学术探索
学术期刊
新闻热点
数据分析
智能评审

TRISOMY-7 IN NONNEOPLASTIC EPITHELIAL KIDNEY-CELLS

被引:29
作者
ELFVING, P [1 ]
AMAN, P [1 ]
MANDAHL, N [1 ]
LUNDGREN, R [1 ]
MITELMAN, F [1 ]
机构
[1] UNIV LUND HOSP,DEPT UROL,S-22185 LUND,SWEDEN
来源
CYTOGENETICS AND CELL GENETICS | 1995年 / 69卷 / 1-2期
关键词
D O I
10.1159/000133945
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Trisomy 7 has been found as the sole clonal chromosome aberration in a number of tumor types, including renal cell carcinomas (RCC), and also in non-neoplastic kidney tissue. It has recently been proposed that the cells harboring trisomy 7 in RCC and in the surrounding tissue may be tumor infiltrating T-helper lymphocytes. We performed cytogenetic analysis of metaphase cells and FISH of interphase nuclei in uncultured and cultured non-neoplastic kidney tissues from 13 patients with renal or urothelial carcinomas, and 4 patients with inflammatory kidney diseases. FISH analysis showed that the frequency of +7 varied between 1.0-8.9% (mean 3.3%) in uncultured cells and between 0.4-8.6% (mean 4.4%) after one week of cell culture. The frequency of + 7 after one week of culture was 1.0-19.0% (mean 6.1%) as determined by cytogenetic analysis. Immunoenzymatic staining of both uncultured and cultured cells with the alkaline phosphatase reaction and monoclonal antibodies for CD3 showed that the frequency of T-cells in uncultured cells and in primary cultures varied between 2.9-10%. The number of T-cells decreased with time and number of in vitro passages to less than 1% after 7-8 weeks, but the frequency of +7 remained fairly constant. Combination of FISH with immunostaining using CD3 for T-lymphocytes and cytokeratins for epithelial cells showed that the cells with +7 were mainly epithelial cells whereas only 0-5% were T-lymphocytes. The results have obvious implications for the interpretation of the significance of trisomy 7 in neoplasia.
引用
收藏
页码:90 / 96
页数:7
相关论文
共 33 条
[1]   DETECTION OF THE PHILADELPHIA-CHROMOSOME IN INTERPHASE NUCLEI [J].
ARNOLDUS, EPJ ;
WIEGANT, J ;
NOORDERMEER, IA ;
WESSELS, JW ;
BEVERSTOCK, GC ;
GROSVELD, GC ;
VANDERPLOEG, M ;
RAAP, AK .
CYTOGENETICS AND CELL GENETICS, 1990, 54 (3-4) :108-&
[2]   CYTOGENETIC STUDY OF 4 CANCERS OF THE PROSTATE [J].
BABU, VR ;
MILES, BJ ;
CERNY, JC ;
WEISS, L ;
VANDYKE, DL .
CANCER GENETICS AND CYTOGENETICS, 1990, 48 (01) :83-87
[3]   TRISOMY 7-IN SHORT-TERM CULTURES OF COLORECTAL ADENOCARCINOMAS [J].
BARDI, G ;
JOHANSSON, B ;
PANDIS, N ;
HEIM, S ;
MANDAHL, N ;
ANDRENSANDBERG, A ;
HAGERSTRAND, I ;
MITELMAN, F .
GENES CHROMOSOMES & CANCER, 1991, 3 (02) :149-152
[4]   TRISOMY-7 IN NONNEOPLASTIC FOCAL STEATOSIS OF THE LIVER [J].
BARDI, G ;
JOHANSSON, B ;
PANDIS, N ;
HEIM, S ;
MANDAHL, N ;
HAGERSTRAND, I ;
HOLMIN, T ;
ANDRENSANDBERG, A ;
MITELMAN, F .
CANCER GENETICS AND CYTOGENETICS, 1992, 63 (01) :22-24
[5]   CHROMOSOMAL EVOLUTION IN MALIGNANT HUMAN GLIOMAS STARTS WITH SPECIFIC AND USUALLY NUMERICAL DEVIATIONS [J].
BIGNER, SH ;
MARK, J ;
BULLARD, DE ;
MAHALEY, MS ;
BIGNER, DD .
CANCER GENETICS AND CYTOGENETICS, 1986, 22 (02) :121-135
[6]  
Dal Cin P, 1988, Cancer Genet Cytogenet, V35, P41, DOI 10.1016/0165-4608(88)90119-7
[7]   TRISOMY-7 AND TRISOMY-10 CHARACTERIZE SUBPOPULATIONS OF TUMOR-INFILTRATING LYMPHOCYTES IN KIDNEY TUMORS AND IN THE SURROUNDING KIDNEY TISSUE [J].
DALCIN, P ;
ALY, MS ;
DELABIE, J ;
CEUPPENS, JL ;
VANGOOL, S ;
VANDAMME, B ;
BAERT, L ;
VANPOPPEL, H ;
VANDENBERGHE, H .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (20) :9744-9748
[8]  
DELOZIERBLANCHE.CD, 1988, PRENAT DIAGN, V8, P281
[9]   TRISOMY-7, TRISOMY-10, AND LOSS OF THE Y-CHROMOSOME IN SHORT-TERM CULTURES OF NORMAL KIDNEY TISSUE [J].
ELFVING, P ;
CIGUDOSA, JC ;
LUNDGREN, R ;
LIMON, J ;
MANDAHL, N ;
KRISTOFFERSSON, U ;
HEIM, S ;
MITELMAN, F .
CYTOGENETICS AND CELL GENETICS, 1990, 53 (2-3) :123-125
[10]   TRISOMY-7 IN NONNEOPLASTIC KIDNEY TISSUE CULTURED WITH AND WITHOUT EPIDERMAL GROWTH-FACTOR [J].
ELFVING, P ;
LUNDGREN, R ;
CIGUDOSA, JCC ;
HEIM, S ;
MANDAHL, N ;
MITELMAN, F .
CANCER GENETICS AND CYTOGENETICS, 1992, 64 (01) :99-100
1234