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Comparison of the antiplatelet and antithrombotic effects of bivalirudin versus unfractionated heparin: A platelet substudy of the HEAT PPCI trial

Comparison of the antiplatelet and antithrombotic effects of bivalirudin versus unfractionated heparin: A platelet substudy of the HEAT PPCI trial
Comparison of the antiplatelet and antithrombotic effects of bivalirudin versus unfractionated heparin: A platelet substudy of the HEAT PPCI trial

In randomised trials, bivalirudin has been associated with higher rates of acute stent thrombosis (AST) compared to unfractionated heparin (UFH), without mechanistic explanation. Furthermore, data are discrepant regards the antiplatelet effects of bivalirudin. This prespecified study, part of a larger HEAT-PPCI Platelet Substudy, aimed to compare the antiplatelet and antithrombotic effects of bivalirudin and UFH using short thrombelastography (s-TEG), an ex vivo whole blood platelet function assay. In HEAT-PPCI, patients were randomised to receive UFH or bivalirudin before angiography. Assay with s-TEG was performed in 184 patients (10.2%) at end of procedure (EOP) and repeated at 24 h. In addition to adenosine diphosphate- (ADP) and arachidonic acid- (AA) mediated platelet aggregation, thrombin-mediated clotting (TMC) was assessed using kaolin with and without heparinase. There were no significant differences between UFH and bivalirudin in ADP- and AA-mediated platelet aggregation at EOP or 24 h. Whilst UFH obliterated TMC at EOP, bivalirudin prolonged R time (19.7 min [15.9-25.4] vs. 8.4 min [7.5-10]; P < 0.0001), K time (2.4 min [1.9-3.4] vs. 2.2 min [1.8-2.7]; P = 0.007) and significantly increased maximum clot strength (MA 62.7 mm [58.7-67.4] vs. 58.6 [55-63]; P = 0.0005), compared to control. In conclusion, there were no significant differences in the antiplatelet effects of UFH and bivalirudin. However, whilst UFH obliterated TMC, bivalirudin prolonged clot initiation but potentiated maximum clot strength. As AST is likely multifactorial in aetiology, in patients treated with bivalirudin, increased clot strength may contribute to this hazard in some individuals and this observation warrants further investigation.

Aged, Antithrombins/pharmacology, Blood Platelets/cytology, Female, Heparin/pharmacology, Hirudins/pharmacology, Humans, Male, Middle Aged, Peptide Fragments/pharmacology, Platelet Aggregation/drug effects, Platelet Aggregation Inhibitors/pharmacology, Recombinant Proteins/pharmacology, Thrombelastography
0049-3848
36-43
Khanna, Vikram
17b557ad-b071-4d1a-84dd-3ba58470cee0
Shahzad, Adeel
f86eaf9e-254e-4acd-999e-6978a780195f
Thayalasamy, Kala
2c826201-a993-43d1-b5ae-da9ffc82201d
Kemp, Ian
b884bce3-f2dd-4374-81a0-a1c7ddcb64a8
Mars, Christine
68734957-1ad4-44a9-8604-111235b72201
Cooper, Rob
3a0ab690-ab62-46b6-9fd5-fc977dcd0423
Roome, Claire
1e1f3888-927c-48cd-92ce-e2bf719678e2
Wilson, Keith
ba657343-ef90-4363-a369-a571caaf001e
Harris, Scott
19ea097b-df15-4f0f-be19-8ac42c190028
Stables, Rod
25839df9-9bcf-4c1d-8e9c-700dd4aa87e1
Curzen, Nick
70f3ea49-51b1-418f-8e56-8210aef1abf4
Khanna, Vikram
17b557ad-b071-4d1a-84dd-3ba58470cee0
Shahzad, Adeel
f86eaf9e-254e-4acd-999e-6978a780195f
Thayalasamy, Kala
2c826201-a993-43d1-b5ae-da9ffc82201d
Kemp, Ian
b884bce3-f2dd-4374-81a0-a1c7ddcb64a8
Mars, Christine
68734957-1ad4-44a9-8604-111235b72201
Cooper, Rob
3a0ab690-ab62-46b6-9fd5-fc977dcd0423
Roome, Claire
1e1f3888-927c-48cd-92ce-e2bf719678e2
Wilson, Keith
ba657343-ef90-4363-a369-a571caaf001e
Harris, Scott
19ea097b-df15-4f0f-be19-8ac42c190028
Stables, Rod
25839df9-9bcf-4c1d-8e9c-700dd4aa87e1
Curzen, Nick
70f3ea49-51b1-418f-8e56-8210aef1abf4

