Your search keyword '"Scherer, Steven S"' showing total 14 results

1. Disruption of Endosomal Sorting in Schwann Cells Leads to Defective Myelination and Endosomal Abnormalities Observed in Charcot-Marie-Tooth Disease.

Author

McLean, John W., Wilson, Julie A., Tian, Tina, Watson, Jennifer A., VanHart, Mary, Bean, Andrew J., Scherer, Steven S., Crossman, David K., Ubogu, Eroboghene, and Wilson, Scott M.

Subjects

SCHWANN cells, CHARCOT-Marie-Tooth disease, MYELINATION, POTASSIUM antagonists, PROTEIN-tyrosine kinases, SCAFFOLD proteins, SCIATIC nerve injuries, MYELIN sheath diseases

Abstract

Endosomal sorting plays a fundamental role in directing neural development. By altering the temporal and spatial distribution of membrane receptors, endosomes regulate signaling pathways that control the differentiation and function of neural cells. Several genes linked to inherited demyelinating peripheral neuropathies, known as Charcot-Marie-Tooth (CMT) disease, encode proteins that directly interact with components of the endosomal sorting complex required for transport (ESCRT). Our previous studies demonstrated that a point mutation in the ESCRT component hepatocyte growth-factor-regulated tyrosine kinase substrate (HGS), an endosomal scaffolding protein that identifies internalized cargo to be sorted by the endosome, causes a peripheral neuropathy in the neurodevelopmentally impaired teetering mice. Here, we constructed a Schwann cell-specific deletion of Hgs to determine the role of endosomal sorting during myelination. Inactivation of HGS in Schwann cells resulted in motor and sensory deficits, slowed nerve conduction velocities, delayed myelination and hypomyelinated axons, all of which occur in demyelinating forms of CMT. Consistent with a delay in Schwann cell maturation, HGS-deficient sciatic nerves displayed increased mRNA levels for several promyelinating genes and decreased mRNA levels for genes that serve as markers of myelinating Schwann cells. Loss of HGS also altered the abundance and activation of the ERBB2/3 receptors, which are essential for Schwann cell development. We therefore hypothesize that HGS plays a critical role in endosomal sorting of the ERBB2/3 receptors during Schwann cell maturation, which further implicates endosomal dysfunction in inherited peripheral neuropathies. [ABSTRACT FROM AUTHOR]

Published

2022

2. Modality-Based Organization of Ascending Somatosensory Axons in the Direct Dorsal Column Pathway.

Author

Jingwen Niu, Long Ding, Li, Jian J., Kim, Hyukmin, Jiakun Liu, Haipeng Li, Moberly, Andrew, Badea, Tudor C., Duncan, Ian D., Young-Jin Son, Scherer, Steven S., and Wenqin Luo

Subjects

SOMATOSENSORY cortex, BRAIN mapping, MEDULLA oblongata, LABORATORY mice, ANIMAL morphology, AXONS

Abstract

The long-standing doctrine regarding the functional organization of the direct dorsal column (DDC) pathway is the "somatotopic map" model, which suggests that somatosensory afferents are primarily organized by receptive field instead of modality. Using modalityspecific genetic tracing, here we show that ascending mechanosensory and proprioceptive axons, two main types of theDDCafferents, are largely segregated into a medial-lateral pattern in the mouse dorsal column and medulla. In addition, we found that this modality-based organization is likely to be conserved in other mammalian species, including human. Furthermore, we identified key morphological differences between these two types of afferents, which explains how modality segregation is formed and why a rough "somatotopic map" was previously detected. Collectively, our results establish a new functional organization model for the mammalian direct dorsal column pathway and provide insight into how somatotopic and modality-based organization coexist in the central somatosensory pathway. [ABSTRACT FROM AUTHOR]

Published

2013

3. Connexin32 Mutations Cause Loss of Function in Schwann Cells and Oligodendrocytes Leading to PNS and CNS Myelination Defects.

Author

Sargiannidou, Irene, Vavlitou, Natalie, Aristodemou, Sophia, Hadjisavvas, Andreas, Kyriacou, Kyriacos, Scherer, Steven S., and Kleopa, Kleopas A.

