Scaling of the Bicoid morphogen gradient by a volume-dependent production rate

Cheung, David T.; Miles, Cecelia M.; Kreitman, Martin; Ma, Jun

doi:10.1242/dev.064402

Cited by 67 publications

(145 citation statements)

References 54 publications

(104 reference statements)

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“…22 In addition, it recapitulates the scaling properties of the Bcd gradient 23 by simply assuming a correlation between the Bcd production rate and embryo volume. 12 This hypothesized correlation was recently observed experimentally 13 through quantitative measurements of bcd mRNA in large and small embryos from selected Drosophila lines. 24 Since our model is based on Bcd diffusion and degradation while incorporating relevant, biologically realistic features of the embryo, our results suggest that the diffusion model-despite the inadequacies of its idealized form in fully capturing Bcd gradient properties-remains a .…”

Section: Bcd Gradient Formation Simulated In a Biologically Realisticmentioning

confidence: 54%

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Morphogen gradient formation and action

Liu

2011

Fly

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Section: Bcd Gradient Formation Simulated In a Biologically Realisticmentioning

confidence: 54%

“…51 Importantly, the scaling properties of hb can also be traced directly to the scaling properties of the Bcd gradient. 12,13,23 These and other results have led us to propose in reference 23 that the Bcd gradient itself is a robust system (see also refs. 34 and 49).…”

Section: ©2 0 1 1 L a N D E S B I O S C I E N C E D O N O T D I S Tmentioning

confidence: 90%

Morphogen gradient formation and action

Liu

2011

Fly

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“…Taking the data from Cheung et al with ( / ) 1/2 = 99 microns [5], assuming = 0.4 is the spatial location where the critical threshold is crossed in the embryo (near the Hunchback boundary), and using = 645 for the large embryo and 0 = 518 for the small embryo, the calculated optimal flux is 67% greater in the large embryo than the flux in the small embryo 0 . This is remarkably close to the increase in amplitude measured for Bcd scaling of 66.9% .…”

Section: B Scaling By Flux Optimizationmentioning

confidence: 99%

“…Recently Cheung et al, [5] investigated the spatial patterns of Bcd patterning between artificially selected populations of an initially wild type Drosophila melanogaster. After successive rounds of selection, two populations were developed that differed in egg length by about 25%.…”

Section: Introductionmentioning

confidence: 99%

Scale invariance of morphogen-mediated patterning by flux optimization

Umulis

Othmer

2012

2012 5th International Conference on BioMedical Engineering and Informatics

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Abstract-The development of an organism from a single cell into an adult requires exquisite control of spatial patterning so that the correct tissues are formed at the correct place and at the correct time. A number of molecular factors that regulate spatial patterning of tissues during development have been identified, however, relatively little is known about how they form consistent spatial patterns of cell signaling or gene expression that scales in proportion to the size of the tissue being patterned. In the model organism Drosophila melanogaster, embryonic morphogen gradients establish the anterior/posterior (AP) and dorsal/ventral (DV) axes to establish the boundaries of gene expression that are further subdivided into distinct cell types. Both AP and DV patterning systems exhibit a high degree of scaling, however, they have evolved distinct mechanisms to achieve scaling. Our analysis herein shows that recently discovered data for Bicoid (the principle AP morphogen) embryonic patterning is consistent for a mechanism that optimizes the flux of Bcd molecules into the anterior end. This mechanism is distinct from mechanisms suggested in other systems that target biophysical properties that regulate morphogen range, thereby stretching or shrinking the morphogen distribution accordingly. Instead, flux optimization changes the morphogen peak levels to provide "approximate" scaling over a large region of space and perfect scaling at a single spatial location. While remarkably simple, this mechanism of scale-invariance is sufficient for increases and decreases in tissue size by 50% and confers less than 10% error in spatial patterning.

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“…The Drosophila activator Bicoid (Bcd) forms a concentration gradient in early embryos and instructs anterior-posterior patterning (Grimm et al, 2010;Lohr et al, 2010;. It offers an excellent system for studying transcriptional activation mechanisms in both space and time (Gregor et al, 2007a, b;He et al, 2008;Deng et al, 2010;He et al, 2010a, b;Cheung et al, 2011;. A recently reported method of simultaneously, and quantitatively, detecting Bcd and the nascent transcripts of its target genes in early Drosophila embryos made it possible to evaluate the role of this activator in the actual events of transcriptional bursts, as opposed to the accumulated products .…”

Section: Transcriptional Burstsmentioning

confidence: 99%