Independent regulation of initiation and maintenance phases ofHoxa3expression in the vertebrate hindbrain involve auto- and cross-regulatory mechanisms-Reference-Cited by-同舟云学术

Independent regulation of initiation and maintenance phases ofHoxa3expression in the vertebrate hindbrain involve auto- and cross-regulatory mechanisms

Published:2001-09-15 Issue:18 Volume:128 Page:3595-3607
ISSN:1477-9129
Container-title:Development
language:en
Short-container-title:

Author:

Manzanares Miguel¹²,Bel-Vialar Sophie¹,Ariza-McNaughton Linda¹³,Ferretti Elisabetta⁴,Marshall Heather¹⁵,Maconochie Mark M.⁶,Blasi Francesco⁴,Krumlauf Robb¹⁵²

Affiliation:

1. Division of Developmental Neurobiology, MRC National Institute for Medical Research, The Ridgeway, Mill Hill, London NW7 1AA, UK

2. Present address: Department of Developmental Neurobiology, Instituto Cajal, CSIC, Av. Doctor Arce 37, 28002 Madrid, Spain

3. Present address: The Sanger Centre, Wellcome Trust Genome Campus, Hinxton, Cambridgshire CB10 1SA, UK

4. Molecular Genetics Unit, DIBIT, Università Vita-Salute S. Raffaele, via Olgettina 58, 20132 Milan, Italy

5. Stowers Institute for Medical Research, 1000 East 50th Street, Kansas City, MO 64110, USA

6. Mammalian Genetics Unit, MRC, Harwell, Oxon OX11 0RD, UK

Abstract

During development of the vertebrate hindbrain, Hox genes play multiples roles in the segmental processes that regulate anteroposterior (AP) patterning. Paralogous Hox genes, such as Hoxa3, Hoxb3 and Hoxd3, generally have very similar patterns of expression, and gene targeting experiments have shown that members of paralogy group 3 can functionally compensate for each other. Hence, distinct functions for individual members of this family may primarily depend upon differences in their expression domains. The earliest domains of expression of the Hoxa3 and Hoxb3 genes in hindbrain rhombomeric (r) segments are transiently regulated by kreisler, a conserved Maf b-Zip protein, but the mechanisms that maintain expression in later stages are unknown. In this study, we have compared the segmental expression and regulation of Hoxa3 and Hoxb3 in mouse and chick embryos to investigate how they are controlled after initial activation. We found that the patterns of Hoxa3 and Hoxb3 expression in r5 and r6 in later stages during mouse and chick hindbrain development were differentially regulated. Hoxa3 expression was maintained in r5 and r6, while Hoxb3 was downregulated. Regulatory comparisons of cis-elements from the chick and mouse Hoxa3 locus in both transgenic mouse and chick embryos have identified a conserved enhancer that mediates the late phase of Hoxa3 expression through a conserved auto/cross-regulatory loop. This block of similarity is also present in the human and horn shark loci, and contains two bipartite Hox/Pbx-binding sites that are necessary for its in vivo activity in the hindbrain. These HOX/PBC sites are positioned near a conserved kreisler-binding site (KrA) that is involved in activating early expression in r5 and r6, but their activity is independent of kreisler. This work demonstrates that separate elements are involved in initiating and maintaining Hoxa3 expression during hindbrain segmentation, and that it is regulated in a manner different from Hoxb3 in later stages. Together, these findings add further strength to the emerging importance of positive auto- and cross-regulatory interactions between Hox genes as a general mechanism for maintaining their correct spatial patterns in the vertebrate nervous system.

Publisher

The Company of Biologists

Subject

Developmental Biology,Molecular Biology

Link

http://journals.biologists.com/dev/article-pdf/128/18/3595/1136775/3595.pdf

Reference82 articles.

1. Alexandre, D., Clarke, J., Oxtoby, E., Yan, Y.-L., Jowett, T. and Holder, N. (1996). Ectopic expression of Hoxa-1 in the zebrafish alters the fate of the mandibular arch neural crest and phenocopies a retinoic acid-induced phenotype. Development122, 735-746.

2. Aparicio, S., Morrison, A., Gould, A., Gilthorpe, J., Chaudhuri, C., Rigby, P. W. J., Krumlauf, R. and Brenner, S. (1995). Detecting conserved regulatory elements with the model genome of the Japanese puffer fish Fugu rubripes. Proc. Natl. Acad. Sci. USA92, 1684-1688.

3. Barrow, J. R., Stadler, H. S. and Capecchi, M. R. (2000). Roles of Hoxa1 and Hoxa2 in patterning the early hindbrain of the mouse. Development127, 933-944.

4. Bell, E., Wingate, R. and Lumsden, A. (1999). Homeotic transformation of rhombomere identity after localized Hoxb1 misexpression. Science284, 2168-2171.

5. Bergson, C. and McGinnis, W. (1990). An auto-regulatory enhancer element of the Drosophila homeotic gene Deformed. EMBO J.9, 4287-4297.

Cited by 49 articles. 订阅此论文施引文献订阅此论文施引文献，注册后可以免费订阅5篇论文的施引文献，订阅后可以查看论文全部施引文献

1. The pioneering function of the hox transcription factors;Seminars in Cell & Developmental Biology;2022-12

2. Hoxb1 Regulates Distinct Signaling Pathways in Neuromesodermal and Hindbrain Progenitors to Promote Cell Survival and Specification;Stem Cells;2022-01-24

3. Transcriptional Regulation and Implications for Controlling Hox Gene Expression;Journal of Developmental Biology;2022-01-10

4. The landscape of regulatory genes in brain-wide neuronal phenotypes of a vertebrate brain;eLife;2021-12-13

5. The Hox protein conundrum: The “specifics” of DNA binding for Hox proteins and their partners;Developmental Biology;2021-09