Subjects

GAP junctions (Cell biology), CELL junctions, OLIGODENDROGLIA, TRANSGENES, NEURAL transmission, NERVOUS system, NEUROSCIENCES

Abstract

The gap junction (GJ) protein connexin32 (Cx32) is expressed by myelinating Schwann cells and oligodendrocytes and is mutated in X-linked Charcot-Marie-Tooth disease. In addition to a demyelinating peripheral neuropathy, some Cx32 mutants are associated with transient or chronic CNS phenotypes. To investigate the molecular basis of these phenotypes, we generated transgenic mice expressing the T55I or the R75W mutation and an IRES-EGFP, driven by the mouse Cnp promoter. The transgene was expressed in oligodendrocytes throughout the CNS and in Schwann cells. Both the T55I and the R75W mutants were localized in the perinuclear cytoplasm, did not form GJ plaques, and did not alter the expression or localization of two other oligodendrocytic GJ proteins, Cx47 and Cx29, or the expression of Cx29 in Schwann cells. On wild type background, the expression of endogenous mCx32 was unaffected by the T55I mutant, but was partly impaired by R75W. Transgenic mice with the R75W mutation and all mutant animals with Gjb1-null background developed a progressive demyelinating peripheral neuropathy along with CNS myelination defects. These findings suggest that Cx32 mutations result in loss of function in myelinated cells without trans-dominant effects on other GJ proteins. Loss of Cx32 function alone in the CNS causes myelination defects. [ABSTRACT FROM AUTHOR]

Published

2009

4. Two Distinct Heterotypic Channels Mediate Gap Junction Coupling between Astrocyte and Oligodendrocyte Connexins.

Author

Orthmann-Murphy, Jennifer L., Freidin, Mona, Fischer, Esther, Scherer, Steven S., and Abrams, Charles K.

Subjects

GAP junctions (Cell biology), ASTROCYTES, CONNEXINS, GENETIC disorders, MYELIN proteins

Abstract

Genetic diseases demonstrate that the normal function of CNS myelin depends on connexin32 (Cx32) and Cx47, gap junction (GJ) proteins expressed by oligodendrocytes. GJs couple oligodendrocytes and astrocytes (O/A channels) as well as astrocytes themselves (A/A channels). Because astrocytes express different connexins (Cx30 and Cx43), O/A channels must be heterotypic, whereas A/A channels may be homotypic or heterotypic. Using electrophysiological and immunocytochemical approaches, we found that Cx47/Cx43 and Cx32/Cx30 efficiently formed functional channels, but other potential heterotypic O/A and A/A pairs did not. These results suggest that Cx30/Cx30 and Cx43/Cx43 channels mediate A/A coupling, and Cx47/Cx43 and Cx32/Cx30 channels mediate O/A coupling. Furthermore, Cx47/Cx43 and Cx32/Cx30 channels have distinct macroscopic and single-channel properties and different dye permeabilities. Finally, Cx47 mutants that cause Pelizaeus-Merzbacher-like disease do not efficiently form functional channels with Cx43, indicating that disrupted Cx47/Cx43 channels cause this disease. [ABSTRACT FROM AUTHOR]

Published

2007

5. Genetic and Physiological Evidence That Oligodendrocyte Gap Junctions Contribute to Spatial Buffering of Potassium Released during Neuronal Activity.

Author

Menichella, Daniela M., Majdan, Marta, Awatramani, Rajeshwar, Goodenough, Daniel A., Sirkowski, Erich, Scherer, Steven S., and Paul, David L.

Subjects

CONNEXINS, NEURAL circuitry, LABORATORY mice, AXONAL transport, MEMBRANE proteins

Abstract

Mice lacking the K+ channel Kir4.1 or both connexin32 (Cx32) and Cx47 exhibit myelin-associated vacuoles, raising the possibility that oligodendrocytes, and the connexins they express, contribute to recycling the K+ evolved during neuronal activity. To study this possibility, we first examined the effect of neuronal activity on the appearance of vacuoles in mice lacking both Cx32 and Cx47. The size and number of myelin vacuoles was dramatically increased when axonal activity was increased, by either a natural stimulus (eye opening) or pharmacological treatment. Conversely, myelin vacuoles were dramatically reduced when axonal activity was suppressed. Second, we used genetic complementation to test for a relationship between the function of Kir4.1 and oligodendrocyte connexins. In a Cx32-null background, haploinsufficiency of either Cx47 or Kir4.1 did not affect myelin, but double heterozygotes developed vacuoles, consistent with the idea that oligodendrocyte connexins and Kir4.1 function in a common pathway. Together, these results implicate oligodendrocytes and their connexins as having critical roles in the buffering of K+ released during neuronal activity. [ABSTRACT FROM AUTHOR]

Published

2006

6. A Common Ankyrin-G-Based Mechanism Retains KCNQ and NaV Channels at Electrically Active Domains of the Axon.

Author

Zongming Pan, Tingching Kao, Horvath, Zsolt, Lemos, Julia, Jai-Yoon Sul, Cranstoun, Stephen D., Bennett, Vann, Scherer, Steven S., and Cooper, Edward C.

