| Literature DB >> 25780780 |
Ghanshyam Palamaner Subash Shantha1, Anita Ashok Kumar1, Mansha Sethi2, Rohit C Khanna3, Samir Bipin Pancholy4.
Abstract
Background. Low molecular weight heparin (LMWH) is an effective anti-coagulant for thrombotic events. However, due to its predominant renal clearance, there are concerns that it might be associated with increased bleeding in patients with renal disease. Objectives. We systematically evaluated the efficacy and safety of LMWH compared to unfractionated heparin (UH) in end stage renal disease (ESRD) patients. Search Methods. Pubmed, Embase and cochrane central were searched for eligible citations. Selection Criteria. Randomized controlled trials, comparing LMWH and UH, involving adult (age > 18 years), ESRD patients receiving outpatient, chronic, intermittent hemodialysis were included. Data Collection and Analysis. Two independent reviewers performed independent data abstraction. I2 statistic was used to assess heterogeneity. Random effects model was used for meta-analysis. Results. Nineteen studies were included for systematic review and 4 were included for meta-analysis. There were no significant differences between LMWH and UFH for extracorporeal circuit thrombosis [risk ratio: 1 (95% CI [0.62-1.62])] and bleeding complications [risk ratio: 1.16 (95% CI [0.62-2.15])]. Conclusions. LMWH is as safe and effective as UFH. Considering the poor quality of studies included for the review, larger well conducted RCTs are required before conclusions can be drawn.Entities:
Keywords: Hemodialysis; Heparin; Meta-analysis; Thromboprophylaxis
Year: 2015 PMID: 25780780 PMCID: PMC4359121 DOI: 10.7717/peerj.835
Source DB: PubMed Journal: PeerJ ISSN: 2167-8359 Impact factor: 2.984
Figure 1Article flow diagram.
Details the process of study inclusion into the review
Characteristics of included studies.
Table details the characteristics of the studies included in the review.
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| 2004 | 1986 | 1997 | 2006 | 1995 | 1998 | 1986 | 2002 | 2004 | 2009 |
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| Parallel RCT | Crossover RCT | Crossover RCT | Crossover RCT | Parallel RCT | Crossover RCT | Crossover RCT | Crossover RCT | Crossover RCT | Parallel RCT |
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| 20 | 10 | 36 | 8 | 20 | 11 | 8 | 32 | 66 | 22 |
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| Enoxaparin | Dalteparin | Tinzaparin | Dalteparin | Dalteparin | LMWH not specified | Dalteparin | Tinzaparin | Tinzaparin | Enoxaparin |
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| Fixed | Fixed | Variable | Fixed | Fixed | Variable | Fixed | Variable | Variable | Fixed |
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| United States | Netherlands | Greece | Netherlands | Germany | France | United Kingdom | Canada | Romania | Poland |
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| Difficult to assess randomization groups for outcomes | Abstract-specific data not provided for circuit thrombosis | ||||||||
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| ADP-induced fibrinogen binding, platelet reactivity | Extracorporeal circuit thrombosis, bleeding complications, factor Xa levels, platelet function, beta-thromboglobulin, thromboxane A2, platelet factor 4, serotonin | Lipid profile (HDL, LDL, total cholesterol, apo A1, apo B, triglycerides, lipoprotein a), albumin, hemoglobin | Platelet factor 4, polymorphonuclear cells and platelet degranulation | Hep test, aPTT, thrombin clotting time | Plasma aldosterone, renin, aldosterone/renin ratio, serum potassium | Fibrinopeptide A, beta-thromboglobulin, kaolin cephalin clotting time, plasma heparin levels, bleeding time | Extracorporeal circuit thrombosis, bleeding complications, vascular compression time, patient/nurse satisfaction, relative cost, nursing time | Extracorporeal circuit thrombosis | Thrombomodulin, von-Willebrand factor, plasminogen activator inhibitor 1, cell surface adhesion molecule, e-selectin, intercellular adhesion molecule 1, prothrombin fragment 1 + 2 |
Patient characteristics (patients in studies that reported outcomes of interest).
