学术探索
学术期刊
新闻热点
数据分析
智能评审

CENP-B IS A HIGHLY CONSERVED MAMMALIAN CENTROMERE PROTEIN WITH HOMOLOGY TO THE HELIX-LOOP-HELIX FAMILY OF PROTEINS

被引:110
作者
SULLIVAN, KF [1 ]
GLASS, CA [1 ]
机构
[1] SCRIPPS RES INST, DEPT MOLEC & EXPTL MED, LA JOLLA, CA 92037 USA
来源
CHROMOSOMA | 1991年 / 100卷 / 06期
关键词
D O I
10.1007/BF00337514
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
CENP-B is a centromere associated protein originally identified in human cells as an 80 kDa autoantigen recognized by sera from patients with anti-centromere antibodies (ACA). Recent evidence indicates that CENP-B interacts with centromeric heterochromatin in human chromosomes and may bind to a specific subset of human alphoid satellite DNA. CENP-B has not been unambiguously identified in non-primates and could, in principal, be a primate-specific alphoid DNA binding protein. In this work, a human genomic DNA segment containing the CENP-B gene was isolated and subjected to DNA sequence analysis. In vitro expression identified the site for translation initiation of CENP-B, demonstrating that it is encoded by an intronless open reading frame (ORF) in human DNA. A homologous mouse gene was also isolated and characterized. It was found to possess a high degree of homology with the human gene, containing an intronless ORF coding for a 599 residue polypeptide with 96% sequence similarity to human CENP-B. 5' and 3' flanking and untranslated sequences were conserved at a level of 94.6% and 82.7%, respectively, suggesting that the regulatory properties of CENP-B may be conserved as well. CENP-B mRNA was detected in mouse cells and tissues and an immunoreactive nuclear protein identical in size to human CENP-B was detected in mouse 3T3 cells using human ACA. Analysis of the sequence of CENP-B revealed a segment of significant similarity to a DNA binding motif identified for the helix-loop-helix (HLH) family of DNA binding proteins. These data demonstrate that CENP-B is a highly conserved mammalian protein that may be a member of the HLH protein family and suggest that it plays a role in a conserved aspect of centromere structure or function.
引用
收藏
页码:360 / 370
页数:11
相关论文
共 61 条
[31]   CLEAVAGE OF STRUCTURAL PROTEINS DURING ASSEMBLY OF HEAD OF BACTERIOPHAGE-T4 [J].
LAEMMLI, UK .
NATURE, 1970, 227 (5259) :680-+
[32]   MYOD IS A SEQUENCE-SPECIFIC DNA-BINDING PROTEIN REQUIRING A REGION OF MYC HOMOLOGY TO BIND TO THE MUSCLE CREATINE-KINASE ENHANCER [J].
LASSAR, AB ;
BUSKIN, JN ;
LOCKSHON, D ;
DAVIS, RL ;
APONE, S ;
HAUSCHKA, SD ;
WEINTRAUB, H .
CELL, 1989, 58 (05) :823-831
[33]  
Maniatis T., 1982, MOL CLONING
[34]   CHROMOSOMAL LOCALIZATION OF COMPLEX AND SIMPLE REPEATED HUMAN DNAS [J].
MANUELIDIS, L .
CHROMOSOMA, 1978, 66 (01) :23-32
[35]   A HUMAN CENTROMERE ANTIGEN (CENP-B) INTERACTS WITH A SHORT SPECIFIC SEQUENCE IN ALPHOID DNA, A HUMAN CENTROMERIC SATELLITE [J].
MASUMOTO, H ;
MASUKATA, H ;
MURO, Y ;
NOZAKI, N ;
OKAZAKI, T .
JOURNAL OF CELL BIOLOGY, 1989, 109 (05) :1963-1973
[36]   AUTOANTIBODIES FROM A PATIENT WITH SCLERODERMA CREST RECOGNIZED KINETOCHORES OF THE HIGHER-PLANT HAEMANTHUS [J].
MOLEBAJER, J ;
BAJER, AS ;
ZINKOWSKI, RP ;
BALCZON, RD ;
BRINKLEY, BR .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1990, 87 (09) :3599-3603
[37]   AUTOANTIBODY TO CENTROMERE (KINETOCHORE) IN SCLERODERMA SERA [J].
MOROI, Y ;
PEEBLES, C ;
FRITZLER, MJ ;
STEIGERWALD, J ;
TAN, EM .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1980, 77 (03) :1627-1631
[38]   A STEM-LOOP IN THE 3' UNTRANSLATED REGION MEDIATES IRON-DEPENDENT REGULATION OF TRANSFERRIN RECEPTOR MESSENGER-RNA STABILITY IN THE CYTOPLASM [J].
MULLNER, EW ;
KUHN, LC .
CELL, 1988, 53 (05) :815-825
[39]   A NEW DNA-BINDING AND DIMERIZATION MOTIF IN IMMUNOGLOBULIN ENHANCER BINDING, DAUGHTERLESS, MYOD, AND MYC PROTEINS [J].
MURRE, C ;
MCCAW, PS ;
BALTIMORE, D .
CELL, 1989, 56 (05) :777-783
[40]   INTERACTIONS BETWEEN HETEROLOGOUS HELIX-LOOP-HELIX PROTEINS GENERATE COMPLEXES THAT BIND SPECIFICALLY TO A COMMON DNA-SEQUENCE [J].
MURRE, C ;
MCCAW, PS ;
VAESSIN, H ;
CAUDY, M ;
JAN, LY ;
JAN, YN ;
CABRERA, CV ;
BUSKIN, JN ;
HAUSCHKA, SD ;
LASSAR, AB ;
WEINTRAUB, H ;
BALTIMORE, D .
CELL, 1989, 58 (03) :537-544
1234567