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1 PLGF significantly increased BBB permeability in NP plas
2 PLGFs elicit diverse biological effects via the activati
3 the C-terminus of placental growth factor-2 (PLGF-2) was selected to enhance the activity of IFNalpha
5 four different splice isoforms of VEGF-A and PLGF, each of which binds to different combinations of t
9 acts through iron to induce pro-arteriogenic PLGF, suggesting iron supplementation as a novel potenti
11 (SIFalpha) by fusing the positively charged PLGF-2 peptide to the C-terminus of the human IFNalpha.
12 expression of the proinflammatory cytokines PLGF (OMIM 601121), TGFbeta (OMIM 190180), END1 (OMIM +1
13 actor (VEGF)/placenta-derived growth factor (PLGF) and soluble Fms-like tyrosine kinase-1 (sFLT-1, th
14 luded, among others, Placenta Growth Factor (PLGF) and Vascular Endothelial Growth Factor (VEGF), bot
15 h factor (VEGF) and placental growth factor (PLGF) are increased in the maternal circulation during p
20 ression of VEGF and Placental growth factor (PLGF) in TNBCs, and inhibited tumor cell migration in vi
22 rete high levels of placental growth factor (PLGF), LLC cells produce high levels of VEGF, but low le
25 xpressed monomers of placenta growth factor (PLGF)129 and vascular endothelial growth factor (VEGF)16
27 human and primate embryonic hearts and find PLGF shows a biphasic expression pattern, as it is expre
34 reviously showed that elevated FSS increases PLGF in a reactive oxygen species (ROS)-dependent fashio
35 develop in all women with high sFLT-1 or low PLGF levels, and it also occurs in some women with low s
36 We also demonstrate the presence of natural PLGF/VEGF heterodimers in the conditioned media of vario
37 We discover that only the application of PLGF modRNA at early time points of hESC-CM differentiat
40 e also confirm in vivo beneficial effects of PLGF modRNA for development of human heart progenitor-de
41 s was restored to LLC cells by expression of PLGF, strongly suggesting that the angiogenic phenotype
42 EGF-induced angiogenesis by the formation of PLGF/VEGF heterodimers in cells producing both factors.
45 e that pharmacologically distinct subsets of PLGF receptors exist that distinguish between cyclic-PA
52 mbilical vein endothelial cells reveals that PLGF/VEGF heterodimers and VEGF165 homodimers, but not P
54 on patterns were established among the three PLGFs by monitoring changes in intracellular Ca2+ in NIH
56 her, we identify the previously unrecognized PLGF-related transcriptional networks driven by EOMES an
57 To determine which HO-1 product upregulates PLGF, co-cultures were treated with a CO donor (CORM-A1)