L-精氨酸：一种改善出血后创伤免疫功能低下的独特氨基酸。

Angele Martin K, Nitsch Stefan M, Hatz Rudolf A, Angele Peter, Hernandez-Richter Thomas, Wichmann Mathias W, Chaudry Irshad H, Schildberg Fredrich W

Department of Surgery, Klinikum Grosshadern, Ludwig Maximilians University, Munich, Germany.

Eur Surg Res. 2002 Jan-Apr;34(1-2):53-60. doi: 10.1159/000048888.

OBJECTIVE

To determine whether L-arginine has any salutary effects on wound immune cell function following trauma-hemorrhage.

BACKGROUND

Depressed wound immune function contributes to an increased incidence of wound infections following hemorrhage. Although administration of L-arginine has been shown to restore depressed cell-mediated immune responses following hemorrhage potentially by maintaining organ blood flow, it remains unknown whether L-arginine has any salutary effects on the depressed local immune response at the wound site.

METHODS

Male mice were subjected to a midline laparotomy and polyvinyl sponges were implanted subcutaneously in the abdominal wound prior to hemorrhage (35 +/- 5 mm Hg for 90 min and resuscitation) or sham operation. During resuscitation mice received 300 mg/kg body weight L-arginine or saline (vehicle). Sponges were harvested 24 h thereafter, wound fluid collected and wound immune cells cultured for 24 h in the presence of LPS. Pro- (IL-1 beta, IL-6) and anti-inflammatory (IL-10) cytokines were determined in the supernatants and the wound fluid. In addition, wounds were stained for IL-6 immunohistochemically. In a separate set of animals, skin and muscle blood flow was determined by microspheres.

RESULTS

The capacity of wound immune cells to release IL-1 beta and IL-6 in vitro was significantly depressed in hemorrhaged mice receiving vehicle. Administration of L-arginine, however, improved wound immune cell function. In contrast, in vivo the increased IL-6 release at the wound site was decreased in L-arginine-treated mice following hemorrhage. Moreover, IL-10 levels were significantly increased in the wound fluid in hemorrhaged animals receiving L-arginine compared to vehicle-treated mice. In addition, the depressed skin and muscle blood flow after hemorrhage was restored by L-arginine.

CONCLUSIONS

Thus, L-arginine might improve local wound cell function by decreasing the inflammatory response at the wound site. Since L-arginine protected wound immune cell function this amino acid might represent a novel and useful adjunct to fluid resuscitation for decreasing wound complications following hemorrhage.

目的

确定L-精氨酸对创伤性出血后伤口免疫细胞功能是否有任何有益作用。

背景

伤口免疫功能低下导致出血后伤口感染发生率增加。尽管已表明给予L-精氨酸可能通过维持器官血流来恢复出血后受抑制的细胞介导免疫反应，但L-精氨酸对伤口部位受抑制的局部免疫反应是否有任何有益作用仍不清楚。

方法

雄性小鼠接受中线剖腹手术，在出血（35±5mmHg，持续90分钟并复苏）或假手术前，将聚乙烯海绵皮下植入腹部伤口。在复苏过程中，小鼠接受300mg/kg体重的L-精氨酸或生理盐水（载体）。此后24小时收集海绵，收集伤口液体，并在LPS存在下将伤口免疫细胞培养24小时。在上清液和伤口液体中测定促炎（IL-1β、IL-6）和抗炎（IL-10）细胞因子。此外，对伤口进行IL-6免疫组织化学染色。在另一组动物中，通过微球测定皮肤和肌肉血流。

结果

接受载体的出血小鼠伤口免疫细胞体外释放IL-1β和IL-6的能力显著降低。然而，给予L-精氨酸可改善伤口免疫细胞功能。相比之下，在体内，L-精氨酸处理的小鼠出血后伤口部位IL-6释放的增加有所减少。此外，与接受载体处理的小鼠相比，接受L-精氨酸的出血动物伤口液体中的IL-10水平显著升高。此外，L-精氨酸可恢复出血后降低的皮肤和肌肉血流。