Subjects

POTASSIUM channels, ACTION potentials, AXONS, IMMUNOGLOBULINS, PEPTIDE hormones, EPITOPES

Abstract

KCNQ (KV7) potassium channels underlie subthreshold M-currents that stabilize the neuronal resting potential and prevent repetitive firing of action potentials. Here, antibodies against four different KCNQ2 and KCNQ3 polypeptide epitopes show these subunits concentrated at the axonal initial segment (AIS) and node of Ranvier. AIS concentration of KCNQ2and KCNQ3, like that of voltage-gated sodium (NaV) channels, is abolished in ankyrin-G knock-out mice. A short motif, common to KCNQ2 and KCNQ3, mediates both in vivo ankyrin-G interaction and retention of the subunits at the AIS. This KCNQ2/KCNQ3 motif is nearly identical to the sequence on NaV α subunits that serves these functions. All identified NaV and KCNQ genes of worms, insects, and molluscs lack the ankyrin-G binding motif. In contrast, vertebrate orthologs of NaV α subunits, KCNQ2, and KCNQ3 (including from bony fish, birds, and mammals) all possess the motif. Thus, concerted ankyrin-G interaction with KCNQ and NaV channels appears to have arisen through convergent molecular evolution, after the division between invertebrate and vertebrate lineages, but before the appearance of the last common jawed vertebrate ancestor. This includes the historical period when myelin also evolved. [ABSTRACT FROM AUTHOR]

Published

2006

7. ErbB2 Signaling in Schwann Cells Is Mostly Dispensable for Maintenance of Myelinated Peripheral Nerves and Proliferation of Adult Schwann Cells after Injury.

Author

Atanasoski, Suzana, Scherer, Steven S., Sirkowski, Erich, Leone, Dino, Garratt, Alistar N., Birchmeier, Carmen, and Suter, Ueli

Subjects

*CELL proliferation, *MYELIN sheath, *PERIPHERAL nervous system, *CYCLINS, *PROTEIN kinases

Abstract

Neuregulin/erbB signaling is critically required for survival and proliferation of Schwann cells as well as for establishing correct myelin thickness of peripheral nerves during development. In this study, we investigated whether erbB2 signaling in Schwann cells is also essential for the maintenance of myelinated peripheral nerves and for Schwann cell proliferation and survival after nerve injury. To this end, we used inducible Cre-loxP technology using a PLP-CreERT2 allele to ablate erbB2 in adult Schwann cells. ErbB2 expression was markedly reduced after induction of erbB2 gene disruption with no apparent effect on the maintenance of already established myelinated peripheral nerves. In contrast to development, Schwann cell proliferation and survival were not impaired in mutant animals after nerve injury, despite reduced levels of MAPK-P (phosphorylated mitogen-activated protein kinase) and cyclin D1. ErbB1 and erbB4 do not compensate for the loss of erbB2. We conclude that adult Schwann cells do not require major neuregulin signaling through erbB2 for proliferation and survival after nerve injury, in contrast to development and in cell culture. [ABSTRACT FROM AUTHOR]

Published

2006

8. Both Laminin and Schwann Cell Dystroglycan Are Necessary for Proper Clustering of Sodium Channels at Nodes of Ranvier.

Author

Occhi, Simona, Zambroni, Desirée, Del Carro, Ubaldo, Amadio, Stefano, Sirkowski, Erich E., Scherer, Steven S., Campbell, Kevin P., Moore, Steven A., Chen, Zulin-L., Strickland, Sidney, Di Muzio, Antonio, Uncini, Antonino, Wrabetz, Lawrence, and Feltri, M. Laura

