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1 ds to a castration-resistant disease that is highly metastatic.
2 tics of human osteosarcomas, including being highly metastatic.
3 e C-alpha (PKC-alpha), is both malignant and highly metastatic.
4  ablation, chemo- and radiotherapy, but also highly metastatic.
5 strogen unresponsive, fully tumorigenic, and highly metastatic.
6                     ARCaP is tumorigenic and highly metastatic.
7 ed as postpartum breast cancer (PPBC) and is highly metastatic.
8                   Colorectal cancer (CRC) is highly metastatic.
9 ancers arising from neuroendocrine cells are highly metastatic.
10             PKCdelta levels are increased in highly metastatic 13762NF mammary tumor cells (MTLn3) co
11                   In vitro incubation of the highly metastatic 253J B-V cells and the IFN-alpha-resis
12 able to suppress the metastatic phenotype in highly metastatic 4T1 and MDA-MB-231 SCP28 cells, as wel
13 w aspirates and mouse models challenged with highly metastatic 4T1 breast cancer cells, we demonstrat
14 tand the chemoresistance mechanism using the highly metastatic 4T1 breast cancer model, which emulate
15 is associated with doxorubicin resistance of highly metastatic 4T1 breast cancer.
16 py was tested against weakly immunogenic and highly metastatic 4T1 breast tumor using SU6668, an angi
17 y, cleaved caspase-3 decreased by 45% in the highly metastatic 4T1 cells after hypoxia.
18 e nonmetastatic 67NR cells and lowest in the highly metastatic 4T1 cells.
19 C expression by small interfering RNA in the highly metastatic 4T1 mammary tumor cell line expressing
20 erapy strategy in the weakly immunogenic and highly metastatic 4T1 murine mammary cancer model.
21                                       In the highly metastatic A375-M human melanoma cells, p190-RhoC
22                    Transfection of AP-2 into highly metastatic A375SM melanoma cells (AP-2-negative a
23         First, the PLD2 gene was silenced in highly metastatic, aggressive breast cancer cells (MDA-M
24                                          The highly metastatic amelanotic C8161 human melanoma line w
25 o a transition from androgen-dependence to a highly metastatic and androgen refractory (androgen depl
26  (TN) breast cancers (ER(-)PR(-)HER2(-)) are highly metastatic and associated with poor prognosis.
27          Pancreatic ductal adenocarcinoma is highly metastatic and current preoperative evaluation of
28                       Because the disease is highly metastatic and difficult to diagnosis until late
29 programmed cell death protein 1 (anti-PD-1), highly metastatic and fibrotic, and secreted TGFbeta/CXC
30 lectively knock down GnT-V expression in the highly metastatic and invasive human breast carcinoma ce
31                   Cells lacking vinculin are highly metastatic and motile.
32 xpressed pluripotency-associated genes, were highly metastatic and showed long-term in vivo tumorigen
33 cer cell lines and selected subpopulation of highly metastatic and tumorigenic cells (ALDH(high)) str
34 hotopic growth and spontaneous metastasis of highly metastatic, androgen-insensitive caveolin-1-secre
35 ane glycoprotein found on the surface of the highly metastatic ascites 13762 rat mammary adenocarcino
36  abundantly expressed on the cell surface of highly metastatic ascites 13762 rat mammary adenocarcino
37 viral Gag-like protein p58gag expressed in a highly metastatic ascites rat mammary adenocarcinoma has
38 f the Mr 85,000 standard form of CD44 in the highly metastatic AT3.1 rat prostatic cells greatly supp
39  containing this region was transferred into highly metastatic AT6.3 rat prostate cancer cells by mic
40 f B16 melanoma and at much reduced levels in highly metastatic B16 variants.
41  that it was substantially down-regulated in highly metastatic B16-F10 melanoma cells, which contribu
42                   In the poorly immunogenic, highly metastatic, B16/F10.9 tumor model a dramatic redu
43 d SENP7L levels lessens the dissemination of highly metastatic BCa cells to the lungs from primary im
44                                Here, using a highly metastatic breast cancer (4T1) model, we show tha
45  breast carcinoma and on the cell surface of highly metastatic breast cancer cell line MDA-MB-231.
