SUMMARY BACKGROUND: The simplified Selvester QRS score is a parameter for estimating myocardial damage in ST-elevation myocardial infarction. ST-elevation myocardial infarction leads to varying degrees of impairment in left ventricular systolic and diastolic function. Myocardial performance index is a single parameter that can predict combined left ventricular systolic and diastolic performance. OBJECTIVE: We investigated the relationship between Selvester score and myocardial performance index in patients undergoing primary percutaneous coronary intervention for acute anterior myocardial infarction. METHODS: The study included 58 patients who underwent primary percutaneous coronary intervention for acute anterior myocardial infarction. Selvester score of all patients was also calculated at 72 h. Patients were categorized into two groups according to the Selvester score. Those with a score <6 (low score) were considered group 1 and those with a score ≥6 (high score) were considered group 2. RESULTS: When compared with group 1, patients in group 2 were older (p=0.01) and had lower left ventricular ejection fractions (50.3±4 vs. 35.6±6.9, p=0.001), and conventional myocardial performance index (0.52±0.06 vs. 0.69±0.08, p=0.001), lateral tissue Doppler-derived myocardial performance index (0.57±0.08 vs. 0.72±0.08, p=0.001), and septal tissue Doppler-derived myocardial performance index (0.62±0.07 vs. 0.76±0.08, p=0.001) were higher. There was a high correlation between lateral tissue Doppler-derived myocardial performance index and conventional myocardial performance index and Selvester score (r=0.80, p<0.001; r=0.86, p<0.001, respectively) and a moderate correlation between septal tissue Doppler-derived myocardial performance index and Selvester score (r=0.67, p<0.001). CONCLUSIONS: The post-procedural Selvester score can predict lateral tissue Doppler-derived myocardial performance index and conventional myocardial performance index with high sensitivity and acceptable specificity in patients undergoing primary percutaneous coronary intervention for acute anterior myocardial infarction. BACKGROUND STelevation ST elevation function OBJECTIVE METHODS 5 7 h 6 < low ≥ RESULTS p=0.01 p001 p 0 01 (p=0.01 50.3±4 5034 50 3 4 (50.3± vs 35669 35 9 35.6±6.9 p=0.001, p0001 p=0.001 , 001 0.52±0.06 052006 52 06 (0.52±0.0 069008 69 08 0.69±0.08 Dopplerderived Doppler derived 0.57±0.08 057008 57 (0.57±0.0 072008 0.72±0.08 0.62±0.07 062007 62 07 (0.62±0.0 076008 76 0.76±0.08 higher r=0.80, r080 r 80 (r=0.80 p<0.001 r086 86 r=0.86 respectively r=0.67, r067 67 (r=0.67 p<0.001. . p<0.001) CONCLUSIONS postprocedural post procedural p=0.0 p00 (p=0.0 50.3± 503 (50.3 3566 35.6±6. p000 p=0.00 00 0.52±0.0 05200 (0.52±0. 06900 0.69±0.0 0.57±0.0 05700 (0.57±0. 07200 0.72±0.0 0.62±0.0 06200 (0.62±0. 07600 0.76±0.0 r=0.80 r08 8 (r=0.8 p<0.00 r=0.8 r=0.67 r06 (r=0.6 p=0. p0 (p=0. 50.3 (50. 356 35.6±6 0.52±0. 0520 (0.52±0 0690 0.69±0. 0.57±0. 0570 (0.57±0 0720 0.72±0. 0.62±0. 0620 (0.62±0 0760 0.76±0. r0 (r=0. p<0.0 r=0. r=0.6 p=0 (p=0 50. (50 35.6± 0.52±0 052 (0.52± 069 0.69±0 0.57±0 057 (0.57± 072 0.72±0 0.62±0 062 (0.62± 076 0.76±0 (r=0 p<0. r=0 p= (p= (5 35.6 0.52± 05 (0.52 0.69± 0.57± (0.57 0.72± 0.62± (0.62 0.76± (r= p<0 r= (p ( 35. 0.52 (0.5 0.69 0.57 0.72 0.62 (0.6 0.76 (r p< 0.5 (0. 0.6 0.7 0. (0