Subjects

AXONS, SODIUM channels, MUSCULAR dystrophy, NEURONS, NERVOUS system

Abstract

Nodes of Ranvier are specialized axonal domains, at which voltage-gated sodium channels cluster. How axons cluster molecules in discrete domains is mostly unknown. Both axons and glia probably provide constraining mechanisms that contribute to domain formation. Proper sodium channel clustering in peripheral nerves depends on contact from Schwann cell microvilli, where at least one molecule, gliomedin, binds the sodium channel complex and induces its clustering. Furthermore, mice lacking Schwann cell dystroglycan have aberrant microvilli and poorly clustered sodium channels. Dystroglycan could interact at the basal lamina or at the axon--glial surface. Because dystroglycan is a laminin receptor, and laminin 2 mutations [merosin-deficient congenital muscular dystrophy (MDC1A)] cause reduced nerve conduction velocity, we asked whether laminins are involved. Here, we show that the composition of both laminins and the dystroglycan complex at nodes differs from that of internodes. Mice defective in laminin 2 have poorly formed microvilli and abnormal sodium clusters. These abnormalities are similar, albeit less severe, than those of mice lacking dystroglycan. However, mice lacking all Schwann cell laminins show severe nodal abnormalities, suggesting that other laminins compensate for the lack of laminin 2. Thus, although laminins are located at a distance from the axoglial junction, they are required for proper clustering of sodium channels. Laminins, through their specific nodal receptors and cytoskeletal linkages, may participate in the formation of mechanisms that constrain clusters at nodes. Finally, abnormal sodium channel clusters are present in a patient with MDC1A, providing a molecular basis for the reduced nerve conduction velocity in this disorder. [ABSTRACT FROM AUTHOR]

Published

2005

9. Prenylation-Defective Human Connexin32 Mutants Are Normally Localized and Function Equivalently to Wild-Type Connexin32 in Myelinating Schwann Cells.

Author

Yan Huang, Sirkowski, Erich E., Stickney, John T., and Scherer, Steven S.

Subjects

MICE, RODENTS, CELLS, PATHOLOGY, GENETIC disorders, SPINAL muscular atrophy, ALTERNATIVE medicine, TRANSGENIC animals, TRANSGENIC mice, GENOTYPE-environment interaction

Abstract

Mutations in GJB1, the gene encoding the gap junction protein connexin32 (Cx32), cause the X-linked form of Charcot-Marie-Tooth disease, an inherited demyelinating neuropathy. The C terminus of human Cx32 contains a putative prenylation motif that is conserved in Cx32 orthologs. Using [³H]mevalonolactone ([³H]MVA) incorporation, we demonstrated that wild-type human connexin32 can be prenylated in COS7 cells, in contrast to disease-associated mutations that are predicted to disrupt the prenylation motif. We generated transgenic mice that express these mutants in myelinating Schwann cells. Male mice expressing a transgene were crossed with female Gjb1-null mice; the male offspring were all Gjb1-null, and one-half were transgene positive; in these mice, all Cx32 was derived from expression of the transgene. The mutant human protein was properly localized in myelinating Schwann cells in multiple transgenic lines and did not alter the localization of other components of paranodes and incisures. Finally, both the C280G and the S281x mutants appeared to "rescue" the phenotype of Gjb1-null mice, because transgene-positive male mice had significantly fewer abnormally myelinated axons than did their transgene-negative male littermates. These results indicate that Cx32 is prenylated, but that prenylation is not required for proper trafficking of Cx32 and perhaps not even for certain aspects of its function, in myelinating Schwann cells. [ABSTRACT FROM AUTHOR]

Published

2005

10. Transgenic Expression of Human Connexin32 in Myelinating Schwann Cells Prevents Demyelination in Connexin32-Null Mice.

Author

Scherer, Steven S., Yi-Tian Xu, Messing, Albee, Willecke, Klaus, Fischbeck, Kenneth H., and Jeng, Linda Jo Bone

Subjects

*GAP junctions (Cell biology), *CELL junctions, *CONNEXINS, *CHARCOT-Marie-Tooth disease, *DEMYELINATION

Abstract

Mutations in Gap junction β1 (GIB1), the gene encoding the gap junction protein connexin32 (Cx32), cause the X-linked form of Charcot-Marie-Tooth disease (CMT1X), an inherited demyelinating neuropathy. We investigated the possibility that the expression of mutant Cx32 in other cells besides myelinating Schwann cells contributes to the development of demyelination. Human Cx32 was expressed in transgenic mice using a rat myelin protein zero (Mpz) promoter, which is exclusively expressed by myelinating Schwann cells. Male mice expressing the human transgene were crossed with female Gjb1/cx32-null mice; the resulting male offspring were all cx32-null (on the X chromosome), and one-half were transgene positive. In these transgenic mice, all of the Cx32 was derived from the expression of the transgene and was found in the sciatic nerve but not in the spinal cord or the liver. Furthermore, the Cx32 protein was properly localized (within incisures and paranodes) in myelinating Schwann cells. Finally, the expression of human Cx32 protein "rescued" the phenotype of cx32-null mice, because the transgenic mice have significantly fewer demyelinated or remyelinated axons than their nontransgenic littermates. These results indicate that the loss of Schwann-cell-autonomous expression of Cx32 is sufficient to account for demyelination in CMT1X. [ABSTRACT FROM AUTHOR]

Published

2005

11. Altered Ion Channels in an Animal Model of Charcot-Marie-Tooth Disease Type IA.

Author

Devaux, Jérôme J. and Scherer, Steven S.