46 re linked to MCT expression in MDA-MB-231, a highly metastatic breast cancer cell line.
47 e show that the loss of KiSS-1 expression in highly metastatic breast cancer cell lines correlates di
48 e 2, I-branching enzyme, is overexpressed in highly metastatic breast cancer cell lines of human and
49 type plasminogen activator, and cytokines in highly metastatic breast cancer cell lines.
50                The restoration of miR-203 in highly metastatic breast cancer cells inhibited tumor ce
51 onditioning of naive mice with exosomes from highly metastatic breast cancer cells revealed the accum
52               These genes are upregulated in highly metastatic breast cancer cells, and their increas
53 verexpression of protein kinase Calpha), and highly metastatic breast cancer cells.
54  miR-203 was significantly down-regulated in highly metastatic breast cancer cells.
55  we found that stable SDPR overexpression in highly metastatic breast cancer model cell lines inhibit
56 on of hyaluronan synthase 2 (HAS2) occurs in highly metastatic breast cancer stem-like cells (CSC) de
57 ve breast cancer (TNBC) is an aggressive and highly metastatic breast cancer subtype.
58             Overexpression of AP-2alpha into highly metastatic breast cell lines did not alter KiSS-1
59  is greater than that in normal tissue, with highly metastatic breast epithelial cells expressing the
60  Furthermore, blockade of activated Stat3 in highly metastatic C4 cells significantly suppressed the
61 e expression of a dominant-negative Stat3 in highly metastatic C4 tumor cells inhibited the MMP-2 pro
62 K-1735 melanoma system, we demonstrated that highly metastatic C4, M2, and X21 tumor cells express el
63 l that Trp consumption and Kyn production by highly metastatic cancer cells (HT29) were significantly
64 and invasion and that MTA1 overexpression in highly metastatic cancer cells drives cell migration and
65                                          For highly metastatic cancer cells, the pH measured at the s
66          Nasopharyngeal carcinoma (NPC) is a highly metastatic cancer that is consistently associated
67                     Uveal melanoma (UM) is a highly metastatic cancer that, in contrast to cutaneous
68 cells from hepatocellular carcinoma (HCC), a highly metastatic cancer, undergo epithelial to amoeboid
69  but significantly reduced the likelihood of highly metastatic cancer.
70 si-mesenchymal state that is associated with highly metastatic capabilities and poor survival of pati
71                           In conclusion, the highly metastatic capability of a unique TS subpopulatio
72 y a poorly metastatic cell line to that by a highly metastatic cell line 24 h after injection in the
73 -2 mRNA stabilization in MDA-MB-231 cells, a highly metastatic cell line derived from a human mammary
74 ential reversal of oncogenic properties of a highly metastatic cell line with the introduction of non
75 ially expressed (greater than 2-fold) in all highly metastatic cell lines relative to their reference
76                        The undifferentiated, highly metastatic cell lines with high metastatic potent
77               We found that in vivo selected highly metastatic cell populations showed little genetic
78                                              Highly metastatic cells (MDA-MB-435) expressing high lev
79              Within minutes of adhesion, the highly metastatic cells acquire the ability of enhanced
80 subset of drug-resisting, self-renewing, and highly metastatic cells called tumor initiating cells or
81 ere we show that loss of c-KIT expression in highly metastatic cells correlates with loss of expressi
82 at up-regulation of MCAM/MUC18 expression in highly metastatic cells correlates with loss of expressi
83 ration of miR-10b antagomirs to mice bearing highly metastatic cells does not reduce primary mammary
84                                              Highly metastatic cells evade this tumor-suppressive pat
85 ompared with poorly metastatic cancer cells, highly metastatic cells expressed increased levels of th
86                                              Highly metastatic cells growing in culture constitutivel
87                                              Highly metastatic cells growing in the prostate expresse
88 usly shown that enforced c-KIT expression in highly metastatic cells inhibited tumor growth and metas
89 ational regulator, and its downregulation in highly metastatic cells leads to the lengthening of 3' u
90                 Silencing of IL-13Ralpha2 in highly metastatic cells led to a decrease in adhesion ca
91            Does it arise from rare, variant, highly metastatic cells or does a primary tumor progress
92                      Introduction of Psap in highly metastatic cells significantly reduced the occurr
93                               Loss of CC3 in highly metastatic cells such as SCLC might render them r
94                                              Highly metastatic cells survived to produce numerous lun
95                                     When the highly metastatic cells were compared with their low met
96                    The pH at the surfaces of highly metastatic cells within tumors was found to be ab
97  kinase expression was first demonstrated in highly metastatic cells, whilst re-expression of the pro
98 s phosphoinositide 3-kinase, AKT, and SRC in highly metastatic cells.
