肺对内皮抗原抗体的摄取:血管免疫靶向的关键决定因素。
Lung uptake of antibodies to endothelial antigens: key determinants of vascular immunotargeting.
作者信息
Danilov S M, Gavrilyuk V D, Franke F E, Pauls K, Harshaw D W, McDonald T D, Miletich D J, Muzykantov V R
机构信息
Department of Anesthesiology, University of Illinois at Chicago, Chicago, IL 60612, USA.
出版信息
Am J Physiol Lung Cell Mol Physiol. 2001 Jun;280(6):L1335-47. doi: 10.1152/ajplung.2001.280.6.L1335.
Vascular immunotargeting is a mean for a site-selective delivery of drugs and genes to endothelium. In this study, we compared recognition of pulmonary and systemic vessels in rats by candidate carrier monoclonal antibodies (MAbs) to endothelial antigens platelet endothelial cell adhesion molecule (PECAM)-1 (CD31), intercellular adhesion molecule (ICAM)-1 (CD54), Thy-1.1 (CD90.1), angiotensin-converting enzyme (ACE; CD143), and OX-43. Tissue immunostaining showed that endothelial cells were Thy-1.1 positive in capillaries but negative in large vessels. In the lung, anti-ACE MAb provided a positive staining in 100% capillaries vs. 5-20% capillaries in other organs. Other MAbs did not discriminate between pulmonary and systemic vessels. We determined tissue uptake after infusion of 1 microg of (125)I-labeled MAbs in isolated perfused lungs (IPL) or intravenously in intact rats. Uptake in IPL attained 46% of the injected dose (ID) of anti-Thy-1.1 and 20-25% ID of anti-ACE, anti-ICAM-1, and anti-OX-43 (vs. 0.5% ID of control IgG). However, after systemic injection at this dose, only anti-ACE MAb 9B9 displayed selective pulmonary uptake (16 vs. 1% ID/g in other organs). Anti-OX-43 displayed low pulmonary (0.5% ID/g) but significant splenic and cardiac uptake (7 and 2% ID/g). Anti-Thy-1.1 and anti-ICAM-1 displayed moderate pulmonary (4 and 6% ID/g, respectively) and high splenic and hepatic uptake (e.g., 18% ID/g of anti-Thy-1.1 in spleen). The lung-to-blood ratio was 5, 10, and 15 for anti-Thy-1.1, anti-ACE, and anti-ICAM-1, respectively. PECAM antibodies displayed low pulmonary uptake in perfusion (2% ID) and in vivo (3-4% ID/g). However, conjugation with streptavidin (SA) markedly augmented pulmonary uptake of anti-PECAM in perfusion (10-54% ID, depending on an antibody clone) and in vivo (up to 15% ID/g). Therefore, ACE-, Thy-1.1-, ICAM-1-, and SA-conjugated PECAM MAbs are candidate carriers for pulmonary targeting. ACE MAb offers a high selectivity of pulmonary targeting in vivo, likely because of a high content of ACE-positive capillaries in the lungs.
血管免疫靶向是一种将药物和基因位点选择性递送至内皮细胞的方法。在本研究中,我们比较了候选载体单克隆抗体(MAb)对大鼠肺血管和体循环血管中内皮抗原血小板内皮细胞黏附分子(PECAM)-1(CD31)、细胞间黏附分子(ICAM)-1(CD54)、Thy-1.1(CD90.1)、血管紧张素转换酶(ACE;CD143)和OX-43的识别情况。组织免疫染色显示,内皮细胞在毛细血管中Thy-1.1呈阳性,但在大血管中呈阴性。在肺中,抗ACE单克隆抗体在100%的毛细血管中呈阳性染色,而在其他器官中为5 - 20%的毛细血管呈阳性。其他单克隆抗体无法区分肺血管和体循环血管。我们在离体灌注肺(IPL)中或在完整大鼠静脉内注射1μg(125)I标记的单克隆抗体后测定了组织摄取情况。在IPL中,抗Thy-1.1的摄取量达到注射剂量(ID)的46%,抗ACE、抗ICAM-1和抗OX-43的摄取量为ID的20 - 25%(而对照IgG为ID的0.5%)。然而,以该剂量进行全身注射后,只有抗ACE单克隆抗体9B9表现出选择性肺摄取(肺摄取量为16% ID/g,其他器官为1% ID/g)。抗OX-43在肺中的摄取量较低(0.5% ID/g),但在脾脏和心脏中有显著摄取(分别为7%和2% ID/g)。抗Thy-1.1和抗ICAM-1在肺中的摄取量中等(分别为4%和6% ID/g),在脾脏和肝脏中的摄取量较高(例如,抗Thy-1.1在脾脏中的摄取量为18% ID/g)。抗Thy-1.1、抗ACE和抗ICAM-1的肺血比分别为5、10和15。PECAM抗体在灌注时肺摄取量较低(2% ID),在体内为(3 - 4% ID/g)。然而,与链霉亲和素(SA)偶联显著增加了抗PECAM在灌注时的肺摄取量(10 - 54% ID,取决于抗体克隆)和体内摄取量(高达15% ID/g)。因此,ACE、Thy-1.1、ICAM-1和SA偶联的PECAM单克隆抗体是肺靶向的候选载体。ACE单克隆抗体在体内具有高度的肺靶向选择性,可能是因为肺中ACE阳性毛细血管含量较高。
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