Your search keyword '"Reese, Benjamin"' showing total 46 results

1. DNER and NFIA are expressed by developing and mature AII amacrine cells in the mouse retina.

Author

Keeley, Patrick W. and Reese, Benjamin E.

Abstract

The present study has taken advantage of publicly available cell type specific mRNA expression databases in order to identify potential genes participating in the development of retinal AII amacrine cells. We profile two such genes, Delta/Notch-like EGF repeat containing ( Dner) and nuclear factor I/A ( Nfia), that are each heavily expressed in AII amacrine cells in the mature mouse retina, and which conjointly identify this retinal cell population in its entirety when using antibodies to DNER and NFIA. DNER is present on the plasma membrane, while NFIA is confined to the nucleus, consistent with known functions of each of these two proteins. DNER also identifies some other subsets of retinal ganglion and amacrine cell types, along with horizontal cells, while NFIA identifies a subset of bipolar cells as well as Muller glia and astrocytes. During early postnatal development, NFIA labels astrocytes on the day of birth, AII amacrine cells at postnatal (P) day 5, and Muller glia by P10, when horizontal cells also transiently exhibit NFIA immunofluorescence. DNER, by contrast, is present in ganglion and amacrine cells on P1, also labeling the horizontal cells by P10. Developing AII amacrine cells exhibit accumulating DNER labeling at the dendritic stalk, labeling that becomes progressively conspicuous by P10, as it is in maturity. This developmental time course is consistent with a prospective role for each gene in the differentiation of AII amacrine cells. [ABSTRACT FROM AUTHOR]

Published

2018

2. Genomic control of neuronal demographics in the retina.

Author

Reese, Benjamin E. and Keeley, Patrick W.

Subjects

*RETINAL anatomy, *GENETIC transcription, *PHENOTYPES, *POPULATION biology, *STATISTICAL correlation

Abstract

The mature retinal architecture is composed of various types of neuron, each population differing in size and constrained to particular layers, wherein the cells achieve a characteristic patterning in their local organization. These demographic features of retinal nerve cell populations are each complex traits controlled by multiple genes affecting different processes during development, and their genetic determinants can be dissected by correlating variation in these traits with their genomic architecture across recombinant-inbred mouse strains. Using such a resource, we consider how the variation in the numbers of twelve different types of retinal neuron are independent of one another, including those sharing transcriptional regulation as well as those that are synaptically-connected, each mapping to distinct genomic loci. Using the populations of two retinal interneurons, the horizontal cells and the cholinergic amacrine cells, we present in further detail examples where the variation in neuronal number, as well as the variation in mosaic patterning or in laminar positioning, each maps to discrete genomic loci where allelic variants modulating these features must be present. At those loci, we identify candidate genes which, when rendered non-functional, alter those very demographic properties, and in turn, we identify candidate coding or regulatory variants that alter protein structure or gene expression, respectively, being prospective contributors to the variation in phenotype. This forward-genetic approach provides an alternative means for dissecting the molecular genetic control of neuronal population dynamics, with each genomic locus serving as a causal anchor from which we may ultimately understand the developmental principles responsible for the control of those traits. [ABSTRACT FROM AUTHOR]

Published

2016

3. HOLDING ON TO CLARITY: RECONCILING THE FEDERAL KIDNAPPING STATUTE WITH THE TRAFFICKING VICTIMS PROTECTION ACT.

Author

Reese, Benjamin

Subjects

*LEGAL status of human trafficking victims, *FEDERAL court decisions, *KIDNAPPING -- Law & legislation, *HUMAN trafficking laws, *LEGAL status of victims of violent crimes, KIDNAPPING Act, 1932 (U.S.), STATE statutes (United States)

Abstract

In recent decades, the international community has come to recognize human trafficking as a problem of epidemic proportions. Congress responded to this global crisis in 2000 by passing the Trafficking Victims Protection Act (TVPA) and has since supplemented that comprehensive enactment. But, in light of the widespread use of psychological rather than physical coercion in trafficking cases, a long-standing split among federal courts regarding the scope of the federal kidnapping statute raises significant concerns about the United States' efforts to combat traffickers. In particular, the broad interpretation adopted by several circuits threatens effective enforcement of statutes designed to prosecute traffickers, endangers the due process rights of potential defendants, and risks rendering the criminal provisions of the TVPA superfluous. This Note argues that those broader interpretations are incorrect as a matter of proper statutory interpretation, and especially when considered in light of the passage of the TVPA. It further contends that, in kidnapping-by-deception cases, the prose- cution must demonstrate that the defendant intended to back up the deception with force or the threat of force if his ruse failed. [ABSTRACT FROM AUTHOR]

Published

2015

4. Design principles and developmental mechanisms underlying retinal mosaics.

Author

Reese, Benjamin E. and Keeley, Patrick W.

Subjects

*RETINAL anatomy, *DEVELOPMENTAL neurobiology, *CENTRAL nervous system, *CELL differentiation, *BRAIN anatomy, *REGENERATIVE medicine, *ANATOMY

Abstract

ABSTRACT Most structures within the central nervous system ( CNS) are composed of different types of neuron that vary in both number and morphology, but relatively little is known about the interplay between these two features, i.e. about the population dynamics of a given cell type. How such arrays of neurons are distributed within a structure, and how they differentiate their dendrites relative to each other, are issues that have recently drawn attention in the invertebrate nervous system, where the genetic and molecular underpinnings of these organizing principles are being revealed in exquisite detail. The retina is one of the few locations where these principles have been extensively studied in the vertebrate CNS, indeed, where the design principles of 'mosaic regularity' and 'uniformity of coverage' were first explicitly defined, quantified, and related to each other. Recent studies have revealed a number of genes that influence the formation of these histotypical features in the retina, including homologues of those invertebrate genes, although close inspection reveals that they do not always mediate comparable developmental processes nor elucidate fundamental design principles. The present review considers just how pervasive these features of 'mosaic regularity' and 'uniform dendritic coverage' are within the mammalian retina, discussing the means by which such features can be assessed in the mature and developing nervous system and examining the limitations associated with those assessments. We then address the extent to which these two design principles co-exist within different populations of neurons, and how they are achieved during development. Finally, we consider the neural phenotypes obtained in mutant nervous systems, to address whether a prospective gene of interest underlies those very design principles. [ABSTRACT FROM AUTHOR]

Published

2015

5. Cell numbers, cell ratios, and developmental plasticity in the rod pathway of the mouse retina.

Author

Keeley, Patrick W., Patel, Shivam S., and Reese, Benjamin E.

Subjects

*PHOTORECEPTORS, *RETINA, *BIPOLAR cells, *APOPTOSIS, *MICE, *FLUORESCENCE angiography

Abstract

The precise specification of cellular fate is thought to ensure the production of the correct number of neurons within a population. Programmed cell death may be an additional mechanism controlling cell number, believed to refine the proper ratio of pre‐ to post‐synaptic neurons for a given species. Here, we consider the size of three different neuronal populations in the rod pathway of the mouse retina: rod photoreceptors, rod bipolar cells, and AII amacrine cells. Across a collection of 28 different strains of mice, large variation in the numbers of all three cell types is present. The variation in their numbers is not correlated, so that the ratio of rods to rod bipolar cells, as well as rod bipolar cells to AII amacrine cells, varies as well. Establishing connectivity between such variable pre‐ and post‐synaptic populations relies upon plasticity that modulates process outgrowth and morphological differentiation, which we explore experimentally for both rod bipolar and AII amacrine cells in a mouse retina with elevated numbers of each cell type. While both rod bipolar dendritic and axonal arbors, along with AII lobular arbors, modulate their areal size in relation to local homotypic cell densities, the dendritic appendages of the AII amacrine cells do not. Rather, these processes exhibit a different form of plasticity, regulating the branching density of their overlapping arbors. Each form of plasticity should ensure uniformity in retinal coverage in the presence of the independent specification of afferent and target cell number. [ABSTRACT FROM AUTHOR]

Published

2023

6. Development of the retina and optic pathway

Author

Reese, Benjamin E.

Subjects

*RETINA, *VISUAL pathways, *CELL proliferation, *CELL differentiation, *MOLECULAR biology, *CELL death, *NEURONS, *THALAMUS

Abstract

Abstract: Our understanding of the development of the retina and visual pathways has seen enormous advances during the past 25years. New imaging technologies, coupled with advances in molecular biology, have permitted a fuller appreciation of the histotypical events associated with proliferation, fate determination, migration, differentiation, pathway navigation, target innervation, synaptogenesis and cell death, and in many instances, in understanding the genetic, molecular, cellular and activity-dependent mechanisms underlying those developmental changes. The present review considers those advances associated with the lineal relationships between retinal nerve cells, the production of retinal nerve cell diversity, the migration, patterning and differentiation of different types of retinal nerve cells, the determinants of the decussation pattern at the optic chiasm, the formation of the retinotopic map, and the establishment of ocular domains within the thalamus. [Copyright &y& Elsevier]

Published

2011

7. Role of Afferents in the Differentiation of Bipolar Cells in the Mouse Retina.

Author

Keeley, Patrick W. and Reese, Benjamin E.