99 n upon miR-200 overexpression toward that of highly metastatic cells.
100 elta levels were relatively increased in the highly metastatic cells.
101  transcripts displaying reduced stability in highly metastatic cells.
102 gainst poorly metastatic cells compared with highly metastatic cells.
103 ignificantly impairs the bone progression of highly metastatic cells.
104 etastatic variants, suggest that not only do highly-metastatic cells display constitutively elevated
105 g ligand activation of the EGFR, but only in highly-metastatic cells.
106 ecause they preferentially activate c-Src in highly-metastatic cells.
107 ces neoplastic transformation and promotes a highly metastatic cellular phenotype.
108 ch, in turn, are likely to contribute to the highly metastatic character of NPC.
109  cancers in humans due to late detection and highly metastatic characteristics.
110                Overexpression of NOS II in a highly metastatic clone by transfection with NOS II gene
111                                            A highly metastatic clone of K1735 cells, SW1-C, and its s
112                 Furthermore, both poorly and highly metastatic clones contained an identical p53 muta
113                                              Highly metastatic clones exhibited higher levels of NOS
114 rays to analyze the secretomes of poorly and highly metastatic colorectal cancer cells.
115            Suppression of Akt2 expression in highly metastatic colorectal carcinoma cells inhibits th
116 e type II TGF-beta receptor (PyMT(mgko)) are highly metastatic compared with control PyMT-induced car
117 noma (NPC), an EBV-associated malignancy, is highly metastatic compared with other head and neck tumo
118 d nitrogen radicals that kill weakly but not highly metastatic CRC cells.
119                                       In the highly metastatic CT26 murine colon cancer cell line, wh
120                          Nearly 10-fold more highly metastatic CX-1 cells survive within the livers o
121 lone A and MIP-101 cells at 24 h but <15% of highly metastatic CX-1 cells.
122 ne A and MIP-101 CRC cells die, whereas many highly metastatic CX-1 CRC cells survive.
123 ndent cells but was significantly reduced in highly metastatic derivative clones.
124 an prostate carcinoma cell line PC-3 and its highly metastatic derivative PC-3M.
125                         Ovarian cancer is an highly metastatic disease characterized by ascites forma
126 s evaluated, all were demonstrated to effect highly metastatic disease involving multiple organs, alt
127 pe of a murine model of pancreatic cancer, a highly metastatic disease that frequently displays p53 m