Characteristics of patients in the included studies.
| Study, year (reference) | Mean age (yrs) ± SD | Excluded patients | Follow-up duration | Patients lost to follow-up | Patients ( | Frequency and duration of dialysis | Type of LMWH | Mean LMWH dose | Mean UFH dose | |
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| Other anticoagulants | Previous bleeding | |||||||||
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| 58.6 | No | NS | NS | 0/0 | 10 | 2-3/wk, 4 h | Dalteparin | (B) 18 IU/kg; | (B) 36 IU/kg; |
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| 68.5 | No | No | 24 weeks | 5 | 36 | 3–4/wk, 3–5 h | Enoxaparin | (B) 1 mg/kg; | (B) 50 IU/kg; |
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| 66.6 ± 14.8 | No | No | 8 weeks | 2 | 32 | 3/wk, 3.5–4 h | Tinzaparin | 4318 IU | (B) 50–75 IU/kg; |
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| 54 ± 15.2 (LMWH), | No | NS | 12 months | 8 | 70 (35/35) | NS, 4.5–5 h | Dalteparin | (B) 34 IU/kg; | (B) 62 IU/kg; |
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| 53.4 ± 19.9 (LMWH), | NS | NS | NS | NS | 20 (10/10) | 3–4 h, 4/wk | Dalteparin | (B) 1750 IU | (B) 2650 IU; |
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| NS | NS | NS | NS | NS | 66 | 3/wk, 4–5 h/session | Tinzaparin | 40 IU/kg | Mean dose 6262 |
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| 52.1 ± 17.2 | NS | NS | NS | NS | 20 | 3/wk, 4–5 h/session | Tinzaparin | (B) 34 IU/kg; | (B) 62 IU/kg; |
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| 55.2 ± 11.7 | NS | NS | NS | NS | 8 | 3/wk, 4–5 h/session | Dalteparin | NS | (B) 62 IU/kg; |
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| 57.1 ± 12.3 | NS | NS | NS | NS | 36 | NS | Tinzaparin | (B) 34 IU/kg; | NS |
Notes.
Not specified
Summary table for meta-analysis (extracorporeal circuit thrombosis).
Table detailing the event rates of comparison between LMWH and UH for extracorporeal circuit thrombosis.
| Study | LMWH | UFH | Risk ratio | 95% CI | ||
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| Events | No. of HD | Events | No. of HD | |||
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| 4 | 10 | 4 | 10 | 1.00 | 0.34–2.93 |
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| 80 | 5,045 | 69 | 5,197 | 1.19 | 0.87–1.64 |
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| 17 | 1,111 | 35 | 1,141 | 0.50 | 0.28–0.89 |
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| 32 | 378 | 21 | 382 | 1.54 | 0.90–2.62 |
| Total | 133 | 6,544 | 129 | 6,730 | 1.00 | 0.62–1.62 |
Figure 2Forest plots: extracorporeal circuit thrombosis.
Forest Plots comparing LMWH Vs UH for extracorporeal circuit thrombosis.
Summary table for meta-analysis (bleeding complications).
Table details the event rates comparison between LMWH and UH for bleeding complications.
| Study | LMWH | UFH | Risk ratio | 95% CI | ||
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| Events | No. of | Events | No. of | |||
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| 2 | 10 | 1 | 10 | 2.00 | 0.21–18.69 |
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| 19 | 35 | 16 | 35 | 1.19 | 0.74–1.90 |
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| 12 | 36 | 6 | 36 | 2.00 | 0.84–4.75 |
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| 3 | 32 | 8 | 32 | 0.38 | 0.11–1.29 |
| Total | 36 | 113 | 31 | 113 | 1.16 | 0.62–2.15 |
Figure 3Forest plots: bleeding complications.
Forest plots comparing LMWH Vs UH for bleeding complications.