Subjects

*BIOLOGICAL neural networks, *DENDRITIC cells, *PHOTORECEPTORS, *NEURONS, *RETINA

Abstract

To establish dendritic arbors that integrate properly into a neural circuit, neurons must rely on cues from the local environment. The neurons presynaptic to these arbors, the afferents, are one potential source of these cues, but the particular dendritic features they regulate remain unclear. Retinal bipolar cells can be classified by the type of photoreceptor, cone or rod, forming synaptic contacts with their dendrites, suggesting a potential role of these afferents in shaping the bipolar cell dendritic arbor. In the present investigation, the role of photoreceptors in directing the differentiation of bipolar cells has been studied using two genetically modified "coneless" and "conefull" mice. Single cone (Type 7/CB4a) and rod bipolar cells were labeled with DiI to reveal the entire dendritic arbor and subsequently analyzed for several morphological features. For both cone and rod bipolar cells, the dendritic field area, number of dendritic terminals, and stratification of terminals in the outer plexiform layer were comparable among coneless, conefull, and wild-type retinas, and the overall morphological appearance of each type of cell was essentially conserved, indicating an independence from afferent specification. The presence of normal afferents was, however, found to be critical for the proper spatial distribution of dendritic terminals, exhibiting a clustered distribution for the cone bipolar cells and a dispersed distribution for the rod bipolar cells. These results demonstrate a selectivity in the afferent dependency of bipolar cell differentiation, their basic morphogenetic plan commanded cell intrinsically, and their fine terminal connectivity directed by the afferents themselves. [ABSTRACT FROM AUTHOR]

Published

2010

8. Afferents and Homotypic Neighbors Regulate Horizontal Cell Morphology, Connectivity, and Retinal Coverage.

Author

Reese, Benjamin E., Raven, Mary A., and Stagg, Stephanie B.

Subjects

*CELLS, *INTERNEURONS, *DENDRITES, *PHOTORECEPTORS, *CELL morphology

Abstract

Horizontal cells are inhibitory interneurons with laterally oriented dendrites that overlap one another, contacting the pedicles of cone photoreceptors. Because of their regular spacing, the network of horizontal cells provides a uniform coverage of the retinal surface. The developmental processes establishing these network properties are undefined, but cell-intrinsic instructions and interactions with other cells have each been suggested to play a role. Here, we show that the intercellular spacing of horizontal cells is essentially independent of genetic background and is predicted by local density, suggesting that horizontal cell positioning is modulated by proximity to other horizontal cells. Dendritic field area compensates for this variation in intercellular spacing, maintaining constant dendritic coverage between strains. Functional dendritic overlap is achieved anatomically at the level of the pedicles, where horizontal cells interact with one another to establish their connectivity: the number of dendritic terminals contacting a pedicle changes, reciprocally, between neighboring horizontal cells during development based on their relative proximity to each pedicle. Cellular morphology is also shown to be regulated by the afferents themselves: afferent elimination before innervation does not alter dendritic field size nor stratification but compromises dendritic branching and prevents terminal formation. Afferent and homotypic interactions therefore generate the morphology, spacing, and connectivity of horizontal cells underlying their functional coverage of the retina. [ABSTRACT FROM AUTHOR]

Published

2005

9. Topography of Photoreceptors and Retinal Ganglion Cells in the Spotted Hyena (Crocuta crocuta).

Author

Calderone, Jack B., Reese, Benjamin E., and Jacobs, Gerald H.

Subjects

*PHOTORECEPTORS, *SPOTTED hyena

Abstract

The spatial distributions of photoreceptors and retinal ganglion cells were examined in the spotted hyena (Crocuta crocuta). Two populations of cones were identified by immunocytochemical labeling. The hyena retina contains approximately 2.3 million middle- to long-wavelength sensitive (M/L) cones that reach peak densities of about 7,500/mm[sup 2] in the vicinity of the optic nerve head. A sparser population of short-wavelength sensitive (S) cones, totaling about 0.3 million, was also detected. There is a striking disparity in the spatial distributions of the two cone types with S cones achieving peak density in a region located well below the optic nerve head. The differences in the spatial distributions of the two cone types have implications both for visual sensitivity and for color vision. Hyena rods outnumber cones by about 100:1 with rod density falling off modestly along a central-peripheral gradient. Ganglion cells were identified in retinal wholemounts by Nissl staining patterns. Their distribution defines a prominent visual streak with highest spatial packing (approx. 4,200/mm[sup 2] ) in an area centralis that is located in the temporal retina. The total number of ganglion cells is estimated at about 260,000. Using standard assumptions the maximum spatial resolution of the spotted hyena is calculated to be about 8.4 cycles/degree, a value similar to estimates obtained for other terrestrial carnivores. Copyright © 2003 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2003

10. The role of tangential dispersion in retinal mosaic formation

Author

Reese, Benjamin E. and Galli-Resta, Lucia

Subjects

*DEVELOPMENTAL neurobiology, *RETINA

Abstract

Individual types of retinal nerve cell are spaced across the retina in an orderly manner, ensuring a uniform sampling of the visual field. This regularity in cellular spacing has been commonly attributed to fate determination mechanisms operating around the time of cell birth, an hypothesis presuming that the position of a nerve cell is fixed within the plane of the retina from the time of its determination. At odds with this view, recent results from X-inactivation mosaic mice indicate that certain classes of retinal nerve cell, those known to form orderly mosaics in the adult retina, disperse tangentially during development. Furthermore, studies defining the spatial characteristics of developing and mature retinal mosaics suggest that cell–cell interactions around the time of morphological differentiation lead to mutual repulsion. Modelling studies in turn show that nothing more than a simple minimal spacing rule between neighboring cells of the same type is sufficient for the creation of the global patterning observed in biological retinal mosaics. For some cell types, the size of this “exclusion zone” surrounding individual cells is shown to be an intrinsic characteristic of each cell type, invariant across the retina, and accounting for the variation in mosaic regularity across changes in cell density. These results show how short-distance movements driven by intercellular interactions at the local level may mediate the emergence of the global patterning characteristic of retinal mosaics during development. [Copyright &y& Elsevier]

Published

2002

11. The Pathophysiology of Acetylcholinesterase Inhibiting Pesticides.

Author

Lessenger, James E. and Reese, Benjamin E.

Subjects

*CHOLINESTERASE-inhibiting insecticides, *PARASYMPATHOMIMETIC agents, *PESTICIDE toxicology

Abstract

The acute effects of anti-cholinesterase pesticides upon humans have long been appreciated, but their pathophysiological basis has been frequently misunderstood. This article reviews the physiology of cholinergic transmission as it relates to pesticide poisoning. It further considers the use of cholinesterase testing for monitoring exposure and defining safe exposure limits. The substantial variation in cholinesterase activity levels across the population is stressed, limiting the use of activity testing in post-exposure diagnosis. Routine monitoring among those potentially exposed to pesticides on a regular basis (e.g., pesticideapplicators, mixer-loaders and flagmen) may reveal decreased activity levels below a threshold. Recent evidence showing chronic long-term effects following low-level exposure is reviewed. [ABSTRACT FROM AUTHOR]

Published

2000

12. From random to regular: Variation in the patterning of retinal mosaics*.

Author

Keeley, Patrick W., Eglen, Stephen J., and Reese, Benjamin E.

Abstract

The various types of retinal neurons are each positioned at their respective depths within the retina where they are believed to be assembled as orderly mosaics, in which like‐type neurons minimize proximity to one another. Two common statistical analyses for assessing the spatial properties of retinal mosaics include the nearest neighbor analysis, from which an index of their "regularity" is commonly calculated, and the density recovery profile derived from autocorrelation analysis, revealing the presence of an exclusion zone indicative of anti‐clustering. While each of the spatial statistics derived from these analyses, the regularity index and the effective radius, can be useful in characterizing such properties of orderly retinal mosaics, they are rarely sufficient for conveying the natural variation in the self‐spacing behavior of different types of retinal neurons and the extent to which that behavior generates uniform intercellular spacing across the mosaic. We consider the strengths and limitations of these and other spatial statistical analyses for assessing the patterning in retinal mosaics, highlighting a number of misconceptions and their frequent misuse. Rather than being diagnostic criteria for determining simply whether a population is "regular," they should be treated as descriptive statistics that convey variation in the factors that influence neuronal positioning. We subsequently apply multiple spatial statistics to the analysis of eight different mosaics in the mouse retina, demonstrating conspicuous variability in the degree of patterning present, from essentially random to notably regular. This variability in patterning has both a developmental as well as a functional significance, reflecting the rules governing the positioning of different types of neurons as the architecture of the retina is assembled, and the distinct mechanisms by which they regulate dendritic growth to generate their characteristic coverage and connectivity. [ABSTRACT FROM AUTHOR]

Published

2020

13. Nfia Is Critical for AII Amacrine Cell Production: Selective Bipolar Cell Dependencies and Diminished ERG.

Author

Keeley, Patrick W., Trod, Stephanie, Gamboa, Bruno N., Coffey, Pete J., and Reese, Benjamin E.

