GENOMIC STABILITY AND WILD-TYPE P53 FUNCTION OF LYMPHOBLASTOID-CELLS WITH GERM-LINE P53 MUTATION

被引：0

作者：

LALLE, P

MOYRETLALLE, C

WANG, Q

VIALLE, JM

NAVARRO, C

BRESSACDEPAILLERETS, B

MAGAUD, JP

OZTURK, M

机构：

[1] CTR LEON BERARD, INSERM, CJF 9302, ONCOL MOLEC LAB, F-69373 LYON 08, FRANCE

[2] HOP EDOUARD HERRIOT, INSERM, CJF 9307, CENT HEMATOL & CYTOGENET LAB, F-69437 LYON, FRANCE

[3] INST GUSTAVE ROUSSY, DIAGNOST MOLEC LAB, F-94805 VILLEJUIF, FRANCE

来源：

ONCOGENE | 1995年 / 10卷 / 12期

关键词：

P53; LI-FRAUMENI SYNDROME; EPSTEIN-BARR VIRUS; LYMPHOBLASTOID CELLS; GENOMIC STABILITY;

D O I：

暂无

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：

Increased cancer risk associated with germ-line p53 mutation was linked to a deficit in the ability to maintain genomic stability. Accordingly, normal fibroblasts from cancer-prone individuals accumulate genomic aberrations with concomitant loss of mild-type p53 allele during in vitro culture. We tested whether such changes also occur in EBV-immortalized lymphoblastoid cells. Both normal and p53 germ-line mutant lymphoblastoid cells maintained functional p53 and genomic stability during long term in vitro culture. These unexpected differences between fibroblastic and lymphoblastic cells suggest that phenotypic expression of p53 deficiency is cell type specific. This could contribute to selective tissular localization of tumours observed in patients with Li-Fraumeni syndrome despite the presence of a mutant p53 allele in all cells.

引用

页码：2447 / 2454

页数：8

共 50 条

[1] A novel germ-line mutation in p53 gene
Roesler, Wojciech
Przybyla, Anna
Mackiewicz, Andrzej
Lamperska, Katarzyna
WSPOLCZESNA ONKOLOGIA-CONTEMPORARY ONCOLOGY, 2006, 10 (01): : 21 - 23
[2] Mutant p53: Gain-of-function oncoproteins and wild-type p53 inactivators
Roemer, K
BIOLOGICAL CHEMISTRY, 1999, 380 (7-8) : 879 - 887
[3] Contribution of the p53 pathway in cancers that carry wild-type p53
Ohki, Rieko
CANCER SCIENCE, 2022, 113 : 1232 - 1232
[4] Aging-associated truncated form of p53 interacts with wild-type p53 and alters p53 stability, localization, and activity
Moore, Lynette
Lu, Xiongbin
Ghebranious, Nader
Tyner, Stuart
Donehower, Lawrence A.
MECHANISMS OF AGEING AND DEVELOPMENT, 2007, 128 (11-12) : 717 - 730
[5] Effects of adenoviral wild-type p53 gene transfer in p53 -mutated lymphoma cells
Peter Buttgereit
Frank Schakowski
Angela Märten
Karsten Brand
Sabine Renoth
Carsten Ziske
Björn Schöttker
Oliver Ebert
Roland Schroers
Ingo GH Schmidt-Wolf
Cancer Gene Therapy, 2001, 8 : 430 - 439
[6] TUMOR SUPPRESSOR P53 - ANALYSIS OF WILD-TYPE AND MUTANT P53 COMPLEXES
MILNER, J
MEDCALF, EA
COOK, AC
MOLECULAR AND CELLULAR BIOLOGY, 1991, 11 (01) : 12 - 19
[7] IDENTIFICATION OF A GERM-LINE MUTATION IN THE P53 GENE IN A PATIENT WITH AN INTRACRANIAL EPENDYMOMA
METZGER, AK
SHEFFIELD, VC
DUYK, G
DANESHVAR, L
EDWARDS, MSB
COGEN, PH
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (17) : 7825 - 7829
[8] GERM-LINE P53 MUTATION IS UNCOMMON IN PATIENTS WITH TRIPLE PRIMARY CANCERS
SHISEKI, M
NISHIKAWA, R
YAMAMOTO, H
OCHIAI, A
SUGIMURA, H
SHITARA, N
SAMESHIMA, Y
MIZOGUCHI, H
SUGIMURA, T
YOKOTA, J
CANCER LETTERS, 1993, 73 (01) : 51 - 57
[9] COTRANSLATION OF ACTIVATED MUTANT P53 WITH WILD-TYPE DRIVES THE WILD-TYPE P53 PROTEIN INTO THE MUTANT CONFORMATION
MILNER, J
MEDCALF, EA
CELL, 1991, 65 (05) : 765 - 774
[10] Germ cell tumors of the testis overexpress wild-type p53
Guillou, L
Estreicher, A
Chaubert, P
Hurlimann, J
Kurt, AM
Metthez, G
Iggo, R
Gray, AC
Jichlinski, P
Benhattar, J
AMERICAN JOURNAL OF PATHOLOGY, 1996, 149 (04): : 1221 - 1228

← 1 2 3 4 5 →