Coadministration of PEGylated apohemoglobin and haptoglobin can limit vascular dysfunction in the microcirculation and prevent acute inflammation.

IF 3.3 3区 医学 Q1 PHYSIOLOGY Journal of applied physiology Pub Date : 2024-10-01 Epub Date: 2024-08-15 DOI:10.1152/japplphysiol.00315.2024
Carlos J Munoz, Daniela Lucas, Cynthia R Muller, Jacinda Martinez, Quintin O'Boyle, Ivan S Pires, Andre F Palmer, Pedro Cabrales
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Abstract

Unfortunately, during pathological conditions resulting in chronic hemolysis cell-free hemoglobin (Hb) is released into the circulation that releases free heme, resulting in several complications. One approach to prevent these toxicities is the administration of supplemental scavenger proteins, haptoglobin (Hp) and hemopexin (Hpx). The goal of this body of work is to objectively measure the levels of vascular reactivity and inflammatory profiles after an infusion of acellular hemoglobin in animals that were given a coadministration of PEGylated human apohemoglobin (PEG-apoHb), a hemopexin (Hpx)-mimetic that can scavenge free heme from hemoglobin, together with human plasma-derived Hp that can scavenge dimerized Hb. Using intravital microscopy, Golden Syrian hamsters instrumented with a dorsal window chamber were used to evaluate the in vivo effects of four experimental groups that were then challenged with a hypovolemic injection (10% of the animal's blood volume) of human Hb (hHb, 5 g/dL). The four experimental groups consisted of: 1) lactated Ringer's solution (control), 2) PEG-apoHb only, 3) Hp only, and 4) PEG-apoHb + Hp. The microvascular hemodynamics (diameter and flow) in arterioles and venules were recorded at baseline, 20 min after treatment, and 20 min after hHb challenge. Systemic parameters (blood pressure and heart rate), blood gases (pH, Pco2, and Po2), blood parameters (Hb concentration and hematocrit), and multiorgan functionality/inflammation were also measured. Our results suggest that coadministration of PEG-apoHb + Hp as a booster before the infusion of acellular hemoglobin significantly prevented vasoconstriction in the microcirculation, significantly increased the number of functional capillaries, and significantly reduced inflammation.NEW & NOTEWORTHY Coadministration of PEGylated human apohemoglobin (PEG-apoHb)-a hemopexin (Hpx) mimetic that can scavenge free heme-and human plasma-derived haptoglobin (Hp) that can scavenge hemoglobin (Hb), reduces microcirculatory dysfunction and cardiac and kidney inflammation in a Hb-challenge model.

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同时服用 PEG 化的载脂蛋白和巯基血红蛋白可限制微循环中的血管功能障碍并预防急性炎症。
不幸的是,在导致慢性溶血的病理情况下,细胞游离血红蛋白(Hb)会释放到血液循环中,从而释放出游离血红素,导致多种并发症。预防这些毒副作用的一种方法是补充清道夫蛋白--血红蛋白(Hp)和血卟啉(Hpx)。本研究的目标是客观测量动物输注无细胞血红蛋白后的血管反应性和炎症特征水平,这些动物同时输注了 PEG 化人促血红蛋白(PEG-apoHb)(一种可清除血红蛋白中游离血红素的仿血红蛋白 (Hpx))和可清除二聚化血红蛋白的人血浆衍生 Hp。利用体视显微镜,使用背窗仓的金色叙利亚仓鼠来评估 4 个实验组的体内效应,然后向这 4 个实验组注射低血容量(动物血容量的 10%)的人血红蛋白(hHb,5 g/dL)。四个实验组包括1)乳酸林格液(对照组);2)仅 PEG-apoHb;3)仅 Hp;4)PEG-apoHb + Hp。分别在基线、治疗后 20 分钟和接受 hHb 挑战后 20 分钟记录动脉和静脉的微血管血液动力学参数(直径和流量)。还测量了全身参数(血压和心率)、血气(pH、pCO2 和 pO2)、血液参数(Hb 浓度和血细胞比容)以及多器官功能/炎症。我们的研究结果表明,在输注无细胞血红蛋白之前联合使用 PEG-apoHb + Hp 作为增效剂可显著防止微循环中的血管收缩,显著增加功能性毛细血管的数量,并显著减轻炎症。
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来源期刊
CiteScore
6.00
自引率
9.10%
发文量
296
审稿时长
2-4 weeks
期刊介绍: The Journal of Applied Physiology publishes the highest quality original research and reviews that examine novel adaptive and integrative physiological mechanisms in humans and animals that advance the field. The journal encourages the submission of manuscripts that examine the acute and adaptive responses of various organs, tissues, cells and/or molecular pathways to environmental, physiological and/or pathophysiological stressors. As an applied physiology journal, topics of interest are not limited to a particular organ system. The journal, therefore, considers a wide array of integrative and translational research topics examining the mechanisms involved in disease processes and mitigation strategies, as well as the promotion of health and well-being throughout the lifespan. Priority is given to manuscripts that provide mechanistic insight deemed to exert an impact on the field.
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