Progressive myoclonic epilepsy-associated geneKctd7regulates retinal neurovascular patterning and function

AbstractNeuron function relies on and instructs the development and precise organization of neurovascular units that in turn support circuit activity. However, our understanding of the molecular cues that regulate this relationship remains sparse. Using a high-throughput screening pipeline, we recently identified several new regulators of vascular patterning. Among these was the potassium channel tetramerization domain-containing protein 7 (KCTD7). Mutations inKCTD7are associated with progressive myoclonic epilepsy, but how KCTD7 regulates neural development and function remains poorly understood. To begin to identify such mechanisms, we focus on mouse retina, a tractable part of the central nervous system that contains precisely ordered neuron subtypes supported by a trilaminar intravascular network. We find that deletion ofKctd7results in defective patterning of the adult retina vascular network, resulting in increased branching, vessel length, and lacunarity. These alterations reflect early and specific defects in vessel development, as emergence of the superficial and deep vascular layers were delayed. These defects are likely due to a role for Kctd7 in inner retina neurons. Kctd7 it is absent from vessels but present in neurons in the inner retina, and its deletion resulted in a corresponding increase in the number of bipolar cells in development and increased vessel branching in adults. These alterations were accompanied by retinal function deficits. Together, these data suggest that neuronal Kctd7 drives growth and patterning of the vasculature and suggest that neurovascular interactions may participate in the pathogenesis of KCTD7-related human diseases.Alevy et al. HighlightsKctd7 is required for normal retinal vascular organization and retinal function in adults.Deletion ofKctd7disrupts the emergence of the superficial and deep vessel layers.Kctd7 may impact vascular patterning through influencing neurons as it is expressed in and regulates bipolar cells.Kctd7 driven neurovascular interactions may participate in the pathogenesis of KCTD7-related human diseases.Lay SummaryNeuron function requires an organized vasculature to maintain brain health and prevent disease, but many neurovasculature regulatory genes remain unknown. Alevy et al. identify the progressive myoclonic epilepsy-associated geneKctd7as a key regulator of vascular development and retinal function. They further show that Kctd7 regulation of vessel patterning likely occurs downstream of its role in regulating the development or activity of specific neuron types. These data suggest that KCTD7-regulated neurovascular interactions may participate in the pathogenesis of associated human diseases.

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Progressive myoclonic epilepsy-associated gene Kctd7 regulates retinal neurovascular patterning and function

Neurochemistry International ◽

10.1016/j.neuint.2019.104486 ◽

2019 ◽

Vol 129 ◽

pp. 104486 ◽

Cited By ~ 1

Author(s):

Jonathan Alevy ◽

Courtney A. Burger ◽

Nicholas E. Albrecht ◽

Danye Jiang ◽

Melanie A. Samuel

Keyword(s):

Myoclonic Epilepsy ◽

Progressive Myoclonic Epilepsy ◽

And Function

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OTX2 non-cell autonomous activity regulates inner retinal function

10.1101/2020.02.12.945584 ◽

2020 ◽

Author(s):

Raoul Torero-Ibad ◽

Bilal Mazhar ◽

Clémentine Vincent ◽

Clémence Bernard ◽

Julie Dégardin ◽

...

Keyword(s):

Visual Acuity ◽

Transcription Factor ◽

Bipolar Cells ◽

Retinal Function ◽

Single Chain ◽

Inner Retina ◽

Cell Functions ◽

Conditional Expression ◽

Autonomous Activity ◽

Retinal Structure

AbstractOTX2 is a homeoprotein transcription factor expressed in photoreceptors and bipolar cells in the retina. OTX2, like many other homeoproteins, transfers between cells and exerts non-cell autonomous effects such as promoting survival of retinal ganglion cells that do not express the protein. Here we used a genetic approach to target extracellular OTX2 in the retina by conditional expression of a secreted single chain anti-OTX2 antibody. Compared to control mice, the expression of this antibody by Parvalbumin-expressing neurons in the retina is followed by a reduction in visual acuity in one-month-old mice with no alteration of the retinal structure or cell type number or aspect. A- and b-waves measured by electroretinogram were also indistinguishable from control mice, suggesting no functional deficit of photoreceptors and bipolar cells. Mice expressing the OTX2-neutralizing antibody did show a significant doubling in the flicker amplitude, consistent with a change in inner retinal function. Our results show that interfering in vivo with OTX2 non-cell autonomous activity in the postnatal retina leads to an alteration in inner retinal cell functions and causes a deficit in visual acuity.Significance statementOTX2 is a homeoprotein transcription factor expressed in retinal photoreceptors and bipolar cells. Although the Otx2 locus is silent in the inner retina, the protein is detected in cells of the ganglion cell layer consistent with the ability of this class of proteins to transfer between cells. We expressed a secreted single chain antibody (scFv) against OTX2 in the retina to neutralize extracellular OTX2. Antibody expression leads to reduced visual acuity with no change in retinal structure, or photoreceptor or bipolar physiology; however, activity in the inner retina was altered. Thus, interfering with OTX2 non-cell autonomous activity in postnatal retina alters inner retinal function and causes vision loss, highlighting the physiological value of homeoprotein direct non-cell autonomous signaling.

