Lipoprotein(a) (Lp(a)) is an important risk factor for coronary artery disease and a prognostic predictor in patients after acute coronary syndrome (ACS), regardless of low-density lipoprotein (LDL) cholesterol levels. The results of recent research have shown that inhibitors of proprotein subtilisin/kexin converting enzyme 9 (PCSK9) are so far the only drugs that significantly lower serum Lp(a) concentration in addition to lowering LDL cholesterol, which is also their main property. However, we have no data on the relationship between Lp(a) concentration and genetic polymorphisms in the LPA gene, inflammation and hemostatic markers, impairment of arterial function and response to treatment with PCSK9 inhibitors in patients after ACS. The aim of our research was to study the relationship between lipid subfractions, inflammation and structural and functional properties of the arterial wall in patients with coronary artery disease, to study the influence of alirocumab and evolocumab on lipid subfractions, inflammation and structural-functional properties of the arterial wall in patients with early coronary atherosclerosis. We studied the influence of Lp(a) and gene polymorphisms in the LPA gene for apolipoprotein(a) on the structural-functional properties of the arterial vessel wall in subjects with a first ACS event before the age of 55, and the influence of alirocumab and evolocumab on the structural-functional properties of the arterial vessel wall in subjects after ACS and with a concentration of Lp(a) above 1000 mg/L or Lp(a) above 600 mg/L and LDL cholesterol above 2.6 mmol/L. We included 70 subjects in an observational, prospective, and randomized study that lasted 6 months. With step-wedge inclusion and randomization, we provided a control group consisting of 31 subjects. We took venous blood from all subjects for laboratory tests and measured the endothelium-dependent vasodilatation of the brachial artery (FMD - "flow-mediated dilatation"), the thickness of the intima-media complex (c-IMT - "carotid intima-media thickness") and the stiffness of the arterial vessel wall of the carotid arteries was measured by ultrasound. The results showed that the GG genotype of the rs10455872 polymorphism and the AT haplotype and the GT of the LPA gene are statistically significantly associated with Lp(a) values. Significantly higher Lp(a) values were recorded in subjects with the GG genotype compared to subjects with the AG genotype. Subjects with the haplotype without the AT allele had significantly higher Lp(a) values compared to the carriers of the haplotype with one allele or the haplotype with two AT alleles. We did not find statistically significant associations between the studied genotypes/haplotypes and arterial wall properties. Lp(a) values were also significantly correlated with the number of KIV-2 repeats (r = -0.601; p <0.0001). We found no statistically significant changes in FMD in the control and alirocumab groups, while a significant increase in FMD was found in the evolocumab group (from 11.2% ±6.8% to 14.1% ±6 .6%; p<0.0001). In the evolocumab group, we found a statistically significant change in c-IMT and pulse wave velocity (PWV). In non-smokers and subjects without diabetes, a significant improvement in FMD (p=0.003), c-IMT (p=0.027) and PWV (p=0.039) was recorded, regardless of which drug they received. There were 9.7% active smokers and 20% diabetics in the control group, 25.7% and 17.1% in the alirocumab group, and 11.8% active smokers and 2.9% diabetics in the evolocumab group. A significant decrease in Lp(a) was found in both treated groups (alirocumab from 1445 mg/l (1231-1793) to 1219 mg/l (845-1709); evolocumab from 1372 mg/l (1021-1608) to 881 mg/ l (800-1433); both p<0.0001), apolipoprotein B (p<0.001), apolipoprotein A1 (alirocumab p=0.019; evolocumab p=0.028), LDL cholesterol (alirocumab from 2.2±0.6 mmol /l to 0.8±0.6 mmol/l; evolocumab from 2.4±0.8 mmol/l to 0.9±0.9 mmol/l; both p<0.0001 and total cholesterol (TC ) (p<0.001). In a linear regression model, FMD at baseline correlated with age at first ACS, high-sensitivity C-reactive protein, and vascular cell adhesion protein 1 (VCAM1). c-IMT significantly correlated with age at first ACS and Lp(a) values. PWV was significantly correlated with systolic blood pressure (β=0.332; p=0.002), tumor necrosis factor alpha and interleukin 8. After treatment, we found a significant association of FMD with systolic blood pressure and VCAM1. PWV and c-IMT correlated with age and systolic blood pressure. Before treatment with PCSK9 inhibitors, TC, LDL cholesterol and triglycerides were significantly correlated with thrombin-activated fibrinolysis inhibitor (TAFI) and plasminogen activator inhibitor 1 (PAI-1) levels. TC and LDL cholesterol concentrations were correlated with total fibrinolytic potential. The concentration of triglycerides is related to the concentration of interleukin 6 and interleukin 8. However, we did not find correlations between Lp(a) and inflammatory or hemostatic markers before and after treatment. These data show that the GG genotype of the rs10455872 polymorphism and the haplotypes of both polymorphisms (rs10455872 and rs3798220) are associated with Lp(a) concentration in patients in the stable phase after ACS and with very high Lp(a) values. We did not find associations between genotypes or haplotypes and functional and morphological properties of the arterial wall. We also found no correlations between Lp(a) concentration and functional and morphological properties of the arterial vessel wall. Risk factors such as smoking, and diabetes weaken the effects of alirocumab and evolocumab on the functional and morphological properties of the arterial wall. In addition to age and arterial blood pressure, arterial vessel wall properties depend on Lp(a) concentration and inflammation before treatment with PCSK9 inhibitors. After treatment, the properties of the arterial vessel wall are affected only by age and blood pressure, and from markers of inflammation, VCAM1. Markers of fibrinolysis and inflammatory cytokines are associated with LDL cholesterol but not Lp(a) levels before or after treatment with PCSK9 inhibitors.