128          Lung squamous carcinoma (LUSC) is a highly metastatic disease with a poor prognosis.
129                     Ovarian cancer (OC) is a highly metastatic disease, but no effective strategies t
130                          Ovarian cancer is a highly metastatic disease.
131                                              Highly metastatic Dunning AT3.1 rat prostate cancer cell
132 eomycin resistance gene, was introduced into highly metastatic Dunning AT6.1 prostate cancer cells by
133 xpression of a dominant-negative CDK5 in the highly metastatic Dunning AT6.3 prostate cancer cell lin
134 results in metastasis suppression in certain highly metastatic Dunning R-3327 rat prostatic cancer su
135 er to introduce human chromosome 16 into the highly metastatic Dunning rat prostatic cancer cell line
136 inally, EGFR-MET signaling was enhanced in a highly metastatic EGFR-mutant cell subpopulation, compar
137 helial (EpCAM(hi)) and quasi-mesenchymal and highly metastatic (EpCAM(lo)) cells in conventional huma
138 minyltransferase (LARGE) gene in a cohort of highly metastatic epithelial cell lines derived from bre
139               This resulted in generation of highly metastatic epithelial-to-mesenchymal transition-l
140 53(R172H) mutation were undifferentiated and highly metastatic, exhibited minimal TP53 transactivatio
141      Here we report that these tumors become highly metastatic following hemizygous deletion of the N
142 e and to an in vivo-derived subline that was highly metastatic for growth in the lungs.
143                            Osteosarcoma is a highly metastatic form of bone cancer in adolescents and
144 crine PrCa (NEPrCa), a highly aggressive and highly metastatic form of PrCa, for which there is no ef
145 c potential and its experimentally selected, highly metastatic form.
146 criptional regulation of the MMP-9 gene in a highly metastatic H-ras and v-myc transformed rat embryo
147                                              Highly metastatic H7 murine pancreatic adenocarcinoma ce
148                 Another cell line, UMRC3, is highly metastatic, having lost TBR3 and TBR2 expression.
149 xpression of TIMP2 open reading frame in the highly metastatic HCC cell line, MHCC-97L, significantly
150 votal role in regulating RUNX2 expression in highly metastatic HNSCC cells, where it was downregulate
151 ricle injection into nude mice to identify a highly metastatic human breast cancer cell line (MDA-MET
152 oRNA-146b (miR-146a/b) when expressed in the highly metastatic human breast cancer cell line MDA-MB-2
153  functionally relevant betaAR subtype in the highly metastatic human breast cancer cell line MDA-MB-2
154 timigratory and antiinvasive effects against highly metastatic human breast cancer MDA-MB-231 cells v
155 in 3F (SEMA3F) was markedly downregulated in highly metastatic human cell lines in vitro and in vivo,
156              MUC2 levels were manipulated in highly metastatic human colon cancer cells using eukaryo
157 nst proteins preferentially expressed by the highly metastatic human epidermoid carcinoma cell line,
158 eLa (human cervical cancer), HCI-H460-LNM35 (highly metastatic human lung cancer) and B16 (murine mel
159 tisense cathepsin B-expressing clones of the highly metastatic human melanoma A375M and prostate carc
160 ected the c-KIT gene into the c-KIT negative highly metastatic human melanoma cell line A375SM and su
161 al human melanocyte cell line and weakly and highly metastatic human melanoma cell lines, we presentl
162                      Medium conditioned by a highly metastatic human pancreatic cancer cell line BxPC
163 i-amino-C1-C3-alkane-sulfonic acid), against highly metastatic human pancreatic carcinoma cells injec
164                                              Highly metastatic human pancreatic carcinoma L3.6pl cell
165                   The highly tumorigenic and highly metastatic human transitional cell carcinoma (TCC
166 nvasive, murine colon cancer cells that were highly metastatic in an immunocompetent mouse model to i
167          The primary neoplasm generated is a highly metastatic islet cell carcinoma of the pancreas.
168 nscript stability measurements in poorly and highly metastatic isogenic human breast cancer lines.
169   Evidence is now provided, using weakly and highly metastatic isogenic melanoma variants, that mda-9
170                                  CD44 on the highly metastatic KM12L4 clone is more heavily substitut
171                                 In addition, highly metastatic L3.6pl cells growing in the pancreas e
172 th transformation of SB2 melanoma cells to a highly metastatic line.
173 cally defective liver stem cells (LSCs) into highly metastatic liver cancer cells in premalignant liv
174 xA also reduced motility and invasiveness of highly metastatic LOX melanoma cells.