Abstract Background Coronary slow flow (CSF) refers to delayed distal vessel opacification in the absence of epicardial coronary artery stenosis. The etiopathogenic mechanism of CSF is still unclear. Objectives This study investigates the relationship between CSF and the triglyceride-glucose (TyG) index. Methods The study sample consisted of 118 CSF patients and 105 patients with normal coronary flow (NCF). The coronary flow rate was measured via the Thrombolysis in Myocardial Infarction (TIMI) frame count (TFC) method in all patients. The TyG index was calculated as the logarithm of the [fasting triglyceride (mg/dL)×fasting glucose (mg/dL)]/2 value. A significance level of < 0.05 was adopted as statistically significant. Results The TyG index, low-density lipoprotein (LDL), body mass index (BMI), neutrophil-to-lymphocyte ratio (NLR) and TFC values, male ratio, and the ratio of smokers were higher, whereas high-density lipoprotein (HDL) levels were significantly lower in the CSF group compared to the NCF group (p<0,05). The correlation analysis revealed that CSF was significantly correlated with TyG index, BMI, NLR, and HDL values. The strongest of these correlations was between CSF and TyG index (r= 0.57, p<0.001). Additionally, the multivariate analysis revealed that TyG index, BMI, NLR ratio, and male gender were independent predictors for CSF (p<0.05). Receiver operating characteristic (ROC) curve analysis indicated that a cut-off value of ≥ 9.28 for the TyG index predicted CSF with a sensitivity of 78% and a specificity of 78.1% [Area under the curve (AUC): 0.868 and 95% Confidence Interval (CI): 0.823-0.914]. Conclusion The findings of this study revealed a very strong relationship between CSF and TyG index. (CSF stenosis unclear triglycerideglucose (TyG 11 10 NCF. . (NCF) TIMI (TIMI (TFC fasting mg/dL×fasting mgdLfasting mg/dL ×fasting mg dL mg/dL/2 mgdL2 mgdL /2 2 (mg/dL)]/ 005 0 05 0.0 significant lowdensity low density LDL, LDL , (LDL) BMI (BMI) neutrophiltolymphocyte neutrophil lymphocyte (NLR values higher highdensity high (HDL p<0,05. p005 p p<0,05 (p<0,05) r= r (r 057 57 0.57 p<0.001. p0001 p<0.001 001 p<0.001) Additionally p<0.05. p<0.05 (p<0.05) ROC (ROC cutoff cut off 928 9 28 9.2 78 781 1 78.1 Area AUC (AUC) 0868 868 0.86 95 CI (CI) 0.8230.914. 08230914 0.823 0.914 823 914 0.823-0.914] (NCF mg/dL/ / (mg/dL)] 00 0. (LDL (BMI p00 p<0,0 (p<0,05 5 0.5 p000 p<0.00 p<0.0 (p<0.05 92 9. 7 78. (AUC 086 86 0.8 (CI 8230 0.8230.914 0823091 0823 0.82 0914 0.91 82 91 0.823-0.914 (mg/dL) p0 p<0, (p<0,0 p<0. (p<0.0 08 8 0.8230.91 082309 082 091 0.9 0.823-0.91 (mg/dL p<0 (p<0, (p<0. 0.8230.9 08230 09 0.823-0.9 p< (p<0 0.8230. 0.823-0. (p< 0.8230 0.823-0 (p 0.823-

Resumo Fundamento O fluxo lento coronariano (FLC) refere-se à opacificação retardada dos vasos distais na ausência de estenose da artéria coronária epicárdica. O mecanismo etiopatogênico do FLC ainda não está claro. Objetivos Este estudo investiga a relação entre o FLC e o índice de triglicerídeos-glicose (TyG). Métodos A amostra do estudo consistiu de 118 pacientes com FLC e 105 pacientes com fluxo coronariano normal (FCN). A taxa de fluxo coronariano foi medida por medio do método de contagem de quadros (TFC) Thrombolysis in Myocardial Infarction (TIMI) em todos os pacientes. O índice TyG foi calculado como o logaritmo do valor [triglicerídeos em jejum (mg/dL)×glicose em jejum (mg/dL)]/2. Adotou-se como estatisticamente significativo o nível de significância < 0,05. Resultados O índice TyG, lipoproteína de baixa densidade (LDL), índice de massa corporal (IMC), relação neutrófilo-linfócito (RNL) e valores de TFC, proporção masculina e proporção de fumantes foram maiores, enquanto os níveis de lipoproteína de alta densidade (HDL) foram significativamente menores no grupo FLC em comparação com o grupo FNC (p<0,05). A análise de correlação revelou que o FLC estava significativamente correlacionado com os valores do índice TyG, IMC, RNL e HDL. A mais forte dessas correlações foi entre o FLC e o índice TyG (r= 0,57, p<0,001). Além disso, a análise multivariada revelou que o índice TyG, IMC, razão RNL e sexo masculino foram preditores independentes para FLC (p<0,05). A análise da curva ROC (Receiver Operating Characteristic) indicou que um valor de corte ≥ 9,28 para o índice TyG previu FLC com sensibilidade de 78% e especificidade de 78,1% [Área sob a curva (AUC): 0,868 e 95% intervalo de confiança (IC): 0,823-0,914]. Conclusão Os achados deste estudo revelaram uma relação muito forte entre o FLC e o índice TyG. (FLC referese refere se epicárdica claro triglicerídeosglicose triglicerídeos glicose . (TyG) 11 10 FCN. FCN (FCN) TFC (TFC TIMI (TIMI mg/dL×glicose mgdLglicose mg/dL ×glicose mg dL mg/dL/2. mgdL2 mgdL /2. 2 (mg/dL)]/2 Adotouse Adotou 005 0 05 0,05 LDL, LDL , (LDL) IMC (IMC) neutrófilolinfócito neutrófilo linfócito (RNL maiores HDL (HDL p<0,05. p005 p p<0,05 (p<0,05) r= r (r 057 57 0,57 p<0,001. p0001 p<0,001 001 p<0,001) disso Receiver Characteristic 928 9 28 9,2 78 781 1 78,1 Área AUC (AUC) 0868 868 0,86 95 IC (IC) 0,8230,914. 08230914 0,823 0,914 823 914 0,823-0,914] (TyG (FCN mg/dL/2 /2 (mg/dL)]/ 00 0,0 (LDL (IMC p00 p<0,0 (p<0,05 5 0,5 p000 p<0,00 92 9, 7 78, (AUC 086 86 0,8 (IC 8230 0,8230,914 0823091 0823 0,82 0914 0,91 82 91 0,823-0,914 mg/dL/ / (mg/dL)] 0, p0 p<0, (p<0,0 08 8 0,8230,91 082309 082 091 0,9 0,823-0,91 (mg/dL) p<0 (p<0, 0,8230,9 08230 09 0,823-0,9 (mg/dL p< (p<0 0,8230, 0,823-0, (p< 0,8230 0,823-0 (p 0,823-

Abstract Background The diagnosis of acute myocarditis is usually made with clinical and laboratory parameters. This can sometimes be mixed up with diseases that have similar clinical features, making the diagnosis difficult. Therefore, the use of more specific biomarkers, in addition to the classically used biomarkers such as troponin, will accelerate the diagnosis. In addition, these biomarkers may help us to understand the mechanism of myocarditis development and thus predict unpredictable clinical outcomes. Objective This study aims to reveal the possible relationship between intestinal permeability and acute myocarditis. Methods In this study, we wanted to evaluate serum levels of zonulin and presepsin in 138 consecutive subjects, including 68 patients with myocarditis and another 70 as the control group, matched for age, gender, and cardiovascular risk factors. P-values <0.05 were considered to be statistically significant. Results Compared to the control group, zonulin and presepsin were significantly higher in the patient group with myocarditis (p < 0.001, for all). Zonulin levels were positively correlated with presepsin, peak CK-MB, and peak troponin levels (r = 0.461, p < 0.001; r = 0.744, p < 0.001; r = 0.627, p < 0.001; respectively). In regression analysis, presepsin and zonulin were determined as independent predictors for myocarditis (OR 1.002, 95% CI 1.001-1.003, p = 0.025; OR 12.331, 95% CI 4.261-35.689; p < 0.001; respectively). The predictive value of acute myocarditis of presepsin and zonulin in ROC curve analysis was statistically significant (p < 0.001, for both). Conclusion This study showed that zonulin and presepsin could be biomarkers that can be used in the diagnosis of myocarditis, and they can also be therapeutic targets by shedding light on the developmental mechanism of myocarditis. parameters features difficult Therefore outcomes 13 subjects 6 7 age gender factors Pvalues P values 005 0 05 <0.0 0001 001 0.001 all. all . all) CKMB, CKMB CK MB, MB CK-MB 0461 461 0.461 0744 744 0.744 0627 627 0.627 respectively. respectively respectively) 1002 1 002 1.002 95 1.0011.003, 10011003 1.001 1.003, 003 1.001-1.003 0.025 0025 025 12331 12 331 12.331 4.26135.689 426135689 4.261 35.689 4 261 35 689 4.261-35.689 both. both both) 00 <0. 000 0.00 046 46 0.46 074 74 0.74 062 62 0.62 100 1.00 9 0011 1.0011.003 1001100 1001 1003 1.003 1.001-1.00 0.02 02 1233 33 12.33 26135 4.26135.68 42613568 4261 4.26 35689 35.68 26 3 4.261-35.68 <0 0.0 04 0.4 07 0.7 06 0.6 10 1.0 1.0011.00 100110 1.001-1.0 123 12.3 2613 4.26135.6 4261356 426 4.2 3568 35.6 2 4.261-35.6 0. 1. 1.0011.0 10011 1.001-1. 12. 4.26135. 426135 42 4. 356 35. 4.261-35. 1.0011. 1.001-1 4.26135 42613 4.261-35 1.0011 1.001- 4.2613 4.261-3 4.261-

Resumo Fundamento O diagnóstico de miocardite aguda geralmente é feito diante de parâmetros clínicos e laboratoriais, podendo, por vezes, ser confundido com doenças que compartilham de características clínicas semelhantes, o que dificulta o diagnóstico. Sendo assim, o uso de biomarcadores mais específicos, para além dos clássicos como a troponina, acelerará o diagnóstico. Além disso, esses biomarcadores podem nos ajudar a compreender melhor o mecanismo de desenvolvimento da miocardite e, assim, prever resultados clínicos imprevisíveis. Objetivo Este estudo tem como objetivo revelar a possível relação entre permeabilidade intestinal e miocardite aguda. Métodos Neste estudo, buscamos avaliar os níveis séricos de zonulina e presepsina em 138 indivíduos consecutivos, incluindo 68 pacientes com miocardite e outros 70 usados como grupo controle, pareados por idade, sexo e fatores de risco cardiovascular. Valores de p < 0,05 foram considerados estatisticamente significativos. Resultados Em comparação com o grupo controle, zonulina e presepsina foram significativamente maiores no grupo de pacientes com miocardite (p < 0,001, para todos). Os níveis de zonulina foram positivamente correlacionados com presepsina, pico de CK-MB e níveis máximos de troponina (r = 0,461, p < 0,001; r = 0,744, p < 0,001; r = 0,627, p < 0,001; respectivamente). Na análise de regressão, presepsina e zonulina foram determinadas como preditores independentes para miocardite (OR de 1,002, IC de 95% 1,001-1,003, p = 0,025; OR de 12,331, IC de 95% 4,261-35,689; p < 0,001; respectivamente). O valor preditivo de miocardite aguda de presepsina e zonulina na análise da curva ROC foi estatisticamente significativo (p < 0,001, para ambos). Conclusão Este estudo mostrou que a zonulina e a presepsina podem ser biomarcadores para o diagnóstico de miocardite e também podem ser alvos terapêuticos para esclarecer o mecanismo de desenvolvimento da miocardite. laboratoriais podendo vezes semelhantes assim específicos disso imprevisíveis 13 consecutivos 6 7 controle idade cardiovascular 005 0 05 0,0 significativos 0001 001 0,001 todos. todos . todos) CKMB CK MB 0461 461 0,461 0744 744 0,744 0627 627 0,627 respectivamente. respectivamente respectivamente) regressão 1002 1 002 1,002 95 1,0011,003, 10011003 1,001 