Mechanisms for controlling Dorsal nuclear levels.

Front Cell Dev Biol

California Institute of Technology, Division of Biology and Biological Engineering, Pasadena, CA, United States.

Published: August 2024

AI Article Synopsis

  • The Dorsal nuclear-cytoplasmic gradient is crucial for establishing proper gene expression patterns along the dorsal-ventral axis during embryo development, which ultimately supports embryo viability.
  • Although Toll signaling is known to assist in forming this gradient, other mechanisms like post-translational modifications, shuttling, and nuclear spacing also play significant roles in achieving the correct levels of Dorsal in the nucleus.
  • Understanding these mechanisms not only illuminates Dorsal's function in early fly embryos but may also provide broader insights into gene expression regulation during critical developmental transitions.

Article Abstract

Formation of the Dorsal nuclear-cytoplasmic gradient is important for the proper establishment of gene expression patterns along the dorsal-ventral (DV) axis during embryogenesis in . Correct patterning of the DV axis leads to formation of the presumptive mesoderm, neurogenic ectoderm, dorsal ectoderm, and amnioserosa, which are tissues necessary for embryo viability. While Toll signaling is necessary for Dorsal gradient formation, a gradient still forms in the absence of Toll, suggesting there are additional mechanisms required to achieve correct nuclear Dorsal levels. Potential mechanisms include post-translational modification, shuttling, and nuclear spacing. Post-translational modification could affect import and export rates either directly through modification of a nuclear localization sequence or nuclear export sequence, or indirectly by affecting interactions with binding partners that alter import and export rates. Shuttling, which refers to the facilitated diffusion of Dorsal through its interaction with its cytoplasmic inhibitor Cactus, could regulate nuclear levels by delivering more Dorsal ventrally. Finally, nuclear spacing could result in higher nuclear levels by leaving fewer nuclei in the ventral domain to uptake Dorsal. This review details how each of these mechanisms may help establish Dorsal nuclear levels in the early fly embryo, which serves as a paradigm for understanding how the dynamics of graded inputs can influence patterning and target gene expression. Furthermore, careful analysis of nuclear Dorsal levels is likely to provide general insights as recent studies have suggested that the regulation of nuclear import affects the timing of gene expression at the maternal-to-zygotic transition.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11330768PMC
http://dx.doi.org/10.3389/fcell.2024.1436369DOI Listing

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