Introduction: Heart failure (HF) is a clinical syndrome characterized by cardinal symptoms that may be accompanied by signs. It results from structural and/or functional abnormalities of the heart leading to elevated intracardiac pressures and/or inadequate cardiac output at rest and/or during exercise. The prevalence of iron deficiency and anemia justifies the current guidelines recommendation of screening. Genes
HP
,
ACE
,
MTHFR, HFE,
and
CYBA
are involved in oxidative mechanisms, iron metabolism, and hematologic homeostasis. This study investigates the contribution of variants Hp1/2 (
HP
), I/D (
ACE
), C677T (
MTHFR
), C282Y and H63D (
HFE
), and C242T (
CYBA
) to the development of HF, either independently or in epistasis.
Methods: We used a database of 389 individuals, 143 HF patients, and 246 healthy controls. Genotypes were characterized through PAGE electrophoresis, PCR, PCR-RFLP, and multiplex-ARMS. Data analysis was performed with the SPSS® 26.0 software (IBM Corp., Armonk, NY).
Results: We observed a significant association between the
MTHFR
gene and HF predisposition. The presence of allele T and genotype CT constituted risk, while genotype CC granted protection. Epistatic interactions revealed risk between genotype II of the
ACE
gene and genotypes CC (
C282Y)
or HH (
H63D)
of the
HFE
gene. Risk was also observed for interactions between genotype CC (
CYBA
)and genotypes 2-2 (
HP)
, CT (
MTHFR
), or HH (
HFE-H63D)
.
Conclusion: We concluded that genes
HP
,
ACE
,
MTHFR, HFE,
and
CYBA
contribute to the susceptibility for HF, individually or in epistasis. This study contributes to the clarification of the role that genes involved in oxidative mechanisms and iron metabolism play in the physiopathology of HF. It is, therefore, a step forward in risk stratification and personalized medicine.