| Literature DB >> 29769031 |
Tejas P Singh1,2,3, Joseph V Moxon1, Genevieve N Healy3, Yvonne Cadet-James4, Jonathan Golledge5,6.
Abstract
BACKGROUND: The risk factors for peripheral artery disease (PAD) are more common in Indigenous than non-Indigenous Australians, however the presentation and outcome of PAD in Indigenous Australians has not been previously investigated. The aim of this prospective cohort study was to compare the presenting characteristics and clinical outcome of Indigenous and non-Indigenous Australians with PAD.Entities:
Mesh:
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Year: 2018 PMID: 29769031 PMCID: PMC5956730 DOI: 10.1186/s12872-018-0835-z
Source DB: PubMed Journal: BMC Cardiovasc Disord ISSN: 1471-2261 Impact factor: 2.298
Demographic and risk factors of included PAD patients
| Characteristics | Indigenous ( | Non-Indigenous ( | |
|---|---|---|---|
| Age (y) | 63.3 (54.7–67.8) | 69.6 (63.3–75.4) |
|
| Sex (% Males) | 10 (62.5%) | 293 (76.1%) | 0.215 |
| Diabetes mellitus | 7 (43.8%) | 103 (26.8%) | 0.135 |
| Smoker |
| ||
| Never | 0 (0%) | 82 (21.3%) | |
| Current | 9 (56.3%) | 121 (31.4%) | |
| Previous | 7 (43.8%) | 182 (47.3%) | |
| Hypertension | 15 (93.8%) | 290 (75.3%) | 0.091 |
| IHD | 10 (62.5%) | 164 (42.6%) | 0.116 |
| Stroke | 1 (6.3%) | 38 (9.9%) | 0.632 |
| eGFR (mL/min/1.73m2) | 79.0 (46.5–85.8) [2]a | 78 (60.0–91.0) [93]a | 0.416 |
| Medications | |||
| Aspirin | 11 (68.88%) | 252 (65.5%) | 0.786 |
| Other antiplatelet | 3 (18.8%) | 66 (17.1%) | 0.867 |
| Frusemide | 4 (25.0%) | 28 (7.3%) |
|
| ACEI | 10 (62.5%) | 152 (39.5%) | 0.066 |
| Beta-Blocker | 6 (37.5%) | 115 (29.9%) | 0.515 |
| Calcium channel blocker | 3 (18.8%) | 115 (29.9%) | 0.339 |
| Metformin | 4 (25.0%) | 69 (17.9%) | 0.472 |
| Insulin | 3 (18.8%) | 20 (5.2%) |
|
| Statin | 13 (81.3%) | 273 (70.9%) | 0.370 |
IHD ischaemic heart disease, eGFR estimated glomerular filtration rate, ACEI angiotensin converting enzyme inhibitor, ARB angiotensin receptor blocker
aRepresents the number of missing data-points. Continuous data are presented as median [interquartile range] and were compared using Mann-Whitney U test. Nominal data are presented as number (%) and were compared using Pearson’s χ2 test. P-values highlighted in bold indicate significant differences
Presenting complaint at entry for Indigenous and non-Indigenous patients
| Characteristics | Indigenous | Non-Indigenous | |
|---|---|---|---|
| Presentationa | 0.385 | ||
| Intermittent Claudication | 8 (50.0%) | 126 (32.7%) | |
| Critical Limb Ischemia | 2 (12.5%) | 24 (6.2%) | |
| Abdominal Aortic or peripheral aneurysm | 3 (18.8%) | 142 (36.9%) | |
| Asymptomatic carotid stenosis | 2 (12.5%) | 46 (11.9%) | |
| Symptomatic carotid stenosis | 1 (6.2%) | 47 (12.2%) |
aIndicates predominant presentation. Some patients had both lower limb symptoms and abdominal aortic aneurysm
Fig. 1Kaplan-Meier curve illustrating the cumulative proportion of Indigenous and non-Indigenous patients with PAD, who had a major cardiovascular event (MI or stroke or death). CV, cardiovascular. Differences between both groups compared using the log-rank test (p = 0.004). The green line represents patients who were Indigenous, and the pink line represents non-Indigenous Australians. Vertical lines represent participants who were censored during follow-up
Cox proportional hazard analyses for the association between Indigenous ethnicity and combined incidence of major cardiovascular events (MI, stroke or death) in PAD patients
| Unadjusted HR (95%CI) | Adjusted HR (95%CI) | |||
|---|---|---|---|---|
| MI, stroke or death | ||||
| Non-Indigenous | 1.00 |
| 1.00 |
|
| Indigenous | 3.59 (1.42–9.07) | 0.007 | 3.12 (1.14–8.49) | 0.026 a |
| – | – | 4.03 (1.17–13.84) | 0.027 b | |
| – | – | 4.72 (1.41–15.78) | 0.012 c | |
MI myocardial infarction, CI confidence interval, HR hazard ratio, IHD ischemic heart disease, ACE angiotensin converting enzyme
aResults are adjusted for hypertension, current smoking, diabetes, IHD, and age
bResults are adjusted for hypertension, current smoking, diabetes, IHD, age, insulin and frusemide prescription
cResults are adjusted for hypertension, current smoking, diabetes, IHD, age, insulin, frusemide, ACE inhibitor, anti-platelet or anti-coagulant prescription and critical limb ischemia