Genetic mapping using microcell-mediated chromosome transfer suggests a locus for Nijmegen breakage syndrome at chromosome 8q21-24

被引：58

作者：

Matsuura, S

Weemaes, C

Smeets, D

Takami, H

Kondo, N

Sakamoto, S

Yano, N

Nakamura, A

Tauchi, H

Endo, S

Oshimura, M

Komatsu, K

机构：

[1] HIROSHIMA UNIV,RES INST RADIAT BIOL & MED,DEPT RADIAT BIOL,MINAMI KU,HIROSHIMA 734,JAPAN

[2] UNIV NIJMEGEN HOSP,DEPT HUMAN GENET,NL-6500 HB NIJMEGEN,NETHERLANDS

[3] UNIV NIJMEGEN HOSP,DEPT PEDIAT,NL-6500 HB NIJMEGEN,NETHERLANDS

[4] TOTTORI UNIV,SCH LIFE SCI,DEPT MOL & CELL GENET,YONAGO,TOTTORI,JAPAN

来源：

AMERICAN JOURNAL OF HUMAN GENETICS | 1997年 / 60卷 / 06期

关键词：

D O I：

10.1086/515461

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Nijmegen breakage syndrome (NBS) is an autosomal recessive disorder characterized by microcephaly, short stature, immunodeficiency, and a high incidence of cancer. Cultured cells from NBS show chromosome instability, an increased sensitivity to radiation-induced cell killing, and an abnormal cell-cycle regulation after irradiation. Hitherto, patients with NBS have been divided into the two complementation groups V1 and V2, on the basis of restoration of radioresistant DNA synthesis, suggesting that each group arises from a different gene, However, the presence of genetic heterogeneity in NBS has been considered to be controversial. To localize the NBS gene, we have performed functional complementation assays using somatic cell fusion between NBS-V1 and NBS-V2 cells, on the basis of hyper-radiosensitivity, and then have performed a genomewide search for the NBS locus, using microcell-mediated chromosome transfer followed by complementation assays based on radiosensitivity, We found that radiation resistance was not restored in the fused NBS-V1 and NBS-V2 cells and that only human chromosome 8 complements the sensitivity to ionizing radiation, in NBS cell lines. In complementation assays performed after the transfer of a reduced chromosome, merely the long arm of chromosome 8 was sufficient for restoring the defect. Our results strongly suggest that NBS is a homogeneous disorder and that the gene for NBS is located at 8q21-24.

引用

页码：1487 / 1494

页数：8

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