PARENTAL ORIGIN OF GERM-LINE AND SOMATIC - MUTATIONS IN THE RETINOBLASTOMA GENE

被引：41

作者：

KATO, MV

ISHIZAKI, K

SHIMIZU, T

EJIMA, Y

TANOOKA, H

TAKAYAMA, J

KANEKO, A

TOGUCHIDA, J

SASAKI, MS

机构：

[1] KYOTO UNIV,CTR RADIAT BIOL,SAKYO KU,KYOTO 606,JAPAN

[2] NATL CANC CTR,RES INST,DIV RADIOBIOL,CHUO KU,TOKYO 104,JAPAN

[3] NATL CANC CTR,DEPT PEDIAT,CHUO KU,TOKYO 104,JAPAN

[4] NATL CANC CTR,DEPT OPHTHALMOL,CHUO KU,TOKYO 104,JAPAN

[5] KYOTO UNIV,FAC MED,DEPT ORTHOPAED SURG,SAKYO KU,KYOTO 606,JAPAN

来源：

HUMAN GENETICS | 1994年 / 94卷 / 01期

关键词：

D O I：

10.1007/BF02272838

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Segregation analysis of polymorphic sites within the retinoblastoma (RB) gene and on chromosome 13, as well as the parental origin of the lost allele in the tumor, were analyzed in 24 families with RB patients. Four mutant alleles transmitted through the germ-line and seven de novo germ-line mutant alleles were identified in 11 patients with hereditary RB. Segregation analysis within the RB gene and on chromosome 13 was useful for DNA diagnosis of susceptibility to RB in relatives of hereditary patients, even if mutations were not identified. All seven de novo germ-line mutant alleles were paternally derived. The bias toward the paternal allele for de novo germ-line mutations of the RB gene was statistically significant. Seven paternal alleles and six maternal alleles were lost in 13 non-hereditary RB tumors with no bias in the parental origin of the somatic allele loss. These results suggest that the physical environment or a deficiency in DNA repair during spermatogenesis may be associated with significant risk factors for de novo germ-line mutations.

引用

页码：31 / 38

页数：8

共 35 条

[1] HUMAN RETINOBLASTOMA GENE - LONG-RANGE MAPPING AND ANALYSIS OF ITS DELETION IN A BREAST-CANCER CELL-LINE
BOOKSTEIN, R
LEE, EYHP
PECCEI, A
LEE, WH
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (04) : 1628 - 1634
[2] PCR-BASED DETECTION OF A POLYMORPHIC BAMHI SITE IN INTRON-1 OF THE HUMAN RETINOBLASTOMA (RB) GENE
BOOKSTEIN, R
LAI, CC
TO, H
LEE, WH
[J]. NUCLEIC ACIDS RESEARCH, 1990, 18 (06) : 1666 - 1666
[3] SHORT, DIRECT REPEATS AT THE BREAKPOINTS OF DELETIONS OF THE RETINOBLASTOMA GENE
CANNING, S
DRYJA, TP
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (13) : 5044 - 5048
[4] EXPRESSION OF RECESSIVE ALLELES BY CHROMOSOMAL MECHANISMS IN RETINOBLASTOMA
CAVENEE, WK
DRYJA, TP
PHILLIPS, RA
BENEDICT, WF
GODBOUT, R
GALLIE, BL
MURPHREE, AL
STRONG, LC
WHITE, RL
[J]. NATURE, 1983, 305 (5937) : 779 - 784
[5] PREDICTION OF FAMILIAL PREDISPOSITION TO RETINOBLASTOMA
CAVENEE, WK
MURPHREE, AL
SHULL, MM
BENEDICT, WF
SPARKES, RS
KOCK, E
NORDENSKJOLD, M
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1986, 314 (19) : 1201 - 1207
[6] PARENTAL AGE IN SPORADIC HEREDITARY RETINOBLASTOMA
DERKINDEREN, DJ
KOTEN, JW
TAN, KEWP
BEEMER, FA
VANROMUNDE, LKJ
DENOTTER, W
[J]. AMERICAN JOURNAL OF OPHTHALMOLOGY, 1990, 110 (06) : 605 - 609
[7] CHROMOSOME-13 RESTRICTION FRAGMENT LENGTH POLYMORPHISMS
DRYJA, TP
RAPAPORT, JM
WEICHSELBAUM, R
BRUNS, GAP
[J]. HUMAN GENETICS, 1984, 65 (04) : 320 - 324
[8] PARENTAL ORIGIN OF MUTATIONS OF THE RETINOBLASTOMA GENE
DRYJA, TP
MUKAI, S
PETERSEN, R
RAPAPORT, JM
WALTON, D
YANDELL, DW
[J]. NATURE, 1989, 339 (6225) : 556 - 558
[9] MUTATIONS IN THE RB1 GENE AND THEIR EFFECTS ON TRANSCRIPTION
DUNN, JM
PHILLIPS, RA
ZHU, X
BECKER, A
GALLIE, BL
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (11) : 4596 - 4604
[10] TYPES, RATES, ORIGIN AND EXPRESSIVITY OF CHROMOSOME MUTATIONS INVOLVING 13Q14 IN RETINOBLASTOMA PATIENTS
EJIMA, Y
SASAKI, MS
KANEKO, A
TANOOKA, H
[J]. HUMAN GENETICS, 1988, 79 (02) : 118 - 123

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