TINF2突变和先天性角化不良患者的组织特异性端粒缩短和退行性改变

Caitlin M. Roake , Marisa Juntilla , Rajni Agarwal-Hashmi , Steven Artandi , Christin S. Kuo
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引用次数: 1

摘要

先天性角化不良症是端粒功能障碍下游组织维持受损的疾病。患者表现为甲营养不良、口腔白斑和皮肤色素沉着缺陷的临床三联征,但该疾病涉及多个器官的退行性改变。端粒结合蛋白如TINF2(与trf1相互作用的核因子2)或端粒酶的突变是导致先天性角化不良的原因,端粒酶可以抵消与年龄相关的端粒缩短。我们提出了一个13岁时出现严重低氧血症的患者。患者有骨髓增生异常综合征病史,5岁时接受骨髓移植治疗。18岁时,她因急性肺炎住院治疗,并发展为呼吸衰竭,肾功能衰竭,最终,她和她的家人选择撤回支持,因为她不适合进行肺移植。患者的TINF2基因座测序显示一个杂合突变(c.844C >T, Arg282Cys),先前在先天性角化不良患者的一个亚群中有报道。多器官组织切片显示退行性改变,包括骨重塑紊乱,肺弥漫性肺泡损伤和小血管增生,皮肤角化过度伴色素沉着。尸检样本显示端粒长度呈双峰分布,来自供体造血组织的端粒长度与年龄相适应,而来自患者组织的端粒显示致病性缩短,其中肺、肝和肾的端粒最短。我们报告了首次调查退行性变化和端粒长度在多器官患者先天性角化不良。
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Tissue-specific telomere shortening and degenerative changes in a patient with TINF2 mutation and dyskeratosis congenita

Dyskeratosis congenita is a disease of impaired tissue maintenance downstream of telomere dysfunction. Characteristically, patients present with the clinical triad of nail dystrophy, oral leukoplakia, and skin pigmentation defects, but the disease involves degenerative changes in multiple organs. Mutations in telomere-binding proteins such as TINF2 (TRF1-interacting nuclear factor 2) or in telomerase, the enzyme that counteracts age related telomere shortening, are causative in dyskeratosis congenita. We present a patient who presented with severe hypoxemia at age 13. The patient had a history of myelodysplastic syndrome treated with bone marrow transplant at the age of 5. At age 18 she was hospitalized for an acute pneumonia progressing to respiratory failure, developed renal failure and ultimately, she and her family opted to withdraw support as she was not a candidate for a lung transplant. Sequencing of the patient’s TINF2 locus revealed a heterozygous mutation (c.844C > T, Arg282Cys) which has previously been reported in a subset of dyskeratosis congenita patients. Tissue sections from multiple organs showed degenerative changes including disorganized bone remodeling, diffuse alveolar damage and small vessel proliferation in the lung, and hyperkeratosis with hyperpigmentation of the skin. Autopsy samples revealed a bimodal distribution of telomere length, with telomeres from donor hematopoietic tissues being an age-appropriate length and those from patient tissues showing pathogenic shortening, with the shortest telomeres in lung, liver, and kidney. We report for the first time a survey of degenerative changes and telomere lengths in multiple organs in a patient with dyskeratosis congenita.

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来源期刊
Human Pathology: Case Reports
Human Pathology: Case Reports Medicine-Pathology and Forensic Medicine
CiteScore
0.50
自引率
0.00%
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0
审稿时长
16 weeks
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