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BRCA1相关的环状结构域(BARD1)蛋白中功能和一级结构的保守性。

Conservation of function and primary structure in the BRCA1-associated RING domain (BARD1) protein.

作者信息

Ayi T C, Tsan J T, Hwang L Y, Bowcock A M, Baer R

机构信息

Department of Microbiology, University of Texas Southwestern Medical Center, Dallas 75235, USA.

出版信息

Oncogene. 1998 Oct 22;17(16):2143-8. doi: 10.1038/sj.onc.1202123.

DOI:10.1038/sj.onc.1202123
PMID:9798686
Abstract

The BRCA1 gene encodes a tumor suppressor that has been implicated in hereditary forms of breast and ovarian cancer. During S phase of the cell cycle, BRCA1 polypeptides are found in discrete nuclear bodies ('BRCA1 nuclear dots') together with HsRad51, a human homolog of the E. coli recA protein, and BARD1, a protein that interacts with BRCA1 to form a stable heterodimer. BARD1 is structurally similar to BRCA1 in that both molecules harbor an amino-terminal RING domain and two carboxy-terminal BRCT domains. Here we describe the amino acid sequence and expression pattern of murine Bard1. A comparison of the mouse and human sequences reveals that the recognizable protein motifs of BARD1 are well conserved, including the RING domain, the three tandem ankyrin repeats, and, to a lesser extent, the two BRCT domains. However, the remaining sequences of BARD1 display a markedly lower degree of phylogenetic conservation, comparable to those reported for BRCA1 and BRCA2. Moreover, murine Bard1 retains the ability to associate in vivo with BRCA1, and its expression pattern in adult mice mirrors that of Brca1, with elevated levels of RNA transcripts found in the testes and spleen. These data suggest that BRCA1 and BARD1 have co-evolved to participate in a common pathway of tumor suppression.

摘要

BRCA1基因编码一种肿瘤抑制因子,它与遗传性乳腺癌和卵巢癌有关。在细胞周期的S期,BRCA1多肽与HsRad51(大肠杆菌recA蛋白的人类同源物)以及BARD1(一种与BRCA1相互作用形成稳定异二聚体的蛋白质)一起存在于离散的核体(“BRCA1核点”)中。BARD1在结构上与BRCA1相似,因为这两个分子都含有一个氨基末端的RING结构域和两个羧基末端的BRCT结构域。在这里,我们描述了小鼠Bard1的氨基酸序列和表达模式。小鼠和人类序列的比较表明,BARD1可识别的蛋白质基序保守性良好,包括RING结构域、三个串联的锚蛋白重复序列,以及在较小程度上的两个BRCT结构域。然而,BARD1的其余序列显示出明显较低的系统发育保守程度,与报道的BRCA1和BRCA2相当。此外,小鼠Bard1在体内仍具有与BRCA1结合的能力,其在成年小鼠中的表达模式与Brca1相似,在睾丸和脾脏中发现RNA转录本水平升高。这些数据表明,BRCA1和BARD1共同进化以参与共同的肿瘤抑制途径。

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