Antithrombin deficiency in three Japanese families: one novel and two reported point mutations in the antithrombin gene

Keiko Maruyama; Eriko Morishita; Megumi Karato; Tadaaki Kadono; Akiko Sekiya; Yukie Goto; Tomomi Sato; Haruka Nomoto; Wataru Omi; Sachie Tsuzura; Hidenori Imai; Hidesaku Asakura; Shigeki Ohtake; Shinji Nakao

doi:10.1016/j.thromres.2013.06.001

Antithrombin deficiency in three Japanese families: one novel and two reported point mutations in the antithrombin gene

Thromb Res. 2013 Aug;132(2):e118-23. doi: 10.1016/j.thromres.2013.06.001. Epub 2013 Jun 25.

Authors

Keiko Maruyama¹, Eriko Morishita, Megumi Karato, Tadaaki Kadono, Akiko Sekiya, Yukie Goto, Tomomi Sato, Haruka Nomoto, Wataru Omi, Sachie Tsuzura, Hidenori Imai, Hidesaku Asakura, Shigeki Ohtake, Shinji Nakao

Affiliation

¹ Department of Clinical Laboratory Science, Kanazawa University Graduate School of Medical Science, Kanazawa, Japan.

PMID: 23809926
DOI: 10.1016/j.thromres.2013.06.001

Abstract

Introduction: Inherited antithrombin (AT) deficiency is associated with a predisposition to familial venous thromboembolic disease. We analyzed the AT gene in three unrelated patients with an AT deficiency who developed thrombosis.

Materials and methods: We analyzed the SERPINC1 gene in three patients. Additionally, we expressed the three mutants in the COS-1 cells and compared their secretion rates and levels of AT activity with those of the wild-type (WT).

Results: We identified three distinct heterozygous mutations of c.2534C>T: p.56Arginine → Cysteine (R56C), c.13398C>A: p.459Alanine → Aspartic acid (A459D) and c.2703C>G: p.112 Proline → Arginine (P112R). In the in vitro expression experiments, the AT antigen levels in the conditioned media (CM) of the R56C mutant were nearly equal to those of WT. In contrast, the AT antigen levels in the CM of the A459D and P112R mutants were significantly decreased. The AT activity of R56C was decreased in association with a shorter incubation time in a FXa inhibition assay and a thrombin inhibition-based activity test. However, the AT activity of R56C was comparable to that of WT when the incubation time was increased.

Conclusions: We concluded that the R56C mutant is responsible for type II HBS deficiency. We considered that the A459D and P112R mutants can be classified as belonging to the type I AT deficiency.

Keywords: AT; Ala; Alanine; Antithrombin; Antithrombin deficiency; Arg; Arginine; Asp; Aspartic acid; CL; CM; COS-1 cells; Cell lysates; Complementary DNA; Conditioned media; Cys; Cysteine; DVT; Deep vein thrombosis; ELISA; Enzyme-linked immunosorbent assay; FXa; Factor Xa; Green monkey kidney cells; Lys; Lysine; PE; PMSF; Phenylmethyl sulfonylfluoride; Pro; Proline; Pulmonary thromboembolism; RCL; RFLP; Reactive center loop; Restriction fragment length polymorphism analysis; Serine protease inhibitor; Type II heparin binding site defects; Type II reactive site defects; Type II with pleiotropic defects; VTE; Venous thromboembolism; WT; Wild-type; cDNA; factor Xa inhibition activity assay; serpin; thrombin inhibition activity assay; type II HBS; type II PE; type II RS.

Publication types

Case Reports
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Animals
Antithrombin III / genetics*
Antithrombin III / metabolism
Antithrombin III Deficiency / blood
Antithrombin III Deficiency / genetics*
Blood Coagulation Tests
COS Cells
Chlorocebus aethiops
Female
Humans
Japan
Point Mutation*
Young Adult

Substances

SERPINC1 protein, human
Antithrombin III