Your search keyword '"Rosalind A. Segal"' showing total 146 results

1. Exploring clinical markers of Axon degeneration processes in Chemotherapy-induced peripheral neuropathy among young adults receiving vincristine or paclitaxel

Author

Robert Knoerl, Emanuele Mazzola, Maria Pazyra-Murphy, Birgitta Ryback, A. Lindsay Frazier, Roy L. Freeman, Marilyn Hammer, Ann LaCasce, Jennifer Ligibel, Marlise R. Luskin, Donna L. Berry, and Rosalind A. Segal

Subjects

Chemotherapy-induced peripheral neuropathy, NAD, human [Supplementary Concept], Young Adult, Neoplasms, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Approximately 70% of patients receiving neurotoxic chemotherapy (e.g., paclitaxel or vincristine) will develop chemotherapy-induced peripheral neuropathy. Despite the known negative effects of CIPN on physical functioning and chemotherapy dosing, little is known about how to prevent CIPN. The development of efficacious CIPN prevention interventions is hindered by the lack of knowledge surrounding CIPN mechanisms. Nicotinamide adenine dinucleotide (NAD+) and cyclic-adenosine diphosphate ribose (cADPR) are potential markers of axon degeneration following neurotoxic chemotherapy, however, such markers have been exclusively measured in preclinical models of chemotherapy-induced peripheral neuropathy (CIPN). The overall objective of this longitudinal, observational study was to determine the association between plasma NAD+, cADPR, and ADPR with CIPN severity in young adults receiving vincristine or paclitaxel. Methods Young adults (18–39 years old) beginning vincristine or paclitaxel were recruited from Dana-Farber Cancer Institute. Young adults completed the QLQ-CIPN20 sensory and motor subscales and provided a blood sample prior to starting chemotherapy (T1) and at increasing cumulative vincristine (T2: 3–5 mg, T3: 7–9 mg) and paclitaxel (T2: 300–500 mg/m2, T3: 700–900 mg/m2) dosages. NAD+, cADPR, and ADPR were quantified from plasma using mass spectrometry. Metabolite levels and QLQ-CIPN20 scores over time were compared using mixed-effects linear regression models and/or paired two-sample tests. Results Participants (N = 50) were mainly female (88%), white (80%), and receiving paclitaxel (78%). Sensory and motor CIPN severity increased from T1–T3 (p

Published

2024

2. Genome-wide CRISPR-Cas9 knockout screens identify DNMT1 as a druggable dependency in sonic hedgehog medulloblastoma

Author

Foteini Tsiami, Chiara Lago, Noemi Pozza, Federica Piccioni, Xuesong Zhao, Fabienne Lülsberg, David E. Root, Luca Tiberi, Marcel Kool, Jens Schittenhelm, Pratiti Bandopadhayay, Rosalind A. Segal, Ghazaleh Tabatabai, and Daniel J. Merk

Subjects

Medulloblastoma, Functional genomics, DNMT1, SHH pathway, Combinatorial treatment, Synergy, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Sonic hedgehog subgroup of medulloblastoma (SHH-MB) is characterized by aberrant activation of the SHH signaling pathway. An inhibition of the positive SHH regulator Smoothened (SMO) has demonstrated promising clinical efficacy. Yet, primary and acquired resistance to SMO inhibitors limit their efficacy. An understanding of underlying molecular mechanisms of resistance to therapy is warranted to bridge this unmet need. Here, we make use of genome-wide CRISPR-Cas9 knockout screens in murine SMB21 and human DAOY cells, in order to unravel genetic dependencies and drug-related genetic interactors that could serve as alternative therapeutic targets for SHH-MB. Our screens reinforce SMB21 cells as a faithful model system for SHH-MB, as opposed to DAOY cells, and identify members of the epigenetic machinery including DNA methyltransferase 1 (DNMT1) as druggable targets in SHH-dependent tumors. We show that Dnmt1 plays a crucial role in normal murine cerebellar development and is required for SHH-MB growth in vivo. Additionally, DNMT1 pharmacological inhibition alone and in combination with SMO inhibition effectively inhibits tumor growth in murine and human SHH-MB cell models and prolongs survival of SHH-MB mouse models by inhibiting SHH signaling output downstream of SMO. In conclusion, our data highlight the potential of inhibiting epigenetic regulators as a novel therapeutic avenue in SMO-inhibitor sensitive as well as resistant SHH-MBs.

Published

2024

3. Developmental basis of SHH medulloblastoma heterogeneity

Author

Maxwell P. Gold, Winnie Ong, Andrew M. Masteller, David R. Ghasemi, Julie Anne Galindo, Noel R. Park, Nhan C. Huynh, Aneesh Donde, Veronika Pister, Raul A. Saurez, Maria C. Vladoiu, Grace H. Hwang, Tanja Eisemann, Laura K. Donovan, Adam D. Walker, Joseph Benetatos, Christelle Dufour, Livia Garzia, Rosalind A. Segal, Robert J. Wechsler-Reya, Jill P. Mesirov, Andrey Korshunov, Kristian W. Pajtler, Scott L. Pomeroy, Olivier Ayrault, Shawn M. Davidson, Jennifer A. Cotter, Michael D. Taylor, and Ernest Fraenkel

Subjects

Science

Abstract

Abstract Many genes that drive normal cellular development also contribute to oncogenesis. Medulloblastoma (MB) tumors likely arise from neuronal progenitors in the cerebellum, and we hypothesized that the heterogeneity observed in MBs with sonic hedgehog (SHH) activation could be due to differences in developmental pathways. To investigate this question, here we perform single-nucleus RNA sequencing on highly differentiated SHH MBs with extensively nodular histology and observed malignant cells resembling each stage of canonical granule neuron development. Through innovative computational approaches, we connect these results to published datasets and find that some established molecular subtypes of SHH MB appear arrested at different developmental stages. Additionally, using multiplexed proteomic imaging and MALDI imaging mass spectrometry, we identify distinct histological and metabolic profiles for highly differentiated tumors. Our approaches are applicable to understanding the interplay between heterogeneity and differentiation in other cancers and can provide important insights for the design of targeted therapies.

Published

2024

4. Mitogenic and progenitor gene programmes in single pilocytic astrocytoma cells

Author

Zachary J. Reitman, Brenton R. Paolella, Guillaume Bergthold, Kristine Pelton, Sarah Becker, Robert Jones, Claire E. Sinai, Hayley Malkin, Ying Huang, Leslie Grimmet, Zachary T. Herbert, Yu Sun, Jessica L. Weatherbee, John A. Alberta, John F. Daley, Orit Rozenblatt-Rosen, Alexandra L. Condurat, Kenin Qian, Prasidda Khadka, Rosalind A. Segal, Daphne Haas-Kogan, Mariella G. Filbin, Mario L. Suva, Aviv Regev, Charles D. Stiles, Mark W. Kieran, Liliana Goumnerova, Keith L. Ligon, Alex K. Shalek, Pratiti Bandopadhayay, and Rameen Beroukhim

Subjects

Science

Abstract

Pilocytic astrocytoma is a low-grade pediatric glioma, characterized by a single BRAF rearrangement. Here, Reitman and colleagues use single-cell RNA sequencing to reveal molecular hallmarks of the disease that might be targeted therapeutically.

Published

2019

5. Prolyl Isomerase Pin1 Regulates Axon Guidance by Stabilizing CRMP2A Selectively in Distal Axons

Author

Martin Balastik, Xiao Zhen Zhou, Meritxell Alberich-Jorda, Romana Weissova, Jakub Žiak, Maria F. Pazyra-Murphy, Katharina E. Cosker, Olga Machonova, Iryna Kozmikova, Chun-Hau Chen, Lucia Pastorino, John M. Asara, Adam Cole, Calum Sutherland, Rosalind A. Segal, and Kun Ping Lu

Subjects

Biology (General), QH301-705.5

Abstract

Axon guidance relies on precise translation of extracellular signal gradients into local changes in cytoskeletal dynamics, but the molecular mechanisms regulating dose-dependent responses of growth cones are still poorly understood. Here, we show that during embryonic development in growing axons, a low level of Semaphorin3A stimulation is buffered by the prolyl isomerase Pin1. We demonstrate that Pin1 stabilizes CDK5-phosphorylated CRMP2A, the major isoform of CRMP2 in distal axons. Consequently, Pin1 knockdown or knockout reduces CRMP2A levels specifically in distal axons and inhibits axon growth, which can be fully rescued by Pin1 or CRMP2A expression. Moreover, Pin1 knockdown or knockout increases sensitivity to Sema3A-induced growth cone collapse in vitro and in vivo, leading to developmental abnormalities in axon guidance. These results identify an important isoform-specific function and regulation of CRMP2A in controlling axon growth and uncover Pin1-catalyzed prolyl isomerization as a regulatory mechanism in axon guidance.

Published

2015

6. A Mechanistic Understanding of Axon Degeneration in Chemotherapy-Induced Peripheral Neuropathy

Author

Yusuke Fukuda, Yihang Li, and Rosalind A. Segal

Subjects

axon, chemotherapy, CIPN, degeneration, DRG, neuropathy, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Chemotherapeutic agents cause many short and long term toxic side effects to peripheral nervous system (PNS) that drastically alter quality of life. Chemotherapy-induced peripheral neuropathy (CIPN) is a common and enduring disorder caused by several anti-neoplastic agents. CIPN typically presents with neuropathic pain, numbness of distal extremities, and/or oversensitivity to thermal or mechanical stimuli. This adverse side effect often requires a reduction in chemotherapy dosage or even discontinuation of treatment. Currently there are no effective treatment options for CIPN. While the underlying mechanisms for CIPN are not understood, current data identify a “dying back” axon degeneration of distal nerve endings as the major pathology in this disorder. Therefore, mechanistic understanding of axon degeneration will provide insights into the pathway and molecular players responsible for CIPN. Here, we review recent findings that expand our understanding of the pathogenesis of CIPN and discuss pathways that may be shared with the axonal degeneration that occurs during developmental axon pruning and during injury-induced Wallerian degeneration. These mechanistic insights provide new avenues for development of therapies to prevent or treat CIPN.

