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轻度β地中海贫血新鲜抽取红细胞的细胞脆性和代谢方面对其输血后的生理功能和表现产生影响:一项体内外三角相关性分析

Corpuscular Fragility and Metabolic Aspects of Freshly Drawn Beta-Thalassemia Minor RBCs Impact Their Physiology and Performance Post Transfusion: A Triangular Correlation Analysis In Vitro and In Vivo.

作者信息

Anastasiadi Alkmini T, Arvaniti Vasiliki-Zoi, Paronis Efthymios C, Kostomitsopoulos Nikolaos G, Stamoulis Konstantinos, Papassideri Issidora S, D'Alessandro Angelo, Kriebardis Anastasios G, Tzounakas Vassilis L, Antonelou Marianna H

机构信息

Department of Biology, Section of Cell Biology and Biophysics, School of Science, National and Kapodistrian University of Athens (NKUA), 15784 Athens, Greece.

Center of Clinical, Experimental Surgery & Translational Research, Biomedical Research Foundation, Academy of Athens (BRFAA), 11527 Athens, Greece.

出版信息

Biomedicines. 2022 Feb 23;10(3):530. doi: 10.3390/biomedicines10030530.

Abstract

The clarification of donor variation effects upon red blood cell (RBC) storage lesion and transfusion efficacy may open new ways for donor-recipient matching optimization. We hereby propose a "triangular" strategy for studying the links comprising the transfusion chain-donor, blood product, recipient-as exemplified in two cohorts of control and beta-thalassemia minor (βThal) donors ( = 18 each). It was unraveled that RBC osmotic fragility and caspase-like proteasomal activity can link both donor cohorts to post-storage states. In the case of heterozygotes, the geometry, size and intrinsic low RBC fragility might be lying behind their higher post-storage resistance to lysis and recovery in mice. Moreover, energy-related molecules (e.g., phosphocreatine) and purine metabolism factors (IMP, hypoxanthine) were specifically linked to lower post-storage hemolysis and phosphatidylserine exposure. The latter was also ameliorated by antioxidants, such as urate. Finally, higher proteasomal conservation across the transfusion chain was observed in heterozygotes compared to control donors. The proposed "triangularity model" can be (a) expanded to additional donor/recipient backgrounds, (b) enriched by big data, especially in the post-transfusion state and (c) fuel targeted experiments in order to discover new quality biomarkers and design more personalized transfusion medicine schemes.

摘要

阐明供体差异对红细胞(RBC)储存损伤和输血疗效的影响可能为优化供体-受体匹配开辟新途径。我们在此提出一种“三角”策略,用于研究输血链(供体、血液制品、受体)各环节之间的联系,以两组对照供体和轻型β地中海贫血(βThal)供体(每组n = 18)为例进行说明。研究发现,RBC渗透脆性和类半胱天冬酶蛋白酶体活性可将两组供体与储存后状态联系起来。对于杂合子而言,其几何形状、大小以及固有的低RBC脆性可能是其在储存后对小鼠溶血和恢复具有较高抵抗力的原因。此外,能量相关分子(如磷酸肌酸)和嘌呤代谢因子(肌苷一磷酸、次黄嘌呤)与储存后较低的溶血和磷脂酰丝氨酸暴露具有特异性联系。后者也可通过抗氧化剂(如尿酸盐)得到改善。最后,与对照供体相比,在杂合子中观察到整个输血链中蛋白酶体的保存情况更好。所提出的“三角模型”可以(a)扩展到其他供体/受体背景,(b)通过大数据进行充实,尤其是在输血后状态下,以及(c)推动靶向实验,以发现新的质量生物标志物并设计更个性化的输血医学方案。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a65f/8945797/eecd9f60ef2c/biomedicines-10-00530-g001.jpg

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