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体内和体外电离辐射暴露对淋巴功能的二分效应。

Dichotomous effects of in vivo and in vitro ionizing radiation exposure on lymphatic function.

作者信息

Singh Reetu, Heaps Cristine L, Muthuchamy Mariappan, Deveau Michael A, Stewart Randolph H, Laine Glen A, Dongaonkar Ranjeet M

机构信息

Michael E. DeBakey Institute for Comparative Cardiovascular Science and Biomedical Devices, Department of Veterinary Physiology and Pharmacology, Texas A&M University, College Station, Texas.

Department of Medical Physiology, Texas A&M University, Bryan, Texas.

出版信息

Am J Physiol Heart Circ Physiol. 2023 Jan 1;324(1):H155-H171. doi: 10.1152/ajpheart.00387.2022. Epub 2022 Dec 2.

Abstract

On the one hand, lymphatic dysfunction induces interstitial edema and inflammation. On the other hand, the formation of edema and inflammation induce lymphatic dysfunction. However, informed by the earlier reports of undetected apoptosis of irradiated lymphatic endothelial cells (LECs) in vivo, lymphatic vessels are commonly considered inconsequential to ionizing radiation (IR)-induced inflammatory injury to normal tissues. Primarily because of the lack of understanding of the acute effects of IR exposure on lymphatic function, acute edema and inflammation, common sequelae of IR exposure, have been ascribed solely to blood vessel damage. Therefore, in the present study, the lymphatic acute responses to IR exposure were quantified to evaluate the hypothesis that IR exposure impairs lymphatic pumping. Rat mesenteric lymphatic vessels were irradiated in vivo or in vitro, and changes in pumping were quantified in isolated vessels in vitro. Compared with sham-treated vessels, pumping was lowered in lymphatic vessels irradiated in vivo but increased in vessels irradiated in vitro. Furthermore, unlike in blood vessels, the acute effects of IR exposure in lymphatic vessels were not mediated by nitric oxide-dependent pathways in either in vivo or in vitro irradiated vessels. After cyclooxygenase blockade, pumping was partially restored in lymphatic vessels irradiated in vitro but not in vessels irradiated in vivo. Taken together, these findings demonstrated that lymphatic vessels are radiosensitive and LEC apoptosis alone may not account for all the effects of IR exposure on the lymphatic system. Earlier studies leading to the common belief that lymphatic vessels are radioresistant either did not characterize lymphatic pumping, deemed necessary for the resolution of edema and inflammation, or did it in vivo. By characterizing pumping in vitro, the present study, for the first time, demonstrated that lymphatic pumping was impaired in vessels irradiated in vivo and enhanced in vessels irradiated in vitro. Furthermore, the pathways implicated in ionizing radiation-induced blood vessel damage did not mediate lymphatic responses.

摘要

一方面,淋巴功能障碍会诱发间质水肿和炎症。另一方面,水肿和炎症的形成会诱发淋巴功能障碍。然而,鉴于此前有报道称在体内未检测到受辐照的淋巴管内皮细胞(LEC)凋亡,淋巴管通常被认为与电离辐射(IR)对正常组织造成的炎性损伤无关。主要是因为对IR暴露对淋巴功能的急性影响缺乏了解,IR暴露常见的后遗症——急性水肿和炎症,一直被认为完全是血管损伤所致。因此,在本研究中,对IR暴露后淋巴系统的急性反应进行了量化,以评估IR暴露会损害淋巴泵功能这一假说。对大鼠肠系膜淋巴管进行体内或体外辐照,并在体外对分离出的淋巴管中泵功能的变化进行量化。与假处理的淋巴管相比,体内辐照的淋巴管泵功能降低,而体外辐照的淋巴管泵功能增加。此外,与血管不同,无论在体内还是体外辐照的淋巴管中,IR暴露的急性效应均不是由一氧化氮依赖性途径介导的。在环氧化酶被阻断后,体外辐照的淋巴管泵功能部分恢复,但体内辐照的淋巴管未恢复。综上所述,这些发现表明淋巴管对辐射敏感,仅LEC凋亡可能无法解释IR暴露对淋巴系统的所有影响。早期的研究导致人们普遍认为淋巴管具有抗辐射性,这些研究要么没有对水肿和炎症消退所必需的淋巴泵功能进行描述,要么是在体内进行描述的。通过在体外对泵功能进行描述,本研究首次证明体内辐照的淋巴管泵功能受损,而体外辐照的淋巴管泵功能增强。此外,与电离辐射诱导血管损伤相关的途径并未介导淋巴反应。

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