Published

2017

7. Table S1 from A Transposon Screen Identifies Loss of Primary Cilia as a Mechanism of Resistance to SMO Inhibitors

Author

Rosalind A. Segal, Joseph F. Kelleher, Tatyana Ponomaryov, Emily J. Chadwick, Ethan L. MacKenzie, Maria F. Pazyra-Murphy, Kimberly J. Ornell, Ekaterina Pak, and Xuesong Zhao

Abstract

Supplementary Table S1, related to Figure 1. A total of 182 transposon insertions were identified in 27 resistant clones. Provided as a separate Excel file

Published

2023

8. Supplemental information from A Transposon Screen Identifies Loss of Primary Cilia as a Mechanism of Resistance to SMO Inhibitors

Author

Rosalind A. Segal, Joseph F. Kelleher, Tatyana Ponomaryov, Emily J. Chadwick, Ethan L. MacKenzie, Maria F. Pazyra-Murphy, Kimberly J. Ornell, Ekaterina Pak, and Xuesong Zhao

Abstract

Supplementary Figures, tables, methods and references

Published

2023

9. Supplemental Methods, Figures 1 - 8, Tables 1 - 2 from RAS/MAPK Activation Drives Resistance to Smo Inhibition, Metastasis, and Tumor Evolution in Shh Pathway–Dependent Tumors

Author

Rosalind A. Segal, Joseph F. Kelleher, Jennifer A. Chan, Anthony E. Oro, Jiang Li, Anne Lynn S. Chang, Ramon J. Whitson, Scott X. Atwood, Wei Li, Ekaterina Pak, Sukriti K. Dabral, Pengcheng Zhou, Kimberly J. Ornell, Tatyana Ponomaryov, and Xuesong Zhao

Abstract

Figure S1. Growth and survival of SMB cells depends on Shh signaling. Figure S2. SMB cell lines are a faithful model to study resistance to Smo inhibitors. Table S1. List of candidate genes with mutations used in the study. Figure S3. RAS signaling confers resistance to Smo inhibitor LDE225. Figure S4. FGF/RAS signaling abrogates dependence on Shh signaling. Figure S5. FGF/RAS-driven resistance to Smo inhibition is reversible and can be treated with MEK inhibitors. Figure S6. MEK inhibitors have therapeutic potential for HRAS SMB cells. Figure S7. Morphology of SMB(HRAS) cells differs from SMB parental cells. Figure S8. Immunohistochemistry of SFRP1, pERK and FGF in primary and metastatic samples from human Shh-subtype medulloblastoma patients. Table S2. Clinical diagnosis for human patient samples shown in Figure 5.

Published

2023

10. An affinity for brainstem microglia in pediatric high-grade gliomas of brainstem origin

Author

Liat Peretz Zats, Labiba Ahmad, Natania Casden, Meelim J Lee, Vitali Belzer, Orit Adato, Shaked Bar Cohen, Seung-Hyun B Ko, Mariella G Filbin, Ron Unger, Douglas A Lauffenburger, Rosalind A Segal, and Oded Behar

Subjects

General Medicine

Abstract

Background High-grade gliomas (HGG) in children have a devastating prognosis and occur in a remarkable spatiotemporal pattern. Diffuse midline gliomas (DMG), including diffuse intrinsic pontine gliomas (DIPG), typically occur in mid-childhood, while cortical HGGs are more frequent in older children and adults. The mechanisms behind this pattern are not clear. Methods We used mouse organotypic slice cultures and glial cell cultures to test the impact of the microenvironment on human DIPG cells. Comparing the expression between brainstem and cortical microglia identified differentially expressed secreted proteins. The impact of some of these proteins on DIPGs was tested. Results DIPGs, pediatric HGGs of brainstem origin, survive and divide more in organotypic slice cultures originating in the brainstem as compared to the cortex. Moreover, brainstem microglia are better able to support tumors of brainstem origin. A comparison between the two microglial populations revealed differentially expressed genes. One such gene, interleukin-33 (IL33), is highly expressed in the pons of young mice and its DIPG receptor is upregulated in this context. Consistent with this observation, the expression levels of IL33 and its receptor, IL1RL1, are higher in DIPG biopsies compared to low-grade cortical gliomas. Furthermore, IL33 can enhance proliferation and clonability of HGGs of brainstem origin, while blocking IL33 in brainstem organotypic slice cultures reduced the proliferation of these tumor cells. Conclusions Crosstalk between DIPGs and the brainstem microenvironment, in particular microglia, through IL33 and other secreted factors, modulates spatiotemporal patterning of this HGG and could prove to be an important future therapeutic target.

Published

2022

11. Synthetic extracellular matrices and astrocytes provide a supportive microenvironment for the cultivation and investigation of primary pediatric gliomas

Author

Christopher M Rota, Alexander T Brown, Emily Addleson, Clara Ives, Ella Trumper, Kristine Pelton, Wei Pin Teh, Matthew J Schniederjan, Robert Craig Castellino, Sara Buhrlage, Douglas A Lauffenburger, Keith L Ligon, Linda G Griffith, and Rosalind A Segal

Subjects

Basic and Translational Investigations, General Medicine

Abstract

Background Pediatric gliomas comprise a diverse set of brain tumor entities that have substantial long-term ramifications for patient survival and quality of life. However, the study of these tumors is currently limited due to a lack of authentic models. Additionally, many aspects of pediatric brain tumor biology, such as tumor cell invasiveness, have been difficult to study with currently available tools. To address these issues, we developed a synthetic extracellular matrix (sECM)-based culture system to grow and study primary pediatric brain tumor cells. Methods We developed a brain-like sECM material as a supportive scaffold for the culture of primary, patient-derived pediatric glioma cells and established patient-derived cell lines. Primary juvenile brainstem-derived murine astrocytes were used as a feeder layer to support the growth of primary human tumor cells. Results We found that our culture system facilitated the proliferation of various primary pediatric brain tumors, including low-grade gliomas, and enabled ex vivo testing of investigational therapeutics. Additionally, we found that tuning this sECM material allowed us to assess high-grade pediatric glioma cell invasion and evaluate therapeutic interventions targeting invasive behavior. Conclusion Our sECM culture platform provides a multipurpose tool for pediatric brain tumor researchers that enables both a wide breadth of biological assays and the cultivation of diverse tumor types.

Published

2022

12. Sarm1 activation produces cADPR to increase intra-axonal Ca++ and promote axon degeneration in PIPN

Author

Yihang Li, Maria F. Pazyra-Murphy, Daina Avizonis, Mariana de Sá Tavares Russo, Sophia Tang, Chiung-Ya Chen, Yi-Ping Hsueh, Johann S. Bergholz, Tao Jiang, Jean J. Zhao, Jian Zhu, Kwang Woo Ko, Jeffrey Milbrandt, Aaron DiAntonio, and Rosalind A. Segal

Subjects

Armadillo Domain Proteins, Cyclic ADP-Ribose, Paclitaxel, Peripheral Nervous System Diseases, Cell Biology, Axons, Mice, Inbred C57BL, Rats, Sprague-Dawley, Cytoskeletal Proteins, HEK293 Cells, Nerve Degeneration, Animals, Humans, Calcium, Female, Calcium Channels

Abstract

Cancer patients frequently develop chemotherapy-induced peripheral neuropathy (CIPN), a painful and long-lasting disorder with profound somatosensory deficits. There are no effective therapies to prevent or treat this disorder. Pathologically, CIPN is characterized by a “dying-back” axonopathy that begins at intra-epidermal nerve terminals of sensory neurons and progresses in a retrograde fashion. Calcium dysregulation constitutes a critical event in CIPN, but it is not known how chemotherapies such as paclitaxel alter intra-axonal calcium and cause degeneration. Here, we demonstrate that paclitaxel triggers Sarm1-dependent cADPR production in distal axons, promoting intra-axonal calcium flux from both intracellular and extracellular calcium stores. Genetic or pharmacologic antagonists of cADPR signaling prevent paclitaxel-induced axon degeneration and allodynia symptoms, without mitigating the anti-neoplastic efficacy of paclitaxel. Our data demonstrate that cADPR is a calcium-modulating factor that promotes paclitaxel-induced axon degeneration and suggest that targeting cADPR signaling provides a potential therapeutic approach for treating paclitaxel-induced peripheral neuropathy (PIPN).

Published

2021

13. Mitogenic and progenitor gene programmes in single pilocytic astrocytoma cells

Author

Kristine Pelton, Prasidda Khadka, Kenin Qian, Zachary T. Herbert, Guillaume Bergthold, Mariella G. Filbin, Liliana Goumnerova, Aviv Regev, Robert T. Jones, John F. Daley, Jessica Weatherbee, Yu Sun, Ying Huang, Keith L. Ligon, Orit Rozenblatt-Rosen, Pratiti Bandopadhayay, Rameen Beroukhim, Claire Sinai, John A. Alberta, Brenton R. Paolella, Alex K. Shalek, Zachary J. Reitman, Sarah Becker, Rosalind A. Segal, Mark W. Kieran, Alexandra L. Condurat, Daphne A. Haas-Kogan, Charles D. Stiles, Hayley Malkin, Leslie Grimmet, and Mario L. Suvà

Subjects

Proto-Oncogene Proteins B-raf, 0301 basic medicine, MAPK/ERK pathway, Oncogene Proteins, Fusion, MAP Kinase Signaling System, Science, General Physics and Astronomy, 02 engineering and technology, Astrocytoma, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Paediatric cancer, Mice, 03 medical and health sciences, Immune system, Neural Stem Cells, Glioma, Tumor Cells, Cultured, medicine, Animals, Humans, lcsh:Science, neoplasms, Progenitor, Multidisciplinary, Pilocytic astrocytoma, Microglia, Brain Neoplasms, RNA sequencing, General Chemistry, 021001 nanoscience & nanotechnology, medicine.disease, Phenotype, 3. Good health, nervous system diseases, CNS cancer, Oligodendroglia, 030104 developmental biology, medicine.anatomical_structure, Cancer cell, Cancer research, lcsh:Q, Mitogen-Activated Protein Kinases, 0210 nano-technology

Abstract

Pilocytic astrocytoma (PA), the most common childhood brain tumor, is a low-grade glioma with a single driver BRAF rearrangement. Here, we perform scRNAseq in six PAs using methods that enabled detection of the rearrangement. When compared to higher-grade gliomas, a strikingly higher proportion of the PA cancer cells exhibit a differentiated, astrocyte-like phenotype. A smaller proportion of cells exhibit a progenitor-like phenotype with evidence of proliferation. These express a mitogen-activated protein kinase (MAPK) programme that was absent from higher-grade gliomas. Immune cells, especially microglia, comprise 40% of all cells in the PAs and account for differences in bulk expression profiles between tumor locations and subtypes. These data indicate that MAPK signaling is restricted to relatively undifferentiated cancer cells in PA, with implications for investigational therapies directed at this pathway., Pilocytic astrocytoma is a low-grade pediatric glioma, characterized by a single BRAF rearrangement. Here, Reitman and colleagues use single-cell RNA sequencing to reveal molecular hallmarks of the disease that might be targeted therapeutically.

