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1 PDGFB can mediate the development of mouse spinal tumors
3 creased expression of EMP-1, NOTCH-1, FLT-1, PDGFB, and several other genes that may contribute to th
6 n were positive for fusion of the COL1A1 and PDGFB loci in 7 patients; and RT-PCR showed the COL1A1-P
7 of three genes (coding for CXCR7, ITGB2, and PDGFB) significantly inhibits C. pneumoniae entry, but t
9 CTTNBP2, MYC (alias c-myc), PTEN, MEN1, and PDGFB] in six nonrecurrent and seven recurrent radical p
10 alysis of the array data identified NFIB and PDGFB as the 2 major candidate target oncogenes that may
11 past 2 years, 3 genes (SLC20A2, PDGFRB, and PDGFB) were identified as causative of primary familial
13 results confirmed the association of VWF and PDGFB with VTE after correction for multiple testing, wh
15 cell genes platelet-derived growth factor B (PDGFB) and vascular endothelial cell growth factor recep
17 naling via platelet-derived growth factor B (PDGFB), expressed by endothelial cells, and its receptor
32 iplatelet therapy or selective inhibition of PDGFB might reduce biliary fibrosis in patients with liv
33 this patient demonstrates that inhibition of PDGFB receptor tyrosine kinase activity can significantl
34 uced circulating serum and hepatic levels of PDGFB and significantly reduced progression of fibrosis
36 MDR2-null mice normalized hepatic levels of PDGFB within 48 hours, reducing levels of a marker of HS
38 ion that results in dermal overexpression of PDGFB and favors the development of fibrotic tumors migh
40 reveals that it is not just the presence of PDGFB, but how it is presented to pericytes, that determ
45 e Akt pathway and collaborates with K-Ras or PDGFB in the development and progression of two major ty
46 on decreased expression of oncogenes (PDGFA, PDGFB, and TGFB1) and increased expression of tumor supp
47 arkers near PDGFalpha (PDGFA) and PDGFbeta, (PDGFB) also failed to maintain significance after correc
49 elet-derived growth factor beta polypeptide [PDGFB], vascular endothelial growth factor [VEGF], vascu
51 involving 9p23-p22.3 (NFIB) and 22q12-qter (PDGFB) may be of importance for disease progression in a
55 moving inhibitory regulatory elements in the PDGFB mRNA, we are able to substantially elevate its exp
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