Khanna, Vikram, Shahzad, Adeel, Thayalasamy, Kala, Kemp, Ian, Mars, Christine, Cooper, Rob, Roome, Claire, Wilson, Keith, Harris, Scott, Stables, Rod and Curzen, Nick (2018) Comparison of the antiplatelet and antithrombotic effects of bivalirudin versus unfractionated heparin: A platelet substudy of the HEAT PPCI trial. Thrombosis Research, 172, 36-43. (doi:10.1016/j.thromres.2018.09.062).

Record type: Article

Abstract

In randomised trials, bivalirudin has been associated with higher rates of acute stent thrombosis (AST) compared to unfractionated heparin (UFH), without mechanistic explanation. Furthermore, data are discrepant regards the antiplatelet effects of bivalirudin. This prespecified study, part of a larger HEAT-PPCI Platelet Substudy, aimed to compare the antiplatelet and antithrombotic effects of bivalirudin and UFH using short thrombelastography (s-TEG), an ex vivo whole blood platelet function assay. In HEAT-PPCI, patients were randomised to receive UFH or bivalirudin before angiography. Assay with s-TEG was performed in 184 patients (10.2%) at end of procedure (EOP) and repeated at 24 h. In addition to adenosine diphosphate- (ADP) and arachidonic acid- (AA) mediated platelet aggregation, thrombin-mediated clotting (TMC) was assessed using kaolin with and without heparinase. There were no significant differences between UFH and bivalirudin in ADP- and AA-mediated platelet aggregation at EOP or 24 h. Whilst UFH obliterated TMC at EOP, bivalirudin prolonged R time (19.7 min [15.9-25.4] vs. 8.4 min [7.5-10]; P < 0.0001), K time (2.4 min [1.9-3.4] vs. 2.2 min [1.8-2.7]; P = 0.007) and significantly increased maximum clot strength (MA 62.7 mm [58.7-67.4] vs. 58.6 [55-63]; P = 0.0005), compared to control. In conclusion, there were no significant differences in the antiplatelet effects of UFH and bivalirudin. However, whilst UFH obliterated TMC, bivalirudin prolonged clot initiation but potentiated maximum clot strength. As AST is likely multifactorial in aetiology, in patients treated with bivalirudin, increased clot strength may contribute to this hazard in some individuals and this observation warrants further investigation.

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More information

Accepted/In Press date: 27 September 2018
e-pub ahead of print date: 28 September 2018
Published date: December 2018
Keywords: Aged, Antithrombins/pharmacology, Blood Platelets/cytology, Female, Heparin/pharmacology, Hirudins/pharmacology, Humans, Male, Middle Aged, Peptide Fragments/pharmacology, Platelet Aggregation/drug effects, Platelet Aggregation Inhibitors/pharmacology, Recombinant Proteins/pharmacology, Thrombelastography

Identifiers

Local EPrints ID: 427319
URI: http://eprints.soton.ac.uk/id/eprint/427319
DOI: doi:10.1016/j.thromres.2018.09.062
ISSN: 0049-3848
PURE UUID: c54fc542-f2a7-4f44-b14e-a13640726892
ORCID for Nick Curzen: ORCID iD orcid.org/0000-0001-9651-7829

Catalogue record

Date deposited: 11 Jan 2019 17:30
Last modified: 18 Mar 2024 03:01

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Contributors

Author: Vikram Khanna
Author: Adeel Shahzad
Author: Kala Thayalasamy
Author: Ian Kemp
Author: Christine Mars
Author: Rob Cooper
Author: Claire Roome
Author: Keith Wilson
Author: Scott Harris
Author: Rod Stables
Author: Nick Curzen ORCID iD

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