| Literature DB >> 26403081 |
Katja-Nicole Adamik1, Emmanuelle Butty2, Judith Howard3.
Abstract
BACKGROUND: Hyperosmolar therapy, using either mannitol or hypertonic saline (HTS), is considered the treatment of choice for intracranial hypertension. However, hyperosmolar agents may impair coagulation and platelet function, limiting their use in patients at risk for hemorrhage. Despite this, studies evaluating the effects of mannitol compared to other hyperosmolar agents in dogs are largely lacking. The aim of this study was to compare the in vitro effects on global hemostasis and platelet function of 20% mannitol and 3% HTS on canine blood.Entities:
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Year: 2015 PMID: 26403081 PMCID: PMC4582639 DOI: 10.1186/s12917-015-0555-x
Source DB: PubMed Journal: BMC Vet Res ISSN: 1746-6148 Impact factor: 2.741
Thromboelastometry and platelet function analyses in undiluted blood samples and samples diluted with 0.9 % saline, 3 % hypertonic saline, and 20 % mannitol in a ratio of 1:16 and 1:8 in 15 dogs
| Variable | Baseline (undiluted) | 0.9 % NaCl (dilution 1:16) | 0.9 % NaCl (dilution 1:8) | 3 % HTS (dilution 1:16) | 3 % HTS (dilution 1:8) | 20 % mannitol (dilution 1:16) | 20 % mannitol (dilution 1:8) |
|---|---|---|---|---|---|---|---|
| PFA-100 | |||||||
| CtPFA (s) | 60 (51–88) | 73 (64–83) | 72 (68–81) | 77 (70–90) | 108 (84–126)*,** | 108 (89–132)* | 172 (124–300)*,**,*** |
| Ex-tem | |||||||
| CT (s) | 35 (28–55) | 38 (36–60) | 44 (31–62) | 37 (33–83) | 40 (34–48) | 51 (38–99)* | 90 (46–134)*,*** |
| CFT (s) | 149 (131–159) | 151 (128–184) | 151 (123–175) | 186 (148–206) | 196 (176–249)*,** | 204 (158–249)* | 252 (222–314)*,**,*** |
| MCF (mm) | 59 (55–62) | 56 (50–60) | 55 (53–57) | 54 (51–57) | 50 (46–53)*,** | 53 (51–56) | 49 (45–50)*,** |
| Fib-tem | |||||||
| CT (s) | 38 (30–43) | 41 (33–51) | 38 (32–47) | 36 (32–42) | 36 (32–43) | 54 (28–66) | 48 (38–58) |
| MCF (mm) | 8 (8–10) | 7 (5–9) | 7 (6–8) | 7 (6–9) | 7 (6–9) | 7 (4–9) | 5 (4–5)*,**,*** |
Values are presented as median (interquartile range) *significant difference (P < 0.05) compared with baseline; **significant difference (P < 0.05) compared with 0.9 % saline at the same dilution; ***significant difference (P > 0.05) compared with 3 % HTS at the same dilution. Ct closure time, CT clotting time, CFT clot formation time, HTS hypertonic saline, MCF maximum clot firmness
Fig. 1Box plots showing platelet function analyzer closure times (CtPFA) in undiluted blood samples and samples diluted with 0.9 % saline, 3 % HTS, and 20 % mannitol in 1:16 and 1:8 dilutions
Fig. 2Box plots showing Ex-tem CT measurements in undiluted blood samples and samples diluted with 0.9 % saline, 3 % HTS, and 20 % mannitol in 1:16 and 1:8 dilutions
Fig. 3Box plots showing Ex-tem CFT measurements in undiluted blood samples and samples diluted with 0.9 % saline, 3 % HTS, and 20 % mannitol in 1:16 and 1:8 dilutions
Fig. 4Box plots showing Ex-tem MCF measurements in undiluted blood samples and samples diluted with 0.9 % saline, 3 % HTS, and 20 % mannitol in 1:16 and 1:8 dilutions
Fig. 5Box plots showing Fib-tem MCF measurements in undiluted blood samples and samples diluted with 0.9 % saline, 3 % HTS, and 20 % mannitol in 1:16 and 1:8 dilutions