A Comparative Study of Neuroepithelial Cells and O2 Sensitivity in the Gills of Goldfish (Carrasius auratus) and Zebrafish (Danio rerio)

Zachar, Peter C.

January 2014

Serotonin (5-HT)-containing neuroepithelial cells (NECs) of the gill filament are believed to be the primary O2 chemosensors in fish. In the mammalian carotid body (CB), 5-HT is one of many neurotransmitters believed to play a role in transduction of hypoxic stimuli, with acetylcholine (ACh) being the primary fast-acting excitatory neurotransmitter. Immunohistochemistry and confocal microscopy was used to observe the presence of the vesicular acetylcholine transporter (VAChT), a marker for the presence of ACh, and its associated innervation in the gills of zebrafish. VAChT-positive cells were observed primarily along the afferent side of the filament, with some cells receiving extrabranchial innervation. No VAChT-positive cells were observed in the gills of goldfish; however, certain key morphological differences in the innervation of goldfish gills was observed, as compared to zebrafish. In addition, in zebrafish NECs, whole-cell current is dominated by an O2-sensitive background K+ current; however, this is just one of several currents observed in the mammalian CB. In zebrafish NECs and the CB, membrane depolarization in response to hypoxia, mediated by inhibition of the background K+ (KB) channels, is believed to lead to activation of voltage-gated Ca2+ (CaV) channels and Ca2+-dependent neurosecretion. Using patch-clamp electrophysiology, I discovered several ion channel types not previously observed in the gill chemosensors, including Ca2+-activated K+ (KCa), voltage-dependent K+ (KV), and voltage-activated Ca2+ (CaV) channels. Under whole-cell patch-clamp conditions, the goldfish NECs did not respond to hypoxia (PO2 ~ 11 mmHg). Employing ratiometric calcium imaging and an activity-dependent fluorescent vital dye, I observed that intact goldfish NECs respond to hypoxia (PO2 ~ 11 mmHg) with an increase in intracellular Ca2+ ([Ca2+]i) and increased synaptic vesicle activity. The results of these experiments demonstrate that (1) ACh appears to play a role in the zebrafish, but not goldfish gill, (2) goldfish NECs likely signal hypoxic stimuli primarily via the central nervous system (CNS), (3) goldfish NECs express a broad range of ion channels as compared to the NECs of zebrafish, and (4) goldfish NECs rely on some cytosolic factor(s) when responding to hypoxia (PO2 ~ 11 mmHg). This thesis represents a further step in the study of neurochemical and physiological adaptations to tolerance of extreme hypoxia.

hypoxia

anoxia

oxygen

neuroepithelial cell

goldfish

zebrafish

electrophysiology

patch-clamp

confocal microscopy

calcium imaging

Study of ribosome biogenesis factors in zebrafish neural progenitors / Étude des facteurs de la biogenèse des ribosomes dans les progéniteurs neuraux de poisson zèbre

Bouffard, Stéphanie

22 September 2017

Alors que la biogénèse des ribosomes a étéconsidérée comme un mécanisme ubiquiste, lesétapes de ce processus ont récemment étédémontrées comme étant tissu-spécifiques. Letoit optique (OT) du poisson-zèbre est un modèleapproprié pour étudier la prolifération cellulairepuisque les cellules à différents états dedifférenciation se trouvent dans des domainesséparés.Au cours de mon doctorat, j'ai examiné si lesgènes de la biogenèse des ribosomes peuventavoir des rôles spécifiques dans les cellulesprogénitrices neuroépithéliales (CPNe). Profitantd'une analyse transcriptomique antérieure, j'aid'abord examiné les nouveaux candidatsaccumulés dans les CPNe. J'ai décidé de meconcentrer sur proliferation-associated 2G4(pa2G4/ebp1) qui est exprimé de manièrepréférentielle dans les CPNe.Ce gène favorise ou réprime la proliférationcellulaire dans des organismes normaux oupendant la tumorigénèse. J'ai conçu une stratégiepour l'expression inductible et cellule-spécifiquede ce gène.Fibrillarin (Fbl), une méthyltranférasenucléolaire est également préférentiellementexprimée dans CPNe. Ce gène joue un rôleimportant dans le cancer. J'ai montré que lesmutants fbl présentaient des défauts OTspécifiques,en lien avec une apoptose massive etune absence de différenciation neurale. J'aiégalement démontré une diminution de l'activitéde traduction des ribosomes. En outre, lesmutants fbl montrent une progression de la phaseS altérée. Nos données suggèrent que fbl estessentiel à la prolifération des progéniteursneuronaux du poisson-zèbre. / While ribosome biogenesis has been consideredas an ubiquitous mechanism, steps of thisprocess have recently been shown to be tissuespecific. Zebrafish optic tectum (OT) is asuitable model to study cell proliferation sincecells at different differentiation states arespatially partitioned.During my PhD, I examined whether ribosomebiogenesis genes may have specific roles inneuroepithelial progenitor cells (NePCs).Taking advantage of a previous transcriptomicanalysis, I first screened for new candidatesaccumulated in NePCs. I decided to focus onproliferation-associated 2G4 (pa2g4/ebp1),which was expressed preferentially in NePCs.This gene promotes or represses cellproliferation in normal organisms or duringtumorigenesis. I designed a strategy for theinducible expression and cell specificexpression of this gene.Fibrillarin (Fbl), a small nucleolarmethyltransferase is also preferentiallyexpressed in NePCs. It plays an important rolein cancer. I showed that fbl mutants displayedspecific OT defects linked to a massiveapoptosis and an absence of neuraldifferentiation. I also demonstrated deficienciesin the ribosome translational activity.Additionally, fbl mutants showed impaired Sphaseprogression. Our data suggest that fbl isessential for the proliferation of zebrafishneuronal progenitors.