Published

2019

14. A large-scale drug screen identifies selective inhibitors of class I HDACs as a potential therapeutic option for SHH medulloblastoma

Author

Daniel L. Shaw, Lee L. Rubin, Maria F. Pazyra-Murphy, Jun Qi, Suzanne S Cayer, Xuesong Zhao, Nathalie Y. R. Agar, Paul M.C. Park, Ethan L. MacKenzie, Begona G-C Lopez, Ekaterina Pak, Emily C Addleson, Rosalind A. Segal, Lei Wu, and Daniel Merk

Subjects

Cancer Research, Cell Survival, Pyridines, Biology, Hydroxamic Acids, Inhibitory Concentration 50, Mice, In vivo, Cell Line, Tumor, medicine, Animals, Anilides, Hedgehog Proteins, Sonic hedgehog, Cerebellar Neoplasms, Medulloblastoma, Biphenyl Compounds, Editorials, Proteins, medicine.disease, Smoothened Receptor, Hedgehog signaling pathway, High-Throughput Screening Assays, Histone Deacetylase Inhibitors, Repressor Proteins, Oncology, Drug Resistance, Neoplasm, Cell culture, biology.protein, Cancer research, Neurology (clinical), Histone deacetylase, Signal transduction, Smoothened, Signal Transduction

Abstract

Background Medulloblastoma (MB) is one of the most frequent malignant brain tumors of children, and a large set of these tumors is characterized by aberrant activation of the sonic hedgehog (SHH) pathway. While some tumors initially respond to inhibition of the SHH pathway component Smoothened (SMO), tumors ultimately recur due to downstream resistance mechanisms, indicating a need for novel therapeutic options. Methods Here we performed a targeted small-molecule screen on a stable, SHH-dependent murine MB cell line (SMB21). Comprehensive isotype profiling of histone deacetylase (HDAC) inhibitors was performed, and effects of HDAC inhibition were evaluated in cell lines both sensitive and resistant to SMO inhibition. Lastly, distinct mouse models of SHH MB were used to demonstrate pharmacologic efficacy in vivo. Results A subset of the HDAC inhibitors tested significantly inhibit tumor growth of SMB21 cells by preventing SHH pathway activation. Isotype profiling of HDAC inhibitors, together with genetic approaches suggested that concerted inhibition of multiple class I HDACs is necessary to achieve pathway inhibition. Of note, class I HDAC inhibitors were also efficacious in suppressing growth of diverse SMO inhibitor‒resistant clones of SMB21 cells. Finally, we show that the novel HDAC inhibitor quisinostat targets multiple class I HDACs, is well tolerated in mouse models, and robustly inhibits growth of SHH MB cells in vivo as well as in vitro. Conclusions Our data provide strong evidence that quisinostat or other class I HDAC inhibitors might be therapeutically useful for patients with SHH MB, including those resistant to SMO inhibition.

Published

2019

15. Uncomfortably numb: how Na(v)1.7 mediates paclitaxel-induced peripheral neuropathy

Author

Elizabeth S. Silagi and Rosalind A. Segal

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Paclitaxel, Sensory Receptor Cells, Axonal Transport, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Text mining, Internal medicine, Ganglia, Spinal, medicine, Animals, Humans, business.industry, NAV1.7 Voltage-Gated Sodium Channel, medicine.disease, Scientific Commentaries, Antineoplastic Agents, Phytogenic, humanities, Axons, Rats, Protein Transport, 030104 developmental biology, Peripheral neuropathy, chemistry, nervous system, NAV1, NUMB, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

The microtubule-stabilizing chemotherapy drug paclitaxel (PTX) causes dose-limiting chemotherapy-induced peripheral neuropathy (CIPN), which is often accompanied by pain. Among the multifaceted effects of PTX is an increased expression of sodium channel Nav1.7 in rat and human sensory neurons, enhancing their excitability. However, the mechanisms underlying this increased Nav1.7 expression have not been explored, and the effects of PTX treatment on the dynamics of trafficking and localization of Nav1.7 channels in sensory axons have not been possible to investigate to date. In this study we used a recently developed live imaging approach that allows visualization of Nav1.7 surface channels and long-distance axonal vesicular transport in sensory neurons to fill this basic knowledge gap. We demonstrate concentration and time-dependent effects of PTX on vesicular trafficking and membrane localization of Nav1.7 in real-time in sensory axons. Low concentrations of PTX increase surface channel expression and vesicular flux (number of vesicles per axon). By contrast, treatment with a higher concentration of PTX decreases vesicular flux. Interestingly, vesicular velocity is increased for both concentrations of PTX. Treatment with PTX increased levels of endogenous Nav1.7 mRNA and current density in dorsal root ganglion neurons. However, the current produced by transfection of dorsal root ganglion neurons with Halo-tag Nav1.7 was not increased after exposure to PTX. Taken together, this suggests that the increased trafficking and surface localization of Halo-Nav1.7 that we observed by live imaging in transfected dorsal root ganglion neurons after treatment with PTX might be independent of an increased pool of Nav1.7 channels. After exposure to inflammatory mediators to mimic the inflammatory condition seen during chemotherapy, both Nav1.7 surface levels and vesicular transport are increased for both low and high concentrations of PTX. Overall, our results show that PTX treatment increases levels of functional endogenous Nav1.7 channels in dorsal root ganglion neurons and enhances trafficking and surface distribution of Nav1.7 in sensory axons, with outcomes that depend on the presence of an inflammatory milieu, providing a mechanistic explanation for increased excitability of primary afferents and pain in CIPN.

Published

2021

16. Activation of Sarm1 produces cADPR to increase intra-axonal calcium and promote axon degeneration in CIPN

Author

Daina Avizonis, Maria F. Pazyra-Murphy, Jiang Zhu, Stephanie Tang, Rosalind A. Segal, Li Y, Jeffrey Milbrandt, Jiangning Zhao, Johann Bergholz, Aaron DiAntonio, Russo MdST, Tao Jiang, and Kwang Woo Ko

Subjects

business.industry, chemistry.chemical_element, Degeneration (medical), Calcium, medicine.disease, chemistry.chemical_compound, Allodynia, Peripheral neuropathy, Paclitaxel, chemistry, Calcium flux, medicine, medicine.symptom, Signal transduction, business, Neuroscience, Intracellular

Abstract

SUMMARYCancer patients frequently develop chemotherapy-induced peripheral neuropathy (CIPN), a painful and long-lasting disorder with profound somatosensory deficits. There are no effective therapies to prevent or treat this disorder. Pathologically, CIPN is characterized by a “dying-back” axonopathy that begins at intra-epidermal nerve terminals of sensory neurons and progresses in a retrograde fashion. Calcium dysregulation constitutes a critical event in CIPN, but it is not known how chemotherapies such as paclitaxel alter intra-axonal calcium and cause degeneration. Here, we demonstrate that paclitaxel triggers Sarm1-dependent cADPR production in distal axons, promoting intra-axonal calcium flux from both intracellular and extracellular calcium stores. Genetic or pharmacologic antagonists of cADPR signaling prevent paclitaxel-induced axon degeneration and allodynia symptoms, without mitigating the anti-neoplastic efficacy of paclitaxel. Our data demonstrate that cADPR is a calcium modulating factor that promotes paclitaxel-induced axon degeneration and suggest that targeting cADPR signaling provides a potential therapeutic approach for treating CIPN.HIGHLIGHTSPaclitaxel induces intra-axonal calcium fluxSarm1-dependent cADPR production promotes axonal calcium elevation and degenerationAntagonizing cADPR signaling pathway protects against paclitaxel-induced peripheral neuropathy in vitro and in vivo

Published

2021

17. Diversity of developing peripheral glia revealed by single cell RNA sequencing

Author

Sébastien Vigneau, Lisa V. Goodrich, Alexander A. Gimelbrant, Noah R. Druckenbrod, Olubusola Olukoya, I. Bastille, Rosalind A. Segal, Andrea R. Yung, Peter V. Kharchenko, Maria F. Pazyra-Murphy, Ozge E. Tasdemir-Yilmaz, Austen A. Sitko, and E. B. Hale

Subjects

Nervous system, medicine.anatomical_structure, nervous system, Peripheral nervous system, Gene expression, Cell, medicine, Neural crest, Sensory system, Biology, Somatosensory system, Gene, Neuroscience

Abstract

The peripheral nervous system responds to a wide variety of sensory stimuli, a process that requires great neuronal diversity. These diverse peripheral sensory neurons are closely associated with glial cells that originate from the neural crest (NC). However, the molecular nature and origins of diversity among peripheral glia is not understood. Here we used single cell RNA sequencing to profile and compare developing and mature glia from somatosensory lumbar dorsal root ganglia (DRG) and auditory spiral ganglia (SG). We found that the glial precursors (GPs) differ in their transcriptional profile and prevalence in these two systems. Despite their unique features, somatosensory and auditory GPs undergo convergent differentiation to generate myelinating and non-myelinating Schwann cells that are molecularly uniform. By contrast, although satellite glia surround the neuronal cell bodies in both ganglia, we found that those in the SG express multiple myelination-associated genes, while DRG satellite cells express components that suppress myelination. Lastly, we identified a set of glial signature genes that are also expressed by placode-derived supporting cells, providing new insights into commonalities among glia across the nervous system. This comprehensive survey of gene expression in peripheral glia constitutes a valuable resource for understanding how glia acquire specialized functions and how their roles differ across sensory modalities.