175                          Mucin purified from highly metastatic LS-Lim6 human colon cancer cells bound
176 ated with the Epstein-Barr virus (EBV), is a highly metastatic malignant tumor.
177 e expression of CXCR4 in murine 4T1 cells, a highly metastatic mammary cancer cell line that is a mod
178           Suppression of Twist expression in highly metastatic mammary carcinoma cells specifically i
179 early completely inhibits lung metastasis of highly metastatic mammary carcinoma cells.
180       We define ECM signatures of poorly and highly metastatic mammary carcinomas and these signature
181                                      Using a highly metastatic mammary tumor cell line that expresses
182             In the mouse, the development of highly metastatic mammary tumors is associated with an a
183 icantly, the HMG-Y protein isolated from the highly metastatic MCF-7/PKC-alpha cells possesses a uniq
184 tion of methylation reduces migration of the highly metastatic MDA-MB-231 breast cancer cell line.
185 gnificantly increased the penetration of the highly metastatic MDA-MB-231 breast cancer cells across
186  20S proteasome and 26S proteasome in intact highly metastatic MDA-MB-231 breast cancer cells, result
187 urthermore, forced expression of KLF4 in the highly metastatic MDA-MB-231 breast tumor cell line was
188 n-invasive MCF7 (56%) cells, but not for the highly metastatic MDA-MB-231 cell.
189 oduced a normal human chromosome 11 into the highly metastatic MDA-MB-435 breast carcinoma cell line
190 ry matrix supported motility and invasion in highly metastatic MDA-MB-435 cells, but not in cells wit
191 s found to suppress motility and invasion in highly metastatic MDA-MB-435 cells, whereas involution m
192 nes, nor was a difference observed between a highly metastatic melanoma cell line (A375SM) or its par
193  progression, we conducted a microarray on a highly metastatic melanoma cell line in which NFAT1 expr
194 ated receptor-1 (PAR-1)] is overexpressed in highly metastatic melanoma cell lines and in patients wi
195 wth (P < 0.01) and metastasis (P < 0.001) of highly metastatic melanoma cell lines in vivo.
196  showed that inducible expression of CD82 in highly metastatic melanoma cells significantly increased
197    Forced expression of TRAF2DeltaN in HHMSX highly metastatic melanoma cells that lack Fas expressio
198 on of the invasive and migratory behavior in highly metastatic melanoma cells, similar to the overexp
199 we use an in vivo selection scheme to select highly metastatic melanoma cells.
200 anocytes, we observed variably pigmented and highly metastatic melanoma with 100% penetrance.
201 onal CDK5 knockout mice and a mouse model of highly metastatic melanoma, we found that CDK5 is dispen
202                                Exosomes from highly metastatic melanomas increased the metastatic beh
203  using retroviral vectors in EpRas cells and highly metastatic mesenchymal mouse colon carcinoma cell
204 a critical role in keeping cancer cells in a highly metastatic mesenchymal state.
205                                              Highly metastatic MeWo human melanoma cells were transfe
206                                        It is highly metastatic, migrating through lymph nodes to dist
207             To explore this possibility, the highly metastatic MMTV-PyMT mice were crossed with 25 AK
208                                 Furthermore, highly metastatic MNNG-HOS cells have increased levels o
209                                      Using a highly metastatic model of mammary cancer, we identified
210                       In vitro analysis of a highly metastatic mouse mammary tumor cell line ectopica
211                        Here we observed that highly metastatic mouse mammary tumours acquired more in
212                         Cells derived from a highly metastatic mouse model of SCCHN were used to conf
213             The two cell lines used were the highly metastatic MTLn3 cells and nonmetastatic MTC cell
214 erinuclear and at the leading edge), whereas highly metastatic MTLn3 cells have only a perinuclear di
215 beta 2m protein and RNA are not expressed in highly metastatic, multidrug-resistant MCF-7/Adr cells w
216  fluorescently labeled exosomes derived from highly metastatic murine breast cancer cells distributed
217 ting angiogenesis and lymphangiogenesis in a highly metastatic murine model of Burkitt's lymphoma (E
218 a human alveolar basal epithelial (A549) and highly metastatic murine osteosarcoma (K7M2) cells lines
219                                    PANC02-H7 highly metastatic murine pancreatic adenocarcinoma cells
220 Ab induces a substantial survival benefit in highly metastatic murine TNBC models poorly responsive t
221  vivo gene therapy modalities to counter the highly metastatic nature of human melanoma.
