypic spectrum. HFS can be recognized easily with distinctive clinical features. Nevertheless, it has poor prognosis with increased mortality due to severe clinical decompensation.
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