Published

2020

18. The Eya1 Phosphatase Mediates Shh-Driven Symmetric Cell Division of Cerebellar Granule Cell Precursors

Author

Samuel M. Cohen, Jennifer A. Chan, Christopher M. Reid, Xuesong Zhao, Maria F. Pazyra-Murphy, Kristina J. Rehm, Corey C. Harwell, Grace H. Hwang, Pin-Xian Xu, Eun Young Park, Kellie J. Nazemi, Daniel Merk, Pengcheng Zhou, Rosalind A. Segal, Michael J. Eck, and Jose Alfaro

Subjects

Cerebellum, Neurogenesis, Symmetric cell division, Cell fate determination, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Developmental Neuroscience, Neural Stem Cells, Precursor cell, medicine, Animals, Hedgehog Proteins, Sonic hedgehog, biology, Chemistry, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Cell cycle, Mice, Mutant Strains, 030227 psychiatry, Cell biology, medicine.anatomical_structure, Neurology, NUMB, biology.protein, Protein Tyrosine Phosphatases, Neural development, 030217 neurology & neurosurgery, Cell Division, Signal Transduction

Abstract

During neural development, stem and precursor cells can divide either symmetrically or asymmetrically. The transition between symmetric and asymmetric cell divisions is a major determinant of precursor cell expansion and neural differentiation, but the underlying mechanisms that regulate this transition are not well understood. Here, we identify the Sonic hedgehog (Shh) pathway as a critical determinant regulating the mode of division of cerebellar granule cell precursors (GCPs). Using partial gain and loss of function mutations within the Shh pathway, we show that pathway activation determines spindle orientation of GCPs, and that mitotic spindle orientation correlates with the mode of division. Mechanistically, we show that the phosphatase Eya1 is essential for implementing Shh-dependent GCP spindle orientation. We identify atypical protein kinase C (aPKC) as a direct target of Eya1 activity and show that Eya1 dephosphorylates a critical threonine (T410) in the activation loop. Thus, Eya1 inactivates aPKC, resulting in reduced phosphorylation of Numb and other components that regulate the mode of division. This Eya1-dependent cascade is critical in linking spindle orientation, cell cycle exit and terminal differentiation. Together these findings demonstrate that a Shh-Eya1 regulatory axis selectively promotes symmetric cell divisions during cerebellar development by coordinating spindle orientation and cell fate determinants.

Published

2020

19. Recognizing Team Science Contributions in Academic Hiring, Promotion, and Tenure

Author

Rosalind A. Segal, Hollis T. Cline, Steven E. Hyman, Saskia E. J. de Vries, Lique M. Coolen, and Oswald Steward

Subjects

medicine.medical_specialty, Biomedical Research, media_common.quotation_subject, MEDLINE, 03 medical and health sciences, 0302 clinical medicine, Promotion (rank), medicine, Humans, Narrative, Sociology, Cooperative Behavior, 030304 developmental biology, media_common, 0303 health sciences, Ideal (set theory), business.industry, General Neuroscience, Public health, Financing, Organized, Public relations, Team science, Career Mobility, Epiphany, Commentary, business, 030217 neurology & neurosurgery

Abstract

The vision of a scientist as a lone investigator reaching an epiphany is a widely cherished narrative. Consistent with this ideal, single-author papers were frequent 50 years ago, when the Society for Neuroscience started. However, the basic and translational questions and the public health

Published

2020

20. Fast Transport of RNA Granules by Direct Interactions with KIF5A/KLC1 Motors Prevents Axon Degeneration

Author

Lynda M. Rose, Yusuke Fukuda, Rosalind A. Segal, Ozge E. Tasdemir-Yilmaz, Jarrod A. Marto, Li Y, Sirano Dhe-Paganon, Bird Gh, Maria F. Pazyra-Murphy, Nicholas E. Vangos, Loren D. Walensky, Hyuk-Soo Seo, Ezekiel A. Geffken, Guillaume Adelmant, and Zoe C. Yeoh

Subjects

medicine.anatomical_structure, Chemistry, Organelle, Biological neural network, medicine, RNA, Kinesin, Translation (biology), Axon, Axon degeneration, Cell biology

Abstract

Complex neural circuitry requires stable connections formed by lengthy axons. To maintain these functional circuits, fast transport delivers RNAs to distal axons where they undergo local translation. However, the mechanism that enables long distance transport of non-membrane enclosed organelles such as RNA granules is not known. Here we demonstrate that a complex containing RNA and the RNA-binding protein (RBP) SFPQ interacts directly with a tetrameric kinesin containing the adaptor KLC1 and the motor KIF5A. We show that binding of SFPQ to KIF5A/KLC1 motor complex is required for axon survival and is impacted by KIF5A mutations that cause Charcot-Marie-Tooth (CMT) Disease. Moreover, therapeutic approaches that bypass the need for local translation of SFPQ-bound proteins prevent axon degeneration in CMT models. Collectively, these observations show that non-membrane enclosed organelles can move autonomously and that replacing axonally translated proteins provides a therapeutic approach to axonal degenerative disorders.

Published

2020

21. A Transposon Screen Identifies Loss of Primary Cilia as a Mechanism of Resistance to SMO Inhibitors

Author

Tatyana Ponomaryov, Xuesong Zhao, Maria F. Pazyra-Murphy, Rosalind A. Segal, Ethan L. MacKenzie, Ekaterina Pak, Joseph Kelleher, Kimberly J. Ornell, and Emily J. Chadwick

Subjects

0301 basic medicine, Genetics, Retroelements, Cilium, Cancer, Drug resistance, Biology, medicine.disease, Smoothened Receptor, Hedgehog signaling pathway, Cell biology, Mice, 03 medical and health sciences, 030104 developmental biology, Oncology, Ciliogenesis, medicine, Animals, Humans, Hedgehog Proteins, Transposon mutagenesis, Cilia, Signal transduction, Hedgehog, Signal Transduction

Abstract

Drug resistance poses a great challenge to targeted cancer therapies. In Hedgehog pathway–dependent cancers, the scope of mechanisms enabling resistance to SMO inhibitors is not known. Here, we performed a transposon mutagenesis screen in medulloblastoma and identified multiple modes of resistance. Surprisingly, mutations in ciliogenesis genes represent a frequent cause of resistance, and patient datasets indicate that cilia loss constitutes a clinically relevant category of resistance. Conventionally, primary cilia are thought to enable oncogenic Hedgehog signaling. Paradoxically, we find that cilia loss protects tumor cells from susceptibility to SMO inhibitors and maintains a “persister” state that depends on continuous low output of the Hedgehog program. Persister cells can serve as a reservoir for further tumor evolution, as additional alterations synergize with cilia loss to generate aggressive recurrent tumors. Together, our findings reveal patterns of resistance and provide mechanistic insights for the role of cilia in tumor evolution and drug resistance. Significance: Using a transposon screen and clinical datasets, we identified mutations in ciliogenesis genes as a new class of resistance to SMO inhibitors. Mechanistically, cilia-mutant tumors can either grow slowly in a “persister” state or evolve and progress rapidly in an “aggressive” state. Cancer Discov; 7(12); 1436–49. ©2017 AACR. See related commentary by Goranci-Buzhala et al., p. 1374. This article is highlighted in the In This Issue feature, p. 1355

Published

2017

22. EXTH-71. FUNCTIONAL GENOMICS IDENTIFIES EPIGENETIC REGULATORS AS NOVEL THERAPEUTIC TARGETS FOR SONIC HEDGEHOG MEDULLOBLASTOMA

Author

David E. Root, Rosalind A. Segal, Pratiti Bandopadhayay, Ghazaleh Tabatabai, Daniel Merk, Foteini Tsiami, and Federica Piccioni

Subjects

Medulloblastoma, Cancer Research, animal structures, biology, Computational biology, Brain tumor childhood, medicine.disease, Signal pathway, Hedgehog signaling pathway, Oncology, embryonic structures, biology.protein, medicine, CRISPR, Neurology (clinical), Epigenetics, Sonic hedgehog, Functional genomics

Abstract

Medulloblastoma (MB) is among the most common malignant pediatric brain tumors. Among its four molecularly heterogeneous clinical variants, sonic hedgehog (SHH) subgroup comprises 30% of all MBs and is characterized by constitutive activation of the canonical SHH signaling pathway. Although Smoothened (Smo) inhibition has emerged as a promising therapeutic target for this tumor entity, primary or acquired resistance impedes its clinical efficacy. Thus, further insight into the molecular mechanisms underlying acquired resistance to Smo inhibition are urgently needed to overcome this challenge. Here, we performed a genome-wide CRISPR/Cas9 knockout screen in a murine and a human SHH-MB cell line, SMB21 and DAOY, respectively, in order to unravel tumor-specific genetic vulnerabilities. Our data provide functional evidence that SMB21 cells highly depend on key members of the SHH pathway such as Smo and Gli1 for their survival. In contrast, none of those positive regulators of SHH signaling scored in DAOY cells, suggesting that they are not a faithful human model of this tumor subtype. Of note, functional genomics identified SMB21-context specific essentialities beyond the SHH pathway that include epigenetic regulators such as Dnmt1, Smarca5 and Smarca4. Further in vitro pharmacological validations demonstrate that Dnmt1 inhibition is efficacious in clinically relevant concentrations in SHH-associated cell lines, both sensitive and resistant to Smo inhibition, suggesting novel therapeutic avenues for SHH-MB. By employing genome-scale knockout screens in murine cell lines faithfully recapitulating the biology of human SHH-MB, we aim to decipher synthetic lethal interactors for Dnmt1 inhibitors that could potentially serve as a combinatorial treatment approach for SHH-MB. Finally, genetic ablation and pharmacological inhibition of epigenetic regulators will be evaluated in in vivo mouse models of SHH-MB. Summarizing, our data highlight the potential of inhibitors of epigenetic regulators in SHH-MB sensitive, as well as resistant to Smo inhibition.