Subjects

*DEMYELINATION, *NEUROLOGICAL disorders, *AXONS, *NEUROPATHY, *MYELIN sheath diseases

Abstract

How demyelination and remyelination affect the function of myelinated axons is a fundamental aspect of demyelinating diseases. We examined this issue in Trembler-J mice, a genetically authentic model of a dominantly inherited demyelinating neuropathy of humans. The K+ channels Kv1.1 and Kv1.2 channels were often improperly located in the paranodal axon membrane, typically associated with improperly formed paranodes, and in unmyelinated segments between internodes. As in wild-type nerves, Trembler-J nodes contained Nav1.6, ankyrin-G, βIV-spectrin, and KCNQ2, but, unlike wild-type nerves, they also contained Kv3.1b and Nav1.8. In unmyelinated segments bordered by myelin sheaths, these proteins were clustered in heminodes and did not appear to be diffusely localized in the unmyelinated segments themselves. Nodes and heminodes were contacted by Schwann cells processes that did not have the ultrastructural or molecular characteristics of mature microvilli. Despite the presence of Nav1.8, a tetrodotoxin-resistant sodium channel, sciatic nerve conduction was at least as sensitive to tetrodotoxin in Trembler-J nerves as in wild-type nerves. Thus, the profound reorganization of axonal ion channels and the aberrant expression of novel ion channels likely contribute to the altered conduction in Trembler-J nerves. [ABSTRACT FROM AUTHOR]

Published

2005

12. KCNQ2 Is a Nodal K+ Channel.

Author

Devaux, Jérôme J., Kleopa, Kleopas A., Cooper, Edward C., and Scherer, Steven S.

Subjects

GENETIC mutation, AXONS, NEURONS, EPILEPSY, BRAIN diseases, PHYSIOLOGICAL control systems

Abstract

Mutations in the gene encoding the K+ channel KCNQ2 cause neonatal epilepsy and myokymia, indicating that KCNQ2 regulates the excitability of CNS neurons and motor axons, respectively. We show here that KCNQ2 channels are functional components of axon initial segments and nodes of Ranvier, colocalizing with ankyrin-G and voltage-dependent Na+ channels throughout the CNS and PNS. Retigabine, which opens KCNQ channels, diminishes axonal excitability. Linopirdine, which blocks KCNQ channels, prolongs the repolarization of the action potential in neonatal nerves. The clustering of KCNQ2 at nodes and initial segments lags that of ankyrin-G during development, and both ankyrin-G and KCNQ2 can be coimmunoprecipitated in the brain. KCNQ3 is also a component of some initial segments and nodes in the brain. The diminished activity of mutant KCNQ2 channels accounts for neonatal epilepsy and myokymia; the cellular locus of these effects may be axonal initial segments and nodes. [ABSTRACT FROM AUTHOR]

Published

2004

13. Connexins Are Critical for Normal Myelination in the CNS.

Author

Menichella, Daniela M., Goodenough, Daniel A., Sirkowski, Erich, Scherer, Steven S., and Paul, David L.

Subjects

CONNEXINS, OLIGODENDROGLIA, MYELINATION, CENTRAL nervous system, NERVOUS system

Abstract

Presents a study that explored the role of oligodendrocyte connexins in normal myelination in the central nervous system. Procedures used in investigating the unaffection of central myelination with regard to mutations in Cx32, a gap-junction channel-forming protein; Assessment of the reaction of animal specimens that lack connexins resulting from cell death; Significance of intercellular communication in oligodendrocytes.

Published

2003

14. Kv3.1b Is a Novel Component of CNS Nodes.

Author

Devaux, Jerome, Alcaraz, Gisele, Grinspan, Judith, Bennett, Vann, Jobo, Rolf, Crest, Marcel, and Scherer, Steven S.

Subjects

NODES of Ranvier, NERVES, CENTRAL nervous system, SPINAL cord, BRAIN

Abstract

Presents a study that investigated Kv3.1b as a novel component of central nervous system nodes. Materials and methods; Results; Discussion.

Published

2003