222 any potential link between the virus and the highly metastatic nature of MCC.
223 k between MCPyV T antigen expression and the highly metastatic nature of MCC.
224 ancreatic cancer to other organs, due to the highly metastatic nature of the disease.
225 nduce apoptosis of human melanomas including highly metastatic ones despite their low surface Fas lev
226 in the majority of osteosarcoma cases and in highly metastatic osteosarcoma cell lines.
227  metastasis, poorly metastatic Panc02-H0 and highly metastatic Panc02-H7 cells were injected into the
228 B with an oncogenic Kras allele, we observed highly metastatic pancreatic adenocarcinomas.
229 ciency cooperates with Kras(G12D) to promote highly metastatic pancreatic cancer.
230                    We then demonstrated in a highly metastatic pancreatic mouse tumor model (Panc-02)
231 lencing MUC4 expression in an aggressive and highly metastatic pancreatic tumor cell line CD18/HPAF t
232 t case, the invasive ascents of the Tepui by highly metastatic PC-3 and noninvasive LNCaP prostate ca
233 nt LNCaP, hormone-independent DU145, PC-3 to highly metastatic PC-3M cancer cell lines.
234                                              Highly metastatic PC-3M human prostate cancer cells were
235                                              Highly metastatic PC-3M human prostate cancer cells were
236                                              Highly metastatic PC3 and PC3M-LN4 cells were found to a
237 poptosis in poorly metastatic PC3 M-Pro4 and highly metastatic PC3 M-LN4 subclones demonstrated that
238                                       In the highly metastatic PC3-MM2 cells, expression of a non-pho
239 sitively regulates E-cadherin and suppresses highly metastatic PCA cell invasion by modulating Rho pa
240 a1 in regulation of INPPB, we engineered the highly metastatic PCa cell line, PC3, to express ERbeta1
241 that miR-25 can act as a tumor suppressor in highly metastatic PCSCs by direct functional interaction
242          In a mouse model of osteosarcoma, a highly metastatic pediatric cancer, we found ezrin to be
243 ggest a possible molecular mechanism for the highly metastatic phenotype associated with MCC.
244 beta4 integrin was sufficient to revert this highly metastatic phenotype in the MNNG-HOS model withou
245 wth factor (EGF) receptor (EGFR) indicates a highly metastatic phenotype of breast cancer.
246 vels of GLI1 are likely to contribute to the highly metastatic phenotype of PDAC.
247 ogressively lost as the cells take on a more highly metastatic phenotype.
248 onsive, estrogen receptor (ER) negative, and highly metastatic phenotype.
249 s of proteases and angiogenic factors, and a highly metastatic phenotype.
250 opically to regulate an undifferentiated and highly metastatic phenotype.
251 dermal growth factor receptor)-positive, and highly metastatic phenotype.
252 oma (PDAC), a cancer type characterized by a highly metastatic phenotype.
253                             p27 knockdown in highly metastatic PI3K-activated cells reduces STAT3 bin
254                         Cell velocity in the highly metastatic population shows a relative insensitiv
255 lusters are both increasingly appreciated as highly metastatic precursors and virtually unexplored.
256                  Rapid, specific adhesion of highly metastatic prostate adenocarcinoma cells (PC3M-LN
257 n at both the mRNA and protein levels in the highly metastatic prostate cancer cell line PC3.