Published

2021

23. Diversity of developing peripheral glia revealed by single-cell RNA sequencing

Author

Noah R. Druckenbrod, Rosalind A. Segal, Maria F. Pazyra-Murphy, Weixiu Dong, Ozge E. Tasdemir-Yilmaz, Austen A. Sitko, Lisa V. Goodrich, Andrea R. Yung, Olubusola Olukoya, Evan B. Hale, Peter V. Kharchenko, Alexander A. Gimelbrant, Sébastien Vigneau, and Isle Bastille

Subjects

Nervous system, Mice, Transgenic, Sensory system, Biology, Somatosensory system, Article, General Biochemistry, Genetics and Molecular Biology, Dorsal root ganglion, Gene expression, medicine, Animals, Molecular Biology, Gene, Neurons, Base Sequence, Sequence Analysis, RNA, Neural crest, Cell Differentiation, Cell Biology, medicine.anatomical_structure, nervous system, Neural Crest, Peripheral nervous system, Schwann Cells, Neuroglia, Neuroscience, Developmental Biology

Abstract

The peripheral nervous system responds to a wide variety of sensory stimuli, a process that requires great neuronal diversity. These diverse neurons are closely associated with glial cells originating from the neural crest. However, the molecular nature and diversity among peripheral glia are not understood. Here, we used single-cell RNA sequencing to profile developing and mature glia from somatosensory dorsal root ganglia and auditory spiral ganglia. We found that glial precursors (GPs) in these two systems differ in their transcriptional profiles. Despite their unique features, somatosensory and auditory GPs undergo convergent differentiation to generate molecularly uniform myelinating and non-myelinating Schwann cells. By contrast, somatosensory and auditory satellite glial cells retain system-specific features. Lastly, we identified a glial signature gene set, providing new insights into commonalities among glia across the nervous system. This survey of gene expression in peripheral glia constitutes a resource for understanding functions of glia across different sensory modalities.

Published

2021

24. EPCT-17. DEVELOPING EYA PHOSPHATASE INHIBITORS WITH ON-TARGET EFFECTS IN SHH-MEDULLOBLASTOMA

Author

Rosalind A. Segal, Grace H. Hwang, and David A. Scott

Subjects

Medulloblastoma, Cancer Research, Cerebellum, animal structures, Phosphoric monoester hydrolases, Phosphatase, Cancer, Protein tyrosine phosphatase, Biology, medicine.disease, Hedgehog signaling pathway, Translational/Early Phase Clinical Trials, nervous system diseases, stomatognathic diseases, medicine.anatomical_structure, Oncology, embryonic structures, medicine, Cancer research, AcademicSubjects/MED00300, AcademicSubjects/MED00310, Neurology (clinical), Signal transduction, neoplasms

Abstract

Medulloblastoma, one of the most frequent malignant pediatric brain tumors, encompasses four molecularly and clinically distinct cancers. Sonic hedgehog (SHH)-subtype medulloblastoma constitutes about 30% of medulloblastomas, and therapies targeting the SHH pathway can lead to new highly selective treatment. The haloacid dehalogenase (HAD) phosphatase Eyes Absent 1 (EYA1) is critically involved in the development and progression of SHH-medulloblastoma: Eya1 is highly expressed in SHH-medulloblastomas, and single cell sequencing indicates that Eya1 is a consistent feature that can be detected in every individual cancer cell. Inhibition of EYA1 interrupts SHH pathway signaling. During normal development, EYA1 promotes symmetric division of cerebellar granule cell precursors (GCPs), the cells of origin for SHH-subtype medulloblastoma, and reduced levels of EYA1 decrease medulloblastoma mortality rates in mouse models. Therefore, targeting EYA1 may be a novel therapeutic avenue for these pediatric cancers. Benzarone derivatives have been suggested as allosteric EYA-inhibitors, and benzarone provides a promising platform for chemical derivatives. Here, we develop 60 novel benzarone derivatives and assess their efficacy in inhibiting SHH-medulloblastoma growth through the inhibition of EYA1. Several of the new compounds inhibit EYA1 phosphotyrosine phosphatase activity in a cell-based assay, interrupt SHH pathway, and prevent SHH-medulloblastoma growth in vitro. Our results show that these novel benzarone derivatives are a new promising avenue for developing therapeutics for pediatric SHH-medulloblastoma via inhibition of EYA phosphatases.

Published

2021

25. An Architect of the Hindbrain: DDX3X Regulates Normal and Malignant Development

Author

Grace H. Hwang and Rosalind A. Segal

Subjects

animal structures, Tumor suppressor gene, Carcinogenesis, Hindbrain, Cell fate determination, Biology, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, DEAD-box RNA Helicases, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Cerebellar Neoplasms, neoplasms, Molecular Biology, book, 030304 developmental biology, Medulloblastoma, 0303 health sciences, Mutation, Wnt signaling pathway, Developmental cell, Cell Biology, medicine.disease, nervous system diseases, Cell biology, Rhombencephalon, stomatognathic diseases, embryonic structures, book.journal, 030217 neurology & neurosurgery, Developmental Biology

Abstract

DDX3X is frequently mutated in the WNT and SHH subtypes of medulloblastoma - the commonest malignant childhood brain tumor. But whether DDX3X functions as a medulloblastoma oncogene or tumor suppressor gene is not known. Here, we show that Ddx3x regulates hindbrain patterning and development by controlling Hox gene expression and cell stress signaling. In mice predisposed to Wnt or Shh-medulloblastoma, Ddx3x sensed oncogenic stress and suppressed tumor formation. WNT and SHH-medulloblastomas normally arise only in the lower and upper rhombic lips, respectively. Deletion of Ddx3x removed this lineage restriction, enabling both medulloblastoma subtypes to arise in either germinal zone. Thus, DDX3X is a medulloblastoma tumor suppressor that regulates hindbrain development and restricts the competence of cell lineages to form medulloblastoma subtypes.

Published

2020

26. Pathogenesis of paclitaxel-induced peripheral neuropathy: A current review of in vitro and in vivo findings using rodent and human model systems

Author

Sandra Rieger, Nathan P. Staff, Jill C. Fehrenbacher, Rosalind A. Segal, Martial Caillaud, and M. Imad Damaj

Subjects

0301 basic medicine, Cell type, Paclitaxel, medicine.medical_treatment, Rodentia, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Developmental Neuroscience, Dorsal root ganglion, In vivo, medicine, Animals, Humans, Calcium signaling, Chemotherapy, business.industry, Peripheral Nervous System Diseases, medicine.disease, Antineoplastic Agents, Phytogenic, Rats, 030104 developmental biology, Peripheral neuropathy, medicine.anatomical_structure, Neurology, chemistry, Tumor progression, Cancer research, business, 030217 neurology & neurosurgery

Abstract

Paclitaxel (Brand name Taxol) is widely used in the treatment of common cancers like breast, ovarian and lung cancer. Although highly effective in blocking tumor progression, paclitaxel also causes peripheral neuropathy as a side effect in 60-70% of chemotherapy patients. Recent efforts by numerous labs have aimed at defining the underlying mechanisms of paclitaxel-induced peripheral neuropathy (PIPN). In vitro models using rodent dorsal root ganglion neurons, human induced pluripotent stem cells, and rodent in vivo models have revealed a number of molecular pathways affected by paclitaxel within axons of sensory neurons and within other cell types, such as the immune system and peripheral glia, as well skin. These studies revealed that paclitaxel induces altered calcium signaling, neuropeptide and growth factor release, mitochondrial damage and reactive oxygen species formation, and can activate ion channels that mediate responses to extracellular cues. Recent studies also suggest a role for the matrix-metalloproteinase 13 (MMP-13) in mediating neuropathy. These diverse changes may be secondary to paclitaxel-induced microtubule transport impairment. Human genetic studies, although still limited, also highlight the involvement of cytoskeletal changes in PIPN. Newly identified molecular targets resulting from these studies could provide the basis for the development of therapies with which to either prevent or reverse paclitaxel-induced peripheral neuropathy in chemotherapy patients.

Published

2019

27. The Eya1 phosphatase mediates Shh-driven symmetric cell division of cerebellar granule cell precursors

Author

Jennifer A. Chan, Kristina J. Rehm, Pengcheng Zhou, Grace H. Hwang, Samuel M. Cohen, Rosalind A. Segal, Michael J. Eck, Kellie J. Nazemi, Xuesong Zhao, Jose Alfaro, Eun Young Park, Pin-Xian Xu, Daniel Merk, and Maria F. Pazyra-Murphy

Subjects

0303 health sciences, Cell division, biology, Chemistry, Symmetric cell division, Cell cycle, Cell fate determination, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Cell polarity, NUMB, biology.protein, Sonic hedgehog, Mitosis, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

During neural development, stem and precursor cells can divide either symmetrically or asymmetrically. The transition between symmetric and asymmetric cell divisions is a major determinant of precursor cell expansion and neural differentiation, but the underlying mechanisms that regulate this transition are not well understood. Here, we identify the Sonic hedgehog (Shh) pathway as a critical determinant regulating the mode of division of cerebellar granule cell precursors (GCPs). Using partial gain and loss of function mutations within the Shh pathway, we show that pathway activation determines spindle orientation of GCPs, and that mitotic spindle orientation directly correlates with the mode of division. Mechanistically, we show that the phosphatase Eya1 is essential for implementing Shh-dependent GCP spindle orientation. We identify atypical protein kinase C (aPKC) as a direct target of Eya1 activity and show that Eya1 dephosphorylates Threonine (T410) in the activation loop of this polarity complex component. Thus, Eya1 inactivates the cell polarity complex, resulting in reduced phosphorylation of Numb and other components that regulate the mode of division. This Eya1-dependent cascade is critical in linking spindle orientation, cell cycle exit and terminal differentiation. Together these findings demonstrate that a Shh-Eya1 regulatory axis selectively promotes symmetric cell divisions during cerebellar development by coordinating spindle orientation and cell fate determinants.Summary statementBiological responses to Shh signaling are specified by the magnitude of pathway activation and the cellular context. This study shows that potent Shh signaling regulates mitotic orientation and symmetric division of cerebellar granule cell precursors in a process that requires the phosphatase Eya1 and unequal distribution of cell fate determinants to daughter cells.

