Development and Validation of a Targeted Next-Generation Sequencing Gene Panel for Children With Neuroinflammation

神经炎症 医学 生物标志物 生物信息学 遗传学 内科学 生物 疾病
作者
Dara McCreary,Ebun Omoyinmi,Ying Hong,Ciara Mulhern,Charalampia Papadopoulou,Marina Casimir,Yael Hacohen,Rodney Nyanhete,Helena Ahlfors,Thomas Cullup,Ming Lim,Kimberly Gilmour,Kshitij Mankad,Evangeline Wassmer,Stefan Berg,Cheryl Hemingway,Paul Brogan,Despina Eleftheriou
出处
期刊:JAMA network open [American Medical Association]
卷期号:2 (10): e1914274-e1914274 被引量:17
标识
DOI:10.1001/jamanetworkopen.2019.14274
摘要

Importance

Neuroinflammatory disorders are a range of severe neurological disorders causing brain and spinal inflammation and are now increasingly recognized in the pediatric population. They are often characterized by marked genotypic and phenotypic heterogeneity, complicating diagnostic work in clinical practice and molecular diagnosis.

Objective

To develop and evaluate a next-generation sequencing panel targeting genes causing neuroinflammation or mimicking neuroinflammation.

Design, Setting, and Participants

Cohort study in which a total of 257 genes associated with monogenic neuroinflammation and/or cerebral vasculopathy, including monogenic noninflammatory diseases mimicking these entities, were selected. A customized enrichment capture array, the neuroinflammation gene panel (NIP), was created. Targeted high-coverage sequencing was applied to DNA samples taken from eligible patients referred to Great Ormond Street Hospital in London, United Kingdom, between January 1, 2017, and January 30, 2019, because of onset of disease early in life, family history, and/or complex neuroinflammatory phenotypes.

Main Outcomes and Measures

The main outcome was the percentage of individuals with definitive molecular diagnoses, variant classification, and clinical phenotyping of patients with pathogenic variants identified using the NIP panel. The NIP panel was initially validated in 16 patients with known genetic diagnoses.

Results

The NIP was both sensitive (95%) and specific (100%) for detection of known mutations, including gene deletions, copy number variants, small insertions and deletions, and somatic mosaicism with allele fraction as low as 3%. Prospective testing of 60 patients (30 [50%] male; median [range] age, 9.8 [0.8-20] years) presenting with heterogeneous neuroinflammatory phenotypes revealed at least 1 class 5 (clearly pathogenic) variant in 9 of 60 patients (15%); 18 of 60 patients (30%) had at least 1 class 4 (likely pathogenic) variant. Overall, a definitive molecular diagnosis was established in 12 of 60 patients (20%).

Conclusions and Relevance

The NIP was associated with molecular diagnosis in this cohort and complemented routine laboratory and radiological workup of patients with neuroinflammation. Unexpected genotype-phenotype associations in patients with pathogenic variants deviating from the classic phenotype were identified. Obtaining an accurate molecular diagnosis in a timely fashion informed patient management, including successful targeted treatment in some instances and early institution of hematopoietic stem cell transplantation in others.
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