Department of Surgery, Pathology and Immunology, Washington University School of Medicine, St. Louis, MO 63110, USA.
Biochem Biophys Res Commun. 2010 Aug 20;399(2):251-5. doi: 10.1016/j.bbrc.2010.07.063. Epub 2010 Jul 30.
Long term function of human lung allografts is hindered by development of chronic rejection manifested as Bronchiolitis Obliterans Syndrome (BOS). We have previously identified the development of antibodies (Abs) following lung transplantation to K-alpha1-tubulin (KAT), an epithelial surface gap junction cytoskeletal protein, in patients who develop BOS. However, the biochemical and molecular basis of the interactions and signaling cascades mediated by KAT Abs are yet to be defined. In this report, we investigated the biophysical basis of the epithelial cell membrane surface interaction between KAT and its specific Abs. Towards this, we analyzed the role of the lipid raft-domains in the membrane interactions which lead to cell signaling and ultimately increased growth factor expression. Normal human bronchial epithelial (NHBE) cells, upon specific ligation with Abs to KAT obtained either from the serum of BOS(+) patients or monoclonal KAT Abs, resulted in upregulation of growth factors VEGF, PDGF, and bFGF (6.4+/-1.1-, 3.2+/-0.9-, and 3.4+/-1.1-fold increase, respectively) all of which are important in the pathogenesis of BOS. To define the role for lipid raft in augmenting surface interactions, we analyzed the changes in the growth factor expression pattern upon depletion and enrichment with lipid raft following the ligation of the epithelial cell membranes with Abs specific for KAT. NHBE cells cultured in the presence of beta-methyl cyclodextran (betaMCD) had significantly reduced growth factor expression (1.3+/-0.3, vs betaMCD untreated being 6.4+/-1.1-fold increase) upon stimulation with KAT Abs. Depletion of cholesterol on NHBE cells upon treatment with betaMCD also resulted in decreased partitioning of caveolin in the membrane fraction indicating a decrease in raft-domains. In conclusion, our results demonstrate an important role for lipid raft-mediated ligation of Abs to KAT on the epithelial cell membrane, which results in the upregulation of growth factor cascades involved in the pathogenesis of BOS following human lung transplantation.
人类肺移植的长期功能受到慢性排斥反应的阻碍,表现为闭塞性细支气管炎综合征(BOS)。我们之前已经在发生 BOS 的患者中发现了肺移植后针对 K-alpha1-微管蛋白(KAT)的抗体(Abs)的发展,KAT 是一种上皮表面间隙连接细胞骨架蛋白。然而,介导 KAT Abs 的相互作用和信号级联的生化和分子基础仍有待确定。在本报告中,我们研究了 KAT 及其特异性 Abs 之间上皮细胞膜表面相互作用的生物物理基础。为此,我们分析了脂质筏域在导致细胞信号传导并最终增加生长因子表达的膜相互作用中的作用。正常的人支气管上皮(NHBE)细胞,在用来自 BOS(+)患者的血清或单克隆 KAT Abs 特异性结合的 KAT Abs 进行特异性连接后,导致生长因子 VEGF、PDGF 和 bFGF 的表达上调(分别增加 6.4+/-1.1-、3.2+/-0.9-和 3.4+/-1.1 倍),所有这些都在 BOS 的发病机制中很重要。为了确定脂质筏在增强表面相互作用中的作用,我们分析了在用 Abs 特异性结合 KAT 连接上皮细胞膜后,脂质筏的耗竭和富集对生长因子表达模式的影响。在存在β-甲基环糊精(βMCD)的情况下培养的 NHBE 细胞在用 KAT Abs 刺激后,生长因子表达显著降低(1.3+/-0.3,与未经βMCD 处理的相比增加了 6.4+/-1.1 倍)。用βMCD 处理 NHBE 细胞还会导致质膜部分中窖蛋白的分布减少,表明筏域减少。总之,我们的结果表明,脂质筏介导的 Abs 与上皮细胞膜上的 KAT 的结合在人类肺移植后闭塞性细支气管炎综合征发病机制中涉及的生长因子级联的上调中起重要作用。