Subjects

*BIPOLAR cells, *PROGENITOR cells, *TRANSCRIPTION factors, *RETINA

Abstract

The nuclear factor one (NFI) transcription factor genes Nfia, Nfib, and Nfix are all enriched in late-stage retinal progenitor cells, and their loss has been shown to retain these progenitors at the expense of later-generated retinal cell types. Whether they play any role in the specification of those later-generated fates is unknown, but the expression of one of these, Nfia, in a specific amacrine cell type may intimate such a role. Here, Nfia conditional knockout (Nfia-CKO) mice (both sexes) were assessed, finding a massive and largely selective absence of AII amacrine cells. There was, however, a partial reduction in type 2 cone bipolar cells (CBCs), being richly interconnected to AII cells. Counts of dying cells showed a significant increase in Nfia-CKO retinas at postnatal day (P)7, after AII cell numbers were already reduced but in advance of the loss of type 2 CBCs detected by P10. Those results suggest a role for Nfia in the specification of the AII amacrine cell fate and a dependency of the type 2 CBCs on them. Delaying the conditional loss of Nfia to the first postnatal week did not alter AII cell number nor differentiation, further suggesting that its role in AII cells is solely associated with their production. The physiological consequences of their loss were assessed using the ERG, finding the oscillatory potentials to be profoundly diminished. A slight reduction in the b-wave was also detected, attributed to an altered distribution of the terminals of rod bipolar cells, implicating a role of the AII amacrine cells in constraining their stratification. [ABSTRACT FROM AUTHOR]

Published

2023

14. Bistratified starburst amacrine cells in Sox2 conditional knockout mouse retina display ON and OFF responses.

Author

Stincic, Todd L., Keeley, Patrick W., Reese, Benjamin E., and Taylor, W. Rowland

Subjects

*ANIMAL models in research, *NEURAL circuitry, *DENDRITIC cells, *ELECTROPHYSIOLOGY, *NEURAL transmission

Abstract

Cell-intrinsic factors, in conjunction with environmental signals, guide migration, differentiation, and connectivity during early development of neuronal circuits. Within the retina, inhibitory starburst amacrine cells (SBACs) comprise ON types with somas in the ganglion cell layer (GCL) and dendrites stratifying narrowly in the inner half of the inner plexiform layer (IPL) and OFF types with somas in the inner nuclear layer (INL) and dendrites stratifying narrowly in the outer half of the IPL. The transcription factor Sox2 is crucial to this subtype specification. Without Sox2, many ON-type SBACs destined for the GCL settle in the INL while many that reach the GCL develop bistratified dendritic arbors. This study asked whether ON-type SBACs in Sox2-conditional knockout retinas exhibit selective connectivity only with ON-type bipolar cells or their bistratified morphology allows them to connect to both ON and OFF bipolar cells. Physiological data demonstrate that these cells receive ON and OFF excitatory inputs, indicating that the ectopically stratified dendrites make functional synapses with bipolar cells. The excitatory inputs were smaller and more transient in Sox2-conditional knockout compared with wild type; however, inhibitory inputs appeared largely unchanged. Thus dendritic stratification, rather than cellular identification, may be the major factor that determines ON vs. OFF connectivity. NEW & NOTEWORTHY Conditional knockout of the transcription factor Sox2 during early embryogenesis converts a monostratifying starburst amacrine cell into a bistratifying starburst cell. Here we show that these bistratifying starburst amacrine cells form functional synaptic connections with both ON and OFF bipolar cells. This suggests that normal ON vs. OFF starburst connectivity may not require distinct molecular specification. Proximity alone may be sufficient to allow formation of functional synapses. [ABSTRACT FROM AUTHOR]

Published

2018

15. Retinal horizontal cells: challenging paradigms of neural development and cancer biology.

Author

Poché, Ross A. and Reese, Benjamin E.

Subjects

*DEVELOPMENTAL biology, *INTERNEURONS, *NEURONS, *CYTOLOGY, *BIOPHYSICS

Abstract

A group of retinal interneurons known as horizontal cells has recently been shown to exhibit a variety of unique biological properties, as compared with other nerve cells, that challenge many long-standing assumptions in the fields of neural development and cancer biology. These features include their unusual migratory behavior, their unique morphological plasticity, and their propensity to divide at a relatively late stage during development. Here, we review these novel features, discuss their relevance for other cell types, outline open questions in our understanding of horizontal cell development and consider their implications. [ABSTRACT FROM AUTHOR]

Published

2009

16. Neurog2 regulates Isl1 to modulate horizontal cell number.

Author

Keeley, Patrick W., Patel, Pooja S., Ryu, Matthew S., and Reese, Benjamin E.

Subjects

*LOCUS (Genetics), *CHROMOSOMES, *KNOCKOUT mice, *TRANSCRIPTION factors

Abstract

The population sizes of different retinal cell types vary between different strains of mice, and that variation can be mapped to genomic loci in order to identify its polygenic origin. In some cases, controlling genes act independently, whereas in other instances, they exhibit epistasis. Here, we identify an epistatic interaction revealed through the mapping of quantitative trait loci from a panel of recombinant inbred strains of mice. The population of retinal horizontal cells exhibits a twofold variation in number, mapping to quantitative trait loci on chromosomes 3 and 13, where these loci are shown to interact epistatically. We identify a prospective genetic interaction underlying this, mediated by the bHLH transcription factor Neurog2, at the chromosome 3 locus, functioning to repress the LIM homeodomain transcription factor Isl1, at the chromosome 13 locus. Using single and double conditional knockout mice, we confirm the countervailing actions of each gene, and validate in vitro a crucial role for two single nucleotide polymorphisms in the 5'UTR of Isl1, one of which yields a novel E-box, mediating the repressive action of Neurog2. [ABSTRACT FROM AUTHOR]

Published

2023

17. Astrocyte structural reactivity and plasticity in models of retinal detachment.

Author

Luna, Gabriel, Keeley, Patrick W., Reese, Benjamin E., Linberg, Kenneth A., Lewis, Geoffrey P., and Fisher, Steven K.

Subjects

*ASTROCYTES, *NEUROPLASTICITY, *RETINAL detachment, *NEURODEGENERATION, *NEUROGLIA

Abstract

Although retinal neurodegenerative conditions such as age-related macular degeneration, glaucoma, diabetic retinopathy, retinitis pigmentosa, and retinal detachment have different etiologies and pathological characteristics, they also have many responses in common at the cellular level, including neural and glial remodeling. Structural changes in Müller cells, the large radial glia of the retina in retinal disease and injury have been well described, that of the retinal astrocytes remains less so. Using modern imaging technology to describe the structural remodeling of retinal astrocytes after retinal detachment is the focus of this paper. We present both a review of critical literature as well as novel work focusing on the responses of astrocytes following rhegmatogenous and serous retinal detachment. The mouse presents a convenient model system in which to study astrocyte reactivity since the Mϋller cell response is muted in comparison to other species thereby allowing better visualization of the astrocytes. We also show data from rat, cat, squirrel, and human retina demonstrating similarities and differences across species. Our data from immunolabeling and dye-filling experiments demonstrate previously undescribed morphological characteristics of normal astrocytes and changes induced by detachment. Astrocytes not only upregulate GFAP, but structurally remodel, becoming increasingly irregular in appearance, and often penetrating deep into neural retina. Understanding these responses, their consequences, and what drives them may prove to be an important component in improving visual outcome in a variety of therapeutic situations. Our data further supports the concept that astrocytes are important players in the retina's overall response to injury and disease. [ABSTRACT FROM AUTHOR]

Published

2016

18. Quantifying Drug-Induced Nanomechanics and Mechanical Effects to Single Cardiomyocytes for Optimal Drug Administration To Minimize Cardiotoxicity.

Author

Tao Yue, Ki Ho Park, Reese, Benjamin E., Hua Zhu, Seth Lyon, Jianjie Ma, Mohler, Peter J., and Mingjun Zhang

Subjects

*CARDIOTOXICITY, *NANOMECHANICS, *MECHANICS (Physics), *HEART cells, *DRUG administration

Abstract

Contrary to the well-studied dynamics and mechanics at organ and tissue levels, there is still a lack of good understanding for single cell dynamics and mechanics. Single cell dynamics and mechanics may act as an interface to provide unique information reflecting activities at the organ and tissue levels. This research was aimed at quantifying doxorubicin- and dexrazoxane-induced nanomechanics and mechanical effects to single cardiomyocytes, to reveal the therapeutic effectiveness of drugs at the single cell level and to optimize drug administration for reducing cardiotoxicity. This work employed a nanoinstrumentation platform, including a digital holographic microscope combined with an atomic force microscope, which can characterize cell stiffness and beating dynamics in response to drug exposures in real time and obtain time-dose-dependent effects of cardiotoxicity and protection. Through this research, an acute increase and a delayed decrease of surface beating force induced by doxorubicin was characterized. Dexrazoxane treated cells maintained better beating force and mechanical functions than cells without any treatment, which demonstrated cardioprotective effects of dexrazoxane. In addition, combined drug effects were quantitatively evaluated following various drug administration protocols. Preadministration of dexrazoxane was demonstrated to have protective effects against doxorubicin, which could lead to better strategies for cardiotoxicity prevention and anticancer drug administration. This study concluded that quantification of nanomechanics and mechanical effects at the single cell level could offer unique insights of molecular mechanisms involved in cellular activities influencing organ and tissue level responses to drug exposure, providing a new opportunity for the development of effective and time-dose-dependent strategies of drug administration. [ABSTRACT FROM AUTHOR]

Published

2016

19. Quantifying Drug-Induced Nanomechanics and Mechanical Effects to Single Cardiomyocytes for Optimal Drug Administration To Minimize Cardiotoxicity.

