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不同品系的小鼠、大鼠和非人灵长类动物之间辐射诱导肺损伤的差异是否与肥大细胞增生的差异有关?

Do variations in mast cell hyperplasia account for differences in radiation-induced lung injury among different mouse strains, rats and nonhuman primates?

机构信息

Institute for Medical Engineering and Science, Massachusetts Institute of Technology, Cambridge, Massachusetts 02142, USA.

出版信息

Radiat Res. 2013 Aug;180(2):216-21. doi: 10.1667/RR3245.1. Epub 2013 Jul 2.

Abstract

The role of mast cell infiltrates in the pathology of radiation damage to the lung has been a subject of continuing investigation over the past four decades. This has been accompanied by a number of proposals as to how mast cells and the secretory products thereof participate in the generation of acute inflammation (pneumonitis) and the chronic process of collagen deposition (fibrosis). An additional pathophysiology examines the possible connection between mast cell hyperplasia and pulmonary hypertension through the release of vasoactive mediators. The timing and magnitude of pneumonitis and fibrosis are known to vary tremendously among different genetic mouse strains and animal species. Therefore, we have systematically compared mast cell numbers in lung sections from nine mouse strains, two rat strains and nonhuman primates (NHP) after whole thorax irradiation (WTI) at doses ranging from 10-15 Gy and at the time of entering respiratory distress. Mice of the BALB/c strain had a dramatic increase in interstitial mast cell numbers, similar to WAG/Rij and August rats, while relatively low levels of mast cell infiltrate were observed in other mouse strains (CBA, C3H, B6, C57L, WHT and TO mice). Enumeration of mast cell number in five NHPs (rhesus macaque), exhibiting severe pneumonitis at 17 weeks after 10 Gy WTI, also indicated a low response shared by the majority of mouse strains. There appeared to be no relationship between the mast cell response and the strain-dependent susceptibility towards pneumonitis or fibrosis. Further investigations are required to explore the possible participation of mast cells in mediating specific vascular responses and whether a genetically diverse mast cell response occurs in humans.

摘要

过去四十年来,肥大细胞浸润在肺放射性损伤病理学中的作用一直是持续研究的课题。这伴随着许多关于肥大细胞及其分泌产物如何参与急性炎症(肺炎)和胶原沉积的慢性过程(纤维化)的建议。另外一个病理生理学研究检查了肥大细胞增生与肺动脉高压之间通过血管活性介质释放的可能联系。不同遗传小鼠品系和动物物种之间的肺炎和纤维化的时间和程度变化极大。因此,我们系统地比较了 9 种小鼠品系、2 种大鼠品系和非人类灵长类动物(NHP)在接受 10-15Gy 全胸照射(WTI)后的肺组织切片中的肥大细胞数量,以及在出现呼吸窘迫时。BALB/c 品系的小鼠间质肥大细胞数量显著增加,类似于 WAG/Rij 和 August 大鼠,而其他小鼠品系(CBA、C3H、B6、C57L、WHT 和 TO 小鼠)的肥大细胞浸润水平相对较低。在接受 10GyWTI 后 17 周出现严重肺炎的 5 只 NHP(恒河猴)中计数肥大细胞数量也表明,大多数小鼠品系的反应较低。肥大细胞反应与肺炎或纤维化的品系依赖性易感性之间似乎没有关系。需要进一步研究以探索肥大细胞在介导特定血管反应中的可能参与作用,以及人类是否存在遗传多样化的肥大细胞反应。

相似文献

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Compartmental responses after thoracic irradiation of mice: strain differences.小鼠胸部照射后的分区反应:品系差异
Int J Radiat Oncol Biol Phys. 2005 Jul 1;62(3):862-71. doi: 10.1016/j.ijrobp.2005.02.037.

本文引用的文献

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Regulation of mast cell responses in health and disease.健康与疾病状态下肥大细胞反应的调节
Crit Rev Immunol. 2011;31(6):475-529. doi: 10.1615/critrevimmunol.v31.i6.30.

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