A RODENT MODEL FOR WILMS-TUMORS - EMBRYONAL KIDNEY NEOPLASMS INDUCED BY N-NITROSO-N'-METHYLUREA

被引：38

作者：

SHARMA, PM ^{[1
]}

BOWMAN, M ^{[1
]}

YU, BF ^{[1
]}

SUKUMAR, S ^{[1
]}

机构：

[1] SALK INST BIOL STUDIES,MOLEC BIOL BREAST CANC LAB,LA JOLLA,CA 92037

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1994年 / 91卷 / 21期

关键词：

D O I：

10.1073/pnas.91.21.9931

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Embryonal kidney cell tumors develop in rats given the alkylating agent N-nitroso-N'-methylurea as neonates. These tumors resemble the childhood Wilms tumors in their histopathology. Deletions and mutations in the Wilms tumor suppressor gene, WT1, are present in up to 6% of childhood nephroblastomas. To investigate the role of WT1 in rat kidney tumorigenesis, we studied the genetic alterations in WT1 and its target genes. Point mutations were found in WT1 cDNA in 7 of 18 kidney tumors. Mesenchymal tumors contained G --> A transition mutations in codons 128, 364, and 372, typical of the methylating action of N-nitroso-N'methylurea on DNA. Each of the four nephroblastomas contained the same T --> A mutation at codon 111 of WT1, reflective of transversion mutagenesis by N-nitroso-N'methylurea in vivo. Like Wilms tumors, mRNA levels of WT1, IGF2, Pax-2, and MK genes were higher than newborn kidney in the majority of the tumors. The histopathology of the rat kidney tumors and the genetic alterations are reminiscent of those observed in Wilms tumors, establishing this as a relevant model system for the human disease.

引用

页码：9931 / 9935

页数：5

共 44 条

[1] SITE-SPECIFICALLY MODIFIED OLIGODEOXYNUCLEOTIDES AS PROBES FOR THE STRUCTURAL AND BIOLOGICAL EFFECTS OF DNA-DAMAGING AGENTS [J].

BASU, AK ;

ESSIGMANN, JM .

CHEMICAL RESEARCH IN TOXICOLOGY, 1988, 1 (01) :1-18

[2]

BECKWITH J B, 1990, Pediatric Pathology, V10, P1

[3] INVITRO DNA-REPLICATION IMPLICATES O2-ETHYLDEOXYTHYMIDINE IN TRANSVERSION MUTAGENESIS BY ETHYLATING AGENTS [J].

BHANOT, OS ;

GREVATT, PC ;

DONAHUE, JM ;

GABRIELIDES, CN ;

SOLOMON, JJ .

NUCLEIC ACIDS RESEARCH, 1992, 20 (03) :587-594

[4] MODULATION OF DNA-BINDING SPECIFICITY BY ALTERNATIVE SPLICING OF THE WILMS-TUMOR WT1 GENE TRANSCRIPT [J].

BICKMORE, WA ;

OGHENE, K ;

LITTLE, MH ;

SEAWRIGHT, A ;

VANHEYNINGEN, V ;

HASTIE, ND .

SCIENCE, 1992, 257 (5067) :235-237

[5]

BRESLOW N, 1988, CANCER RES, V48, P1653

[6]

Clapp W L, 1993, Curr Opin Nephrol Hypertens, V2, P419, DOI 10.1097/00041552-199305000-00010

[7] SIMULTANEOUS ISOLATION OF DNA, RNA, AND ANTIGENIC PROTEIN EXHIBITING KINASE-ACTIVITY FROM SMALL TUMOR SAMPLES USING GUANIDINE ISOTHIOCYANATE [J].

COOMBS, LM ;

PIGOTT, D ;

PROCTOR, A ;

EYDMANN, M ;

DENNER, J ;

KNOWLES, MA .

ANALYTICAL BIOCHEMISTRY, 1990, 188 (02) :338-343

[8] THE ROLE OF ZINC FINGERS IN TRANSCRIPTIONAL ACTIVATION BY TRANSCRIPTION FACTOR-IIIA [J].

DELRIO, S ;

SETZER, DR .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (01) :168-172

[9] PAX-2 IS A DNA-BINDING PROTEIN EXPRESSED IN EMBRYONIC KIDNEY AND WILMS-TUMOR [J].

DRESSLER, GR ;

DOUGLASS, EC .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (04) :1179-1183

[10] REPRESSION OF THE INSULIN-LIKE GROWTH FACTOR-II GENE BY THE WILMS-TUMOR SUPPRESSOR WT1 [J].

DRUMMOND, IA ;

MADDEN, SL ;

ROHWERNUTTER, P ;

BELL, GI ;

SUKHATME, VP ;

RAUSCHER, FJ .

SCIENCE, 1992, 257 (5070) :674-678

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