258 st completely inhibited lung colonization of highly metastatic prostate cancer cells without affectin
259 tional regulator, is abnormally expressed in highly metastatic prostate cancer cells.
260                                 In contrast, highly metastatic prostate carcinoma cells were resistan
261  pluripotency in embryonic stem cells and in highly metastatic prostate tumors.
262 ersely, recombinant expression of Cav-1 in a highly metastatic PyMT mammary carcinoma-derived cell li
263 were transfected and stably expressed in the highly metastatic rat Dunning MAT-LyLu prostate cancer c
264 d with lycopene against proliferation of the highly metastatic rat prostate adenocarcinoma MAT-LyLu c
265  SPARC selectively supports the migration of highly metastatic relative to less metastatic prostate c
266                       We used J774 tumors (a highly metastatic reticulum cell sarcoma line) and PDT w
267 r to introduce normal human chromosomes into highly metastatic rodent prostatic cancer cells to map t
268 mplete inhibition on invasion (P < 0.001) of highly metastatic SiHa cells via reduced transcriptional
269 6.1, without metastasis suppression in other highly metastatic sublines, such as AT3.1.
270 in-7 expression in poorly differentiated and highly metastatic SW620 colon cancer cells induced epith
271 ong epithelial gene program were enriched in highly metastatic TICs, while a second subpopulation wit
272  for these cells revealed that CSCs that are highly metastatic to bone and brain expressed significan
273 -MB cells, a breast cancer cell line that is highly metastatic to bone.
274                    NME1(LOW) cells were also highly metastatic to lung and liver when xenografted sub
275                  A murine melanoma cell line highly metastatic to lymph nodes (B16F10) was implanted
276 , FAK expression is increased in a number of highly metastatic tumor cell lines.
277 ate that secretion of inhibitory TFPI-2 by a highly metastatic tumor cell markedly inhibits its growt
278  within extracellular vesicles secreted from highly metastatic tumor cells can be internalized by wea
279        In vivo tumor modeling studies with a highly metastatic tumor line, PC-3ML cells, revealed tha
280 titumor efficacy and overall survival in two highly metastatic tumor models.
281 rate that several proteins characteristic of highly metastatic tumors (LTBP3, SNED1, EGLN1, and S100A
282 ant organs, whereas inhibition of miR-105 in highly metastatic tumors alleviates these effects.
283 n, which can be defeated in the evolution of highly metastatic tumors by combined loss of both p66(Sh
284 sing a mouse model of metastasis reveal that highly metastatic tumors express proteolyzed cyclin E an
285                  Instead, these mice develop highly metastatic tumors of neuroendocrine, not epitheli
286                                Consistently, highly metastatic tumors upregulated multiple pyrimidine
287 the control clones produced rapidly growing, highly metastatic tumors within 2 wk of inoculation on c
288 oss in the mouse lung to promote aggressive, highly metastatic tumors, that are initially sensitive t
289  we found that 4.1B expression is reduced in highly metastatic tumors.
290 or discrimination between non-metastatic and highly metastatic tumors.
291  cell lines, POS (low metastatic) and HMPOS (highly metastatic), under normoxia and hypoxia.
292 e human-human somatic cell fusions between a highly metastatic, undifferentiated, ER-negative line of
293 rom the compound mutant prostates, which was highly metastatic upon orthotopic transplantation.
294 o search for metastasis-related mutations in highly metastatic uveal melanomas of the eye.
295 an prostate cancer cell line LNCaP, with its highly metastatic variant LNCaP-LN3, by two-dimensional
296 man breast carcinoma MDA-MB-435-F-L cells, a highly metastatic variant of human breast cancer MDA-MB-
297 c GI101A human breast cancer cell line and a highly metastatic variant, GILM2.
298 y be essential for this process, we isolated highly metastatic variants from a poorly metastatic huma
299 ic vs. immunosuppressed newborn rat-selected highly metastatic variants.
300                          However, HCT116 was highly metastatic with 68% metastasis observed in liver

 
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