异ferlinopathy的基因型-表型相关性和自然史研究:来自印度的单中心经验。

IF 1.6 4区 医学 Q3 CLINICAL NEUROLOGY
Saraswati Nashi, Kiran Polavarapu, Mainak Bardhan, Ram Murthy Anjanappa, Veeramani Preethish-Kumar, Seena Vengalil, Hansashree Padmanabha, Thenral S Geetha, P V Prathyusha, Vedam Ramprasad, Aditi Joshi, Tanushree Chawla, Gopikirshnan Unnikrishnan, Pooja Sharma, Akshata Huddar, Bharathram Uppilli, Abel Thomas, Dipti Baskar, Susi Mathew, Deepak Menon, Gautham Arunachal, Mohammed Faruq, Kumarasamy Thangaraj, Atchayaram Nalini
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引用次数: 1

摘要

肌营养不良症是一组在年轻人群中引起严重残疾的四肢带状肌肉营养不良症。有必要对大型队列进行研究,以描述我们次大陆的临床、基因型和自然史。描述和关联的临床,遗传档案和自然历史的遗传证实的异常蛋白病。我们分析了一个回顾性队列患者从一个单一的四级护理中心在印度的异ferlinopathy。共纳入124例异ferlinopathy患者(40例女性)。中位发病年龄和病程分别为21岁(范围13-50岁)和48个月(范围8-288岁)。平均随访60个月(范围12 ~ 288)。51%的人在发病时有LGMD模式的虚弱;三好型和近远型各占23.4%,孤立性高血血症占1.6%。约60%为近亲出生,26.6%有类似疾病家族史。23例患者(18.6%)在随访中失去行动能力;到丧失独立行走能力的中位时间为120个月(范围72-264)。单核苷酸变异(SNVs)占78.2%;14.5%和7.3%的患者同时存在snv和INDELs。snv的发病年龄较早。其他临床参数和活动状态与基因型无相关性。在总共81个变异中鉴定出37个(45.7%)新的致病/可能致病(P/LP)变异。c.3191G > A变异是最常见的突变。我们的队列构成了一个临床和遗传异质性的异铁蛋白病群体。临床遗传特征与运动状态之间没有明显的相关性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Genotype-phenotype correlation and natural history study of dysferlinopathy: a single-centre experience from India.

Genotype-phenotype correlation and natural history study of dysferlinopathy: a single-centre experience from India.

Dysferlinopathies are a group of limb-girdle muscular dystrophies causing significant disability in the young population. There is a need for studies on large cohorts to describe the clinical, genotypic and natural history in our subcontinent. To describe and correlate the clinical, genetic profile and natural history of genetically confirmed dysferlinopathies. We analysed a retrospective cohort of patients with dysferlinopathy from a single quaternary care centre in India. A total of 124 patients with dysferlinopathy were included (40 females). Median age at onset and duration of illness were 21 years (range, 13-50) and 48 months (range, 8-288), respectively. The average follow-up period was 60 months (range, 12-288). Fifty-one percent had LGMD pattern of weakness at onset; 23.4% each had Miyoshi and proximo-distal type while isolated hyperCKemia was noted in 1.6%. About 60% were born to consanguineous parents and 26.6% had family history of similar illness. Twenty-three patients (18.6%) lost ambulation at follow-up; the median time to loss of independent ambulation was 120 months (range, 72-264). Single-nucleotide variants (SNVs) constituted 78.2% of patients; INDELs 14.5% and 7.3% had both SNVs and INDELs. Earlier age at onset was noted with SNVs. There was no correlation between the other clinical parameters and ambulatory status with the genotype. Thirty-seven (45.7%) novel pathogenic/likely pathogenic (P/LP) variants were identified out of a total of 81 variations. The c.3191G > A variant was the most recurrent mutation. Our cohort constitutes a clinically and genetically heterogeneous group of dysferlinopathies. There is no significant correlation between the clinico-genetic profile and the ambulatory status.

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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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