Correlation of von Willebrand factor and platelets with acute ischemic stroke etiology and revascularization outcome: an immunohistochemical study

Author:

Mereuta Oana MadalinaORCID,Abbasi MehdiORCID,Arturo Larco Jorge LORCID,Dai DayingORCID,Liu Yang,Arul Santhosh,Kadirvel RamanathanORCID,Hanel Ricardo A,Yoo Albert J,Almekhlafi Mohammed AORCID,Layton Kennith F,Delgado Almandoz Josser E,Kvamme Peter,Mendes Pereira VitorORCID,Jahromi Babak SORCID,Nogueira Raul G,Gounis Matthew JORCID,Patel Biraj,Aghaebrahim Amin,Sauvageau Eric,Bhuva Parita,Soomro Jazba,Demchuk Andrew M,Thacker Ike C,Kayan Yasha,Copelan Alexander,Nazari PouyaORCID,Cantrell Donald Robert,Haussen Diogo C,Al-Bayati Alhamza RORCID,Mohammaden Mahmoud,Pisani LeonardoORCID,Rodrigues Gabriel MartinsORCID,Puri Ajit S,Entwistle John,Meves Alexander,Savastano Luis,Cloft Harry J,Nimjee Shahid MORCID,McBane Robert D,Kallmes David F,Brinjikji WaleedORCID

Abstract

BackgroundPlatelets and von Willebrand factor (vWF) are key components of acute ischemic stroke (AIS) emboli. We aimed to investigate the CD42b (platelets)/vWF expression, its association with stroke etiology and the impact these components may have on the clinical/procedural parameters.MethodsCD42b/vWF immunostaining was performed on 288 emboli collected as part of the multicenter STRIP Registry. CD42b/VWF expression and distribution were evaluated. Student’s t-test and χ2test were performed as appropriate.ResultsThe mean CD42b and VWF content in clots was 44.3% and 21.9%, respectively. There was a positive correlation between platelets and vWF (r=0.64, p<0.001**). We found a significantly higher vWF level in the other determined etiology (p=0.016*) and cryptogenic (p=0.049*) groups compared with cardioembolic etiology. No significant difference in CD42b content was found across the etiology subtypes. CD42b/vWF patterns were significantly associated with stroke etiology (p=0.006*). The peripheral pattern was predominant in atherosclerotic clots (36.4%) while the clustering (patchy) pattern was significantly associated with cardioembolic and cryptogenic origin (66.7% and 49.8%, respectively). The clots corresponding to other determined etiology showed mainly a diffuse pattern (28.1%). Two types of platelets were distinguished within the CD42b-positive clusters in all emboli: vWF-positive platelets were observed at the center, surrounded by vWF-negative platelets. Thrombolysis correlated with a high platelet content (p=0.03*). vWF-poor and peripheral CD42b/vWF pattern correlated with first pass effect (p=0.03* and p=0.04*, respectively).ConclusionsThe vWF level and CD42b/vWF distribution pattern in emboli were correlated with AIS etiology and revascularization outcome. Platelet content was associated with response to thrombolysis.

Funder

National Institutes of Health

Publisher

BMJ

Subject

Neurology (clinical),General Medicine,Surgery

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