Author

Tao Yue, Park, Ki Ho, Reese, Benjamin E., Hua Zhu, Lyon, Seth, Jianjie Ma, Mohler, Peter J., and Mingjun Zhang

Subjects

*NANOMECHANICS, *HEART cells, *BIOMECHANICS, *DRUG administration, *CARDIOTOXICITY, *TISSUE engineering

Abstract

Contrary to the well-studied dynamics and mechanics at organ and tissue levels, there is still a lack of good understanding for single cell dynamics and mechanics. Single cell dynamics and mechanics may act as an interface to provide unique information reflecting activities at the organ and tissue levels. This research was aimed at quantifying doxorubicin- and dexrazoxane-induced nanomechanics and mechanical effects to single cardiomyocytes, to reveal the therapeutic effectiveness of drugs at the single cell level and to optimize drug administration for reducing cardiotoxicity. This work employed a nanoinstrumentation platform, including a digital holographic microscope combined with an atomic force microscope, which can characterize cell stiffness and beating dynamics in response to drug exposures in real time and obtain time-dose-dependent effects of cardiotoxicity and protection. Through this research, an acute increase and a delayed decrease of surface beating force induced by doxorubicin was characterized. Dexrazoxane treated cells maintained better beating force and mechanical functions than cells without any treatment, which demonstrated cardioprotective effects of dexrazoxane. In addition, combined drug effects were quantitatively evaluated following various drug administration protocols. Preadministration of dexrazoxane was demonstrated to have protective effects against doxorubicin, which could lead to better strategies for cardiotoxicity prevention and anticancer drug administration. This study concluded that quantification of nanomechanics and mechanical effects at the single cell level could offer unique insights of molecular mechanisms involved in cellular activities influencing organ and tissue level responses to drug exposure, providing a new opportunity for the development of effective and time-dose-dependent strategies of drug administration. [ABSTRACT FROM AUTHOR]

Published

2015

20. Alternative splicing of the LIM-homeodomain transcription factor Isl1 in the mouse retina.

Author

Whitney, Irene E., Kautzman, Amanda G., and Reese, Benjamin E.

Subjects

*HOMEOBOX proteins, *TRANSCRIPTION factors, *RETINAL diseases, *LABORATORY mice, *CENTRAL nervous system diseases, *CELL differentiation

Abstract

Islet-1 (Isl1) is a LIM-homeodomain (LIM-HD) transcription factor that functions in a combinatorial manner with other LIM-HD proteins to direct the differentiation of distinct cell types within the central nervous system and many other tissues. A study of pancreatic cell lines showed that Isl1 is alternatively spliced generating a second isoform, Isl1β, which is missing 23 amino acids within the C-terminal region. This study examines the expression of the canonical and alternative Isl1 transcripts across other tissues, in particular, within the retina, where Isl1 is required for the differentiation of multiple neuronal cell types. The alternative splicing of Isl1 is shown to occur in multiple tissues, but the relative abundance of Isl1 α and Isl1 β expression varies greatly across them. In most tissues, Isl1 α is the more abundant transcript, but in others the transcripts are expressed equally, or the alternative splice variant is dominant. Within the retina, differential expression of the two Isl1 transcripts increases as a function of development, with dynamic changes in expression peaking at E16.5 and again at P10. At the cellular level, individual retinal ganglion cells vary in their expression, with a subset of small-to-medium sized cells expressing only the alternative isoform. The functional significance of the difference in protein sequence between the two Isl1 isoforms was also assessed using a luciferase assay, demonstrating that the alternative isoform forms a less effective transcriptional complex for activating gene expression. These results demonstrate the differential presence of the canonical and alternative isoforms of Isl1 amongst retinal ganglion cell classes. As Isl1 participates in the differentiation of multiple cell types within the CNS, the present results support a role for alternative splicing in the establishment of cellular diversity in the developing nervous system. [ABSTRACT FROM AUTHOR]

Published

2015

21. Experimental Studies and Dynamics Modeling Analysis of the Swimming and Diving of Whirligig Beetles (Coleoptera: Gyrinidae).

Author

Zhonghua Xu, Lenaghan, Scott C., Reese, Benjamin E., Xinghua Jia, and Mingjun Zhang

Subjects

*GYRINIDAE, *SURFACE tension, *DYNAMIC models, *FORCE & energy, *ANGULAR velocity, *COMPUTATIONAL biology

Abstract

Whirligig beetles (Coleoptera, Gyrinidae) can fly through the air, swiftly swim on the surface of water, and quickly dive across the air-water interface. The propulsive efficiency of the species is believed to be one of the highest measured for a thrust generating apparatus within the animal kingdom. The goals of this research were to understand the distinctive biological mechanisms that allow the beetles to swim and dive, while searching for potential bio-inspired robotics applications. Through static and dynamic measurements obtained using a combination of microscopy and high-speed imaging, parameters associated with the morphology and beating kinematics of the whirligig beetle's legs in swimming and diving were obtained. Using data obtained from these experiments, dynamics models of both swimming and diving were developed. Through analysis of simulations conducted using these models it was possible to determine several key principles associated with the swimming and diving processes. First, we determined that curved swimming trajectories were more energy efficient than linear trajectories, which explains why they are more often observed in nature. Second, we concluded that the hind legs were able to propel the beetle farther than the middle legs, and also that the hind legs were able to generate a larger angular velocity than the middle legs. However, analysis of circular swimming trajectories showed that the middle legs were important in maintaining stable trajectories, and thus were necessary for steering. Finally, we discovered that in order for the beetle to transition from swimming to diving, the legs must change the plane in which they beat, which provides the force required to alter the tilt angle of the body necessary to break the surface tension of water. We have further examined how the principles learned from this study may be applied to the design of bio-inspired swimming/diving robots. [ABSTRACT FROM AUTHOR]

Published

2012

22. Interrelationships between Cellular Density, Mosaic Patterning, and Dendritic Coverage of VGluT3 Amacrine Cells.

Author

Keeley, Patrick W., Lebo, Mikayla C., Vieler, Jordan D., Kim, Jason J., St. John, Ace J., and Reese, Benjamin E.

Subjects

*GLUTAMATE transporters, *MOSAICISM, *DISTRIBUTION (Probability theory), *CELL death, *BIPOLAR cells

Abstract

Amacrine cells of the retina are conspicuously variable in their morphologies, their population demographics, and their ensuing functions. Vesicular glutamate transporter 3 (VGluT3) amacrine cells are a recently characterized type of amacrine cell exhibiting local dendritic autonomy. The present analysis has examined three features of this VGluT3 population, including their density, local distribution, and dendritic spread, to discern the extent to which these are interrelated, using male and female mice. We first demonstrate that Bax-mediated cell death transforms the mosaic of VGluT3 cells from a random distribution into a regular mosaic. We subsequently examine the relationship between cell density and mosaic regularity across recombinant inbred strains of mice, finding that, although both traits vary across the strains, they exhibit minimal covariation. Other genetic determinants must therefore contribute independently to final cell number and to mosaic order. Using a conditional KO approach, we further demonstrate that Bax acts via the bipolar cell population, rather than cell-intrinsically, to control VGluT3 cell number. Finally, we consider the relationship between the dendritic arbors of single VGluT3 cells and the distribution of their homotypic neighbors. Dendritic field area was found to be independent of Voronoi domain area, while dendritic coverage of single cells was not conserved, simply increasing with the size of the dendritic field. Bax-KO retinas exhibited a threefold increase in dendritic coverage. Each cell, however, contributed less dendrites at each depth within the plexus, intermingling their processes with those of neighboring cells to approximate a constant volumetric density, yielding a uniformity in process coverage across the population. [ABSTRACT FROM AUTHOR]

Published

2021

23. Straying from the flatfish retinal plan: Cone photoreceptor patterning in the common sole (Solea solea) and the Senegalese sole (Solea senegalensis).

Author

Frau, Sara, Novales Flamarique, Iñigo, Keeley, Patrick W., Reese, Benjamin E., and Muñoz‐Cueto, José A.

