Abstract
Here, we describe a mother and son with a lifelong bleeding tendency and posttraumatic bleeding who were recruited to the UK Genotyping and Phenotyping of Platelets (GAPP) study with a suspected platelet function disorder. However, despite a clinically significant bleeding score, both had normal platelet counts and normal platelet function. The patients’ blood was analyzed by light transmission aggregometry and genotyping by whole exome sequencing, as outlined by the GAPP study. Approximately 25 000 genetic variants were found for each patient as a result of sequencing and were filtered using a specialized bioinformatics pipeline. A heterozygous variant displaying autosomal dominant inheritance (c.1611 C>A) was found in the gene THBD which encodes the glycoprotein thrombomodulin. This sequence change results in a stop codon (p.Cys537Stop) and truncation of the protein and has been previously described in two other families with bleeding events which suggests it may be a recurrent mutation. In summary, this study shows that patients with a suspected platelet disorder but who present with a normal pattern of platelet aggregation should be investigated for defects in nonplatelet genes.
Highlights
Inherited platelet disorders (IPDs) are a heterogeneous group of disorders associated with normal or reduced platelet counts and bleeding diatheses of varying severities [1,2]
We describe a mother and son with a lifelong bleeding tendency and posttraumatic bleeding who were recruited to the UK Genotyping and Phenotyping of Platelets (GAPP) study with a suspected platelet function disorder
A mother and son were recruited to the GAPP study with a lifelong bleeding tendency, including posttraumatic bleeding, but presented with normal platelet and platelet-rich plasma (PRP) counts (4.2 × 108/mL and 3 × 108/mL, respectively), normal clotting factors, and normal platelet function
Summary
Inherited platelet disorders (IPDs) are a heterogeneous group of disorders associated with normal or reduced platelet counts and bleeding diatheses of varying severities [1,2]. The UK Genotyping and Phenotyping of Platelets (GAPP) study recruits patients with mild bleeding who have been clinically diagnosed with a suspected platelet function disorder. A mother and son were recruited to the GAPP study with a lifelong bleeding tendency, including posttraumatic bleeding, but presented with normal platelet and platelet-rich plasma (PRP) counts (4.2 × 108/mL and 3 × 108/mL, respectively), normal clotting factors, and normal platelet function. Factor IX genetics were normal; prothrombin consumption index was abnormal. To study these patients further, we have used a forward genetic approach by
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