Mikols Cassandra L, Yan Le, Norris Jin Y, Russell Tonya D, Khalifah Anthony P, Hachem Ramsey R, Chakinala Murali M, Yusen Roger D, Castro Mario, Kuo Elbert, Patterson G Alexander, Mohanakumar Thalachallour, Trulock Elbert P, Walter Michael J
Division of Pulmonary and Critical Care Medicine, Washington University School of Medicine, St. Louis, MO 63110, USA.
Am J Respir Crit Care Med. 2006 Aug 15;174(4):461-70. doi: 10.1164/rccm.200512-1886OC. Epub 2006 May 25.
Bronchiolitis obliterans syndrome is the leading cause of chronic lung allograft dysfunction. We have demonstrated that respiratory viral infection is a bronchiolitis obliterans syndrome risk factor and virus-dependent injury induces expression of innate airway epithelial genes belonging to the interleukin (IL)-12 family. Thus, we hypothesized that epithelial cell IL-12 family members could mediate lung allograft dysfunction.
We used mouse and human allograft specimens to evaluate the role of epithelial cell IL-12 family members in allograft dysfunction associated with and without viral infection.
Murine and human IL-12 family members were characterized and manipulated in allografts and then correlated with epithelial cell injury, immune cell accumulation, and collagen deposition.
In a mouse model of lung transplantation, concurrent viral infection and allogeneic transplantation increased epithelial injury and this was followed by exaggerated accumulation of macrophages and collagen deposition. This virus-driven allograft dysfunction was associated with an epithelial innate response manifested by a synergistic increase in the production of the macrophage chemoattractant IL-12 p80 (p80), but not IL-12 or IL-23. Blockade or overexpression of donor epithelial p80 resulted in a corresponding abrogation or enhancement of macrophage accumulation and allograft dysfunction. We extended these findings to human recipients with viral infection and transplant bronchitis and again observed excessive epithelial p80 expression that correlated with increased macrophage accumulation.
These experiments support a role for an enhanced epithelial innate response as a central process in allograft dysfunction and identify the macrophage chemoattractant p80 as an innate epithelial effector of disease progression.
闭塞性细支气管炎综合征是慢性肺移植功能障碍的主要原因。我们已经证明,呼吸道病毒感染是闭塞性细支气管炎综合征的一个危险因素,病毒依赖性损伤可诱导属于白细胞介素(IL)-12家族的先天性气道上皮基因的表达。因此,我们推测上皮细胞IL-12家族成员可能介导肺移植功能障碍。
我们使用小鼠和人类移植标本评估上皮细胞IL-12家族成员在伴有和不伴有病毒感染的移植功能障碍中的作用。
对小鼠和人类IL-12家族成员在移植体中进行表征和调控,然后将其与上皮细胞损伤、免疫细胞积聚和胶原沉积相关联。
在肺移植的小鼠模型中,同时发生的病毒感染和同种异体移植增加了上皮损伤,随后巨噬细胞积聚和胶原沉积加剧。这种病毒驱动的移植功能障碍与一种上皮先天性反应相关,表现为巨噬细胞趋化因子IL-12 p80(p80)而非IL-12或IL-23的产生协同增加。供体上皮p80的阻断或过表达导致巨噬细胞积聚和移植功能障碍相应的消除或增强。我们将这些发现扩展到患有病毒感染和移植性支气管炎的人类受者,再次观察到上皮p80过度表达与巨噬细胞积聚增加相关。
这些实验支持增强的上皮先天性反应作为移植功能障碍的核心过程的作用,并确定巨噬细胞趋化因子p80是疾病进展的先天性上皮效应物。
