A novel nonsense variant in TPM4 caused dominant macrothrombocytopenia, mild bleeding tendency and disrupted cytoskeleton remodeling

Ana Marín-Quílez; Elena Vuelta; Lorena Díaz-Ajenjo; Cristina Fernández-Infante; Ignacio García-Tuñón; Rocío Benito; Verónica Palma-Barqueros; Jesús María Hernández-Rivas; José Ramón González-Porras; José Rivera; José María Bastida

doi:10.1111/jth.15672

A novel nonsense variant in TPM4 caused dominant macrothrombocytopenia, mild bleeding tendency and disrupted cytoskeleton remodeling

J Thromb Haemost. 2022 May;20(5):1248-1255. doi: 10.1111/jth.15672. Epub 2022 Feb 28.

Authors

Affiliations

¹ IBSAL, CIC, IBMCC, Universidad de Salamanca-CSIC, Salamanca, Spain.
² Transgenic Facility, Nucleus, University of Salamanca, Salamanca, Spain.
³ Department of Hematology and Oncology, Hospital Universitario Morales Meseguer, Centro Regional de Hemodonación, Universidad de Murcia, IMIB-Arrixaca, Murcia, Spain.
⁴ Department of Hematology, Complejo Asistencial Universitario de Salamanca (CAUSA), Instituto de Investigación Biomédica de Salamanca (IBSAL), Universidad de Salamanca (USAL), Salamanca, Spain.
⁵ On behalf of "Grupo Español de Alteraciones Plaquetarias Congénitas (GEAPC)", SETH, Madrid, Spain.

Abstract

Background: Rare inherited thrombocytopenias are caused by alterations in genes involved in megakaryopoiesis, thrombopoiesis and/or platelet release. Diagnosis is challenging due to poor specificity of platelet laboratory assays, large numbers of culprit genes, and difficult assessment of the pathogenicity of novel variants.

Objectives: To characterize the clinical and laboratory phenotype, and identifying the underlying molecular alteration, in a pedigree with thrombocytopenia of uncertain etiology.

Patients/methods: Index case was enrolled in our Spanish multicentric project of inherited platelet disorders due to lifelong thrombocytopenia and bleeding. Bleeding score was recorded by ISTH-BAT. Laboratory phenotyping consisted of blood cells count, blood film, platelet aggregation and flow cytometric analysis. Genotyping was made by whole-exome sequencing (WES). Cytoskeleton proteins were analyzed in resting/spreading platelets by immunofluorescence and immunoblotting.

Results: Five family members displayed lifelong mild thrombocytopenia with a high number of enlarged platelets in blood film, and mild bleeding tendency. Patient's platelets showed normal aggregation and granule secretion response to several agonists. WES revealed a novel nonsense variant (c.322C>T; p.Gln108*) in TPM4 (NM_003290.3), the gene encoding for tropomyosin-4 (TPM4). This variant led to impairment of platelet spreading capacity after stimulation with TRAP-6 and CRP, delocalization of TPM4 in activated platelets, and significantly reduced TPM4 levels in platelet lysates. Moreover, the index case displayed up-regulation of TPM2 and TPM3 mRNA levels.

Conclusions: This study identifies a novel TPM4 nonsense variant segregating with macrothrombocytopenia and impaired platelet cytoskeletal remodeling and spreading. These findings support the relevant role of TPM4 in thrombopoiesis and further expand our knowledge of TPM4-related thrombocytopenia.

Keywords: TPM4; inherited platelet disorders; macrothrombocytopenia; tropomyosin-4; whole-exome sequencing.

Publication types

Case Reports

MeSH terms

Blood Platelet Disorders* / genetics
Blood Platelets / metabolism
Cytoskeleton / metabolism
Hemorrhage
Humans
Thrombocytopenia*
Thrombopoiesis / genetics
Tropomyosin / genetics
Tropomyosin / metabolism

Substances

TPM4 protein, human
Tropomyosin