1,003, 003 1,001-1,003 0,025 0025 025 12331 12 331 12,331 4,26135,689 426135689 4,261 35,689 4 261 35 689 4,261-35,689 ambos. ambos ambos) 00 0, 000 0,00 046 46 0,46 074 74 0,74 062 62 0,62 100 1,00 9 0011 1,0011,003 1001100 1001 1003 1,003 1,001-1,00 0,02 02 1233 33 12,33 26135 4,26135,68 42613568 4261 4,26 35689 35,68 26 3 4,261-35,68 04 0,4 07 0,7 06 0,6 10 1,0 1,0011,00 100110 1,001-1,0 123 12,3 2613 4,26135,6 4261356 426 4,2 3568 35,6 2 4,261-35,6 1, 1,0011,0 10011 1,001-1, 12, 4,26135, 426135 42 4, 356 35, 4,261-35, 1,0011, 1,001-1 4,26135 42613 4,261-35 1,0011 1,001- 4,2613 4,261-3 4,261-

Abstract Background Correct TIMI frame count (CTFC), myocardial blush grade (MBG), and ST-segment resolution (STR) are parameters used to evaluate reperfusion at the microvascular level in patients that have undergone primary percutaneous coronary intervention (pPCI). Fibrinogen-to-albumin ratio (FAR) has been associated with thrombotic events in patients with ST-elevation myocardial infarction (STEMI) and chronic venous insufficiency. Objectives To investigate the relationship of FAR with CTFC, MBG, and STR. Methods: The study included 167 consecutive patients who underwent successful pPCI for STEMI and achieved TIMI-3 flow. The cases were divided into two groups, high (>0.0765) and low FAR (≤0.0765), according to the cut-off value of this parameter in the receiver operator characteristic analysis (ROC). STR, CTFC, and MBG were used to evaluate myocardial reperfusion. P values<0.05 were considered statistically significant. Results CTFC value, SYNTAX score, neutrophil/lymphocyte ratio, low-density lipoprotein, glucose, and peak cTnT were significantly higher, whereas STR, MBG, and LVEF were lower in the high FAR group. Spearman’s correlation analysis revealed a significant relationship between the FAR and STR (r=-0.666, p<0.001), MBG (-0.523, p<0.001), and CTFC (r=0.731, p≤0.001). According to the logistic regression analysis, FAR, glucose, peak cTnT, and pain to balloon time were the most important independent predictors of MBG 0/1, CTFC>28, and STR<50%).ROC analysis revealed that the cut-off value of FAR≥0.0765 was a predictor of incomplete STR with a sensitivity of 71.9 % and a specificity of 69.8 %, MBG0/1 with a sensitivity of 72.6 % and a specificity of 68.6 %, and CTFC >28 with a sensitivity of 76 % and a specificity of 65.8 %. Conclusions FAR is an important independent predictor of microvascular perfusion in patients undergoing pPCI for STEMI. , (CTFC) (MBG) STsegment ST segment (STR pPCI. . (pPCI) Fibrinogentoalbumin Fibrinogen albumin (FAR STelevation elevation (STEMI insufficiency Methods 16 TIMI3 3 TIMI- flow groups >0.0765 00765 0 0765 (>0.0765 ≤0.0765, ≤0.0765 (≤0.0765) cutoff cut off ROC. ROC (ROC) values005 values 05 values<0.0 score neutrophillymphocyte neutrophil lymphocyte lowdensity density lipoprotein glucose higher group Spearmans Spearman s r=0.666, r0666 r r= 0.666, 666 (r=-0.666 p<0.001, p0001 p p<0.001 001 p<0.001) 0.523, 0523 523 (-0.523 r=0.731, r0731 731 (r=0.731 p≤0.001. p≤0.001 p≤0.001) 01 1 0/1 CTFC28 28 CTFC>28 STR<50%.ROC STR50ROC STRROC STR<50% .ROC 50 FAR00765 FAR≥0.076 719 71 9 71. 698 69 8 69. MBG01 MBG0 MBG0/ 726 72 6 72. 686 68 68. >2 7 658 65 65. (CTFC (MBG (pPCI >0.076 0076 076 (>0.076 ≤0.076 (≤0.0765 (ROC values00 values<0. r=0.666 r066 0666 0.666 66 (r=-0.66 p000 p<0.00 00 0.523 052 52 (-0.52 r=0.731 r073 73 (r=0.73 p≤0.00 0/ CTFC2 2 CTFC>2 STR50 STR<50 5 FAR0076 FAR≥0.07 > >0.07 007 07 (>0.07 ≤0.07 (≤0.076 values0 values<0 r=0.66 r06 066 0.66 (r=-0.6 p00 p<0.0 0.52 (-0.5 r=0.73 r07 (r=0.7 p≤0.0 CTFC> STR5 STR<5 FAR007 FAR≥0.0 >0.0 (>0.0 ≤0.0 (≤0.07 values< r=0.6 r0 06 0.6 (r=-0. p0 p<0. 0.5 (-0. r=0.7 (r=0. p≤0. STR< FAR00 FAR≥0. >0. (>0. ≤0. (≤0.0 r=0. 0. (r=-0 p<0 (-0 (r=0 p≤0 FAR0 FAR≥0 >0 (>0 ≤0 (≤0. r=0 (r=- p< (- (r= p≤ FAR≥ (> ≤ (≤0 ( (r (≤