Abstract

The retinas of nonmammalian vertebrates have cone photoreceptor mosaics that are often organized as highly patterned lattice‐like distributions. In fishes, the two main lattice‐like patterns are composed of double cones and single cones that are either assembled as interdigitized squares or as alternating rows. The functional significance of such orderly patterning is unknown. Here, the cone mosaics in two species of Soleidae flatfishes, the common sole and the Senegalese sole, were characterized and compared to those from other fishes to explore variability in cone patterning and how it may relate to visual function. The cone mosaics of the common sole and the Senegalese sole consisted of single, double, and triple cones in formations that differed from the traditional square mosaic pattern reported for other flatfishes in that no evidence of higher order periodicity was present. Furthermore, mean regularity indices for single and double cones were conspicuously lower than those of other fishes with "typical" square and row mosaics, but comparable to those of goldfish, a species with lattice‐like periodicity in its cone mosaic. Opsin transcripts detected by quantitative polymerase chain reaction (sws1, sws2, rh2.3, rh2.4, lws, and rh1) were uniformly expressed across the retina of the common sole but, in the Senegalese sole, sws2, rh2.4, and rh1 were more prevalent in the dorsal retina. Microspectrophotometry revealed five visual pigments in the retina of the common sole [S(472), M(523), M(536), L(559), and rod(511)] corresponding to the repertoire of transcripts quantified except for sws1. Overall, these results indicate a loss of cone mosaic patterning in species that are primarily nocturnal or dwell in low light environments as is the case for the common sole and the Senegalese sole. The corollary is that lattice‐like patterning of the cone mosaic may improve visual acuity. Ecological and physiological correlates derived from observations across multiple fish taxa that live in low light environments and do not possess lattice‐like cone mosaics are congruent with this claim. [ABSTRACT FROM AUTHOR]

Published

2020

24. Large-scale death of retinal astrocytes during normal development is non-apoptotic and implemented by microglia.

Author

Puñal, Vanessa M., Paisley, Caitlin E., Brecha, Federica S., Lee, Monica A., Perelli, Robin M., Wang, Jingjing, O'Koren, Emily G., Ackley, Caroline R., Saban, Daniel R., Reese, Benjamin E., and Kay, Jeremy N.

Subjects

*ASTROCYTES, *CELL death, *CELL populations, *MICROGLIA, *NERVOUS system, *NEURONS

Abstract

Naturally occurring cell death is a fundamental developmental mechanism for regulating cell numbers and sculpting developing organs. This is particularly true in the nervous system, where large numbers of neurons and oligodendrocytes are eliminated via apoptosis during normal development. Given the profound impact of death upon these two major cell populations, it is surprising that developmental death of another major cell type—the astrocyte—has rarely been studied. It is presently unclear whether astrocytes are subject to significant developmental death, and if so, how it occurs. Here, we address these questions using mouse retinal astrocytes as our model system. We show that the total number of retinal astrocytes declines by over 3-fold during a death period spanning postnatal days 5–14. Surprisingly, these astrocytes do not die by apoptosis, the canonical mechanism underlying the vast majority of developmental cell death. Instead, we find that microglia engulf astrocytes during the death period to promote their developmental removal. Genetic ablation of microglia inhibits astrocyte death, leading to a larger astrocyte population size at the end of the death period. However, astrocyte death is not completely blocked in the absence of microglia, apparently due to the ability of astrocytes to engulf each other. Nevertheless, mice lacking microglia showed significant anatomical changes to the retinal astrocyte network, with functional consequences for the astrocyte-associated vasculature leading to retinal hemorrhage. These results establish a novel modality for naturally occurring cell death and demonstrate its importance for the formation and integrity of the retinal gliovascular network. A study of the neonatal mouse retina shows that developmental cell death of retinal astrocytes does not occur by apoptosis but is instead mediated by microglia, which kill and engulf astrocytes to effect their developmental removal. [ABSTRACT FROM AUTHOR]

Published

2019

25. Dopaminergic amacrine cell number, plexus density, and dopamine content in the mouse retina: Strain differences and effects of Bax gene disruption.

Author

Sankaran, Mathangi, Keeley, Patrick W., He, Li, Iuvone, P. Michael, and Reese, Benjamin E.

Subjects

*DOPAMINERGIC neurons, *DENDRITIC cells, *APOPTOTIC bodies, *RETINA analysis, *HIGH performance liquid chromatography

Abstract

Abstract Many types of retinal neuron modulate the distribution of their processes to ensure a uniform coverage of the retinal surface. Dendritic field area, for instance, is inversely related to the variation in cellular density for many cell types, observed either across retinal eccentricity or between different strains of mice that differ in cell number. Dopaminergic amacrine (DA) cells, by contrast, have dendritic arbors that bear no spatial relationship to the presence of their immediate homotypic neighbors, yet it remains to be determined whether their coverage upon the retina, as a population, is conserved across variation in their total number. The present study assessed the overall density of the dopaminergic plexus in the inner plexiform layer in the presence of large variation in the total number of DA cells, as well as their retinal dopamine content, to determine whether either of these features is conserved. We first compared these traits between two strains of mice (C57BL/6J and A/J) that exhibit a two-fold difference in DA cell number. We subsequently examined these same traits in littermate mice for which the pro-apoptotic Bax gene was either intact or knocked out, yielding a five-fold difference in DA cell number. In both comparisons, we found greater plexus density and DA content in the strain or condition with the greater number of DA cells. The population of DA cells, therefore, does not appear to self-regulate its process coverage to achieve a constant density as the DA mosaic is established during development, nor its functional dopamine content in maturity. Highlights • DA amacrine cell number varies considerably between different strains of mice. • The density of DA processes is significantly greater in retinas with more DA cells. • DA content is also significantly greater in retinas with more DA cells. • Neither DA process outgrowth nor DA content is regulated at the population level. [ABSTRACT FROM AUTHOR]

Published

2018

26. Dendritic stratification differs among retinal OFF bipolar cell types in the absence of rod photoreceptors.

Author

Puller, Christian, Arbogast, Patrick, Keeley, Patrick W., Reese, Benjamin E., and Haverkamp, Silke

Subjects

*DENDRITIC cells, *PHOTORECEPTORS, *SYNAPSES, *BIPOLAR cells, *GLUTAMATE receptors, *ELECTRON microscopy

Abstract

Retinal OFF bipolar cells show distinct connectivity patterns with photoreceptors in the wild-type mouse retina. Some types are cone-specific while others penetrate further through the outer plexiform layer (OPL) to contact rods in addition to cones. To explore dendritic stratification of OFF bipolar cells in the absence of rods, we made use of the ‘cone-full’ Nrl-/- mouse retina in which all photoreceptor precursor cells commit to a cone fate including those which would have become rods in wild-type retinas. The dendritic distribution of OFF bipolar cell types was investigated by confocal and electron microscopic imaging of immunolabeled tissue sections. The cells’ dendrites formed basal contacts with cone terminals and expressed the corresponding glutamate receptor subunits at those sites, indicating putative synapses. All of the four analyzed cell populations showed distinctive patterns of vertical dendritic invasion through the OPL. This disparate behavior of dendritic extension in an environment containing only cone terminals demonstrates type-dependent specificity for dendritic outgrowth in OFF bipolar cells: rod terminals are not required for inducing dendritic extension into distal areas of the OPL. [ABSTRACT FROM AUTHOR]

Published

2017

27. X-ray detectors at the Linac Coherent Light Source.

Author

Blaj, Gabriel, Caragiulo, Pietro, Carini, Gabriella, Carron, Sebastian, Dragone, Angelo, Freytag, Dietrich, Haller, Gunther, Hart, Philip, Hasi, Jasmine, Herbst, Ryan, Herrmann, Sven, Kenney, Chris, Markovic, Bojan, Nishimura, Kurtis, Osier, Shawn, Pines, Jack, Reese, Benjamin, Segal, Julie, Tomada, Astrid, and Weaver, Matt

Subjects

*FREE electron lasers, *LIGHT sources, *X-ray spectroscopy, *OPTICAL coherent transients, *COHERENT scattering

Abstract

Free-electron lasers (FELs) present new challenges for camera development compared with conventional light sources. At SLAC a variety of technologies are being used to match the demands of the Linac Coherent Light Source (LCLS) and to support a wide range of scientific applications. In this paper an overview of X-ray detector design requirements at FELs is presented and the various cameras in use at SLAC are described for the benefit of users planning experiments or analysts looking at data. Features and operation of the CSPAD camera, which is currently deployed at LCLS, are discussed, and the ePix family, a new generation of cameras under development at SLAC, is introduced. [ABSTRACT FROM AUTHOR]

Published

2015

28. Programmed cell death of retinal cone bipolar cells is independent of afferent or target control.

Author

Keeley, Patrick W., Madsen, Nils R., St. John, Ace J., and Reese, Benjamin E.

Subjects

*APOPTOSIS, *RETINAL cone photoreceptor cells, *BIPOLAR cells, *AFFERENT pathways, *HISTOGENESIS, *NERVOUS system, *RETINAL ganglion cells

Abstract

Programmed cell death contributes to the histogenesis of the nervous system, and is believed to be modulated through the sustaining effects of afferents and targets during the period of synaptogenesis. Cone bipolar cells undergo programmed cell death during development, and we confirm that the numbers of three different types are increased when the pro-apoptotic Bax gene is knocked out. When their cone afferents are selectively eliminated, or when the population of retinal ganglion cells is increased, however, cone bipolar cell number remains unchanged. Programmed cell death of the cone bipolar cell populations, therefore, may be modulated cell-intrinsically rather than via interactions with these synaptic partners. [ABSTRACT FROM AUTHOR]

Published

2014

29. Sox2 Regulates Cholinergic Amacrine Cell Positioning and Dendritic Stratification in the Retina.

Author

Whitney, Irene E., Keeley, Patrick W., John, Ace J. St., Kautzman, Amanda G., Kay, Jeremy N., and Reese, Benjamin E.

