Optic cup formation: a calcium-regulated process.

Brady, Richard C.; Hilfer, S. Robert

doi:10.1073/pnas.79.18.5587

Cited by 43 publications

(25 citation statements)

References 16 publications

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“…This interpretation is further supported by the finding that none of 48 stage 11-13 + embryos exhibited reopening of the occluded neurocoels when treated for 4 h r in medium 199 with agents known to mobilize intracellular Ca2+: 10 mM caffeine or theophylline. The concentration of these two drugs was identical to that used by Brady and Hilfer (1982) to show that in chick embryos of stages similar to those used in our study, optic cup morphogenesis was not reversed by 10 mM caffeine or theophylline.…”

Section: Pharmacological Reversal Of Spinal Cord Occlusionsupporting

confidence: 60%

“…To determine whether occlusion requires calmodulin, embryos with occluded neurocoels were treated with three pharmacological agents known to be antagonists of calmodulin: chlorpromazine (CPZ) (Brady and Hilfer, 1982;Levin and Weiss, 1979), trifluperazine (TFP) (Levin and Weiss, 19771, and N-(6-aminohexyl)-5-chloro-1-napthalenesulfonamide (W-7) (Hidaka et al, 1981). The rationale for these treatments was based on the prevailing cell biology theory that all calmodulin reactions require Ca2' (Cheung, 1980).…”

Section: This Brings Up the Interesting Question Of How Ca2mentioning

confidence: 99%

“…It could also be argued that Ca2+ mediated its effect on neurocoel occlusion via a putative intrinsic mechanism: contraction of cytoplasmic actomyosin, considered to be a major force in bending the neural plate into a tube Nagele, 1985, 1988;Moran and Rice, 1976) and the invagination of the optic vesicle to form the optic cup (Brady and Hilfer, 1982). Furthermore, it is well known that actomyosin interaction in nonmuscle cells is a process dependent on Ca2+ (Brady and Hilfer, 1982;Cohen and de Vries, 1973;Korn, 1978) and calmodulin (Cheung, 1980;Yerna et al, 1979). However, when Desmond and Schoenwolf (1986) treated embryos with cytochalasin D a t concentrations effective in depolymerizing microfilaments, the neurocoels remained occluded.…”

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confidence: 99%

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Second messenger regulation of occlusion of the spinal neurocoel in the chick embryo

Desmond

Duzy

Federici

1993

Developmental Dynamics

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We know that, once rostra1 neurulation is completed in the neuroaxis of the chick embryo, the caudal neurocoel becomes occluded and the brain rapidly expands. However, very little is known about the mechanisms maintaining occlusion. Studies had shown that occluded neurocoels reopened in embryos treated with chelators of cations, but the reasons remained unclear and the cations unidentified. To begin defining the role of cations, this study explored the effect of CaZC, calmodulin, and cAMP on maintaining the occluded neurocoel. Chick embryos during the natural phase of neurocoel occlusion (stage 12) were cultured in vitro with drugs known to modulate Ca2+ transport, to inhibit calmodulin activity, or to elevate cAMP levels. To test if occlusion is a Ca2+-dependent process, embryos were treated with verapamil and ionophore A23187. To test if occlusion requires calmodulin, embryos were treated with antipsychotic agents. To test if occlusion is cAMP dependent, embryos were treated with methylisobutylxanthine (MIX), forskolin (FOR), or dibutyl cyclic adenosine (DbC). Following each treatment, occlusion of the neurocoel was tested by injecting dye into the midbrain. All treatments resulted in a predominant number of precocious reopenings of the occluded neurocoels. MIX-treated, naked neural tubes had a fourfold increase in CAMP, whereas FOR-and DbCtreated neural tubes showed ten-and 14-fold increases, respectively. The presence of calmodulin in the cells of the neural tube was confirmed by fluorescent tagging and 3H-chlorpromazine labelling. The combined results of this study show that occlusion of the spinal neurocoel depends on exogenous Ca2+, requires calmodulin, and is cAMP sensitive. 0 1993 Wiley-Liss, Inc.

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Section: Pharmacological Reversal Of Spinal Cord Occlusionsupporting

confidence: 60%

Section: This Brings Up the Interesting Question Of How Ca2mentioning

confidence: 99%

mentioning

confidence: 99%

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Second messenger regulation of occlusion of the spinal neurocoel in the chick embryo

Desmond

Duzy

Federici

1993

Developmental Dynamics

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“…It has been postulated that the cellular cytoskeleton plays a role in the folding of numerous embryonal epithelial primordia (Hilfer and Searls 1986), and changes in the organisation of actin and myosin could bring about constriction of cell apices, inducing epithelial invagination. In this regard experimental manipulation of ATP levels or disruption in the transport of Ca ++ , conditions that interfere with the interaction of cytoskeletal actin and myosin, have been shown to disrupt invagination of the thyroid placode (Hilfer et al 1977), optic vesicle (Brady and Hilfer 1982), nasal placode (Smuts 1981) and neural plate (Lee et al 1983;Schoenwolf et al 1988;Ferreira and Hilfer 1993). Nevertheless, these manipulations apparently have no effect on invagination of the otic placode (Hilfer et al 1989), which indicates that the factors in question do not play a decisive role in the epithelial folds leading to otic vesicle formation.…”

