Suppressor of Fused Is Required to Maintain the Multipotency of Neural Progenitor Cells in the Retina

Cwinn, M.; Mazerolle, Chantal; McNeill, Brian; Ringuette, Randy; Thurig, Sherry; Hui, Chi‐chung; Wallace, Valerie A.

doi:10.1523/jneurosci.5495-10.2011

Cited by 29 publications

(25 citation statements)

References 57 publications

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“…The SHH pathway is the target of receptor (dys)function, as other morphogen pathways are not altered (e.g., Ihh and Bmp4) (Figures 3A and S3B) or decreased secondarily as shown by downregulation of WNT activity by SAG ( Figure 5D). Enhanced RPC proliferation as a consequence of increased Hh signaling is also seen in mice heterozygous for the Ptch1 gene defect (Moshiri and Reh, 2004) or in animals lacking Sufu, an inhibitor of the SHH pathway (Cwinn et al, 2011). In contrast, a WNT signaling defect in mice lacking b-catenin in the retina causes a decrease, rather than an increase, in the progenitor cell pool (Liu et al, 2007).…”

Section: Lrp2 Deficiency Causes Ectopic Induction Of Shh Activity In mentioning

confidence: 99%

LRP2 Acts as SHH Clearance Receptor to Protect the Retinal Margin from Mitogenic Stimuli

et al. 2015

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During forebrain development, LRP2 promotes morphogen signaling as an auxiliary SHH receptor. However, in the developing retina, LRP2 assumes the opposing function, mediating endocytic clearance of SHH and antagonizing morphogen action. LRP2-mediated clearance prevents spread of SHH activity from the central retina into the retinal margin to protect quiescent progenitor cells in this niche from mitogenic stimuli. Loss of LRP2 in mice increases the sensitivity of the retinal margin for SHH, causing expansion of the retinal progenitor cell pool and hyperproliferation of this tissue. Our findings document the ability of LRP2 to act, in a context-dependent manner, as activator or inhibitor of the SHH pathway. Our current findings uncovered LRP2 activity as the molecular mechanism imposing quiescence of the retinal margin in the mammalian eye and suggest SHH-induced proliferation of the retinal margin as cause of the large eye phenotype observed in mouse models and patients with LRP2 defects.

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Section: Lrp2 Deficiency Causes Ectopic Induction Of Shh Activity In mentioning

confidence: 99%

LRP2 Acts as SHH Clearance Receptor to Protect the Retinal Margin from Mitogenic Stimuli

et al. 2015

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“…Our own results support these findings, as expression of Su(fu) reduces the ability of Ci ACT to activate a Ci-dependent luciferase reporter. Within the mouse eye, loss of Su(fu) leads to an increase in Hh signaling which in turn results in retinal hyperplasia, late onset premature exit from the cell cycle, and an increase in the number of horizontal and amacrine cells at the expense of other cell types (Cwinn et al, 2011). By contrast, Su(fu) does not appear to be a rate-limiting component of the Hh pathway in Drosophila and, as such, null mutants are completely viable and have normally constructed eyes (Préat, 1992;Shi et al, 2011;Zhou and Kalderon, 2011).…”

Section: Developmentmentioning

confidence: 99%

Extramacrochaetae imposes order on the Drosophila eye by refining the activity of the Hedgehog signaling gradient

Spratford

Kumar

2013

Development

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The compound eye of Drosophila melanogaster is configured by a differentiating wave, the morphogenetic furrow, that sweeps across the eye imaginal disc and transforms thousands of undifferentiated cells into a precisely ordered repetitive array of 800 ommatidia. The initiation of the furrow at the posterior margin of the epithelium and its subsequent movement across the eye field is controlled by the activity of the Hedgehog (Hh) signaling pathway. Differentiating photoreceptors that lie behind the furrow produce and secrete the Hh morphogen, which is captured by cells within the furrow itself. This leads to the stabilization of the full-length form of the zinc-finger transcription factor Cubitus interruptus (Ci155), the main effector of Hh signaling. Ci155 functions as a transcriptional activator of a number of downstream targets, including decapentaplegic (dpp), a TGFβ homolog. In this report, we describe a mechanism that is in place within the fly retina to limit Hh pathway activity within and ahead of the furrow. We demonstrate that the helix-loop-helix (HLH) protein Extramacrochaetae (Emc) regulates Ci155 levels. Loss of emc leads to an increase in Ci155 levels, nuclear migration, apical cell constriction and an acceleration of the furrow. We find that these roles are distinct from the bHLH protein Hairy (H), which we show restricts atonal (ato) expression ahead of the furrow. Secondary furrow initiation along the dorsal and ventral margins is blocked by the activity of the Wingless (Wg) pathway. We also show that Emc regulates and cooperates with Wg signaling to inhibit lateral furrow initiation.

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“…2) while centrally localized RPC require Pax6 to retain multipotency (Oron-Karni et al, 2008). Recently, Pax6 was identified as being downstream of suppressor-of-fused (Sufu), a negative regulator of the Hedgehog signaling pathway (Cwinn et al, 2011;Svard et al, 2006;Varjosalo et al, 2006). Conditional loss of Sufu in the proximal retina results in Pax6 down-regulation and phenocopies the Pax6 conditional knockout described above Pax6 is required to maintain multipotency of RPC and restrict Crx expression in peripheral RPC.…”

Section: Irx6mentioning

confidence: 99%

“…Up-regulation of Crx also positively regulates its own expression. (Cwinn et al, 2011). In addition to its role in the neural retina, Pax6 is required for lens development.…”

Section: Irx6mentioning

confidence: 99%

The role of homeobox genes in retinal development and disease

Zagozewski

Zhang

Pinto

et al. 2014

Developmental Biology

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Homeobox genes are an evolutionarily conserved class of transcription factors that are critical for development of many organ systems, including the brain and eye. During retinogenesis, homeodomain-containing transcription factors, which are encoded by homeobox genes, play essential roles in the regionalization and patterning of the optic neuroepithelium, specification of retinal progenitors and differentiation of all seven of the retinal cell classes that derive from a common progenitor. Homeodomain transcription factors control retinal cell fate by regulating the expression of target genes required for retinal progenitor cell fate decisions and for terminal differentiation of specific retinal cell types. The essential role of homeobox genes during retinal development is demonstrated by the number of human eye diseases, including colobomas and anophthalmia, which are attributed to homeobox gene mutations. In the following review, we highlight the role of homeodomain transcription factors during retinogenesis and regulation of their gene targets. Understanding the complexities of vertebrate retina development will enhance our ability to drive differentiation of specific retinal cell types towards novel cell-based replacement therapies for retinal degenerative diseases.

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Suppressor of Fused Is Required to Maintain the Multipotency of Neural Progenitor Cells in the Retina

Cited by 29 publications

References 57 publications

LRP2 Acts as SHH Clearance Receptor to Protect the Retinal Margin from Mitogenic Stimuli

LRP2 Acts as SHH Clearance Receptor to Protect the Retinal Margin from Mitogenic Stimuli

Extramacrochaetae imposes order on the Drosophila eye by refining the activity of the Hedgehog signaling gradient

The role of homeobox genes in retinal development and disease

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