Biogenèse des ribosomes

Cellules neuroépithéliales

Poisson zèbre

Ribosome biogenesis

Neuroepithelial cells

Zebrafish

Processus régénératifs du cerveau moyen dorsal chez le poisson zèbre adulte / Midbrain regeneration in adult zebrafish

Heuzé, Aurélie

08 December 2017

Contrairement aux mammifères, le système nerveux central du poisson téléostéen adulte possède un potentiel énorme de neurogenèse et de régénération après une lésion cérébrale. Chez le poisson zèbre adulte, de nouveaux neurones peuvent être régénérés à partir de progéniteurs constitutifs ou latents. Au cours de mon doctorat, je me suis intéressée aux capacités de régénération neuronale du cerveau moyen dorsal (le toit optique, TO) chez le poisson zèbre. Le TO présente à sa périphérie une zone de progéniteurs de type neuroépithélial à l’origine des neurones et des cellules épendymogliales qui le constituent. J’ai tout d’abord identifié un enhancer potentiel du gène meis2a, qui m’a permis d’effectuer des lignages cellulaires de progéniteurs neuroépithéliaux. En contexte homéostatique, j’ai montré que ces progéniteurs construisent la totalité du TO pendant le développement et soutiennent sa neurogenèse continue pendant la croissance post-embryonnaire. A la suite d’une lésion cérébrale chez la larve et l’adulte, le TO à la capacité de générer de nouveaux neurones, toutefois sa structure topographique n’est pas restaurée. Chez l’adulte, j’ai montré que les progéniteurs constitutifs neuroépithéliaux et des progéniteurs latents épendymogliaux sont activés lors du processus de régénération. / Unlike mammals, the adult teleost brain exhibits widespread neurogenic activity and can regenerate after injury. The adult zebrafish has the capacity to regenerate neurons from constitutive or latent progenitors. During my PhD, I studied the neuronal regeneration in the zebrafish dorsal midbrain (optic tectum, OT). At adult stage, neuroepithelial-like progenitors at the OT periphery contribute to neuronal and glial lineages during homeostasis.I identified a putative enhancer of meis2a, which allowed me to trace the progeny of neuroepithelial-like progenitors. In a non-regenerative context I showed that enhancer-targeted progenitors were at the origin of the whole structure during development and of its continued neurogenesis during post-embryonic growth.Following lesion, OT displayed reactive neurogenesis, at larval and adult stages, nevertheless its topographical structure remained altered. In adults, I showed that both constitutive neuroepithelial-like progenitors and latent ependymoglial progenitors were activated in a regenerative context.

Régénération

Poisson-Zèbre

Toit optique

Cellules neuroépithéliales

Regeneration

Zebrafish

Optic tectum

Neuroepithelial cells

Metabolic, cardiac and ventilatory regulation in early larvae of the South African clawed frog, Xenopus laevis.

Pan, Tien-Chien

12 1900

Early development of O2 chemoreception and hypoxic responses under normoxic (150 mmHg) and chronically hypoxic (110 mmHg) conditions were investigated in Xenopus laevis from hatching to 3 weeks post fertilization. Development, growth, O2 consumption, ventilatory and cardiac performance, and branchial neuroepithelial cells (NEC) density and size were determined. At 3 days post fertilization (dpf), larvae started gill ventilation at a rate of 28 ± 4 beats/min and showed increased frequency to 60 ± 2 beats/min at a PO2 of 30 mmHg. Also at 3 dpf, NECs were identified in the gill filament buds using immunohistochemical methods. Lung ventilation began at 5 dpf and exhibited a 3-fold increase in frequency from normoxia to a PO2 of 30 mmHg. Hypoxic tachycardia developed at 5 dpf, causing an increase of 20 beats/min in heart rate, which led to a 2-fold increase in mass-specific cardiac output at a PO2 of 70 mmHg. At 10 dpf, gill ventilatory sensitivity to hypoxia increased, which was associated with the increase in NEC density, from 15 ± 1 to 29 ± 2 cells/mm of filament at 5 and 10 dpf, respectively. Unlike the elevated rate, cardiac and ventilatory volumes were independent of acute hypoxia. Despite increased cardioventilatory frequency, larvae experienced an average of 80% depression in during acute hypoxia. Chronic hypoxia (PO2 of 110 mmHg) decreased mass-specific cardiac performance before 10 dpf. In older larvae (10 to 21 dpf), chronic hypoxia decreased acute branchial and pulmonary hypoxic hyperventilation and increased NEC size. Collectively, these data suggest that larvae exhibit strong O2-driven acute hypoxic responses post-hatching, yet are still O2 conformers. All acute hypoxic responses developed before 5 dpf, and then the effects of chronic hypoxia started to show between 7 and 21 dpf. Thus, the early formation of acute hypoxic responses is susceptible to the environment and can be shaped by the ambient PO2.

Metabolism

Xenopus development

hypoxia

neuroepithelial cell

ventilation

Xenopus laevis -- Larvae.

Xenopus laevis -- Metabolism.

Xenopus laevis -- Cardiovascular system.

Xenopus laevis -- Respiration.