Section: Introductionmentioning

confidence: 99%

Basal lamina heparan sulphate proteoglycan is involved in otic placode invagination in chick embryos

Moro-Balbás

Gato

Alonso

et al. 2000

Anatomy and Embryology

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Formation of the otocyst from the otic placode appears to differ from invagination of other cup-shaped organ primordia. It is known that the cellular cytoskeleton plays a limited role in otic placode invagination, whilst the extracellular matrix underlying the otic primordium intervenes in the folding process. In this study we have analysed the role of the basal lamina heparan sulphate proteoglycan in otic primordium invagination. At 10 H.H. stage, heparan sulphate proteoglycan immunomarking begins to appear on the otic placode basal lamina, increasing noticeably at 13 H.H. stage, coinciding with maximum folding of the otic epithelium, and is still present at later stages. Enzyme degradation of heparan sulphate proteoglycan in the otic primordium basal lamina, by means of microinjection with heparinase III prior to folding, significantly disrupts invagination of the otic placode, which remains practically flat, with a significant reduction in the depth of the otic pit and an increase in the diameter of the otic opening. The immunocytochemistry analysis revealed a notable depletion of basal lamina heparan sulphate proteoglycan in the otic primordia microinjected with heparinase, with no statistically significant differences observed in the volume or rate of cell proliferation in the otic epithelium relative to the control, which suggests that heparan sulphate proteoglycan disruption does not interfere with the epithelial growth. In addition, a study of apoptosis distribution by the TUNEL method confirmed that treatment with heparinase does not cause interference with cell survival in the otic epithelium. Our findings support the theory that otic primordium invagination may be regulated, at least in part, by the basal lamina components, which might contribute towards anchoring the otic epithelium to adjacent structures.

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“…It has been suggested that this mechanism operates during the invagination of different ectodermic placodes such as the lens itself, the otic and nasal placodes and the neural tube, among others (Wrenn and Wessells, 1969;Bancroft and Bellairs, 1977;Brady and Hilfer, 1982;Ferreira and Hilfer, 1993); (2) a high rate of cell replication in the lens placode, with respect to the surrounding surface ectoderm, has been proposed as the mechanism responsible for creating forces involved in lens placode invagination (Modak, Morris and Yamada, 1968;Harding et al, 1971;Hendrix and Zwaan, 1974;A Â lvarez and Navascues, 1990;Hendrix, Madras and Johnson, 1993); (3) certain extracellular factors and, more speci®cally, extracellular matrix molecules, appear to be associated with epithelial invagination. What is more, it is known that alteration of the synthesis or enzyme degrading of particular matrix molecules such as collagen, certain proteoglycans and glycoproteins, may disrupt epithelial folding, as occurs in the branching of the salivary gland, lung and kidney primordia (Spooner and Faubion, 1980;Thompson and Spooner, 1983;Spooner, Bassett and Stokes, 1985;Nakanishi et al, 1986;Klein et al, 1989).…”

Section: Introductionmentioning

confidence: 99%

Chondroitin Sulphate Proteoglycan is Involved in Lens Vesicle Morphogenesis in Chick Embryos

Gato

Martín

Alonso

et al. 2001

Experimental Eye Research

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Proteoglycans have been implicated in the invagination and formation of various embryonal cavitied primordia. In this paper the expression of chondroitin sulphate proteoglycan is analysed (CSPG) in the lens primordium during lens vesicle formation, and demonstrate that this proteoglycan has a speci®c distribution pattern with regard to invagination and fusion processes in the transformation of placode into lens vesicle. More speci®cally, CSPG was detached in: (1) the apical surface of lens epithelial cells, where early CSPG expression was observed in the whole of the lens placode whilst in the vesicle phase it was restricted to the posterior epithelium; (2) intense CSPG expression in the basal lamina, which remained constant for the entire period under study; (3) CSPG expression in the intercellular spaces of the lens primordium epithelium, which increased during the invagination of the primordium and which at the vesicle stage was more evident in the posterior epithelium; and (4) CSPG expression on the edges of the lens placode both prior to and during fusion. Treatment with b-D-xyloside causes signi®cant CSPG depletion in the lens primordium together with severe alterations in the invagination and fusion of the lens vesicle; this leads to the formation of lens primordia which in some cases remain practically¯at or show partial invagination defects or fusion disruption. Similar results were obtained by enzyme digestion with chondroitinase AC but not with type II heparinase, which indicates that alterations induced by b-Dxyloside were due to interference in CSPG synthesis. The ®ndings demonstrate that CSPG is a common component of the lens primordium at the earliest developmental stages during which it undergoes speci®c modi®cations. It also includes experimental evidence to show that`in vivo' CSPG plays an important role in the invagination and fusion processes of the lens primordium.

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Optic cup formation: a calcium-regulated process.

Cited by 43 publications

References 16 publications

Second messenger regulation of occlusion of the spinal neurocoel in the chick embryo

Second messenger regulation of occlusion of the spinal neurocoel in the chick embryo

Basal lamina heparan sulphate proteoglycan is involved in otic placode invagination in chick embryos

Chondroitin Sulphate Proteoglycan is Involved in Lens Vesicle Morphogenesis in Chick Embryos

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