Clin Lab. 2020 Apr 1;66(4). doi: 10.7754/Clin.Lab.2019.190715.
Congenital thrombotic thrombocytopenic purpura (TTP) is rare and is prone to misdiagnosis or missed diagnosis in clinical. The relationship between genotype and phenotype needs further study.
A 15-hour-old Chinese girl develops jaundice. Her platelet counts suddenly decreases with bleeding spots on the left side of chest, upper abdomen, and bilateral groin on the fourth day after birth. The plasma ADAMTS13 activity and inhibitor are detected by residual collagen binding assay. ADAMTS 13 gene is detected by next generation sequencing.
The plasma ADAMTS13 activity of the patient is shown to be severely deficient, but without inhibitor. Gene sequencing analysis shows that the patient carries a compound heterozygote mutation of ADAMTS13 gene, one is c.1564T>C, p.(Cys522Arg) on exon 13 of the ADAMTS13 gene, a heterozygote missense mutation. It is identified as a de novo suspected pathological variation. The other is c.330+1G>A on intron 3 of the ADAMTS13 gene, a heterozygote splicing mutation. Her father and elder sister carry c.1564T>C, p.(Cys522Arg) on exon 13 of the ADAMTS13 gene, a heterozygote missense mutations. Her mother carries c.330+1G>A on intron 3 of the ADAMTS13 gene, a heterozygote splicing mutation.
The deficiency of ADAMTS13 caused by one heterozygote missense mutation and the other heterozygote splicing mutation are responsible for the episode of this congenital TTP patient.
先天性血栓性血小板减少性紫癜(TTP)较为罕见,临床上易误诊或漏诊。基因型与表型的关系尚需进一步研究。
一名 15 小时大的中国女婴出现黄疸。出生后第 4 天,其血小板计数突然下降,并出现左侧胸部、上腹部和双侧腹股沟的出血点。采用残余胶原结合试验检测血浆 ADAMTS13 活性和抑制剂。采用下一代测序检测 ADAMTS13 基因。
患者的血浆 ADAMTS13 活性严重缺乏,但无抑制剂。基因测序分析显示,该患者携带 ADAMTS13 基因的复合杂合突变,一种是 ADAMTS13 基因外显子 13 上的 c.1564T>C,p.(Cys522Arg),为杂合错义突变,被鉴定为疑似新生病理性变异。另一种是 ADAMTS13 基因内含子 3 上的 c.330+1G>A,为杂合剪接突变。其父亲和姐姐携带 ADAMTS13 基因外显子 13 上的 c.1564T>C,p.(Cys522Arg),杂合错义突变。其母亲携带 ADAMTS13 基因内含子 3 上的 c.330+1G>A,杂合剪接突变。
该先天性 TTP 患者的 ADAMTS13 活性缺乏由一个杂合错义突变和另一个杂合剪接突变引起。
