The association between early neurological deterioration and whole blood purine concentration during acute stroke

Abstract Background Early neurological deterioration (END) is common after stroke. Prediction could identify patients requiring additional monitoring and intervention. Purines, breakdown products of adenosine triphosphate which accumulate during acute hypoxia, may reflect the subclinical presence of...

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Main Authors: Alexander J. Martin, Nicholas Dale, Christopher H. E. Imray, Christine Roffe, Craig J. Smith, Faming Tian, Christopher I. Price
Format: Article
Language:English
Published: BMC 2019-04-01
Series:Biomarker Research
Subjects:
Online Access:http://link.springer.com/article/10.1186/s40364-019-0158-y
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spelling doaj-d700c53965f54ebe80c73ff25c86c90a2020-11-25T02:07:11ZengBMCBiomarker Research2050-77712019-04-01711510.1186/s40364-019-0158-yThe association between early neurological deterioration and whole blood purine concentration during acute strokeAlexander J. Martin0Nicholas Dale1Christopher H. E. Imray2Christine Roffe3Craig J. Smith4Faming Tian5Christopher I. Price6NIHR Newcastle Biomedical Research Centre and Institute of Neuroscience, Newcastle UniversitySchool of Life Sciences, University of WarwickCoventry and Warwickshire County Vascular Unit, University Hospitals Coventry and Warwickshire NHS Foundation TrustInstitute for Science and Technology in Medicine, University of KeeleDivision of Cardiovascular Sciences, University of ManchesterSarissa Biomedical LtdNIHR Newcastle Biomedical Research Centre and Institute of Neuroscience, Newcastle UniversityAbstract Background Early neurological deterioration (END) is common after stroke. Prediction could identify patients requiring additional monitoring and intervention. Purines, breakdown products of adenosine triphosphate which accumulate during acute hypoxia, may reflect the subclinical presence of vulnerable tissue. We considered whether whole blood purine concentration (WBPC) measurements during acute stroke were associated with subsequent END. Methods Patients within 4.5 h of stroke onset underwent point-of-care finger-prick measurement of WBPC and blinded assessment of symptom severity using the National Institutes of Health Stroke Scale (NIHSS). END was defined as an NIHSS increase ≥2 points at 24–36 h compared to baseline. Results 15/152 (9.8%) patients experienced END with a median [IQR] NIHSS increase of 4 [2–7] points. There were no strong associations between END and baseline NIHSS, clinical stroke subtype, thrombolytic therapy, physiological characteristics or time to assay. The median [IQR] WBPC concentration (uM) was higher before the occurrence of END but without statistical significance (7.21 [4.77–10.65] versus 4.83 [3.00–9.02]; p = 0.1). Above a WBPC threshold of 6.05uM, the risk of END was significantly greater (odds ratio 3.7 (95% CI 1.1–12.4); p = 0.03). Conclusion Although the study lacked statistical power, early WBPC measurement could be a convenient biomarker for identifying acute stroke patients at risk of END, but further evaluation is required.http://link.springer.com/article/10.1186/s40364-019-0158-yStrokeCerebrovascular diseaseDeteriorationPurinesPenumbra
collection DOAJ
language English
format Article
sources DOAJ
author Alexander J. Martin
Nicholas Dale
Christopher H. E. Imray
Christine Roffe
Craig J. Smith
Faming Tian
Christopher I. Price
spellingShingle Alexander J. Martin
Nicholas Dale
Christopher H. E. Imray
Christine Roffe
Craig J. Smith
Faming Tian
Christopher I. Price
The association between early neurological deterioration and whole blood purine concentration during acute stroke
Biomarker Research
Stroke
Cerebrovascular disease
Deterioration
Purines
Penumbra
author_facet Alexander J. Martin
Nicholas Dale
Christopher H. E. Imray
Christine Roffe
Craig J. Smith
Faming Tian
Christopher I. Price
author_sort Alexander J. Martin
title The association between early neurological deterioration and whole blood purine concentration during acute stroke
title_short The association between early neurological deterioration and whole blood purine concentration during acute stroke
title_full The association between early neurological deterioration and whole blood purine concentration during acute stroke
title_fullStr The association between early neurological deterioration and whole blood purine concentration during acute stroke
title_full_unstemmed The association between early neurological deterioration and whole blood purine concentration during acute stroke
title_sort association between early neurological deterioration and whole blood purine concentration during acute stroke
publisher BMC
series Biomarker Research
issn 2050-7771
publishDate 2019-04-01
description Abstract Background Early neurological deterioration (END) is common after stroke. Prediction could identify patients requiring additional monitoring and intervention. Purines, breakdown products of adenosine triphosphate which accumulate during acute hypoxia, may reflect the subclinical presence of vulnerable tissue. We considered whether whole blood purine concentration (WBPC) measurements during acute stroke were associated with subsequent END. Methods Patients within 4.5 h of stroke onset underwent point-of-care finger-prick measurement of WBPC and blinded assessment of symptom severity using the National Institutes of Health Stroke Scale (NIHSS). END was defined as an NIHSS increase ≥2 points at 24–36 h compared to baseline. Results 15/152 (9.8%) patients experienced END with a median [IQR] NIHSS increase of 4 [2–7] points. There were no strong associations between END and baseline NIHSS, clinical stroke subtype, thrombolytic therapy, physiological characteristics or time to assay. The median [IQR] WBPC concentration (uM) was higher before the occurrence of END but without statistical significance (7.21 [4.77–10.65] versus 4.83 [3.00–9.02]; p = 0.1). Above a WBPC threshold of 6.05uM, the risk of END was significantly greater (odds ratio 3.7 (95% CI 1.1–12.4); p = 0.03). Conclusion Although the study lacked statistical power, early WBPC measurement could be a convenient biomarker for identifying acute stroke patients at risk of END, but further evaluation is required.
topic Stroke
Cerebrovascular disease
Deterioration
Purines
Penumbra
url http://link.springer.com/article/10.1186/s40364-019-0158-y
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