Published

2019

28. LGG-05. SINGLE CELL RNA SEQUENCING REVEALS MITOGENIC AND PROGENITOR GENE PROGRAMS IN BRAF-REARRANGED PILOCYTIC ASTROCYTOMAS

Author

Liliana Goumnerova, Zachary J. Reitman, Sarah Becker, Orit Rozenblatt-Rozen, Daphne A. Haas-Kogan, Rosalind A. Segal, Mariella G. Filbin, Claire Sinai, Zachary T. Herbert, Kenin Qian, Brenton R. Paolella, Alexandra-Larisa Condurat, Alex K. Shalek, Guillaume Bergthold, Yu Sun, Ying Huang, John F. Daley, Kristine Pelton, Robert T. Jones, Jessica Weatherbee, Rameen Beroukhim, John A. Alberta, Keith L. Ligon, Hayley Malkin, Leslie Grimmet, Pratiti Bandopadhayay, Mario L. Suvà, Charles D. Stiles, Mark W. Kieran, and Aviv Regev

Subjects

Cancer Research, Cell, Pilocytic Astrocytomas, RNA, Low Grade Glioma, Biology, medicine.anatomical_structure, Oncology, Cancer research, medicine, Neurology (clinical), Gene, neoplasms, Progenitor

Abstract

Pilocytic astrocytoma (PA) is the most common pediatric low-grade glioma. While PAs exhibit a favorable prognosis compared to higher-grade gliomas, treatment morbidity and tumor recurrence still represent major challenges for some PA patients. PAs frequently harbor rearrangements resulting in expression of oncogenic KIAA1549-BRAF fusion transcripts. We performed scRNAseq of both tumor and non-tumor cells in newly-diagnosed PAs that contained KIAA1549-BRAF rearrangements. To confidently distinguish tumor cells from nontumor cells, we sorted cells by glial progenitor marker A2B5 status and profiled KIAA1549-BRAF fusion status of cells using a quantitative PCR-based assay. Results were validated using RNA in situ hybridization and compared to bulk expression data from 151 pediatric low grade gliomas. When compared to higher-grade gliomas, a higher proportion of the PA tumor cells exhibited a differentiated, astrocyte-like phenotype. A smaller proportion of cells exhibited a progenitor-like phenotype with evidence of proliferation. These progenitor-like tumor cells expressed a mitogen-activated protein kinase (MAPK) gene program that was absent from higher-grade gliomas. Similar patterns of expression of genes associated with the astrocyte-like and MAPK gene programs were also seen in formalin fixed, paraffin embedded PA tissues using RNA in situ hybridization. Immune cells, especially microglia, comprised almost half of all cells in the PAs and accounted for many differences seen in bulk pediatric low grade glioma expression profiles. These single cell transcriptional data reveal a transcriptional developmental hierarchy in a pediatric low-grade glioma that is skewed towards more mature brain cells compared to higher-grade gliomas. The results indicate that future analyses of bulk PA tissues should attempt to account for considerable infiltration by nontumor cells. Finally, the finding that a MAPK gene program is not uniformly expressed in PA tumor cells has implications for ongoing clinical investigations of therapies directed at the MAPK pathway for the treatment of PA.

Published

2019

29. The National Cancer Institute Clinical Trials Planning Meeting for Prevention and Treatment of Chemotherapy-Induced Peripheral Neuropathy

Author

Ann M. O'Mara, Michelle C. Janelsins, Ellen M. Lavoie Smith, Judith O. Hopkins, Andrea G. Hohmann, Rosalind A. Segal, Judith A. Paice, Ahmet Hoke, Ian R. Kleckner, Debra L. Barton, Guido Cavaletti, Suzanne C. Danhauer, Karen M. Mustian, Daniela Salvemini, Worta Mc Caskill Stevens, Diane St. Germain, Charles L. Loprinzi, Dawn L. Hershman, Howard L. McLeod, Katherine Patterson Kelly, Julia H. Rowland, Supriya G. Mohile, and Susan G. Dorsey

Subjects

Cancer Research, medicine.medical_specialty, business.industry, Psychological intervention, MEDLINE, Cancer, medicine.disease, law.invention, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Quality of life (healthcare), Oncology, Randomized controlled trial, Chemotherapy-induced peripheral neuropathy, law, 030220 oncology & carcinogenesis, medicine, Commentary, Working group, Intensive care medicine, business, 030217 neurology & neurosurgery

Abstract

Although recent scientific advances have improved our understanding of basic biological mechanisms underlying chemotherapy-induced peripheral neuropathy (CIPN), few interventions are available to prevent or treat CIPN. Although some biological targets from preclinical studies show promise in nonhuman animal models, few targets have been translated to successful clinical trials. To address this problem, the National Cancer Institute’s Symptom Management and Health-Related Quality of Life Steering Committee convened a meeting of experts in the CIPN and oncology symptom management fields to participate in a Clinical Trials Planning Meeting (CTPM). Investigators presented data from preclinical and translational studies for possible CIPN interventions; these were evaluated for readiness of randomized clinical trial testing by experts, and recommendations were provided. Breakout sessions were convened to discuss and develop future studies. The CTPM experts concluded that there is compelling evidence to move forward with selected pharmacological and nonpharmacological clinical trials for the prevention and treatment of CIPN. Several key feasibility issues need to be addressed, however. These include identification of optimal outcome measures to define the CIPN phenotype, establishment of parameters that guide the evaluation of clinically meaningful effects, and adoption of approaches for inclusion of translational and biomarker and/or genetic measures. The results of the CTPM provide support for conducting clinical trials that include both pharmacological and nonpharmacological approaches, alone or in combination, with biomarkers, genetics, or other measures designed to inform underlying CIPN mechanisms. Several working groups were formed to design rigorous CIPN clinical trials, the results of which are ongoing.

Published

2019

30. Hedgehog Signal Transduction: Key Players, Oncogenic Drivers, and Cancer Therapy

Author

Rosalind A. Segal and Ekaterina Pak

Subjects

0301 basic medicine, Hh signaling, Cancer therapy, Tumor initiation, Biology, Bioinformatics, Article, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, Transduction (genetics), Animals, Humans, Hedgehog Proteins, Molecular Biology, Hedgehog, Extramural, Cell Biology, Cell biology, Cell Transformation, Neoplastic, 030104 developmental biology, Carcinoma, Basal Cell, Signal transduction, Pathway activity, Medulloblastoma, Signal Transduction, Transcription Factors, Developmental Biology

Abstract

The Hedgehog (Hh) signaling pathway governs complex developmental processes, including proliferation and patterning within diverse tissues. These activities rely on a tightly regulated transduction system that converts graded Hh input signals into specific levels of pathway activity. Uncontrolled activation of Hh signaling drives tumor initiation and maintenance. However, recent entry of pathway-specific inhibitors into the clinic reveals mixed patient responses and thus prompts further exploration of pathway activation and inhibition. In this review, we share emerging insights into regulated and oncogenic Hh signaling, supplemented with updates on the development and use of Hh pathway-targeted therapies.

Published

2016

31. Tyrosine receptor kinase B is a drug target in astrocytomas

Author

Jing Ni, Rosalind A. Segal, Victor Luu, Charles D. Stiles, Pratiti Bandopadhayay, Rameen Beroukhim, Jean J. Zhao, William C. Hahn, Shakti Ramkissoon, Yu Sun, Keith L. Ligon, Shaozhen Xie, and Thomas M. Roberts

Subjects

0301 basic medicine, Cancer Research, biology, Astrocytoma, Tropomyosin receptor kinase B, Tropomyosin receptor kinase A, medicine.disease, Molecular biology, Tropomyosin receptor kinase C, Receptor tyrosine kinase, nervous system diseases, 03 medical and health sciences, 030104 developmental biology, nervous system, Oncology, Trk receptor, embryonic structures, ROR1, biology.protein, medicine, Neurology (clinical), neoplasms, Platelet-derived growth factor receptor

Abstract

Background. Astrocytomas are the most common primary human brain tumors. Receptor tyrosine kinases (RTKs), including tyrosine receptor kinase B (TrkB, also known as tropomyosin-related kinase B; encoded by neurotrophic tyrosine kinase receptor type 2 [NTRK2]), are frequently mutated by rearrangement/fusion in high-grade and low-grade astrocytomas. We found that activated TrkB can contribute to the development of astrocytoma and might serve as a therapeutic target in this tumor type. Methods. To identify RTKs capable of inducing astrocytoma formation, a library of human tyrosine kinases was screened for the ability to transform murine Ink4a−/−/Arf−/− astrocytes. Orthotopic allograft studies were conducted to evaluate the effects of RTKs on the development of astrocytoma. Since TrkB was identified as a driver of astrocytoma formation, the effect of the Trk inhibitors AZD1480 and RXDX-101 was assessed in astrocytoma cells expressing activated TrkB. RNA sequencing, real-time PCR, western blotting, and enzyme-linked immunosorbent assays were conducted to characterize NTRK2 in astrocytomas. Results. Activated TrkB cooperated with Ink4a/Arf loss to induce the formation of astrocytomas through a mechanism mediated by activation of signal transducer and activator of transcription 3 (STAT3). TrkB activation positively correlated with Ccl2 expression. TrkB-induced astrocytomas remained dependent on TrkB signaling for survival, highlighting a role of NTRK2 as an addictive oncogene. Furthermore, the QKI-NTRK2 fusion associated with human astrocytoma transformed Ink4a−/−/Arf−/− astrocytes, and this process was also mediated via STAT3 signaling. Conclusions. Our findings provide evidence that constitutively activated NTRK2 alleles, notably the human tumor-associated QKI-NTRK2 fusion, can cooperate with Ink4a/Arf loss to drive astrocytoma formation. Therefore, we propose NTRK2 as a potential therapeutic target in the subset of astrocytoma patients defined by QKI-NTRK2 fusion.