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Molecular mechanisms regulating cytotoxic lymphocyte development and function, and their associations to human diseases

10.3389/978-2-88919-279-3 ◽

2015 ◽

Keyword(s):

Molecular Mechanisms ◽

Human Diseases ◽

Lymphocyte Development ◽

Cytotoxic Lymphocyte ◽

And Function

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Insect Behavioral Change and the Potential Contributions of Neuroinflammation—A Call for Future Research

Genes ◽

10.3390/genes12040465 ◽

2021 ◽

Vol 12 (4) ◽

pp. 465

Author(s):

Colleen A. Mangold ◽

David P. Hughes

Keyword(s):

Behavioral Change ◽

Potential Role ◽

Insect Behavior ◽

Future Research ◽

Cell Physiology ◽

Behavioral Manipulation ◽

Neuroimmune Communication ◽

And Function ◽

Neuron Function ◽

Insect Innate Immunity

Many organisms are able to elicit behavioral change in other organisms. Examples include different microbes (e.g., viruses and fungi), parasites (e.g., hairworms and trematodes), and parasitoid wasps. In most cases, the mechanisms underlying host behavioral change remain relatively unclear. There is a growing body of literature linking alterations in immune signaling with neuron health, communication, and function; however, there is a paucity of data detailing the effects of altered neuroimmune signaling on insect neuron function and how glial cells may contribute toward neuron dysregulation. It is important to consider the potential impacts of altered neuroimmune communication on host behavior and reflect on its potential role as an important tool in the “neuro-engineer” toolkit. In this review, we examine what is known about the relationships between the insect immune and nervous systems. We highlight organisms that are able to influence insect behavior and discuss possible mechanisms of behavioral manipulation, including potentially dysregulated neuroimmune communication. We close by identifying opportunities for integrating research in insect innate immunity, glial cell physiology, and neurobiology in the investigation of behavioral manipulation.

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Subcellular Localization and Complements of GABAA and GABAC Receptors on Bullfrog Retinal Bipolar Cells

Journal of Neurophysiology ◽

10.1152/jn.2000.84.2.666 ◽

2000 ◽

Vol 84 (2) ◽

pp. 666-676 ◽

Cited By ~ 37

Author(s):

Jiu-Lin Du ◽

Xiong-Li Yang

Keyword(s):

Subcellular Localization ◽

Receptor Antagonist ◽

Gaba Receptor ◽

Drug Application ◽

Bipolar Cells ◽

Visual Signals ◽

Receptor Subtypes ◽

Inner Retina ◽

Axon Terminals ◽

Retinal Bipolar Cells

γ-Aminobutyric acid (GABA) receptors on retinal bipolar cells (BCs) are highly relevant to spatial and temporal integration of visual signals in the outer and inner retina. In the present work, subcellular localization and complements of GABAA and GABACreceptors on BCs were investigated by whole cell recordings and local drug application via multi-barreled puff pipettes in the bullfrog retinal slice preparation. Four types of the BCs (types 1–4) were identified morphologically by injection of Lucifer yellow. According to the ramification levels of the axon terminals and the responses of these cells to glutamate (or kainate) applied at their dendrites, types 1 and 2 of BCs were supposed to be off type, whereas types 3 and 4 of BCs might be on type. Bicuculline (BIC), a GABAA receptor antagonist, and imidazole-4-acetic acid (I4AA), a GABAC receptor antagonist, were used to distinguish GABA receptor-mediated responses. In all BCs tested, not only the axon terminals but also the dendrites showed high GABA sensitivity mediated by both GABAA and GABACreceptors. Subcellular localization and complements of GABAA and GABAC receptors at the dendrites and axon terminals were highly related to the dichotomy of offand on BCs. In the case of off BCs, GABAA receptors were rather evenly distributed at the dendrites and axon terminals, but GABAC receptors were predominantly expressed at the axon terminals. Moreover, the relative contribution of GABAC receptors to the axon terminals was prevalent over that of GABAA receptors, while the situation was reversed at the dendrites. In the case of on BCs, GABAA and GABAC receptors both preferred to be expressed at the axon terminals; relative contributions of these two GABA receptor subtypes to both the sites were comparable, while GABAC receptors were much less expressed than GABAA receptors. GABAA, but not GABAC receptors, were expressed clusteringly at axons of a population of BCs. In a minority of BCs, I4AA suppressed the GABAC responses at the dendrites, but not at the axon terminal, implying that the GABAC receptors at these two sites may be heterogeneous. Taken together, these results suggest that GABAA and GABAC receptors may play different roles in the outer and inner retina and the differential complements of the two receptors on off and on BCs may be closely related to physiological functions of these cells.

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