| Literature DB >> 35155608 |
Sang Heon Suh1, Tae Ryom Oh1, Hong Sang Choi1, Chang Seong Kim1, Eun Hui Bae1, Kook-Hwan Oh2, Kyu-Beck Lee3, Seung Hyeok Han4, Suah Sung5, Seong Kwon Ma1, Soo Wan Kim1.
Abstract
BACKGROUND: We investigated whether high body weight variability (BWV) is associated with a higher prevalence of coronary artery calcification (CAC) or more rapid progression of CAC in patients with predialysis chronic kidney disease (CKD).Entities:
Keywords: body weigh variability; cardiovascular disease; cardiovascular event; chronic kidney disease; coronary artery calcification
Year: 2022 PMID: 35155608 PMCID: PMC8826058 DOI: 10.3389/fcvm.2021.794957
Source DB: PubMed Journal: Front Cardiovasc Med ISSN: 2297-055X
Figure 1Flow diagram of the study participants. ASV, average successive variability; BW, body weight; CACS, coronary artery calcium score; T1, 1st tertile; T2, 2nd tertile; T3, 3rd tertile.
Baseline characteristics of study participants in the tertile by BWV.
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| Follow-up duration (year) | 6.466 ± 1.450 | 6.569 ± 1.413 | 6.466 ± 1.450 | 0.594 |
| CACS (AU) | 0.804 | |||
| 0 | 216 (55.8) | 198 (51.2) | 204 (52.6) | |
| 0 <, ≤ 400 | 178 (38.2) | 157 (40.6) | 155 (39.9) | |
| 400 <, ≤ 1000 | 14 (3.6) | 22 (5.7) | 20 (5.2) | |
| 1,000 < | 9 (2.3) | 10 (2.6) | 9 (2.3) | |
| Age (year) | 54.065 ± 10.334 | 53.390 ± 11.171 | 50.353 ± 13.246 | <0.001 |
| Male | 208 (53.7) | 229 (59.2) | 253 (65.2) | 0.005 |
| Charlson comorbidity index | 0.007 | |||
| 0–3 | 340 (87.9) | 312 (80.6) | 304 (78.4) | |
| 4–5 | 44 (11.4) | 73 (18.9) | 81 (20.9) | |
| 6–7 | 3 (0.8) | 2 (0.5) | 3 (0.8) | |
| DM | 72 (18.6) | 107 (27.6) | 121 (31.2) | 0.001 |
| CAD | 2 (0.5) | 9 (2.3) | 10 (2.6) | 0.162 |
| Arrhythmia | 8 (2.1) | 3 (0.8) | 4 (1.0) | 0.426 |
| Medication | ||||
| ACEi/ARBs | 336 (86.8) | 344 (88.9) | 327 (84.3) | 0.167 |
| Diuretics | 91 (23.5) | 91 (23.5) | 108 (27.8) | 0.276 |
| Number of anti-HTN drugs ≥ 3 | 78 (20.2) | 81 (20.9) | 111 (28.6) | 0.009 |
| Statins | 204 (52.7) | 192 (49.6) | 186 (47.9) | 0.403 |
| BMI (kg/m2) | 23.788 ± 2.2924 | 24.363 ± 3.058 | 25.616 ± 3.746 | <0.001 |
| SBP (mmHg) | 125.295 ± 14.014 | 125.645 ± 14.326 | 126.894 ± 15.551 | 0.279 |
| DBP (mmHg) | 77.220 ± 9.984 | 76.259 ± 10.358 | 77.090 ± 10.766 | 0.377 |
| Laboratory findings | ||||
| Hemoglobin (g/dl) | 13.261 ± 1.664 | 13.414 ± 1.887 | 13.408 ± 1.946 | 0.429 |
| Albumin (g/dl) | 4.226 ± 0.333 | 4.273 ± 0.335 | 4.296 ± 0.363 | 0.016 |
| Total cholesterol (mg/dl) | 174.434 ± 35.000 | 174.179 ± 36.672 | 175.917 ± 35.720 | 0.768 |
| HDL-C (mg/dl) | 52.278 ± 15.914 | 51.237 ± 15.047 | 48.970 ± 14.017 | 0.008 |
| LDL-C (mg/dl) | 95.937 ± 29.055 | 96.560 ± 30.792 | 98.829 ± 30.224 | 0.375 |
| TG (mg/dl) | 142.621 ± 91.443 | 151.832 ± 91.224 | 162.992 ± 101.510 | 0.013 |
| Fasting glucose (mg/dl) | 102.632 ± 25.048 | 109.135 ± 33.699 | 108.190 ± 31.623 | 0.006 |
| 25(OH) vitamin D | 18.835 ± 7.286 | 18.854 ± 7.712 | 17.180 ± 6.765 | 0.001 |
| hsCRP (mg/dl) | 0.600 [0.200, 1.400] | 0.510 [0.200, 1.400] | 0.700 [0.200, 1.900] | 0.809 |
| Spot urine ACR (mg/gCr) | 245.079 [42.450, 616.708] | 217.470 [34.877, 597.054] | 241.744 [56.312, 625.118] | 0.623 |
| eGFR (ml/min./1.73 m2) | 57.441 ± 27.405 | 59.227 ± 28.337 | 61.375 ± 30.714 | 0.165 |
| CKD stages | 0.167 | |||
| Stage 1 | 72 (18.6) | 79 (20.4) | 100 (25.8) | |
| Stage 2 | 96 (24.8) | 101 (26.1) | 97 (25.0) | |
| Stage 3a | 84 (21.7) | 78 (20.2) | 63 (16.2) | |
| Stage 3b | 91 (23.5) | 88 (22.7) | 79 (20.4) | |
| Stage 4 | 41 (10.6) | 41 (10.6) | 44 (11.3) | |
| Stage 5 | 3 (0.8) | 0 (0.0) | 5 (1.3) | |
Values for categorical variables are given as number (percentage); values for continuous variables, as mean ± SD or median (interquartile range).