Published

2016

32. The RNA-binding protein SFPQ orchestrates an RNA regulon to promote axon viability

Author

Hunter L. Elliott, Sara J. Fenstermacher, Maria F. Pazyra-Murphy, Rosalind A. Segal, and Katharina E. Cosker

Subjects

0301 basic medicine, Sensory Receptor Cells, Cell Survival, RNA-binding protein, Biology, Axonal Transport, Regulon, Article, Mice, 03 medical and health sciences, Splicing factor, Ganglia, Spinal, Gene expression, medicine, Gene Knockdown Techniques, Animals, Axon, PTB-Associated Splicing Factor, Mice, Knockout, Lamin Type B, General Neuroscience, Proteins, RNA, Translation (biology), Axons, 030104 developmental biology, medicine.anatomical_structure, nervous system, Apoptosis Regulatory Proteins, Neuroscience

Abstract

To achieve accurate spatiotemporal patterns of gene expression, RNA-binding proteins (RBPs) guide nuclear processing, intracellular trafficking, and local translation of target mRNAs. In neurons, RBPs direct transport of target mRNAs to sites of translation in remote axons and dendrites. However, it is not known whether an individual RBP coordinately regulates multiple mRNAs within these morphologically complex cells. Here we identify SFPQ (Splicing factor, proline-glutamine rich) as an RBP that binds and regulates multiple mRNAs in dorsal root ganglion (DRG) sensory neurons and thereby promotes neurotrophin-dependent axonal viability. SFPQ acts within nuclei, cytoplasm and axons to regulate multiple functionally related mRNAs essential for axon survival. Notably SFPQ is required for co-assembly of laminb2 and bclw within RNA granules and for axonal trafficking of these mRNAs. Together these data demonstrate that SFPQ orchestrates spatial gene expression of a newly identified RNA regulon essential for axonal viability.

Published

2016

33. Sonic Hedgehog Signaling is Blue: Insights from the Patched Mutant Mice

Author

Rosalind A. Segal and Daniel Merk

Subjects

0301 basic medicine, Medulloblastoma, Patched, General Neuroscience, Neurogenesis, Mutant, Biology, medicine.disease, Hedgehog signaling pathway, Cell biology, Patched-1 Receptor, 03 medical and health sciences, Mice, 030104 developmental biology, Genetically Engineered Mouse, Mutation, medicine, Animals, Hedgehog Proteins, Receptor, Hedgehog, Gene

Abstract

The Hedgehog (Hh) pathway is a highly conserved signaling system regulating a range of developmental processes. A 1997 paper by Goodrich and colleagues provided major contributions to understanding the Hh pathway by mutating the gene encoding the Hh receptor, Patched, and thereby developing a mouse model for a human cancer predisposition syndrome, known as Gorlin syndrome. These studies provided one of the first genetically engineered mouse models for brain tumors.

Published

2018

34. A transatlantic cooperation for enriched neuroscience training

Author

Menno P. Witter, Elisabeth J. Van Bockstaele, Rosalind A. Segal, and Domna Karagogeos

Subjects

Cognitive science, Europe, Societies, Scientific, General Neuroscience, International Cooperation, North America, Neurosciences, Humans, Psychology, Training (civil), Intersectoral Collaboration

Published

2018

35. PCLN-07. A 3D HYDROGEL CULTURE SYSTEM FACILITATES STUDY OF PRIMARY PEDIATRIC LOW-GRADE GLIOMA CELLS IN VITRO

Author

Liliana Goumnerova, Karen Wright, Christopher Rota, Mark W. Kieran, Linda Stockdale, Emily C. Chadwick, Rosalind A. Segal, Alexander Brown, Keith L. Ligon, Douglas A. Lauffenburger, and Linda G. Griffith

Subjects

Cancer Research, Abstracts, Primary (chemistry), Text mining, Oncology, business.industry, Cancer research, Medicine, Low-Grade Glioma, Neurology (clinical), business, In vitro

Abstract

Gliomas are the most common solid tumor of childhood and while children with low grade gliomas (LGGs) are likely to survive their disease, their course is complicated by significant treatment-related neurocognitive and endocrinological sequelae. Few accurate preclinical LGG models exist, thereby limiting development and testing of novel targeted agents. We developed a 3D, hydrogel-based co-culture system utilizing mouse astrocytes to support growth of primary human pediatric LGG cells in vitro. This tunable hydrogel system recapitulates many features of brain extracellular matrix, while the co-cultured astrocytes provide growth factors and other components normally present in vivo. In this system, patients’ tumor cells are dissociated, and functionalized polyethylene glycol-based hydrogels are produced to surround tumor cells. These tumor-containing hydrogels are then placed adjacent to adherent layers of primary mouse astrocytes and the co-cultures grown for an extended period of time. Using this system, multiple types of human LGG cells and other pediatric tumor cells can be successfully cultured in hydrogels for up to one month. Moreover, these hydrogels can be enzymatically dissolved, releasing tumor cells to passage into new gels. Fluorescent 5-ethynyl-2’-deoxyuridine labeling followed by confocal microscopy of co-cultures reveals viable, proliferating cell clusters even one month later. While high grade gliomas in this setting proliferate rapidly, cultured LGG cells proliferate slowly, much like their original tumor counterparts. These methods can be used to provide patient-specific avatars to identify the best personalized targeted therapies. Moreover, the system enables investigations of the brain tumor microenvironment as a modulator of tumor growth.

Published

2018

36. The Eya1 Phosphatase Promotes Shh Signaling during Hindbrain Development and Oncogenesis

Author

Matthew P. Scott, Xuesong Zhao, Emily C. Chadwick, Pengcheng Zhou, Adriana Eisner, R. Tyler Hillman, Maria F. Pazyra-Murphy, Ershela Durresi, Pin-Xian Xu, Rosalind A. Segal, and Michael E. Greenberg

Subjects

Patched Receptors, Chromatin Immunoprecipitation, animal structures, Carcinogenesis, Blotting, Western, Kruppel-Like Transcription Factors, Regulator, Receptors, Cell Surface, Hindbrain, Protein tyrosine phosphatase, Real-Time Polymerase Chain Reaction, Zinc Finger Protein GLI1, Article, General Biochemistry, Genetics and Molecular Biology, Immunoenzyme Techniques, Small hairpin RNA, Mice, Biomarkers, Tumor, Animals, Humans, Immunoprecipitation, Hedgehog Proteins, RNA, Messenger, RNA, Small Interfering, Sonic hedgehog, Nuclear protein, Molecular Biology, Cells, Cultured, Oligonucleotide Array Sequence Analysis, Homeodomain Proteins, Mice, Knockout, biology, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Cell Biology, Rhombencephalon, Mutation, embryonic structures, Cancer research, biology.protein, Protein Tyrosine Phosphatases, Signal transduction, Medulloblastoma, Signal Transduction, Developmental Biology

Abstract

SummarySonic hedgehog (Shh) signaling is critical in development and oncogenesis, but the mechanisms regulating this pathway remain unclear. Although protein phosphorylation clearly affects Shh signaling, little is known about phosphatases governing the pathway. Here, we conducted a small hairpin RNA (shRNA) screen of the phosphatome and identified Eya1 as a positive regulator of Shh signaling. We find that the catalytically active phosphatase Eya1 cooperates with the DNA-binding protein Six1 to promote gene induction in response to Shh and that Eya1/Six1 together regulate Gli transcriptional activators. We show that Eya1, which is mutated in a human deafness disorder, branchio-oto-renal syndrome, is critical for Shh-dependent hindbrain growth and development. Moreover, Eya1 drives the growth of medulloblastoma, a Shh-dependent hindbrain tumor. Together, these results identify Eya1 and Six1 as key components of the Shh transcriptional network in normal development and in oncogenesis.

