人类FOX基因家族（综述）

Human FOX gene family (Review).

作者信息

Katoh Masuko, Katoh Masaru

机构信息

M&M Medical BioInformatics, Hongo 113-0033, Japan.

出版信息

Int J Oncol. 2004 Nov;25(5):1495-500.

PMID:15492844

Abstract

Human Forkhead-box (FOX) gene family consists of at least 43 members, including FOXA1, FOXA2, FOXA3, FOXB1, FOXC1, FOXC2, FOXD1, FOXD2, FOXD3, FOXD4, FOXD5 (FOXD4L1), FOXD6 (FOXD4L3), FOXE1, FOXE2, FOXE3, FOXF1, FOXF2, FOXG1 (FOXG1B), FOXH1, FOXI1, FOXJ1, FOXJ2, FOXJ3, FOXK1, FOXK2, FOXL1, FOXL2, FOXM1, FOXN1, FOXN2 (HTLF), FOXN3 (CHES1), FOXN4, FOXN5 (FOXR1), FOXN6 (FOXR2), FOXO1 (FOXO1A), FOXO2 (FOXO6), FOXO3 (FOXO3A), FOXO4 (MLLT7), FOXP1, FOXP2, FOXP3, FOXP4, and FOXQ1. FOXE3-FOXD2 (1p33), FOXQ1-FOXF2-FOXC1 (6p25.3), and FOXF1-FOXC2-FOXL1 (16q24.1) loci are FOX gene clusters within the human genome. Members of FOX subfamilies A-G, I-L and Q were grouped into class 1 FOX proteins, while members of FOX subfamilies H and M-P were grouped into class 2 FOX proteins. C-terminal basic region within the FOX domain was the common feature of class 1 FOX proteins. FOXH1 and FOXO1 mRNAs are expressed in human embryonic stem (ES) cells. FOXC1, FOXC2, FOXE1, FOXE3, FOXL2, FOXN1, FOXP2 and FOXP3 genes are mutated in human congenital disorders. FOXA1 gene is amplified and over-expressed in esophageal and lung cancer. FOXM1 gene is up-regulated in pancreatic cancer and basal cell carcinoma due to the transcriptional regulation by Sonic Hedgehog (SHH) pathway. FOXO1 gene is fused to PAX3 or PAX7 genes in rhabdomyosarcoma. FOXO3 and FOXO4 genes are fused to MLL gene in hematological malignancies. Deregulation of FOX family genes leads to congenital disorders, diabetes mellitus, or carcinogenesis. Expression profiles, genetic alterations and epigenetic changes of FOX family genes as well as binding proteins and target genes of FOX family transcription factors should be comprehensively investigated to develop novel therapeutics and preventives for human diseases.

摘要

人类叉头框（FOX）基因家族至少由43个成员组成，包括FOXA1、FOXA2、FOXA3、FOXB1、FOXC1、FOXC2、FOXD1、FOXD2、FOXD3、FOXD4、FOXD5（FOXD4L1）、FOXD6（FOXD4L3）、FOXE1、FOXE2、FOXE3、FOXF1、FOXF2、FOXG1（FOXG1B）、FOXH1、FOXI1、FOXJ1、FOXJ2、FOXJ3、FOXK1、FOXK2、FOXL1、FOXL2、FOXM1、FOXN1、FOXN2（HTLF）、FOXN3（CHES1）、FOXN4、FOXN5（FOXR1）、FOXN6（FOXR2）、FOXO1（FOXO1A）、FOXO2（FOXO6）、FOXO3（FOXO3A）、FOXO4（MLLT7）、FOXP1、FOXP2、FOXP3、FOXP4和FOXQ1。FOXE3 - FOXD2（1p33）、FOXQ1 - FOXF2 - FOXC1（6p25.3）以及FOXF1 - FOXC2 - FOXL1（16q24.1）位点是人类基因组中的FOX基因簇。FOX亚家族A - G、I - L和Q的成员被归类为1类FOX蛋白，而FOX亚家族H和M - P的成员被归类为2类FOX蛋白。FOX结构域内的C端碱性区域是1类FOX蛋白的共同特征。FOXH1和FOXO1 mRNA在人类胚胎干细胞中表达。FOXC1、FOXC2、FOXE1、FOXE3、FOXL2、FOXN1、FOXP2和FOXP3基因在人类先天性疾病中发生突变。FOXA1基因在食管癌和肺癌中扩增并过度表达。由于Sonic Hedgehog（SHH）信号通路的转录调控，FOXM1基因在胰腺癌和基底细胞癌中上调。在横纹肌肉瘤中，FOXO1基因与PAX3或PAX7基因融合。在血液系统恶性肿瘤中，FOXO3和FOXO4基因与MLL基因融合。FOX家族基因的失调会导致先天性疾病、糖尿病或癌症发生。应全面研究FOX家族基因的表达谱、基因改变和表观遗传变化，以及FOX家族转录因子的结合蛋白和靶基因，以开发针对人类疾病的新型治疗方法和预防措施。