Diesen Diana L, Hess Douglas T, Stamler Jonathan S
Departments of Surgery, Duke University Medical Center, Durham, NC 27710, USA.
Circ Res. 2008 Aug 29;103(5):545-53. doi: 10.1161/CIRCRESAHA.108.176867. Epub 2008 Jul 24.
Red blood cells (RBCs) have been ascribed an essential role in matching blood flow to local metabolic demand during hypoxic vasodilation. The vasodilatory function of RBCs evidently relies on the allosteric properties of hemoglobin (Hb), which couple the conformation of Hb to tissue oxygen tension (Po(2)) and thereby provide a basis for the graded vasodilatory activity that is inversely proportional to Hb oxygen saturation. Although a large body of evidence indicates that the Po(2)-coupled allosteric transition from R (oxy)-state to T (deoxy)-state subserves the release from Hb of vasodilatory nitric oxide (NO) bioactivity, it has not yet been determined whether the NO-based signal is a necessary and sufficient source of RBC-mediated vasoactivity and it has been suggested that ATP or nitrite may also contribute. We demonstrate here by bioassay that untreated human RBCs rapidly and substantially relax thoracic aorta from both rabbit and mouse at low Po(2) (approximately 1% O(2)) but not at high Po(2) (approximately 21% O(2)). RBC-mediated vasorelaxation is inhibited by prior depletion of S-nitroso-Hb, potentiated by low-molecular-weight thiols, and dependent on cGMP. Furthermore, these relaxations are largely endothelium-independent and unaffected by NO synthase inhibition or nitrite. Robust relaxations by RBCs are also elicited in the absence of endothelial, neuronal or inducible NO synthase. Finally, contractions that appear following resolution of RBC-mediated relaxations are dependent on NO derived from RBCs as well as the endothelium. Our results suggest that an S-nitrosothiol-based signal originating from RBCs mediates hypoxic vasodilation by RBCs, and that vasorelaxation by RBCs dominates NO-based vasoconstriction under hypoxic conditions.
在低氧性血管舒张过程中,红细胞(RBCs)被认为在使血流与局部代谢需求相匹配方面发挥着重要作用。红细胞的血管舒张功能显然依赖于血红蛋白(Hb)的变构特性,这种特性将Hb的构象与组织氧张力(Po₂)联系起来,从而为与Hb氧饱和度成反比的分级血管舒张活性提供了基础。尽管大量证据表明,Po₂耦合的从R(氧合)状态到T(脱氧)状态的变构转变有助于从Hb释放血管舒张性一氧化氮(NO)生物活性,但基于NO的信号是否是红细胞介导的血管活性的必要和充分来源尚未确定,并且有人提出ATP或亚硝酸盐也可能起作用。我们在此通过生物测定证明,未经处理的人红细胞在低Po₂(约1% O₂)时能迅速且显著地舒张兔和小鼠的胸主动脉,但在高Po₂(约21% O₂)时则不能。红细胞介导的血管舒张受到先前S-亚硝基-Hb耗竭的抑制,被低分子量硫醇增强,并且依赖于cGMP。此外,这些舒张在很大程度上不依赖于内皮,不受NO合酶抑制或亚硝酸盐的影响。在没有内皮型、神经元型或诱导型NO合酶的情况下,红细胞也能引起强烈的舒张。最后,红细胞介导的舒张消退后出现的收缩依赖于源自红细胞以及内皮的NO。我们的结果表明,源自红细胞的基于S-亚硝基硫醇的信号介导了红细胞的低氧性血管舒张,并且在低氧条件下红细胞介导的血管舒张主导了基于NO的血管收缩。