Subjects

*CHOLINERGIC receptors, *RETINAL ganglion cells, *NEURONS, *LABORATORY mice, *LOCUS (Genetics)

Abstract

The retina contains two populations of cholinergic amacrine cells, one positioned in the ganglion cell layer (GCL) and the other in the inner nuclear layer (INL), that together comprise ~1/2 of apercent of all retinal neurons. The present study examined the genetic control of cholinergic amacrine cell number and distribution between these two layers. The total number of cholinergic amacrine cells was quantified in the C57BL/6J and A/J inbred mouse strains, and in 25 recombinant inbred strains derived from them, and variations in their number and ratio (GCL/INL) across these strains were mapped to genomic loci. The total cholinergic amacrine cell number was found to vary across the strains, from 27,000 to 40,000 cells, despite little variation within individual strains. The number of cells was always lower within the GCL relative to the INL, and the sizes of the two populations were strongly correlated, yet there was variation in their ratio between the strains. Approximately 1/3 of that variation in cell ratio was mapped to a locus on chromosome 3, where Sex determining region Y box 2 (Sox2) was identified as a candidate gene due to the presence of a 6-nucleotide insertion in the protein-coding sequence in C57BL/6J and because of robust and selective expression in cholinergic amacrine cells. Conditionally deleting Sox2 from the population of nascent cholinergic amacrine cells perturbed the normal ratio of cells situated in the GCL versus the INL and induced a bistratifying morphology, with dendrites distributed to both ON and OFF strata within the inner plexiform layer. [ABSTRACT FROM AUTHOR]

Published

2014

30. Independent Genomic Control of Neuronal Number across Retinal Cell Types.

Author

Keeley, Patrick W., Whitney, Irene E., Madsen, Nils R., St. John, Ace J., Borhanian, Sarra, Leong, Stephanie A., Williams, Robert W., and Reese, Benjamin E.

Subjects

*NEURONS, *POPULATION biology, *GENETIC regulation, *GENOMICS, *DEVELOPMENTAL biology, *LABORATORY mice

Abstract

The sizes of different neuronal populations within the CNS are precisely controlled, but whether neuronal number is coordinated between cell types is unknown. We examined the covariance structure of 12 different retinal cell types across 30 genetically distinct lines of mice, finding minimal covariation when comparing synaptically connected or developmentally related cell types. Variation mapped to one or more genomic loci for each cell type, but rarely were these shared, indicating minimal genetic coregulation of final number. Multiple genes, therefore, participate in the specification of the size of every population of retinal neuron, yet genetic variants work largely independent of one another during development to modulate those numbers, yielding substantial variability in the convergence ratios between pre- and postsynaptic populations. Density-dependent cellular interactions in the outer plexiform layer overcome this variability to ensure the formation of neuronal circuits that maintain constant retinal coverage and complete afferent sampling. [ABSTRACT FROM AUTHOR]

Published

2014

31. Pituitary tumor-transforming gene 1 regulates the patterning of retinal mosaics.

Author

Keeley, Patrick W., Cuiqi Zhou, Lu Lu, Williams, Robert W., Melmed, Shlomo, and Reese, Benjamin E.

Subjects

*PITUITARY tumors, *GENETIC regulation, *MOSAICISM, *INTERNEURONS, *NUCLEOTIDES, *LOCUS (Genetics)

Abstract

Neurons are commonly organized as regular arrays within a structure, and their patterning is achieved by minimizing the proximity between like-type cells, but molecular mechanisms regulating this process have, until recently, been unexplored. We performed a forward genetic screen using recombinant inbred (RI) strains derived from two parental A/J and C57BL/6J mouse strains to identify genomic loci controlling spacing of cholinergic amacrine cells, which is a subclass of retinal interneuron. We found conspicuous variation in mosaic regularity across these strains and mapped a sizeable proportion of that variation to a locus on chromosome 11 that was subsequently validated with a chromosome substitution strain. Using a bioinformatics approach to narrow the list of potential candidate genes, we identified pituitary tumor-transforming gene 1 (Pttg1) as the most promising. Expression of Pttg1 was significantly different between the two parental strains and correlated with mosaic regularity across the RI strains. We identified a seven-nucleotide deletion in the Pttg1 promoter in the C57BL/6J mouse strain and confirmed a direct role for this motif in modulating Pttg1 expression. Analysis of Pttg1 KO mice revealed a reduction in the mosaic regularity of cholinergic amacrine cells, as well as horizontal cells, but not in two other retinal cell types. Together, these results implicate Pttg1 in the regulation of homotypic spacing between specific types of retinal neurons. The genetic variant identified creates a binding motif for the transcriptional activator protein 1 complex, which may be instrumental in driving differential expression of downstream processes that participate in neuronal spacing. [ABSTRACT FROM AUTHOR]

Published

2014

32. Development and Plasticity of Outer Retinal Circuitry Following Genetic Removal of Horizontal Cells.

Author

Keeley, Patrick W., Luna, Gabriel, Fariss, Robert N., Skyles, Kimberly A., Raven, Mary A., Poché, Ross A., Swindell, Eric C., Jamrich, Milan, Oh, Edwin C., Swaroop, Anand, Fisher, Steven K., and Reese, Benjamin E.

Subjects

*RETINA physiology, *NEURAL circuitry, *NEUROPLASTICITY, *DEVELOPMENTAL neurobiology, *NEUROGENETICS, *EMBRYOLOGY

Abstract

The present study examined the consequences of eliminating horizontal cells from the outer retina during embryogenesis upon the organization and assembly of the outer plexiform layer (OPL). Retinal horizontal cells exhibit a migration defect in Lim1-conditional knock-out (Lim1-CKO) mice and become mispositioned in the inner retina before birth, redirecting their dendrites into the inner plexiform layer. The resultant (mature) OPL, developing in the absence of horizontal cells, shows a retraction of rod spherules into the outer nuclear layer and a sprouting of rod bipolar cell dendrites to reach ectopic ribbon-protein puncta. Cone pedicles and the dendrites of type 7 cone bipolar cells retain their characteristic stratification and colocalization within the collapsed OPL, although both are atrophic and the spatial distribution of the pedicles is disrupted. Developmental analysis of Lim1-CKO retina reveals that components of the rod and cone pathways initially co-assemble within their normal strata in the OPL, indicating that horizontal cells are not required for the correct targeting of photoreceptor terminals or bipolar cell dendrites. As the rod spherules begin to retract during the second postnatal week, rod bipolar cells initially show no signs of ectopic growth, sprouting only subsequently and continuing to do so well after the eighth postnatal week. These results demonstrate the critical yet distinctive roles for horizontal cells on the rod and cone pathways and highlight a unique and as-yet-unrecognized maintenance function of an inhibitory interneuron that is not required for the initial targeting and co-stratification of other components in the circuit. [ABSTRACT FROM AUTHOR]

Published

2013

33. Apoptosis Regulates ipRGC Spacing Necessary for Rods and Cones to Drive Circadian Photoentrainment

Author

Chen, Shih-Kuo, Chew, Kylie S., McNeill, David S., Keeley, Patrick W., Ecker, Jennifer L., Mao, Buqing Q., Pahlberg, Johan, Kim, Bright, Lee, Sammy C.S., Fox, Michael A., Guido, William, Wong, Kwoon Y., Sampath, Alapakkam P., Reese, Benjamin E., Kuruvilla, Rejji, and Hattar, Samer

Subjects

*APOPTOSIS, *PHOTORECEPTORS, *CIRCADIAN rhythms, *RETINAL ganglion cells, *BAX protein, *MELANOPSIN, *SYNAPSES

Abstract

Summary: The retina consists of ordered arrays of individual types of neurons for processing vision. Here, we show that such order is necessary for intrinsically photosensitive retinal ganglion cells (ipRGCs) to function as irradiance detectors. We found that during development, ipRGCs undergo proximity-dependent Bax-mediated apoptosis. Bax mutant mice exhibit disrupted ipRGC spacing and dendritic stratification with an increase in abnormally localized synapses. ipRGCs are the sole conduit for light input to circadian photoentrainment, and either their melanopsin-based photosensitivity or ability to relay rod/cone input is sufficient for circadian photoentrainment. Remarkably, the disrupted ipRGC spacing does not affect melanopsin-based circadian photoentrainment but severely impairs rod/cone-driven photoentrainment. We demonstrate reduced rod/cone-driven cFos activation and electrophysiological responses in ipRGCs, suggesting that impaired synaptic input to ipRGCs underlies the photoentrainment deficits. Thus, for irradiance detection, developmental apoptosis is necessary for the spacing and connectivity of ipRGCs that underlie their functioning within a neural network. [ABSTRACT FROM AUTHOR]

Published

2013

34. Neuronal clustering and fasciculation phenotype in Dscam- and Bax-deficient mouse retinas.

Author

Keeley, Patrick W., Sliff, Buranee J., Lee, Sammy C.S., Fuerst, Peter G., Burgess, Robert W., Eglen, Stephen J., and Reese, Benjamin E.

