Modular development of the teleost trunk along the dorsoventral axis and <i>zic1/zic4</i> as selector genes in the dorsal module

Kawanishi, Toru; Kaneko, Takuya; Moriyama, Yuuta; Kinoshita, Masato; Yokoi, Hayato; Suzuki, Tohru; Shimada, Atsuko; Takeda, Hiroyuki

doi:10.1242/dev.088567

Cited by 20 publications

(42 citation statements)

References 61 publications

(73 reference statements)

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“…Given that HMD size correlates with transcriptional repression level, this HMD shortening might promote zic1/zic4 expression. To examine when this HMD shortening occurs during development, we additionally investigated the DNA methylation pattern in dorsal and ventral myotome at the hatching stage, a stage when the dorsal-specific expression of zic1/zic4 is already induced (Kawanishi et al, 2013). As expected, ChIP-qPCR revealed that the pattern of active and repressive histone modifications was already established in the dorsal and ventral myotome by the hatching stage ( Fig.…”

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 71%

“…We focused on the zic1 and zic4 (zic1/zic4) genes because they have a particularly large K27HMD (26 kb) in medaka blastula embryos (Fig. 5A) and their function has been extensively studied in medaka (Kawanishi et al, 2013;Moriyama et al, 2012). zic1/ zic4, organized head-to-head with a small intergenic sequence (∼3.4 kb), encode zinc-finger transcription factors and function in the neuronal development and specification of dorsal fate in the trunk (Kawanishi et al, 2013;Merzdorf, 2007).…”

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 99%

“…5A) and their function has been extensively studied in medaka (Kawanishi et al, 2013;Moriyama et al, 2012). zic1/ zic4, organized head-to-head with a small intergenic sequence (∼3.4 kb), encode zinc-finger transcription factors and function in the neuronal development and specification of dorsal fate in the trunk (Kawanishi et al, 2013;Merzdorf, 2007). They are thought to share cis-regulatory elements and thus their expression is nearly identical.…”

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 99%

“…It is known that their expression is activated by secreted factors during embryogenesis, and is autonomously maintained throughout life in the dorsal parts of somite derivatives, i.e. the myotome, dermis and vertebrae (Kawanishi et al, 2013). Thus, these genes served as a good example with which to analyze the change in epigenetic states of key developmental genes from embryo to adult.…”

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 99%

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Large hypomethylated domains serve as strong repressive machinery for key developmental genes in vertebrates

et al. 2014

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DNA methylation is a fundamental epigenetic modification in vertebrate genomes and a small fraction of genomic regions is hypomethylated. Previous studies have implicated hypomethylated regions in gene regulation, but their functions in vertebrate development remain elusive. To address this issue, we generated epigenomic profiles that include base-resolution DNA methylomes and histone modification maps from both pluripotent cells and mature organs of medaka fish and compared the profiles with those of human ES cells. We found that a subset of hypomethylated domains harbor H3K27me3 (K27HMDs) and their size positively correlates with the accumulation of H3K27me3. Large K27HMDs are conserved between medaka and human pluripotent cells and predominantly contain promoters of developmental transcription factor genes. These key genes were found to be under strong transcriptional repression, when compared with other developmental genes with smaller K27HMDs. Furthermore, human-specific K27HMDs show an enrichment of neuronal activityrelated genes, which suggests a distinct regulation of these genes in medaka and human. In mature organs, some of the large HMDs become shortened by elevated DNA methylation and associate with sustained gene expression. This study highlights the significance of domain size in epigenetic gene regulation. We propose that large K27HMDs play a crucial role in pluripotent cells by strictly repressing key developmental genes, whereas their shortening consolidates long-term gene expression in adult differentiated cells.

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Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 71%

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 99%

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 99%

Section: Human-specific K27hmds Mark Genes Related To Neuronal Activimentioning

confidence: 99%

See 2 more Smart Citations

Large hypomethylated domains serve as strong repressive machinery for key developmental genes in vertebrates

et al. 2014

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“…All of these five genes can act as transcription factors to affect early embryo development. For instances, Dmrta2 in mice is essential in the early development of the telencephalon via the formation of the cortical hem and maintaining of neural progenitors [39]; homeobox genes HOXA9 and HOXA7 spatially and temporally regulate morphogenesis and differentiation during embryonic development [40]; homeobox gene SIX3 provides necessary instructions for the formation of the forebrain and eye development [41]; ZIC4 has been proposed to regulate lateemerging characteristics in the dorsal surface with ZIC1 [42]. Due to their important roles in embryo development, methylation of these genes could affect important cellular functions and eventually promote tumorigenesis.…”

Section: Discussionmentioning

confidence: 99%

Selection of Sensitive Methylation Markers for the Detection of Non-small Cell Lung Cancer

Zhao¹,

Jen²,

Peikert³

2015

J Mol Biomark Diagn

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Platyfish bypass the constraint of the caudal fin ventral identity in teleosts

Rees

König

Jaźwińska

2022

Developmental Dynamics

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Background: The caudal fin of teleosts is characterized by dorsoventral symmetry. Despite this external morphology, the principal rays of this appendage connect to bones below the notochord, indicating the ventral (hypochordal) identity of this organ. Results: Here, we report that this typical architecture of the caudal fin is not fully conserved in the platyfish (Xiphophorus maculatus) and the guppy (Poecilia reticulata), representatives of the Poeciliidae family. We show that in these species, 3–4 principal rays connect to bones above the notochord, suggesting an epichordal contribution. Consistently, as examined in platyfish, dorsal identity genes zic1/4 were highly expressed in these rays, providing molecular evidence of their epichordal origin. Developmental analysis revealed that the earliest rays above the notochord emerge at the 10‐ray stage of fin morphogenesis. In contrast to zebrafish and medaka, platyfish and guppies display a mirrored shape of dorsal and ventral processes of the caudal endoskeleton. Our study suggests that an ancestral bauplan expanded in poeciliids by advancing its symmetrical pattern. Conclusion: The platyfish evolved a fin architecture with the epichordal origin of its upper principal rays and a high level of symmetry in the caudal endoskeleton. This innovative architecture highlights the adaptation of the teleost skeleton.

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Modular development of the teleost trunk along the dorsoventral axis and zic1/zic4 as selector genes in the dorsal module

Cited by 20 publications

References 61 publications

Large hypomethylated domains serve as strong repressive machinery for key developmental genes in vertebrates

Large hypomethylated domains serve as strong repressive machinery for key developmental genes in vertebrates

Selection of Sensitive Methylation Markers for the Detection of Non-small Cell Lung Cancer

Platyfish bypass the constraint of the caudal fin ventral identity in teleosts

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