Summary
Background
Hemostasis biomarkers are known to have an impact on venous thromboembolism (VTE) occurrence and survival in cancer patients.
Objectives
As there are almost no data on longitudinal changes, we aimed to evaluate those in the present prospective observational study during chemotherapy and the course of disease.
Patients/Methods
Patients with cancer of the brain (n = 39), lung (n = 41), colon (n = 15) or pancreas (n = 17) were included before initiation of antitumor therapy. Blood samples for determination of factor VIII, thrombin peak height, D‐dimer, F1 + 2, fibrinogen and soluble P‐selectin (sP‐selectin) were drawn on a monthly basis. The study endpoints were death, VTE occurrence, or completion of the study period.
Results
Overall, 546 blood samples of 112 patients were analyzed. D‐dimer and sP‐selectin levels were significantly higher in patients with distant metastasis than in those without. Patients with complete remission had significantly lower levels of F1 + 2, D‐dimer and fibrinogen. Peak height thrombin levels showed a decrease over time in all tumor types. Levels of biomarkers behaved differently in the various tumor types. Patients who developed VTE (n = 14) showed increasing levels of FVIII, sP‐selectin, and D‐dimer. At the last blood sampling time‐point before VTE occurrence, in 13 patients the D‐dimer level was above the median, and in seven of these patients it was even above the 75th percentile; however, the individual course was highly variable. Regarding survival, steadily increased FVIII, sP‐selectin and D‐dimer levels were associated with higher mortality.
Conclusions
Hemostatic parameters show an association with disease state, prognosis, and the risk of VTE, not only at diagnosis, but also during the course of antineoplastic treatment.