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患有急性肺移植排斥反应的犬类的单核细胞会导致肺动脉收缩。

Mononuclear cells from dogs with acute lung allograft rejection cause contraction of pulmonary arteries.

作者信息

Cale A R, Ricagna F, Wiklund L, McGregor C G, Miller V M

机构信息

Department of Surgery, Mayo Clinic and Foundation, Rochester, Minn. 55905.

出版信息

Circulation. 1994 Aug;90(2):952-8. doi: 10.1161/01.cir.90.2.952.

Abstract

PURPOSE

Experiments were designed to determine whether or not leukocytes activated by acute pulmonary rejection cause contractions of isolated pulmonary arteries.

METHODS AND RESULTS

Separate suspensions of (a) polymorphonuclear cells (> 95%) and (b) mononuclear cells (85% lymphocytes/10% monocytes/5% polymorphonuclear cells), respectively, were obtained from the arterial blood of four groups of adult male mongrel dogs: unoperated dogs (controls), dogs with single-lung autotransplants, dogs with rejecting single-lung allotransplants, and unoperated dogs treated with the same immunosuppressants as allotransplanted dogs. These suspensions were added to rings of control intralobar pulmonary arteries suspended in organ chambers for measurement of isometric force. The endothelium was removed mechanically from selected rings. No significant change in basal tension of pulmonary arterial rings occurred by adding suspensions of polymorphonuclear cells from any of the four groups of dogs. Significant cell-number-dependent increases in tension occurred with suspensions of mononuclear cells from unoperated dogs, autotransplanted dogs, and unoperated, medicated dogs. These increases in tension were less in rings with compared to those without endothelium. Addition of a synthetic analogue of L-arginine abolished this difference. Suspensions of mononuclear cells from rejecting allotransplanted dogs caused significantly greater contractions in rings with endothelium than those observed with suspended cells from either unoperated, autotransplanted dogs or unoperated, medicated dogs. Addition of superoxide dismutase plus catalase or an antagonist of endothelin-A receptors (BQ-123) reduced contractions in rings with endothelium but not in those without endothelium to suspensions of mononuclear cells from rejecting allotransplanted dogs.

CONCLUSIONS

The results of this study suggest that mononuclear cells cause contraction of pulmonary arteries, which can be partially inhibited by endothelium-derived nitric oxide. However, if the mononuclear cells are activated by acute pulmonary rejection, contractions are no longer inhibited by the endothelium. Under conditions of rejection, contractions are mediated in part by oxygen radicals and endothelin(s).

摘要

目的

设计实验以确定急性肺排斥反应激活的白细胞是否会引起离体肺动脉收缩。

方法与结果

分别从四组成年雄性杂种犬的动脉血中获取(a)多形核细胞(>95%)和(b)单核细胞(85%淋巴细胞/10%单核细胞/5%多形核细胞)的单独悬液:未手术犬(对照组)、单肺自体移植犬、单肺同种异体移植排斥反应犬以及接受与同种异体移植犬相同免疫抑制剂治疗的未手术犬。将这些悬液添加到悬浮于器官腔室中的对照叶内肺动脉环中,以测量等长力。从选定的环中机械去除内皮。添加来自四组犬中任何一组的多形核细胞悬液后,肺动脉环的基础张力无显著变化。未手术犬、自体移植犬以及接受药物治疗的未手术犬的单核细胞悬液可引起张力显著的细胞数量依赖性增加。与无内皮的环相比,有内皮的环中这种张力增加较小。添加L-精氨酸的合成类似物消除了这种差异。来自排斥同种异体移植犬的单核细胞悬液在有内皮的环中引起的收缩明显大于未手术犬、自体移植犬或接受药物治疗的未手术犬的悬浮细胞所观察到的收缩。添加超氧化物歧化酶加过氧化氢酶或内皮素-A受体拮抗剂(BQ-123)可减少来自排斥同种异体移植犬的单核细胞悬液对有内皮环的收缩作用,但对无内皮环无此作用。

结论

本研究结果表明,单核细胞可引起肺动脉收缩,内皮衍生的一氧化氮可部分抑制这种收缩。然而,如果单核细胞被急性肺排斥反应激活,内皮不再抑制收缩。在排斥反应条件下,收缩部分由氧自由基和内皮素介导。

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