ACEi, angiotensin-converting enzyme inhibitor; ACR, albumin-to-creatinine ratio; ARB, angiotensin receptor blocker; AU, Agatston unit; BMI, body mass index; BWV, body weight variability; CACS, coronary artery calcium score; CAD, coronary artery disease; CKD, chronic kidney disease; Cr, creatinine; DBP, diastolic blood pressure; DM, diabetes mellitus; eGFR, estimated glomerular filtration rate; HDL-C, high density lipoprotein cholesterol; hs-CRP, high-sensitivity C-reactive protein; HTN, hypertension; LDL-C, low-density lipoprotein cholesterol; SBP, systolic blood pressure; T1, 1st tertile; T2, 2nd tertile; T3, 3rd tertile; TG, triglyceride; 25(OH) vitamin D, 25-hydroxyvitamin D.
Figure 2Comparison of the CACS at the baseline and at 4-year follow-up and the CACS change during 4-year follow-up period by BWV. CACS at the baseline (A) and at 4-year follow-up (B) and the CACS change during the 4-year follow-up period (C) were compared by BWV. *P < 0.05 vs. T1 by one-way ANOVA with Scheffe's post-hoc test. Error bars indicate SE of means. AU, Agatston unit; BWV, body weight variability; CACS, coronary artery calcium score; T1, 1st tertile; T2, 2nd tertile; T3, 3rd tertile.
Binary logistic regression of BWV for rapid progression of CAC.
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| BWV, T1 | Reference | Reference | ||
| BWV, T2 | 2.021 (1.194, 3.422) | 0.009 | 2.118 (1.075, 4.175) | 0.030 |
| BWV, T3 | 2.121 (1.259, 3.572) | 0.005 | 2.602 (1.304, 5.191) | 0.007 |
Models were adjusted for age, gender, Charlson comorbidity index, smoking history, BMI, SBP, DBP, medication (ACEi/ARBs, diuretics, number of antihypertensive drugs, statins), hemoglobin, albumin, HDL-C, fasting serum glucose, 25(OH) vitamin D, hs-CRP, eGFR, spot urine ACR, and baseline CACS.
BWV, body weight variability; OR, odds ratio; T1, 1st tertile; T2, 2nd tertile; T3, 3rd tertile.
Figure 3The restricted cubic spline of BWV on the risk of rapid progression of CAC. Adjusted OR of BWV as a continuous variable for the risk of rapid progression of CAC is depicted. The model was adjusted for age, gender, Charlson comorbidity index, smoking history, BMI, SBP, DBP, medication (ACEi/ARBs, diuretics, number of antihypertensive drugs, statins), hemoglobin, albumin, HDL-C, fasting serum glucose, 25(OH) vitamin D, hs-CRP, eGFR, spot urine ACR, and baseline CACS. BWV, body weight variability; OR, odds ratio.
Binary logistic regression of BWV for rapid progression of CAC in subjects with BW maintenance during follow-up periods.
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| BWV, T1 | Reference | Reference | ||
| BWV, T2 | 1.925 (1.130, 3.280) | 0.016 | 2.007 (1.011, 3.984) | 0.046 |
| BWV, T3 | 1.910 (1.110, 3.287) | 0.019 | 2.054 (1.003, 4.207) | 0.049 |
Models were adjusted for age, gender, Charlson comorbidity index, smoking history, BMI, SBP, DBP, medication (ACEi/ARBs, diuretics, number of antihypertensive drugs, statins), hemoglobin, albumin, HDL-C, fasting serum glucose, 25(OH) vitamin D, hs-CRP, eGFR, spot urine ACR, and baseline CACS.
