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搏动血流期间红细胞与血管细胞黏附分子-1的黏附增加:微流控流动黏附生物测定法的应用

Increased erythrocyte adhesion to VCAM-1 during pulsatile flow: Application of a microfluidic flow adhesion bioassay.

作者信息

White Jennell, Lancelot Moira, Sarnaik Sharada, Hines Patrick

机构信息

Department of Pediatrics, Wayne State University School of Medicine, Detroit, MI, USA.

Division of Hematology/Oncology, Children's Hospital of Michigan, Detroit, MI, USA.

出版信息

Clin Hemorheol Microcirc. 2015;60(2):201-13. doi: 10.3233/CH-141847.

Abstract

Sickle cell disease (SCD) is characterized by microvascular occlusion mediated by adhesive interactions of sickle erythrocytes (SSRBCs) to the endothelium. Most in vitro flow adhesion assays measure SSRBC adhesion during continuous flow, although in vivo SSRBC adhesive interactions occur during pulsatile flow. Using a well-plate microfluidic flow adhesion system, we demonstrate that isolated SSRBCs adhere to vascular cell adhesion molecule (VCAM-1) at greater levels during pulsatile versus continuous flow. A significant increase in adhesive interactions was observed between all pulse frequencies 1 Hz to 2 Hz (60-120 beats/min) when compared to non-pulsatile flow. Adhesion of isolated SSRBCs and whole blood during pulsatile flow was unaffected by protein kinase A (PKA) inhibition, and exposure of SSRBCs to pulsatile flow did not affect the intrinsic adhesive properties of SSRBCs. The cell type responsible for increased adhesion of whole blood varied from patient to patient. We conclude that low flow periods of the pulse cycle allow more adhesive interactions between sickle erythrocytes and VCAM-1, and sickle erythrocyte adhesion in the context of whole blood may better reflect physiologic cellular interactions. The microfluidic flow adhesion bioassay used in this study may have applications for clinical assessment of sickle erythrocyte adhesion during pulsatile flow.

摘要

镰状细胞病(SCD)的特征是镰状红细胞(SSRBCs)与内皮细胞发生黏附相互作用介导的微血管闭塞。大多数体外流动黏附试验测量的是连续流动过程中SSRBC的黏附情况,尽管在体内,SSRBC的黏附相互作用发生在脉动血流期间。使用微孔板微流控流动黏附系统,我们证明,与连续流动相比,分离的SSRBCs在脉动血流期间与血管细胞黏附分子(VCAM-1)的黏附水平更高。与非脉动血流相比,在1Hz至2Hz(60 - 120次/分钟)的所有脉冲频率下,黏附相互作用均显著增加。脉动血流期间,分离的SSRBCs和全血的黏附不受蛋白激酶A(PKA)抑制的影响,并且将SSRBCs暴露于脉动血流中不会影响SSRBCs的固有黏附特性。导致全血黏附增加的细胞类型因患者而异。我们得出结论,脉冲周期的低血流期允许镰状红细胞与VCAM-1之间发生更多的黏附相互作用,并且在全血环境中镰状红细胞的黏附可能更好地反映生理细胞相互作用。本研究中使用的微流控流动黏附生物测定法可能在临床评估脉动血流期间镰状红细胞黏附方面具有应用价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe4e/4923762/1e9df787a2cc/ch-60-2-ch1847-g001.jpg

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