Day-Williams Aaron G, Sun Chao, Jelcic Ilijas, McLaughlin Helen, Harris Tim, Martin Roland, Carulli John P
Translational Sciences, Biogen Idec, Cambridge, MA, USA.
Department of Neurology, University Hospital Zurich, Zurich, Switzerland.
J Clin Immunol. 2015 Jan;35(1):92-6. doi: 10.1007/s10875-014-0114-4. Epub 2014 Nov 12.
A 30 year-old man with a history of recurrent skin infections as well as elevated serum IgE and eosinophils developed neurological symptoms and had T2-hyperintense lesions observed in cerebral MRI. The immune symptoms were attributed to Hyper IgE syndrome (HIES) and the neurological symptoms with presence of JC virus in cerebrospinal fluid were diagnosed as Progressive Multifocal Leukoencephalopathy (PML). The patient was negative for STAT3 mutations. To determine if other mutations explain HIES and/or PML in this subject, his DNA was analyzed by whole genome sequencing.
Whole genome sequencing was completed to 30X coverage, and whole genome SNP typing was used to complement these data. The methods revealed single nucleotide variants, structural variants, and copy number variants across the genome. Genome-wide data were analyzed for homozygous or compound heterozygous null mutations for all protein coding genes. Mutations were confirmed by PCR and/or Sanger sequencing.
Whole genome analysis revealed deletions near the telomere of both copies of chromosome 9p. Several genes, including DOCK8, were impacted by the deletions but it was unclear whether each chromosome had identical or distinct deletions. PCR across the impacted region combined with Sanger sequencing of selected fragments confirmed a homozygous deletion from position 10,211 to 586,751.
While several genes are impacted by the deletion, DOCK8 deficiency is the most probable cause of HIES in this patient. DOCK8 deficiency may have also predisposed the patient to develop PML.
一名30岁男性,有复发性皮肤感染病史,血清IgE和嗜酸性粒细胞升高,出现神经症状,脑部MRI显示有T2高信号病变。免疫症状归因于高IgE综合征(HIES),脑脊液中存在JC病毒的神经症状被诊断为进行性多灶性白质脑病(PML)。该患者STAT3突变检测为阴性。为了确定是否有其他突变可解释该患者的HIES和/或PML,对其DNA进行了全基因组测序。
全基因组测序完成至30倍覆盖度,并使用全基因组SNP分型来补充这些数据。这些方法揭示了全基因组的单核苷酸变异、结构变异和拷贝数变异。对所有蛋白质编码基因的纯合或复合杂合无效突变进行全基因组数据分析。通过PCR和/或Sanger测序确认突变。
全基因组分析显示9号染色体短臂两个拷贝的端粒附近存在缺失。包括DOCK8在内的几个基因受到缺失影响,但尚不清楚每条染色体的缺失是否相同或不同。对受影响区域进行PCR并结合选定片段的Sanger测序,证实了从位置10,211到586,751的纯合缺失。
虽然有几个基因受到缺失影响,但DOCK8缺陷最有可能是该患者HIES的病因。DOCK8缺陷也可能使该患者易患PML。
