DIRECT SEQUENCING FROM TOUCH PREPARATIONS OF HUMAN CARCINOMAS - ANALYSIS OF P53 MUTATIONS IN BREAST CARCINOMAS

被引：108

作者：

KOVACH, JS

MCGOVERN, RM

CASSADY, JD

SWANSON, SK

WOLD, LE

VOGELSTEIN, B

SOMMER, SS

机构：

[1] MAYO CLIN & MAYO FDN, DEPT BIOCHEM & MOLEC BIOL, 200 1ST ST, ROCHESTER, MN 55905 USA

[2] MAYO CLIN & MAYO FDN, DEPT ONCOL, ROCHESTER, MN 55905 USA

[3] MAYO CLIN & MAYO FDN, DEPT LAB MED & PATHOL, ROCHESTER, MN 55905 USA

[4] MAYO CLIN & MAYO FDN, DEPT BIOCHEM & MOLEC BIOL, ROCHESTER, MN 55905 USA

来源：

JNCI-JOURNAL OF THE NATIONAL CANCER INSTITUTE | 1991年 / 83卷 / 14期

关键词：

D O I：

10.1093/jnci/83.14.1004

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

A new technique for characterizing somatic mutations in very small samples of cellularly heterogeneous human cancer tissue was developed and tested using mutations in the p53 gene in breast carcinomas as a model system. The technique combines touch preparation of specimens to obtain homogeneous clusters of carcinoma cells free of normal cells with a nested pair of polymerase chain reaction (PCR) amplifications of DNA to increase the amount of target gene sequence sufficiently to permit direct sequencing of the p53 gene. Touch preparations of fresh or previously frozen tissue from human adenocarcinomas derived from several organs were stained, and clusters of 10-50 malignant cells were transferred by pipette into microfuge tubes for PCR amplification. Exons 5-9 of the p53 gene, which contain the major mutational hot spots associated with most human cancers, were sequenced by the following steps: 1) two rounds of PCR amplification using DNA Taq polymerase and two sets of oligonucleotide primers, the second set being nested within the segment amplified by the first set and having attached T7 and SP6 phage promoter sequences, 2) transcription of the amplified DNA sequences with T7 and SP6 RNA polymerases, and 3) dideoxy sequencing of single-stranded RNA transcripts with reverse transcriptase and with additional oligonucleotide primers to achieve specificity for this unique region of the genome. The utility of this approach is illustrated by our success in detecting and analyzing point mutations in cell clusters from four of 11 primary adenocarcinomas of the human breast.

引用

页码：1004 / 1009

页数：6

共 36 条

[1] SUPPRESSION OF HUMAN COLORECTAL-CARCINOMA CELL-GROWTH BY WILD-TYPE-P53
BAKER, SJ
MARKOWITZ, S
FEARON, ER
WILLSON, JKV
VOGELSTEIN, B
[J]. SCIENCE, 1990, 249 (4971) : 912 - 915
[2] CHROMOSOME-17 DELETIONS AND P53 GENE-MUTATIONS IN COLORECTAL CARCINOMAS
BAKER, SJ
FEARON, ER
NIGRO, JM
HAMILTON, SR
PREISINGER, AC
JESSUP, JM
VANTUINEN, P
LEDBETTER, DH
BARKER, DF
NAKAMURA, Y
WHITE, R
VOGELSTEIN, B
[J]. SCIENCE, 1989, 244 (4901) : 217 - 221
[3] BARTEK J, 1990, ONCOGENE, V5, P893
[4] PHOSPHORYLATION OF THE RETINOBLASTOMA GENE-PRODUCT IS MODULATED DURING THE CELL-CYCLE AND CELLULAR-DIFFERENTIATION
CHEN, PL
SCULLY, P
SHEW, JY
WANG, JYJ
LEE, WH
[J]. CELL, 1989, 58 (06) : 1193 - 1198
[5] CHIBA I, 1990, ONCOGENE, V5, P1603
[6] SINGLE-SPERM TYPING - DETERMINATION OF GENETIC-DISTANCE BETWEEN THE G-GAMMA-GLOBIN AND PARATHYROID-HORMONE LOCI BY USING THE POLYMERASE CHAIN-REACTION AND ALLELE-SPECIFIC OLIGOMERS
CUI, XF
LI, HH
GORADIA, TM
LANGE, K
KAZAZIAN, HH
GALAS, D
ARNHEIM, N
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (23) : 9389 - 9393
[7] WILD-TYPE P53 CAN INHIBIT ONCOGENE-MEDIATED FOCUS FORMATION
ELIYAHU, D
MICHALOVITZ, D
ELIYAHU, S
PINHASIKIMHI, O
OREN, M
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (22) : 8763 - 8767
[8] ELIYAHU D, 1988, ONCOGENE, V3, P313
[9] A GENETIC MODEL FOR COLORECTAL TUMORIGENESIS
FEARON, ER
VOGELSTEIN, B
[J]. CELL, 1990, 61 (05) : 759 - 767
[10] ACTIVATING MUTATIONS FOR TRANSFORMATION BY P53 PRODUCE A GENE-PRODUCT THAT FORMS AN HSC70-P53 COMPLEX WITH AN ALTERED HALF-LIFE
FINLAY, CA
HINDS, PW
TAN, TH
ELIYAHU, D
OREN, M
LEVINE, AJ
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1988, 8 (02) : 531 - 539

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