Abstract

Individual types of retinal neurons are distributed to minimize proximity to neighboring cells. Many of these same cell types extend dendrites to provide coverage of the retinal surface. These two cardinal features of retinal mosaics are disrupted, for certain cell types, in mice deficient for the Down syndrome cell adhesion molecule, Dscam, exhibiting an aberrant clustering of somata and fasciculation of dendrites. The Dscam mutant mouse retina also exhibits excess numbers of these same cell types. The present study compared these two features in Dscam mutant retinas with the Bax knockout retina, in which excess numbers of two of these cell types, the melanopsin-positive retinal ganglion cells (MRGCs) and the dopaminergic amacrine cells (DACs), are also present. Whole retinas were immunolabeled for both populations, and every labeled soma was plotted. For the MRGCs, we found a gene dosage effect for Dscam, with the Dscam+/− retinas showing smaller increases in cell number, clustering, and fasciculation. Curiously, Bax−/− retinas, showing numbers of MRGCs intermediate to those found in the Dscam−/− and Dscam+/− retinas, also had clustering and fasciculation phenotypes that were intermediate to retinas with those genotypes. DACs, by comparison, showed changes in both the Dscam−/− and the Bax−/− retinas that did not correlate with their increases in DAC number. The fasciculation phenotype in the Dscam−/− retina was particularly prominent despite only modest clustering. These results demonstrate that the somal clustering and fasciculation observed in the Dscam mutant retina are not unique to Dscam deficiency and are manifested distinctively by different retinal cell types. J. Comp. Neurol. 520:1349-1364, 2012. © 2011 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

35. Cell-Type Specific Roles for PTEN in Establishing a Functional Retinal Architecture.

Author

Cantrup, Robert, Dixit, Rajiv, Palmesino, Elena, Bonfield, Stephan, Shaker, Tarek, Tachibana, Nobuhiko, Zinyk, Dawn, Dalesman, Sarah, Yamakawa, Kazuhiro, Stell, William K., Wong, Rachel O., Reese, Benjamin E., Kania, Artur, Sauvé, Yves, and Schuurmans, Carol

Subjects

*RETINA, *NEURONS, *DENDRITIC cells, *HYPERTROPHY, *VISUAL acuity, *PHOSPHATASES

Abstract

Background: The retina has a unique three-dimensional architecture, the precise organization of which allows for complete sampling of the visual field. Along the radial or apicobasal axis, retinal neurons and their dendritic and axonal arbors are segregated into layers, while perpendicular to this axis, in the tangential plane, four of the six neuronal types form patterned cellular arrays, or mosaics. Currently, the molecular cues that control retinal cell positioning are not wellunderstood, especially those that operate in the tangential plane. Here we investigated the role of the PTEN phosphatase in establishing a functional retinal architecture. Methodology/Principal Findings: In the developing retina, PTEN was localized preferentially to ganglion, amacrine and horizontal cells, whose somata are distributed in mosaic patterns in the tangential plane. Generation of a retina-specific Pten knock-out resulted in retinal ganglion, amacrine and horizontal cell hypertrophy, and expansion of the inner plexiform layer. The spacing of Pten mutant mosaic populations was also aberrant, as were the arborization and fasciculation patterns of their processes, displaying cell type-specific defects in the radial and tangential dimensions. Irregular oscillatory potentials were also observed in Pten mutant electroretinograms, indicative of asynchronous amacrine cell firing. Furthermore, while Pten mutant RGC axons targeted appropriate brain regions, optokinetic spatial acuity was reduced in Pten mutant animals. Finally, while some features of the Pten mutant retina appeared similar to those reported in Dscam-mutant mice, PTEN expression and activity were normal in the absence of Dscam. Conclusions/Significance: We conclude that Pten regulates somal positioning and neurite arborization patterns of a subset of retinal cells that form mosaics, likely functioning independently of Dscam, at least during the embryonic period. Our findings thus reveal an unexpected level of cellular specificity for the multi-purpose phosphatase, and identify Pten as an integral component of a novel cell positioning pathway in the retina. [ABSTRACT FROM AUTHOR]

Published

2012

36. Homotypic Regulation of Neuronal Morphology and Connectivity in the Mouse Retina.

Author

Lee, Sammy C. S., Cowgill, Erin J., Al-Nabulsi, Ali, Quinn, Emma J., Evans, Sylvia M., and Reese, Benjamin E.

Abstract

The establishment of neuronal circuitry during development relies upon the action of cell-intrinsic mechanisms that specify neuronal form as well as plastic processesthat requirethetransmission of neural activity between afferents andtheirtargets. Here, we examinethe role of interactions between neighboring like-type cells withinthe mouse retina upon neuronal differentiation and circuitformation. Two different genetically modified mouse models were used to modulate the density of homotypic neighbors, the Type 7 cone bipolar cells, without affectingthe density oftheir afferents,the cone photoreceptors.We demonstrate a corresponding plasticityin dendriticfield area whenthe density of Type 7 cone bipolar cells is elevated or reduced. In accord withthis variation in dendriticfield area across an invariant population of afferents, individual Type 7 cone bipolar cells are also shown to modulate the number of cone pedicles contacted without varying the number of contacts at each cone pedicle. Analysis of developing Type 7 cone bipolar cells reveals that the dendritic tiling present in maturity is achieved secondarily, after an initial stage of dendritic overlap, when the dendritic terminals are stratified at the level ofthe cone pedicles but are not localizedtothem. These results demonstrate a conspicuous developmental plasticity in neural circuit formation independent of neural activity, requiring homotypic interactions between neighboring cells that ultimately regulate connectivity within the retina. [ABSTRACT FROM AUTHOR]

Published

2011

37. Specific Interaction of Gαi3 with the Oa1 G-Protein Coupled Receptor Controls the Size and Density of Melanosomes in Retinal Pigment Epithelium.

Author

Young, Alejandra, Jiang, Meisheng, Wang, Ying, Ahmedli, Novruz B., Ramirez, John, Reese, Benjamin E., Birnbaumer, Lutz, and Farber, Debora B.

Subjects

*G protein coupled receptors, *PROTEIN-protein interactions, *PIGMENT epithelium-derived factor, *AXONS, *OPTIC chiasm, *PRECIPITIN reaction, *GENETIC mutation, *MELANOCYTES

Abstract

Background: Ocular albinism type 1, an X-linked disease characterized by the presence of enlarged melanosomes in the retinal pigment epithelium (RPE) and abnormal crossing of axons at the optic chiasm, is caused by mutations in the OA1 gene. The protein product of this gene is a G-protein-coupled receptor (GPCR) localized in RPE melanosomes. The Oa1-/- mouse model of ocular albinism reproduces the human disease. Oa1 has been shown to immunoprecipitate with the Gαi subunit of heterotrimeric G proteins from human skin melanocytes. However, the Gαi subfamily has three highly homologous members, Gαi1, Gαi2 and Gαi3 and it is possible that one or more of them partners with Oa1. We had previously shown by in-vivo studies that Gαi3-/- and Oa1-/- mice have similar RPE phenotype and decussation patterns. In this paper we analyze the specificity of the Oa1-Gαi interaction. Methodology: By using the genetic mouse models Gαi1-/-, Gαi2-/-, Gαi3-/- and the double knockout Gαi1-/-, Gαi3-/- that lack functional Gαi1, Gαi2, Gαi3, or both Gαi1 and Gαi3 proteins, respectively, we show that Gαi3 is critical for the maintenance of a normal melanosomal phenotype and that its absence is associated with changes in melanosomal size and density. GSTpull- down and immunoprecipitation assays conclusively demonstrate that Gαi3 is the only Gαi that binds to Oa1. Western blots show that Gαi3 expression is barely detectable in the Oa1-/- RPE, strongly supporting a previously unsuspected role for Gαi3 in melanosomal biogenesis. Conclusion: Our results identify the Oa1 transducer Gai3 as the first downstream component in the Oa1 signaling pathway. [ABSTRACT FROM AUTHOR]

Published

2011

38. Genetic modulation of horizontal cell number in the mouse retina.

Author

Whitney, Irene E., Raven, Mary A., Ciobanu, Daniel C., Poché, Ross A., Qian Ding, Elshatory, Yasser, Lin Gan, Williams, Robert W., and Reese, Benjamin E.

Subjects

*ANIMAL models in research, *NEURONS, *RETINA, *GENES, *NUCLEOTIDES, *GENETIC polymorphisms

Abstract

Neuronal populations display conspicuous variability in their size among individuals, but the genetic sources of this variation are largely undefined. We demonstrate a large and highly heritable variation in neuron number within the mouse retina, affecting a critical population of interneurons, the horizontal cells. Variation in the size of this population maps to the distal end of chromosome (Chr) 13, a region homologous to human Chr 5q11.1-11.2. This region contains two genes known to modulate retinal cell number. Using conditional knock-out mice, we demonstrate that one of these genes, the LIM homeodomain gene Islet-1 (Isl1), plays a role in regulating horizontal cell number. Genetic differences in Isl1 expression are high during the period of horizontal cell production, and cis-regulation of Isl1 expression within the retina is demonstrated directly. We identify a single nucleotide polymorphism in the 5′ UTR of Isl1 that creates an E-box sequence as a candidate causal variant contributing to this variation in horizontal cell number. [ABSTRACT FROM AUTHOR]

Published

2011

39. Somal positioning and dendritic growth of horizontal cells are regulated by interactions with homotypic neighbors.

Author

Poché, Ross A., Raven, Mary A., Kwan, Kin Ming, Furuta, Yasuhide, Behringer, Richard R., and Reese, Benjamin E.

