Interaction of SP-A (surfactant protein A) with bacterial rough lipopolysaccharide (Re-LPS), and effects of SP-A on the binding of Re-LPS to CD14 and LPS-binding protein

Cristina Casals; Fernando Sánchez-Barbero; Ignacio García-Verdugo; Katrin Soldau; Peter?S. Tobias

摘要

pSP-A (surfactant protein A) is a lipid-binding collectin primarily involved in innate lung immunity. SP-A interacts with the bacterial rough LPS (lipopolysaccharide) Re-LPS (Re595 mutant of LPS from iSalmonella minnesota/i), but not with smooth LPS. In the present study, we first examined the characteristics of the interaction of human SP-A with Re-LPS. Fluorescence intensity and anisotropy measurements of FITC-labelled Re-LPS in the presence and absence of SP-A indicated that SP-A bound to Re-LPS in solution in a Casup2+/sup-independent manner, with a dissociation constant of 2.8×10sup?8/sup M. In the presence of calcium, a high-mobility complex of SP-A and [sup3/supH]Rb-LPS (Rb mutant of LPS from iEscherichia coli/i strain LCD 25) micelles was formed, as detected by sucrose density gradients. Re-LPS aggregation induced by SP-A was further characterized by light scattering. On the other hand, human SP-A inhibited TNF-α (tumour necrosis factor-α) secretion by human macrophage-like U937 cells stimulated with either Re-LPS or smooth LPS. We further examined the effects of human SP-A on the binding of Re-LPS to LBP (LPS-binding protein) and CD14. SP-A decreased the binding of Re-LPS to CD14, but not to LBP, as detected by cross-linking experiments with sup125/supI-ASD-Re-LPS [sup125/supI-labelled sulphosuccinimidyl-2-(ip/i-azidosalicylamido)-1,3-dithiopropionate derivative of Re-LPS] and fluorescence analysis with FITC-Re-LPS. When SP-A, LBP and CD14 were incubated together, SP-A reduced the ability of LBP to transfer sup125/supI-ASD-Re-LPS to CD14. These SP-A effects were not due to the ability of SP-A to aggregate Re-LPS in the presence of calcium, since they were observed in both the absence and the presence of calcium. These studies suggest that SP-A could contribute to modulate Re-LPS responses by altering the competence of the LBP–CD14 receptor complex./p

机译：SP-A（表面活性蛋白A）是一种脂质结合型集合蛋白，主要参与先天性肺免疫。 SP-A与细菌粗糙的LPS（脂多糖）Re-LPS（来自明尼苏达沙门氏菌的LPS的Re595突变体）相互作用，但不与光滑LPS相互作用。在本研究中，我们首先研究了人SP-A与Re-LPS相互作用的特征。在存在和不存在SP-A的情况下，FITC标记的Re-LPS的荧光强度和各向异性测量表明，SP-A以Ca 2 + 独立的方式与溶液中的Re-LPS结合，解离常数为2.8×10 ？8 ＆nbsp; M。在钙存在下，SP-A和[ 3 H] Rb-LPS（大肠杆菌 LCD 25菌株的LPS的Rb突变体）高迁移率复合物如通过蔗糖密度梯度所检测到的那样，形成了α。 SP-A诱导的Re-LPS聚集通过光散射进一步表征。另一方面，人SP-A抑制了被Re-LPS或平滑LPS刺激的人巨噬细胞样U937细胞分泌的TNF-α（肿瘤坏死因子-α）。我们进一步检查了人SP-A对Re-LPS与LBP（LPS结合蛋白）和CD14结合的影响。通过与 125 I-ASD-Re-LPS [ 125 ]的交联实验发现，SP-A降低了Re-LPS与CD14的结合，但并未降低与LBP的结合。 I-标记的磺基琥珀酰亚胺基-2-（ p -叠氮基水杨酰胺基）-1,3-二硫代丙酸酯的Re-LPS衍生物]，并用FITC-Re-LPS进行荧光分析。将SP-A，LBP和CD14一起孵育时，SP-A降低了LBP将 125 I-ASD-Re-LPS转移到CD14的能力。这些SP-A的作用不是由于SP-A在钙存在下聚集Re-LPS的能力，因为它们在钙的存在和不存在下均被观察到。这些研究表明，SP-A可能通过改变LBP-CD14受体复合物的能力来调节Re-LPS反应。

Interaction of SP-A (surfactant protein A) with bacterial rough lipopolysaccharide (Re-LPS), and effects of SP-A on the binding of Re-LPS to CD14 and LPS-binding protein

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