We studied the molecular basis and genetic heterogeneity of hereditary antithrombin (III) deficiency in nine Dutch families. Polymerase chain reaction (PCR) amplification and direct sequencing of all antithrombin gene exons and flanking intronic regions identified mutations in eight families. Given the opportunity to correlate the molecular basis with survival, we addressed the relevance of molecular defects to mortality in inherited antithrombin deficiency. The defects included single nucleotide deletions (7671 del G, 7768–69 del G) and insertions (5501 ins A, 2463 G-->TC) that lead to frameshifts, a single base substitution [5381 C-->T (129Arg-->stop)] leading to a premature termination codon, and single base substitutions resulting in amino acid substitutions [2652 A-->C (63Tyr-->Ser), 13380 T-->C (421Ile-->Thr), and 13407 G-->T (430Cys-->Phe)]. All affected individuals were heterozygous for the defects. Previously we found in Dutch families that antithrombin deficiency did not lead to higher mortality compared with the general population. In accordance with these findings, we observed no excess mortality in the nine families [Observed:Expected, 52:52.6; standardised mortality ratio (SMR) 1.0, 95% confidence interval (CI), 0.7–1.3]. Our findings confirmed a considerable genetic heterogeneity underlying antithrombin deficiency. We therefore concluded that the lack of excess mortality in these families is not caused by a Dutch mild defect. We suggest that the longevity is not affected by molecular defects in the antithrombin gene and hypothesize that differences in mortality or natural history between families most likely result from other (genetic) risk factors.
ARTICLES|
December 15, 1994
Hereditary antithrombin deficiency: heterogeneity of the molecular basis and mortality in Dutch families
HH van Boven,
HH van Boven
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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RJ Olds,
RJ Olds
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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SL Thein,
SL Thein
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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PH Reitsma,
PH Reitsma
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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DA Lane,
DA Lane
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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E Briet,
E Briet
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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JP Vandenbroucke,
JP Vandenbroucke
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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FR Rosendaal
FR Rosendaal
Department of Clinical Epidemiology, University Hospital, Leiden, The Netherlands.
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Blood (1994) 84 (12): 4209–4213.
Citation
HH van Boven, RJ Olds, SL Thein, PH Reitsma, DA Lane, E Briet, JP Vandenbroucke, FR Rosendaal; Hereditary antithrombin deficiency: heterogeneity of the molecular basis and mortality in Dutch families. Blood 1994; 84 (12): 4209–4213. doi: https://doi.org/10.1182/blood.V84.12.4209.bloodjournal84124209
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