Table 2.
Prognostic value of H-FABP in studies recruiting exclusively patients with ‘confirmed’ acute coronary syndrome.
| Author and year of publication | N | H-FABP assay | Clinical setting | MI (%) | Follow-up duration | Biomarkers measured | Key findings |
|---|---|---|---|---|---|---|---|
| Ishii et al. 200544 | 328 | Dainippon | Consecutive CCU admissions, sample on admission | 73.5% | 6 mths | TnT | Increased H-FABP was independently associated with cardiac events (cardiac death or non-fatal MI) RR=9; p=0.0004 |
| Erlikh et al. 200545 | 203 | Hycult | Sample 6 h from symptom onset | NA | 12 mths | TnI, CKMB | Elevated H-FABP was independent predictor of death or non-fatal MI, OR 2.45 95% CI (1.1–5.2); p=0.02 |
| O’Donoghue et al. 200632 | 2287 | In-house (Alere San Diego) | Clinical trial subset, mean time to randomisation = 41h | 55% | 10 mths | TnI, BNP, myoglobin | Elevated H-FABP was an independent predictor of death, recurrent MI, congestive heart failure or the composite of these end points (HR, 1.9; 95% CI, 1.3 to 2.7). In a multimarker approach, H-FABP, TnI, and BNP provided complementary information |
| Kilcullen et al. 200731 | 1448 | Dainippon | Consecutive confirmed ACS, sample 12–24 h from symptoms | 85% | 12 mths | TnI, hsCRP | H-FABP predicts long-term mortality independent of GRACE clinical risk factors, troponin and hsCRP. The adjusted all-cause mortality HR among unstable angina patients (Trop-ve) was 11.35 (95% CI 2.00 to 64.34; p=0.006) |