Resumo Fundamento A contagem corrigida de quadros TIMI (CTFC), o grau de blush miocárdico (MBG) e a resolução do segmento ST (STR) são parâmetros utilizados para avaliar a reperfusão em nível microvascular em pacientes submetidos à intervenção coronária percutânea primária (ICPp). A relação fibrinogênio/albumina (FAR) tem sido associada a eventos trombóticos em pacientes com infarto do miocárdio com elevação do segmento ST (IAMCSST) e insuficiência venosa crônica. Objetivos Investigar a relação do FAR com CTFC, MBG e STR.Métodos: O estudo incluiu 167 pacientes consecutivos que foram submetidos a ICPp com sucesso para IAMCSST e alcançaram fluxo TIMI-3. Os casos foram divididos em dois grupos, FAR alto (> 0,0765) e FAR baixo (≤ 0,0765), de acordo com o valor de corte desse parâmetro na análise característica do operador do receptor (ROC). STR, CTFC e MBG foram utilizados para avaliar a reperfusão miocárdica. Valores de p<0,05 foram considerados estatisticamente significativos. Resultados O valor CTFC, escore SYNTAX, relação neutrófilos/linfócitos, lipoproteína de baixa densidade, glicose e pico de cTnT foram significativamente maiores, enquanto STR, MBG e FEVE foram menores no grupo FAR alto. A análise de correlação de Spearman revelou relação significativa entre FAR e STR (r=-0,666, p<0,001), MBG (-0,523, p<0,001) e CTFC (r=0,731, p≤0,001). De acordo com a análise de regressão logística, FAR, glicose, pico de cTnT e dor até o tempo de Balão foram os preditores independentes mais importantes de MBG 0/1, CTFC>28 e STR<50%). A análise ROC revelou que o ponto de corte o valor de FAR≥0,0765 foi preditor de STR incompleto com sensibilidade de 71,9% e especificidade de 69,8%, MBG0/1 com sensibilidade de 72,6% e especificidade de 68,6%, e CTFC>28 com sensibilidade de 76% e uma especificidade de 65,8%. Conclusões A FAR é um importante preditor independente de perfusão microvascular em pacientes submetidos a ICPp por IAMCSST. , (CTFC) (MBG (STR ICPp. . (ICPp) fibrinogênioalbumina fibrinogênio albumina (FAR (IAMCSST crônica STR.Métodos STRMétodos Métodos 16 TIMI3. TIMI3 3. 3 TIMI-3 grupos > ( 0,0765 00765 0 0765 ≤ 0,0765, ROC. (ROC) miocárdica p005 p 05 p<0,0 significativos SYNTAX neutrófiloslinfócitos neutrófilos linfócitos neutrófilos/linfócitos densidade maiores r=0,666, r0666 r r= 0,666, 666 (r=-0,666 p<0,001, p0001 p<0,001 001 0,523, 0523 523 (-0,523 r=0,731, r0731 731 (r=0,731 p≤0,001. p≤0,001 p≤0,001) logística 01 1 0/1 CTFC28 28 CTFC>2 STR<50%. STR50 STR<50% 50 STR<50%) FAR00765 FAR≥0,076 719 71 9 71,9 698 69 8 69,8% MBG01 MBG0 MBG0/ 726 72 6 72,6 686 68 68,6% 76 658 65 65,8% (CTFC (ICPp TIMI- 0,076 0076 076 (ROC p00 p<0, r=0,666 r066 0666 0,666 66 (r=-0,66 p000 p<0,00 00 0,523 052 52 (-0,52 r=0,731 r073 73 (r=0,73 p≤0,00 0/ CTFC2 2 CTFC> STR5 STR<50 5 FAR0076 FAR≥0,07 7 71, 69,8 72, 68,6 65,8 0,07 007 07 p0 p<0 r=0,66 r06 066 0,66 (r=-0,6 0,52 (-0,5 r=0,73 r07 (r=0,7 p≤0,0 STR<5 FAR007 FAR≥0,0 69, 68, 65, 0,0 p< r=0,6 r0 06 0,6 (r=-0, 0,5 (-0, r=0,7 (r=0, p≤0, STR< FAR00 FAR≥0, 0, r=0, (r=-0 (-0 (r=0 p≤0 FAR0 FAR≥0 r=0 (r=- (- (r= p≤ FAR≥ (r