Down-modulation of p210(bcr/abl) induces apoptosis/differentiation in K562 leukemic blast cells

被引：10

作者：

Deora, AB ^{[1
]}

Miranda, MB ^{[1
]}

Rao, SGA ^{[1
]}

机构：

[1] TATA MEM HOSP,CANC RES INST,CHEMOTHERAPY & STEM CELL BIOL DIV,BOMBAY 400012,MAHARASHTRA,INDIA

来源：

TUMORI | 1997年 / 83卷 / 04期

关键词：

apoptosis; differentiation; quercetin; genistein;

D O I：

10.1177/030089169708300409

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Aims and background: K562 cells are growth factor independent and neither function as stem cells nor differentiate into functional end cells. They are blast cells. There is evidence that the constitutively expressed bcr-abl tyrosine kinase might be responsible for the maintenance of the blast state of CML cells. We have studied the effect of two tyrosine kinase inhibitors, quercetin and genistein, on K562 cells. Methods: K562 cells were treated with quercetin/genistein for a period of 72 hrs and then subjected to staining for apoptosis and erythroid differentiation and Western blotting with c-abl and phosphotyrosine monoclonal antibodies, Results: The IC50 value was found to be 9.2 mu g/ml for quercetin and 11.8 mu g/ml for genistein. Quercetin-treated cells did not show any differentiation but showed 68% apoptosis as compared to 7% in control. Genistein-treated cells showed 16% apoptosis and 15% erythroid differentiation. Quercetin reduced the level of p210 by 74% and its phosphotyrosine content by 67.6%. Genistein reduced p210 by 77.8% and its phosphotyrosine content by 16%, Conclusion: Both quercetin and genistein are able to down-modulate the tyrosine kinase activity of p210 as well as bring about a decrease in the content of the protein with different effects: quercetin induced apoptosis while genistein brought about both differentiation and apoptosis.

引用

页码：756 / 761

页数：6

共 20 条

[1]

AKIYAMA T, 1987, J BIOL CHEM, V262, P5592

[2]

BEDI A, 1994, BLOOD, V83, P2038

[3] LINEAGE-SPECIFIC REQUIREMENT OF C-ABL FUNCTION IN NORMAL HEMATOPOIESIS [J].

CARACCIOLO, D ;

VALTIERI, M ;

VENTURELLI, D ;

PESCHLE, C ;

GEWIRTZ, AM ;

CALABRETTA, B .

SCIENCE, 1989, 245 (4922) :1107-1110

[4] A CELLULAR ONCOGENE IS TRANSLOCATED TO THE PHILADELPHIA-CHROMOSOME IN CHRONIC MYELOCYTIC-LEUKEMIA [J].

DEKLEIN, A ;

VANKESSEL, AG ;

GROSVELD, G ;

BARTRAM, CR ;

HAGEMEIJER, A ;

BOOTSMA, D ;

SPURR, NK ;

HEISTERKAMP, N ;

GROFFEN, J ;

STEPHENSON, JR .

NATURE, 1982, 300 (5894) :765-767

[5]

EVANS CA, 1993, CANCER RES, V53, P1735

[6] CHRONIC MYELOCYTIC-LEUKEMIA - CLONAL ORIGIN IN A STEM-CELL COMMON TO GRANULOCYTE, ERYTHROCYTE, PLATELET AND MONOCYTE-MACROPHAGE [J].

FIALKOW, PJ ;

JACOBSON, RJ ;

PAPAYANNOPOULOU, T .

AMERICAN JOURNAL OF MEDICINE, 1977, 63 (01) :125-130

[7] CALCIUM AND PHOSPHOLIPID-DEPENDENT PROTEIN-KINASE ACTIVITY IN MOUSE EPIDERMIS CYTOSOL - STIMULATION BY COMPLETE AND INCOMPLETE TUMOR PROMOTERS AND INHIBITION BY VARIOUS COMPOUNDS [J].

GSCHWENDT, M ;

HORN, F ;

KITTSTEIN, W ;

FURSTENBERGER, G ;

BESEMFELDER, E ;

MARKS, F .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1984, 124 (01) :63-68

[8] PROTEIN-TYROSINE KINASES [J].

HUNTER, T ;

COOPER, JA .

ANNUAL REVIEW OF BIOCHEMISTRY, 1985, 54 :897-930

[9] CELL-LINES AND CLINICAL ISOLATES DERIVED FROM PH1-POSITIVE CHRONIC MYELOGENOUS LEUKEMIA PATIENTS EXPRESS C-ABL PROTEINS WITH A COMMON STRUCTURAL ALTERATION [J].

KONOPKA, JB ;

WATANABE, SM ;

SINGER, JW ;

COLLINS, SJ ;

WITTE, ON .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1985, 82 (06) :1810-1814

[10] AN ALTERATION OF THE HUMAN C-ABL PROTEIN IN K562 LEUKEMIA-CELLS UNMASKS ASSOCIATED TYROSINE KINASE-ACTIVITY [J].

KONOPKA, JB ;

WATANABE, SM ;

WITTE, ON .

CELL, 1984, 37 (03) :1035-1042

← 1 2 →