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Published November 7, 2008 | Published + Supplemental Material
Journal Article Open

A Precise Bicoid Gradient Is Nonessential during Cycles 11–13 for Precise Patterning in the Drosophila Blastoderm

Abstract

Background: During development, embryos decode maternal morphogen inputs into highly precise zygotic gene expression. The discovery of the morphogen Bicoid and its profound effect on developmental programming in the Drosophila embryo has been a cornerstone in understanding the decoding of maternal inputs. Bicoid has been described as a classical morphogen that forms a concentration gradient along the antero-posterior axis of the embryo by diffusion and initiates expression of target genes in a concentration-dependent manner in the syncytial blastoderm. Recent work has emphasized the stability of the Bicoid gradient as a function of egg length and the role of nuclear dynamics in maintaining the Bicoid gradient. Bicoid and nuclear dynamics were observed but not modulated under the ideal conditions used previously. Therefore, it has not been tested explicitly whether a temporally stable Bicoid gradient prior to cellularization is required for precise patterning. Principal Findings: Here, we modulate both nuclear dynamics and the Bicoid gradient using laminar flows of different temperature in a microfluidic device to determine if stability of the Bicoid gradient prior to cellularization is essential for precise patterning. Dramatic motion of both cytoplasm and nuclei was observed prior to cellularization, and the Bicoid gradient was disrupted by nuclear motion and was highly abnormal as a function of egg length. Despite an abnormal Bicoid gradient during cycles 11–13, Even-skipped patterning in these embryos remained precise. Conclusions: These results indicate that the stability of the Bicoid gradient as a function of egg length is nonessential during syncytial blastoderm stages. Further, presumably no gradient formed by simple diffusion on the scale of egg length could be responsible for the robust antero-posterior patterning observed, as severe cytoplasmic and nuclear motion would disrupt such a gradient. Additional mechanisms for how the embryo could sense its dimensions and interpret the Bicoid gradient are discussed.

Additional Information

Copyright: © 2008 Lucchetta et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. We thank Eric F. Wieschaus for providing the Bcd-eGFP stock, Gerold Schubiger for providing the His2AvD-GFP stock, Nipam H. Patel and Manfred Frasch for providing antibodies, Nipam H. Patel and Kevin P. White for helpful discussions, and Elizabeth W. Boyd for contributions to writing and editing this manuscript. We thank referees for helpful suggestions. Author Contributions: Conceived and designed the experiments: EML RFI. Performed the experiments: EML MEV. Analyzed the data: EML. Contributed reagents/materials/analysis tools: RFI. Wrote the paper: EML RFI. Funding: This work was funded by NIH Grant No. R01 GM077331 and the Yen Postdoctoral Fellowship (E.M.L.). Competing interests: The authors have declared that no competing interests exist.

Attached Files

Published - Ismagilov_PLoSONE_2008_3_e3651_bcd_elena.pdf

Supplemental Material - Ismagilov_Bcd_PLoS_ONE_EML_SI_v1.pdf

Supplemental Material - journal.pone.0003651.s012.avi

Supplemental Material - journal.pone.0003651.s013.avi

Supplemental Material - journal.pone.0003651.s014.avi

Supplemental Material - journal.pone.0003651.s015.avi

Supplemental Material - journal.pone.0003651.s016.avi

Supplemental Material - journal.pone.0003651.s017.avi

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