Localization of BRCA1 and a splice variant identifies the nuclear localization signal

被引：227

作者：

Thakur, S

Zhang, HB

Peng, Y

Le, H

Carroll, B

Ward, T

Yao, J

Farid, LM

Couch, FJ

Wilson, RB

Weber, BL

机构：

[1] UNIV PENN, PHILADELPHIA, PA 19104 USA

[2] UNIV PENN, DEPT MED, PHILADELPHIA, PA 19104 USA

[3] UNIV PENN, DEPT BIOCHEM, PHILADELPHIA, PA 19104 USA

[4] UNIV PENN, DEPT GENET, PHILADELPHIA, PA 19104 USA

[5] UNIV PENN, DEPT LAB MED & PATHOL, PHILADELPHIA, PA 19104 USA

来源：

MOLECULAR AND CELLULAR BIOLOGY | 1997年 / 17卷 / 01期

关键词：

D O I：

10.1128/MCB.17.1.444

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Inherited mutations in BRCA1 confer susceptibility to breast and ovarian neoplasms. However, the function of BRCA1 and the role of BRCA1 in noninherited cancer remain unknown. Characterization of alternately spliced forms of BRCA1 may identify functional regions; thus, we constructed expression vectors of BRCA1 and a splice variant lacking exon II, designated BRCA1 Delta 672-4095. Immunofluorescence studies indicate nuclear localization of BRCA1 but cytoplasmic localization of BRCA1 Delta 672-4095. Two putative nuclear localization signals (designated NLS1 and NLS2) were identified in exon II; immunofluorescence studies indicate that only NLS1 is required for nuclear localization RNA analysis indicates the expression of multiple, tissue-specific forms of BRCA1 RNAs; protein analysis with multiple antibodies suggests that at least three BRCA1 isoforms are expressed, including those lacking exon 11, The results suggest that BRCA1 is a nuclear protein and raise the possibility that splicing is one form of regulation of BRCA1 function by alteration of the subcellular localization of expressed proteins.

引用

页码：444 / 452

页数：9

共 29 条

[21] A STRONG CANDIDATE FOR THE BREAST AND OVARIAN-CANCER SUSCEPTIBILITY GENE BRCA1
MIKI, Y
SWENSEN, J
SHATTUCKEIDENS, D
FUTREAL, PA
HARSHMAN, K
TAVTIGIAN, S
LIU, QY
COCHRAN, C
BENNETT, LM
DING, W
BELL, R
ROSENTHAL, J
HUSSEY, C
TRAN, T
MCCLURE, M
FRYE, C
HATTIER, T
PHELPS, R
HAUGENSTRANO, A
KATCHER, H
YAKUMO, K
GHOLAMI, Z
SHAFFER, D
STONE, S
BAYER, S
WRAY, C
BOGDEN, R
DAYANANTH, P
WARD, J
TONIN, P
NAROD, S
BRISTOW, PK
NORRIS, FH
HELVERING, L
MORRISON, P
ROSTECK, P
LAI, M
BARRETT, JC
LEWIS, C
NEUHAUSEN, S
CANNONALBRIGHT, L
GOLDGAR, D
WISEMAN, R
KAMB, A
SKOLNICK, MH
[J]. SCIENCE, 1994, 266 (5182) : 66 - 71
[22] NUCLEAR-LOCALIZATION OF THE ADENOVIRUS DNA-BINDING PROTEIN - REQUIREMENT FOR 2 SIGNALS AND COMPLEMENTATION DURING VIRAL-INFECTION
MORIN, N
DELSERT, C
KLESSIG, DF
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (10) : 4372 - 4380
[23] Rao VN, 1996, ONCOGENE, V12, P523
[24] PROTEIN IMPORT INTO NUCLEI - ASSOCIATION AND DISSOCIATION REACTIONS INVOLVING TRANSPORT SUBSTRATE, TRANSPORT FACTORS, AND NUCLEOPORINS
REXACH, M
BLOBEL, G
[J]. CELL, 1995, 83 (05) : 683 - 692
[25] Location of BRCA1 in human breast and ovarian cancer cells
Scully, R
Ganesan, S
Brown, M
DeCaprio, JA
Cannistra, SA
Feunteun, J
Schnitt, S
Livingston, DM
[J]. SCIENCE, 1996, 272 (5258) : 123 - 125
[26] MURINE BRCA1 - SEQUENCE AND SIGNIFICANCE FOR HUMAN MISSENSE MUTATIONS
SHARAN, SK
WIMS, M
BRADLEY, A
[J]. HUMAN MOLECULAR GENETICS, 1995, 4 (12) : 2275 - 2278
[27] A KARYOPHILIC SIGNAL SEQUENCE IN ADENOVIRUS TYPE-5 E1A IS FUNCTIONAL IN XENOPUS OOCYTES BUT NOT IN SOMATIC-CELLS
SLAVICEK, JM
JONES, NC
RICHTER, JD
[J]. JOURNAL OF VIROLOGY, 1989, 63 (09) : 4047 - 4050
[28] DECREASED EXPRESSION OF BRCA1 ACCELERATES GROWTH AND IS OFTEN PRESENT DURING SPORADIC BREAST-CANCER PROGRESSION
THOMPSON, ME
JENSEN, RA
OBERMILLER, PS
PAGE, DL
HOLT, JT
[J]. NATURE GENETICS, 1995, 9 (04) : 444 - 450
[29] THE MOUSE TYPE-IV C-ABL GENE-PRODUCT IS A NUCLEAR-PROTEIN, AND ACTIVATION OF TRANSFORMING ABILITY IS ASSOCIATED WITH CYTOPLASMIC LOCALIZATION
VANETTEN, RA
JACKSON, P
BALTIMORE, D
[J]. CELL, 1989, 58 (04) : 669 - 678

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