Sheibani N, Newman P J, Frazier W A
Washington University School of Medicine, Department of Biochemistry and Molecular Biophysics, St. Louis, Missouri 63110, USA.
Mol Biol Cell. 1997 Jul;8(7):1329-41. doi: 10.1091/mbc.8.7.1329.
Expression of thrombospondin-1 (TS1) in polyoma middle-sized T (tumor)-transformed mouse brain endothelial cells (bEND.3) restores a normal phenotype and suppresses their ability to form hemangiomas in mice. We show that TS1 expression results in complete suppression of platelet-endothelial cell adhesion molecule-1 (PECAM-1) expression and altered cell-cell interactions in bEND.3 cells. To further investigate the role of PECAM-1 in regulation of endothelial cell-cell interactions and morphogenesis, we expressed human (full length) or murine (delta 15) PECAM-1 isoforms in TS1-transfected bEND.3 (bEND/TS) cells. Expression of either human or murine PECAM-1 resulted in an enhanced ability to organize and form networks of cords on Matrigel, an effect that was specifically blocked by antibodies to PECAM-1. Anti-PECAM-1 antibodies also inhibited tube formation in Matrigel by normal human umbilical vein endothelial cells. However, PECAM-1-transfected bEND/TS cells did not regain the ability to form hemangiomas in mice and the expressed PECAM-1, unlike the endogenous PECAM-1 expressed in bEND.3 cells, failed to localize to sites of cell-cell contact. This may be, in part, attributed to the different isoforms of PECAM-1 expressed in bEND.3 cells. Using reverse transcription-polymerase chain reaction, we determined that bEND.3 cells express mRNA encoding six different PECAM-1 isoforms, the isoform lacking both exons 14 and 15 (delta 14&15) being most abundant. Expression of the murine delta 14&15 PECAM-1 isoform in bEND/TS cells resulted in a similar phenotype to that described for the full-length human or murine delta 15 PECAM-1 isoform. The delta 14&15 isoform, despite the lack of exon 14, failed to localize to sites of cell-cell contact even in clones that expressed it at very high levels. Thus, contrary to recent reports, lack of exon 14 is not sufficient to result in junctional localization of PECAM-1 isoforms in bEND/TS cells.
血小板反应蛋白-1(TS1)在多瘤中T(肿瘤)转化的小鼠脑内皮细胞(bEND.3)中的表达可恢复正常表型,并抑制其在小鼠体内形成血管瘤的能力。我们发现TS1的表达导致血小板内皮细胞黏附分子-1(PECAM-1)表达完全受抑制,并改变了bEND.3细胞中的细胞间相互作用。为了进一步研究PECAM-1在调节内皮细胞间相互作用和形态发生中的作用,我们在转染了TS1的bEND.3(bEND/TS)细胞中表达了人(全长)或小鼠(δ15)PECAM-1异构体。人或小鼠PECAM-1的表达均导致在基质胶上组织和形成索状网络的能力增强,这一效应被PECAM-1抗体特异性阻断。抗PECAM-1抗体也抑制正常人脐静脉内皮细胞在基质胶中的管形成。然而,转染了PECAM-1的bEND/TS细胞在小鼠体内并未恢复形成血管瘤的能力,且所表达的PECAM-1与bEND.3细胞中内源性表达的PECAM-1不同,未能定位于细胞间接触部位。这可能部分归因于bEND.3细胞中表达的PECAM-1的不同异构体。通过逆转录-聚合酶链反应,我们确定bEND.3细胞表达编码六种不同PECAM-1异构体的mRNA,其中缺少外显子14和15(δ14&15)的异构体最为丰富。在bEND/TS细胞中表达小鼠δ14&15 PECAM-1异构体导致的表型与全长人或小鼠δ15 PECAM-1异构体所描述的表型相似。δ14&15异构体尽管缺少外显子14,但即使在表达水平非常高的克隆中也未能定位于细胞间接触部位。因此,与最近的报道相反,缺少外显子14不足以导致PECAM-1异构体在bEND/TS细胞中定位于连接部位。
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