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1 ent precursors of hepatoblasts and thence of hepatocytic and biliary epithelia, are located in ductal
2 red to host hepatocytes, differentiated into hepatocytic and biliary epithelial cells, and generated
3 ar1-positive, or CK19-positive, has revealed hepatocytic and biliary poles, respectively, in the DRs.
5 iron-restricted media, reduced its growth in hepatocytic and epithelial cells, and impaired its acqui
7 dary inflammatory cellular reaction, induces hepatocytic apoptosis and suggest that future therapeuti
8 V/HIV envelope proteins cooperatively induce hepatocytic apoptosis by activating a novel downstream S
12 ) of F. tularensis grown in the FL83B murine hepatocytic cell line compared to that of F. tularensis
13 uman HBV nucleocapsids in a variety of human hepatocytic cell lines and in primary rat hepatocytes an
14 These were predifferentiated in vitro into hepatocytic cells and delivered to the liver by splenic
16 storation of DDD expression in DDD-deficient hepatocytic cells, we found that both caspase-3 sites in
20 ate lobular lymphoplasmacytic hepatitis with hepatocytic coagulative necrosis, but the hydrogenase mu
22 ure hepatocyte markers are expressed; mature hepatocytic differentiation and cell size are also augme
23 9.2% displayed histological diversity: focal hepatocytic differentiation and ductular areas (mixed-IC
24 ividually throughout the liver, resulting in hepatocytic differentiation by tumor cells with concomit
25 Sustained activation of mTOR impaired the hepatocytic differentiation capability of these cells as
27 l to study factors that may be important for hepatocytic differentiation from precursor cells and a m
28 and a fibroblast feeder layer that supports hepatocytic differentiation from precursor epithelial (o
29 ome P450 (CYP) enzymes, and other markers of hepatocytic differentiation in SHPCs during the protract
30 but differentially express tumorigenicity or hepatocytic differentiation in the liver depending on ho
31 cell pool, impaired migration, and decreased hepatocytic differentiation in vivo, as demonstrated by
32 dged by high expression of c-kit and lack of hepatocytic differentiation markers, whereas OV1(high) c
35 further identified miR-148a as an inducer of hepatocytic differentiation that is down-regulated in HC
36 e alpha/NUMB/NOTCH pathway and an inducer of hepatocytic differentiation that when deregulated promot
37 e-like cells also expressed other markers of hepatocytic differentiation, including albumin, transfer
43 monolayered Madin-Darby canine kidney cells, hepatocytic epithelial cells, which typically feature ti
44 ation, mainly cells with a single phenotype, hepatocytic (expressing AFP and albumin) or bile ductula
45 suggest that Mist1 partially induces mature hepatocytic expression and function accompanied by the d
49 c steatohepatitis significantly up-regulated hepatocytic HRG expression, which was associated with M1
52 ontrast, cotransfection into an AFP-negative hepatocytic line produced moderate activation of the AFP
53 or (rat liver epithelial [RLE]) cells toward hepatocytic lineage affects the response to TNFalpha-med
55 in cell culture and differentiated along the hepatocytic lineage in the presence of dexamethasone, ex
57 factor, Mist1, induced expression of mature hepatocytic markers such as carbamoyl-phosphate syntheta
60 transmission electron microscopy, and fewer hepatocytic microvilli were evident, indicating impaired
61 f human fetal hepatocytes (HFHs) that retain hepatocytic morphology and gene expression patterns for
62 ve (HNF4alpha(+)) biphenotypic cells showing hepatocytic morphology appeared near EpCAM(+) ductular s
64 C engrafted into the parenchyma exhibited an hepatocytic phenotype and generated new hepatic cord str
65 These problems include the rapid loss of the hepatocytic phenotype in primary culture and the limited
69 stem cells derived from the bone marrow have hepatocytic potential, a topic that has been covered ext
72 receptor system to elucidate the pathway of hepatocytic processing of ligands such as asialoorosomuc
73 ic-transplant recipients are allowed to age, hepatocytic progeny of BAG2-GN6TF cells proliferate to f
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