Coagulation Profile of Convalescent Plasma Donors and Recipients.

IF 2.3 4区 医学 Q2 HEMATOLOGY
Hanna H Pitkänen, Tuukka Helin, Tamim Khawaja, Jukka-Pekka Pietilä, Mikael Kajova, Hanna Välimaa, Tero Vahlberg, Jarkko Ihalainen, Antti Vierikko, Olli Vapalahti, Anu Kantele, Riitta Lassila
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Abstract

Convalescent plasma (CP) therapy for COVID-19 infection may have favorable safety but varying efficacy, with concerns about its procoagulant impact. We investigated whether administration of CP to hospitalized patients affects their coagulation profile. Fifty-four patients randomized in a double-blinded fashion received either placebo, low-titer CP (LCP) or high-titer CP (HCP). Donor blood samples were obtained at the time of the plasmapheresis, while recipient blood samples were collected before infusion, one day post-infusion and between two and six days after infusion. Routine laboratory follow-up, coagulation biomarkers, antiphospholipid antibodies, and thrombin generation (TG) were assessed. CP donors had normal blood cell counts and coagulation profiles, without differences between LCP and HCP donors at the baseline. All CP recipients were on low-molecular-weight heparin thromboprophylaxis at the time of the infusion. Despite randomization, the HCP group had lower baseline (p = 0.004) and Day 1 platelet counts (p = 0.019) than the LCP group. Von Willebrand antigen (VWF:Ag) levels clearly exceeded normal without differences at baseline. At Day 1, LCP recipients had higher VWF:Ag (mean ± SD 224 ± 15%) than HCP recipients (210 ± 8%) (p = 0.012). In all groups, overall 80% lupus anticoagulant was positive. Baseline TG variables were comparable, but again LCP recipients exhibited higher endogenous thrombin potential (ETP) (1313 ± 535 nM.min) (p = 0.038) and peak TG (184 ± 106 nM) (p = 0.037) than the HCP group (870 ± 425 nM.min and 86 ± 54 nM). Our findings show that LCP increases VWF:Ag levels and enhances TG despite the thromboprophylaxis. These results suggest that HCP induces less hypercoagulability than LCP, which may contribute to the variability in CP efficacy.

恢复期血浆供体和受体的凝血状况。
恢复期血浆(CP)治疗COVID-19感染可能具有良好的安全性,但疗效不一,值得关注的是其促凝作用。我们调查了给住院患者服用CP是否会影响他们的凝血状况。54名患者随机以双盲方式接受安慰剂、低效价CP (LCP)或高效价CP (HCP)。供体血样采集于血浆置换时,受体血样采集于输注前、输注后1天及输注后2 - 6天。评估常规实验室随访、凝血生物标志物、抗磷脂抗体和凝血酶生成(TG)。CP供者的血细胞计数和凝血情况正常,在基线时LCP和HCP供者之间没有差异。所有接受CP的患者在输注时均使用低分子肝素预防血栓形成。尽管随机分组,HCP组的基线(p = 0.004)和第1天血小板计数(p = 0.019)低于LCP组。血管性血友病抗原(VWF:Ag)水平明显高于正常水平,基线无差异。在第1天,LCP受体的VWF:Ag(平均±SD 224±15%)高于HCP受体(210±8%)(p = 0.012)。在所有组中,80%的狼疮抗凝剂呈阳性。基线TG变量具有可比性,但LCP受体的内源性凝血酶电位(ETP)(1313±535 nM.min) (p = 0.038)和峰值TG(184±106 nM) (p = 0.037)高于HCP组(870±425 nM)。min和86±54 nM)。我们的研究结果表明,LCP增加VWF:Ag水平并提高TG,尽管有血栓预防。这些结果表明,与LCP相比,HCP诱导的高凝性更低,这可能导致CP疗效的变异性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
4.40
自引率
3.40%
发文量
150
审稿时长
2 months
期刊介绍: CATH is a peer-reviewed bi-monthly journal that addresses the practical clinical and laboratory issues involved in managing bleeding and clotting disorders, especially those related to thrombosis, hemostasis, and vascular disorders. CATH covers clinical trials, studies on etiology, pathophysiology, diagnosis and treatment of thrombohemorrhagic disorders.
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