BWV, body weight variability; OR, odds ratio; T1, 1st tertile; T2, 2nd tertile; T3, 3rd tertile.
Binary logistic regression of BWV for rapid progression of CAC in various subgroups.
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| Age <60 years | BWV, T1 | Reference | 0.172 | Reference | 0.176 |
| BWV, T2 | 1.461 (0.663, 3.220) | 1.224 (0.330, 4.533) | |||
| BWV, T3 | 1.400 (0.642, 3.053) | 1.445 (0.347, 6.007) | |||
| Age ≥ 60 years | BWV, T1 | Reference | Reference | ||
| BWV, T2 | 2.676 (1.283, 5.578) | 3.167 (1.237, 8.104) | |||
| BWV, T3 | 3.696 (1.767, 7.730) | 4.462 (1.729, 11.517) | |||
| Male | BWV, T1 | Reference | 0.435 | Reference | 0.719 |
| BWV, T2 | 1.674 (0.918, 3.055) | 2.193 (0.996, 4.830) | |||
| BWV, T3 | 1.590 (0.880, 2.871) | 2.395 (1.068, 5.371) | |||
| Female | BWV, T1 | Reference | Reference | ||
| BWV, T2 | 3.184 (0.991, 10.235) | 2.428 (0.293, 20.118) | |||
| BWV, T3 | 3.748 (1.163, 12.073) | 10.033 (1.088, 92.508) | |||
| Charlson comorbidity index ≤ 3 | BWV, T1 | Reference | 0.858 | Reference | 0.582 |
| BWV, T2 | 0.812 (0.297, 2.221) | 1.091 (0.223, 5.343) | |||
| BWV, T3 | 0.767 (0.281, 2.097) | 1.906 (0.396, 9.163) | |||
| Charlson comorbidity index ≥ 4 | BWV, T1 | Reference | Reference | ||
| BWV, T2 | 2.741 (1.400, 5.370) | 2.690 (1.181, 6.129) | |||
| BWV, T3 | 3.180 (1.629, 6.209) | 3.216 (1.384, 7.476) | |||
| DM (-) | BWV, T1 | Reference | 0.877 | Reference | 0.459 |
| BWV, T2 | 1.316 (0.579, 2.995) | 1.709 (0.527, 5.538) | |||
| BWV, T3 | 1.345 (0.591, 3.060) | 1.786 (0.521, 6.128) | |||
| DM (+) | BWV, T1 | Reference | Reference | ||
| BWV, T2 | 1.990 (0.933, 4.246) | 2.235 (0.868, 5.756) | |||
| BWV, T3 | 1.894 (0.898, 3.994) | 2.398 (0.928, 6.194) | |||
| eGFR ≥ 45 ml/min./1.73 m2 | BWV, T1 | Reference | 0.743 | Reference | 0.970 |
| BWV, T2 | 1.742 (0.836, 3.631) | 1.730 (0.687, 4.359) | |||
| BWV, T3 | 2.106 (1.036, 4.284) | 2.513 (0.985, 6.411) | |||
| eGFR <45 ml/min./1.73 m2 | BWV, T1 | Reference | Reference | ||
| BWV, T2 | 2.440 (1.134, 5.251) | 3.071 (1.022, 9.225) | |||
| BWV, T3 | 2.237 (1.029, 4.859) | 2.769 (0.895, 8.568) | |||
| Spot urine ACR <300 mg/g | BWV, T1 | Reference | 0.081 | Reference | 0.151 |
| BWV, T2 | 1.011 (0.469, 2.180) | 1.245 (0.461, 3.365) | |||
| BWV, T3 | 1.604 (0.791, 3.254) | 2.461 (0.911, 6.652) | |||
| Spot urine ACR ≥ 300 mg/g | BWV, T1 | Reference | Reference | ||
| BWV, T2 | 3.672 (1.679, 8.031) | 2.633 (0.928, 7.470) | |||
| BWV, T3 | 2.846 (1.289, 6.282) | 2.606 (0.895, 7.589) |
Models were adjusted for age, gender, Charlson comorbidity index, smoking history, BMI, SBP, DBP, medication (ACEi/ARBs, diuretics, number of antihypertensive drugs, statins), hemoglobin, albumin, HDL-C, fasting serum glucose, 25(OH) vitamin D, hs-CRP, eGFR, spot urine ACR, and baseline CACS.
ACR, albumin-to-creatinine ratio; BMI, body mass index; DM, diabetes mellitus; eGFR, estimated glomerular filtration rate, OR, odd ratio; T1, 1st tertile; T2, 2nd tertile; T3, 3rd tertile.