Turtle interacts with borderless in regulating glial extension and axon ensheathment

Chen, Yixu; Cameron, Scott A.; Chang, Wen-Tzu; Rao, Yong

doi:10.1186/s13041-017-0299-6

Cited by 13 publications

(28 citation statements)

References 19 publications

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“…knocking down CadN disrupted the organization of R-cell axonal terminals in the optic lobe, and also caused abnormal axonal terminal morphology. However, the fact that WG projected normally in CadN knockdown animals suggests that unlike that of Tutl and Bdl [9,10], the adhesive property of CadN is not involved in mediating the recognition between Rcell axons and WG for the extension of WG processes.…”

Section: Discussionmentioning

confidence: 94%

“…And Tutl protein expressed on R-cell axons binds to the WG-specific Bdl in promoting WG extension [9]. Thus, a decrease in the number of R cells may reduce the levels of R-cell-derived factors for WG differentiation and extension.…”

Section: Discussionmentioning

confidence: 99%

“…Recent studies identify several neuron-derived factors that coordinate the development of R cells and WG [8,9]. It is shown that the neuron-derived FGF8like ligand Thisbe promotes the differentiation of PG into WG, which migrate along the surface of R-cell axons and subsequently insulate R-cell axons [8].…”

Section: Introductionmentioning

confidence: 99%

“…It is shown that the neuron-derived FGF8like ligand Thisbe promotes the differentiation of PG into WG, which migrate along the surface of R-cell axons and subsequently insulate R-cell axons [8]. Our previous studies reveal that the immunoglobulin (Ig) superfamily transmembrane protein Turtle (Tutl) expressed on R-cell axons binds to the WG-specific cell-surface receptor Borderless (Bdl) to promote WG extension and axonal ensheathment [9,10]. While it is reported that WG also plays an active role in regulating the topographic projection of R-cell axons in the optic lobe [11], the underlying mechanisms remain unclear.…”

Section: Introductionmentioning

confidence: 99%

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An RNAi screen for secreted factors and cell-surface players in coordinating neuron and glia development in Drosophila

2020

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The establishment of the functional nervous system requires coordinated development of neurons and glia in the embryo. Our understanding of underlying molecular and cellular mechanisms, however, remains limited. The developing Drosophila visual system is an excellent model for understanding the developmental control of the nervous system. By performing a systematic transgenic RNAi screen, we investigated the requirements of secreted proteins and cell-surface receptors for the development of photoreceptor neurons (R cells) and wrapping glia (WG) in the Drosophila visual system. From the screen, we identified seven genes whose knockdown disrupted the development of R cells and/or WG, including amalgam (ama), domeless (dome), epidermal growth factor receptor (EGFR), kuzbanian (kuz), N-Cadherin (CadN), neuroglian (nrg), and shotgun (shg). Cell-type-specific analysis revealed that ama is required in the developing eye disc for promoting cell proliferation and differentiation, which is essential for the migration of glia in the optic stalk. Our results also suggest that nrg functions in both eye disc and WG for coordinating R-cell and WG development.

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Section: Discussionmentioning

confidence: 94%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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An RNAi screen for secreted factors and cell-surface players in coordinating neuron and glia development in Drosophila

2020

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“…Furthermore, EGF secreted by photoreceptor neurons activates EGFR signaling in wrapping glia. In response, wrapping glial cells secrete insulin like peptides to induce neuronal differentiation in the lamina and thereby function as a signaling relay (Fernandes, Chen, Rossi, Zipfel, & Desplan, ). Thus, wrapping glial cells are not only necessary for photoreceptor clustering and insulation but also function in the communication between the different cell types.…”

Section: Optic Nerve Modelmentioning

confidence: 99%

Drosophila glia: Few cell types and many conserved functions

Yildirim

Petri

Kottmeier

et al. 2018

Glia

138

153

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Glial cells constitute without any dispute an essential element in providing an efficiently operating nervous system. Work in many labs over the last decades has demonstrated that neuronal function, from action potential generation to its propagation, from eliciting synaptic responses to the subsequent postsynaptic integration, is evolutionarily highly conserved. Likewise, the biology of glial cells appears conserved in its core elements and therefore, a deeper understanding of glial cells is expected to benefit from analyzing model organisms such as Drosophila melanogaster. Drosophila is particularly well suited for studying glial biology since in the fly nervous system only a limited number of glial cells exists, which can be individually identified based on position and a set of molecular markers. In combination with the well‐known genetic tool box an unprecedented level of analysis is feasible, that not only can help to identify novel molecules and principles governing glial cell function but also will help to better understand glial functions first identified in the mammalian nervous system. Here we review the current knowledge on Drosophila glia to spark interest in using this system to analyze complex glial traits in the future.

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