DIFFERENTIATION STATE AND INVASIVENESS OF HUMAN BREAST-CANCER CELL-LINES

被引：257

作者：

SOMMERS, CL

BYERS, SW

THOMPSON, EW

TORRI, JA

GELMANN, EP

机构：

[1] GEORGETOWN UNIV,VINCENT T LOMBARDI CANC RES CTR,WASHINGTON,DC 20007

[2] GEORGETOWN UNIV,DEPT CELL BIOL,WASHINGTON,DC 20007

来源：

BREAST CANCER RESEARCH AND TREATMENT | 1994年 / 31卷 / 2-3期

关键词：

BREAST CANCER; VIMENTIN; INVASION; INTEGRINS; CADHERINS; EPITHELIAL;

D O I：

10.1007/BF00666165

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Eighteen breast cancer cell lines were examined for expression of markers of epithelial and fibroblastic differentiation: E-cadherin, desmoplakins, ZO-1, vimentin, keratin and beta(1) and beta(4) integrins. The cell lines were distributed along a spectrum of differentiation from epithelial to fibroblastic phenotypes. The most well-differentiated, epithelioid cell lines contained proteins characteristic of desmosomal, adherens and tight junctions, were adherent to one another on plastic and in the basement membrane matrix Matrigel and were keratin-positive and vimentin-negative. These cell lines were all weakly invasive in an in vitro chemoinvasion assay. The most poorly-differentiated, fibroblastic cell lines were E-cadherin-, desmoplakin- and ZO-1-negative and formed branching structures in Matrigel. They were vimentin-positive, contained only low levels of keratins and were highly invasive in the in vitro chemoinvasion assay. Of all of the markers analyzed, vimentin expression correlated best with in vitro invasive ability and fibroblastic differentiation. In a cell line with unstable expression of vimentin, T47D(CO), the cells that were invasive were of the fibroblastic type. The differentiation markers described here may be useful for analysis of clinical specimens and could potentially provide a more precise measure of differentiation grade yielding more power for predicting prognosis.

引用

页码：325 / 335

页数：11

共 50 条

[1] NEW CELL-LINES OF HUMAN BREAST-CANCER ORIGIN
CALAF, G
ABARCAQUINONES, J
FEUILHADE, F
BEAUNE, J
DUPRE, G
ORRICO, M
BARNABASSOHI, N
KOUYOUMDJIAN, JC
[J]. BREAST CANCER RESEARCH AND TREATMENT, 1992, 21 (01) : 63 - 75
[2] OXYTOCIN INHIBITS PROLIFERATION OF HUMAN BREAST-CANCER CELL-LINES
CASSONI, P
SAPINO, A
NEGRO, F
BUSSOLATI, G
[J]. VIRCHOWS ARCHIV, 1994, 425 (05) : 467 - 472
[3] COMBINED EFFECTS OF LONIDAMINE AND TAMOXIFEN IN HUMAN BREAST-CANCER CELL-LINES
GORNATI, D
ZAFFARONI, N
ORLANDI, L
DIFRONZO, G
SILVESTRINI, R
[J]. INTERNATIONAL JOURNAL OF ONCOLOGY, 1995, 6 (05) : 993 - 996
[4] MECHANISMS OF RESISTANCE TO ANSAMYCIN ANTIBIOTICS IN HUMAN BREAST-CANCER CELL-LINES
BENCHEKROUN, MN
SCHNEIDER, E
SAFA, AR
TOWNSEND, AJ
SINHA, BK
[J]. MOLECULAR PHARMACOLOGY, 1994, 46 (04) : 677 - 684
[5] STUDIES ON CONFRONTATION OF DIFFERENT BREAST-CANCER CELL-LINES WITH PRECULTURED EMBRYONIC CHICK HEART - AN ASSAY FOR INVASIVENESS
MANDEVILLE, R
BERRADA, F
[J]. BREAST CANCER RESEARCH AND TREATMENT, 1986, 8 (01) : 108 - 108
[6] GLUTATHIONE DEPLETION IN HUMAN AND IN RAT MULTIDRUG RESISTANT BREAST-CANCER CELL-LINES
BATIST, G
SCHECTER, R
WOO, A
GREENE, D
LEHNERT, S
[J]. BIOCHEMICAL PHARMACOLOGY, 1991, 41 (04) : 631 - 635
[7] REGULATION OF VIMENTIN GENE-TRANSCRIPTION IN HUMAN BREAST-CANCER CELL-LINES
SOMMERS, CL
SKERKER, JM
CHRYSOGELOS, SA
BOSSELER, M
GELMANN, EP
[J]. CELL GROWTH & DIFFERENTIATION, 1994, 5 (08): : 839 - 846
[8] IGFS AND IGF BINDING-PROTEINS IN HUMAN BREAST-CANCER CELL-LINES
WILSON, DM
DELEON, DD
BAKKER, B
LAMSON, G
ROSENFELD, RG
[J]. INSULIN-LIKE GROWTH FACTOR BINDING PROTEINS, 1989, 881 : 241 - 247
[9] INSULIN-RECEPTOR EXPRESSION AND FUNCTION IN HUMAN BREAST-CANCER CELL-LINES
MILAZZO, G
GIORGINO, F
DAMANTE, G
SUNG, C
STAMPFER, MR
VIGNERI, R
GOLDFINE, ID
BELFIORE, A
[J]. CANCER RESEARCH, 1992, 52 (14) : 3924 - 3930
[10] 1-ALPHA-25-DIHYDROXYCHOLECALCIFEROL AND HUMAN BREAST-CANCER CELL-LINES
DEGREMOUX, P
CALVO, F
GAUVILLE, C
JABRANE, N
ABITA, JP
LAGIER, G
LECHAT, P
[J]. THERAPIE, 1987, 42 (03): : 327 - 327

← 1 2 3 4 5 →