Subjects

*CELLS, *GROWTH factors, *NEURONS, *NERVOUS system, *GENE targeting

Abstract

Retinal neurons extend their dendritic fields to achieve a degree of dendritic overlap with homotypic neighbors that is cell-type specific. How these neurons regulate their dendritic growth is unclear. The dendritic field of a retinal horizontal cell varies inversely with horizontal cell density across different strains of mice, suggesting that proximity to neighboring cells regulates dendritic growth. To test this directly, we have employed the Cre-loxP conditional gene targeting strategy to achieve inactivation of Lim1 function in developing horizontal cells. Through this approach, Lim1 function was prevented within a subset of horizontal cells that in turn fail to migrate to the horizontal cell layer and differentiate normally. For those remaining horizontal cells with Lim1 intact (about half of the normal population in these mice), we show that they spread themselves out tangentially and differentiate a dendritic morphology that is essentially normal but for the fact that it has nearly doubled in area. Such larger horizontal cells, sampling from an area of retina containing twice their normal afferent number, differentiate a dendritic field with nearly double the number of higher order branches and terminal clusters. These results demonstrate directly that positioning and dendritic growth are regulated by interactions with homotypic neighbors, whereas afferents instruct the differentiation of dendritic patterning. [ABSTRACT FROM AUTHOR]

Published

2008

40. Lim1 Is Essential for the Correct Laminar Positioning of Retinal Horizontal Cells.

Author

Poché, Ross A., Kin Ming Kwan, Raven, Mary A., Furuta, Yasuhide, Reese, Benjamin E., and Behringer, Richard R.

Subjects

*RETINAL ganglion cells, *RETINA, *NEURONS, *CELLS, *TRANSCRIPTION factors

Abstract

Although much is known about the transcriptional regulation that coordinates retinal cell fate determination, very little is known about the developmental processes that establish the characteristic laminar architecture of the retina, in particular, the specification of neuronal positioning. The LIM class homeodomain transcription factor Lim1 (Lhx1) is expressed in postmitotic, differentiating, and mature retinal horizontal cells. We show that conditional ablation of Lim1 results in the ectopic localization of horizontal cells to inner aspects of the inner nuclear layer, among the retinal amacrine cells. The ectopic cells maintain a molecular phenotype consistent with horizontal cell identity; however, these neurons adopt a unique morphology more reminiscent of amacrine cells, including a dendritic arbor positioned within the inner plexiform layer. All other retinal cell populations appear unaltered. Our data suggest a model whereby Lim1 lies downstream of horizontal cell fate determination factors and functions cell autonomously to instruct differentiating horizontal cells to the appropriate laminar position in the developing retina. This study is the first to describe a cell type- specific genetic program that is essential for targeting a discrete retinal neuron population to the proper lamina. [ABSTRACT FROM AUTHOR]

Published

2007

41. Afferent Control of Horizontal Cell Morphology Revealed by Genetic Respecification of Rods and Cones.

Author

Raven, Mary A., Oh, Edwin C. T., Swaroop, Anand, and Reese, Benjamin E.

Subjects

*INTERNEURONS, *RETINA, *PHOTORECEPTORS, *AXONS, *MORPHOLOGY, *TRANSGENIC mice

Abstract

The first inhibitory interneurons of the retina, the horizontal cells, stratify within the outer plexiform layer, extending dendritic terminals that connect to the pedicles of cone photoreceptors and an axon terminal system contacting the spherules of rod photoreceptors. How the horizontal cells acquire this morphology is unknown, but instructive interactions with afferents are suggested to play a role in the development of synaptic circuits. Here, we show that the morphology of the axon terminal system and the dendritic field are selectively regulated by innervation from their respective afferents: genetic respecification of all cones to become rods, in Crxp-Nrl transgenic mice, produces an atrophic dendritic field yet leaves the axon terminal system largely intact. In contrast, in the retinas of Nrl-/- mice, in which the population of rod photoreceptors is respecified to adopt a cone fate, the dendritic field is hypertrophic, whereas the axon terminal system is underdeveloped. Our studies reveal that, although cell-intrinsic mechanisms drive the formation of independent dendritic versus axonal domains, the afferents play a selectively instructive role in defining their respective morphologies. [ABSTRACT FROM AUTHOR]

Published

2007

42. Genetically engineered mice with an additional class of cone photoreceptors: Implications for the evolution of color vision.

Author

Smallwood, Philip M., Ölveczky, Bence P., Williams, Gary L., Jacobs, Gerald H., Reese, Benjamin E., Meister, Markus, and Nathans, Jeremy

Subjects

*PHOTORECEPTORS, *ANIMAL genetic engineering

Abstract

Examines a genetically engineered mice with an additional class of cone photoreceptors. Immunostaining of mouse retinae; Recording of glanglion cell action potentials; Design of the red knock-in allele.

Published

2003

43. Gap Junctions Mediate Bystander Cell Death in Developing Retina.

Author

Cusato, Karen, Bosco, Alejandra, Rozental, Renato, Guimaraes, Cinthya A., Reese, Benjamin E., Linden, Rafael, and Spray, David C.

Subjects

*GAP junctions (Cell biology), *CELL death, *RETINA cytology, *CELL junctions, *CELL communication

Abstract

Presents a study which investigated the role of gap junctions in cell death in developing retina. Review of related literature; Materials and methods used; Results and discussion.

Published

2003

44. Cell death in the inner nuclear layer of the retina is modulated by BDNF

Author

Cusato, Karen, Bosco, Alejandra, Linden, Rafael, and Reese, Benjamin E.

Subjects

*RETINA, *CELL death, *RETINAL ganglion cells

Abstract

Developing amacrine cells in the vertebrate retina undergo naturally-occurring cell death which is accentuated by the early removal of retinal ganglion cells. We show that providing BDNF or decreasing endogenous BDNF via competitive binding with soluble TrkB receptors in a whole-retina culture assay modulates the frequency of dying cells in the amacrine cell layer. Ganglion cells synthesize BDNF, and amacrine cells express TrkB receptors, suggesting a likely signaling mechanism. [Copyright &y& Elsevier]

Published

2002

45. Development of a large active area beam telescope based on the SiD microstrip sensor.

Author

Wu, Mengqing, Breidenbach, Martin, Freytag, Dietrich, Herbst, Ryan, Kraemer, Uwe, Reese, Benjamin, Roelofs, Sebastiaan, and Stanitzki, Marcel

Subjects

*SILICON detectors, *PARTICLE beams, *MAGNETS, *DETECTORS, *SUPERCONDUCTING magnets, *CHERENKOV counters, *TESTING laboratories, *TESTING equipment

Abstract

A beam telescope as one of the most important and often requested test beam equipment provides particle tracking to test beam users. At the DESY II test beam facility, a new beam telescope called Lycoris based on a microstrip sensor has been designed to address the user demands for momentum measurement in a 1 T solenoid magnet or large area tracking with limited space (3.5 cm between the potential user device and the magnet inner wall). Lycoris is designed to provide a high-precision resolution of at least ∼ 10 µm along the bending direction, and a large active area of 10 × 10 cm2 to cover at least 90% of the beam particles at energies of 1-6 GeV. The microstrip sensor was originally designed for the Silicon Detector (SiD) at the International Linear Collider (ILC), which adopted a hybrid-less design, i.e. a second metallization layer is used to route signals from strips to the bump-bonded ASIC, and from the ASIC to a wire-bond pad to the outside. This hybrid-less arrangement eliminates the need for a complex hybrid design, and its functioning is first-time tested in this project. The performance of the sensor modules was firstly tested in the lab then at the DESY II test beam facility in August/September 2018, and the results will be presented here. In addition, a summary will be given at the end with an overview of the ongoing test beam campaign of the Lycoris prototype in February 2019. [ABSTRACT FROM AUTHOR]

Published

2020

46. Neuronal clustering and fasciculation phenotype in Dscam- and Bax-deficient mouse retinas.

Author

Keeley, Patrick W., Sliff, Buranee J., Lee, Sammy C.S., Fuerst, Peter G., Burgess, Robert W., Eglen, Stephen J., and Reese, Benjamin E.

Abstract

Wild-type mouse retina immunofluorescently labeled to reveal the populations of melanopsin-positive ganglion cells (green) and dopaminergic amacrine cells (magenta). Each cell type shows abnormal clustering and fasciculation in both Dscam- and Bax- deficient mice, though the profile of these features is distinct in the two mutants. The Journal of Comparative Neurology, Volume 520, Number 7, pages 1349-1364. [ABSTRACT FROM AUTHOR]

Published

2012