Published

2015

37. DIPG-29. GENOMIC LANDSCAPE OF DIFFUSE INTRINSIC PONTINE GLIOMA: AN ANALYSIS OF THE DIPG-BATS COHORT

Author

D.A. Haas-Kogan, Nathan Robison, Arthur J DiPatri, Sabine Mueller, Matija Snuderl, Maneka Puligandla, Jason Fangusaro, Eric Sandler, Sridharan Gururangan, Lianne Greenspan, Nada Jabado, Rosalind A. Segal, Joshua B. Rubin, Oren J. Becher, David D. Limbrick, Paul G. Fisher, Kristen Lawler, Peter E. Manley, Patricia Ho, Bradley E. Weprin, Matthias A. Karajannis, Zhihong Joanne Wang, Melanie Comito, Kellie J. Nazemi, Stewart Goldman, Erin N. Kiehna, Ziab Khatib, Dolly Aguilera, Herbert E. Fuchs, Noah F. Greenwald, Liliana Goumnerova, Kaynalakshmi Ayyanar, Daniel C. Bowers, Mark D. Krieger, Karen J. Marcus, Hayley Malkin, Adam Tracy, Sandeep Sood, Michael H. Handler, Ofer Sharpira, Philipp Aldana, Jeffrey R. Leonard, Sharon Gardner, Mark S. Dias, Samuel R. Browd, Mario L. Suvà, David H. Harter, Lissa C. Baird, Mark W. Kieran, Russ Geyer, Susan N. Chi, Jennifer D. Elster, Tadanori Tomita, Michael D. Prados, Amy-Lee Bredlau, Karen Gauvain, Jeremiah Wala, Karen Wright, Ryan O’Rourke, Sarah Leary, Anne Bendel, Kenneth J. Cohen, Nalin Gupta, Pratiti Bandopadhayay, William Gump, Tobey J. McDonald, Claire Sinai, Kristine Pelton, Mariella G. Filbin, Jeffrey C. Murray, Barun Brahma, Tord D. Alden, Donna Neuberg, Anu Banerjee, Mahmoud Nagib, John Ragheb, Sanjiv Bhatia, Rameen Beroukhim, Keith L. Ligon, and Michelle Monje

Subjects

0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Biology, 03 medical and health sciences, Abstracts, 030104 developmental biology, 0302 clinical medicine, Oncology, PIK3CA gene, 030220 oncology & carcinogenesis, Cohort, medicine, Neurology (clinical), Protein p53

Abstract

INTRODUCTION: Diffuse intrinsic pontine glioma (DIPG) remains a devastating and incurable disease. The DIPG-BATs clinical trial incorporates diagnostic biopsy with molecularly determined treatment stratification. Here we present the initial genomic analysis of the DIPG-BATs cohort. METHODS: Children enrolled on the DIPG-BATs clinical trial underwent upfront diagnostic biopsies prior to commencement of therapy. RNA and DNA were extracted from single core biopsies and subjected to whole-genome sequencing (WGS) and RNA-sequencing. Tumor samples were also collected at autopsy if there was parental consent. RESULTS: Fifty-three patients were enrolled on study, of whom 50 underwent biopsy. There were no biopsy-related deaths. A mean of 5ug of RNA and 10ug of DNA were extracted from single frozen cores. WGS on 41 DIPG samples (including eight autopsy samples) revealed a mean mutation rate of 0.753 mutations per Mb. We confirmed TP53, PIK3CA, H3F3A, ACVR1, PPM1D, and HIST1H3B to be recurrently mutated in DIPG. Additional mutations were found in epigenetic modifiers including ASXL1. Copy-number analysis revealed PDGFRA to meet statistical significance as a recurrent amplification peak in DIPG (q

Published

2017

38. A brain-penetrant RAF dimer antagonist for the noncanonical BRAF oncoprotein of pediatric low-grade astrocytomas

Author

Nathalie Y. R. Agar, Neal Rosen, Emily J. Chadwick, Nathanael S. Gray, David Calligaris, Liliana Goumnerova, Keith L. Ligon, Levi A. Garraway, Mark W. Kieran, Catherine Pilarz, Lori A. Ramkissoon, Shakti Ramkissoon, John A. Alberta, Charles D. Stiles, Rosalind A. Segal, Veronica Matia Garcia, Zhan Yao, Emanuele Mazzola, William C. Hahn, Sara J. Buhrlage, Yu Sun, and Michael F. Kane

Subjects

0301 basic medicine, Proto-Oncogene Proteins B-raf, Cancer Research, Oncogene Proteins, Mutant, Astrocytoma, 03 medical and health sciences, chemistry.chemical_compound, medicine, Humans, Child, neoplasms, Kinase, Melanoma, Antagonist, Brain, Glioma, medicine.disease, Small molecule, Penetrance, digestive system diseases, PLGA, 030104 developmental biology, Oncology, chemistry, Basic and Translational Investigations, Cancer research, Neurology (clinical)

Abstract

Background Activating mutations or structural rearrangements in BRAF are identified in roughly 75% of all pediatric low-grade astrocytomas (PLGAs). However, first-generation RAF inhibitors approved for adult melanoma have poor blood-brain penetrance and are only effective on tumors that express the canonical BRAFV600E oncoprotein, which functions as a monomer. These drugs (type I antagonists that target the "DFG-in" conformation of the kinase) fail to block signaling via KIAA1549:BRAF, a truncation/fusion BRAF oncoprotein which functions as a dimer and is found in the most common form of PLGA. Methods A panel of small molecule RAF inhibitors (including type II inhibitors, targeting the "DFG-out" conformation of the kinase) was screened for drugs showing efficacy on murine models of PLGA and on authentic human PLGA cells expressing KIAA1549:BRAF. Results We identify a type II RAF inhibitor that serves as an equipotent antagonist of BRAFV600E, KIAA1549:BRAF, and other noncanonical BRAF oncoproteins that function as dimers. This drug (MLN2480, also known as TAK-580) has good brain penetrance and is active on authentic human PLGA cells in brain organotypic cultures. Conclusion MLN2480 may be an effective therapeutic for BRAF mutant pediatric astrocytomas.

Published

2017

39. Shh-proteoglycan interactions regulate maturation of olfactory glomerular circuitry

Author

Sandeep Robert Datta, Adriana Eisner, Laura Persson, Paul L. Greer, Rosalind A. Segal, Maria F. Pazyra-Murphy, Rochelle M. Witt, and Meghan M. Galligan

Subjects

Olfactory system, Olfactory receptor, biology, Neurogenesis, Subventricular zone, Sensory system, Olfactory bulb, Cellular and Molecular Neuroscience, medicine.anatomical_structure, Developmental Neuroscience, medicine, biology.protein, Olfactory ensheathing glia, Olfactory marker protein, Neuroscience

Abstract

The olfactory system relies on precise circuitry connecting olfactory sensory neurons (OSNs) and appropriate relay and processing neurons of the olfactory bulb (OB). In mammals, the exact correspon- dence between specific olfactory receptor types and indi- vidual glomeruli enables a spatially precise map of glomerular activation that corresponds to distinct odors. However, the mechanisms that govern the establishment and maintenance of the glomerular circuitry are largely unknown. Here we show that high levels of Sonic Hedge- hog (Shh) signaling at multiple sites enable refinement and maintenance of olfactory glomerular circuitry. Mice expressing a mutant version of Shh (Shh Ala/Ala ), with impaired binding to proteoglycan co-receptors, exhibit disproportionately small olfactory bulbs containing fewer glomeruli. Notably, in mutant animals the correspon- dence between individual glomeruli and specific olfactory receptors is lost, as olfactory sensory neurons expressing different olfactory receptors converge on the same glo- meruli. These deficits arise at late stages in post-natal development and continue into adulthood, indicating impaired pruning of erroneous connections within the olfactory bulb. In addition, mature Shh Ala/Ala mice exhibit decreased proliferation in the subventricular zone (SVZ), with particular reduction in neurogenesis of calbindin-expressing periglomerular cells. Thus, Shh interactions with proteoglycan co-receptors function at multiple locations to regulate neurogenesis and precise olfactory connectivity, thereby promoting functional neu- ronal circuitry. V C 2014 Wiley Periodicals, Inc. Develop Neurobiol 00: 000-000, 2014

Published

2014

40. Paclitaxel Reduces Axonal Bclw to Initiate IP

Author

Sarah E, Pease-Raissi, Maria F, Pazyra-Murphy, Yihang, Li, Franziska, Wachter, Yusuke, Fukuda, Sara J, Fenstermacher, Lauren A, Barclay, Gregory H, Bird, Loren D, Walensky, and Rosalind A, Segal

Subjects

Male, Mice, Knockout, Paclitaxel, Antineoplastic Agents, Phytogenic, Axons, Article, Rats, Mice, Inbred C57BL, Rats, Sprague-Dawley, Mice, Proto-Oncogene Proteins c-bcl-2, Ganglia, Spinal, Nerve Degeneration, Animals, Inositol 1,4,5-Trisphosphate Receptors, Female, Amino Acid Sequence, Cells, Cultured

Abstract

Chemotherapy induced peripheral neuropathy (CIPN) is a debilitating side effect of many cancer treatments. The hallmark of CIPN is degeneration of long axons required for transmission of sensory information; axonal degeneration causes impaired tactile sensation and persistent pain. Currently the molecular mechanisms of CIPN are not understood, and there are no available treatments. Here we show that the chemotherapeutic agent paclitaxel triggers CIPN by altering IP3 receptor phosphorylation and intracellular calcium flux, and activating calcium-dependent calpain proteases. Concomitantly paclitaxel impairs axonal trafficking of RNA-granules and reduces synthesis of Bclw (bcl2l2), a Bcl2 family member that binds IP3R1 and restrains axon degeneration. Surprisingly, Bclw or a stapled peptide corresponding to the Bclw BH4 domain interact with axonal IP3R1 and prevent paclitaxel-induced degeneration, while Bcl2 and BclxL cannot do so. Together these data identify a Bclw-IP3R1-dependent cascade that causes axon degeneration, and suggest Bclw-mimetics could provide effective therapy to prevent CIPN.

Published

2016

41. Abstract 3647: Single cell RNA sequencing reveals mitogenic and progenitor gene programs inBRAF-rearranged pilocytic astrocytomas

Author

Robert T. Jones, Liliana Goumnerova, Mariella G. Filbin, Zachary T. Herbert, Ying Huang, Mark W. Kieran, Alex K. Shalek, Orit Rozenblatt-Rosen, Kristine Pelton, Zachary J. Reitman, Sarah Becker, Rameen Beroukhim, Rosalind A. Segal, Guillaume Bergthold, Brenton R. Paolella, John A. Alberta, Jessica Weatherbee, John F. Daley, Pratiti Bandopadhayay, Yu Sun, Mario L. Suvà, Leslie Grimmett, Keith L. Ligon, Haley Malkin, Charles D. Stiles, Daphne A. Haas-Kogan, Claire Sinai, and Aviv Regev

Subjects

Cancer Research, Pilocytic astrocytoma, Microglia, Cell, RNA, In situ hybridization, Biology, medicine.disease, Phenotype, medicine.anatomical_structure, Oncology, Glioma, Cancer research, medicine, Gene

Abstract

Single-cell RNA sequencing (scRNAseq) has been performed across a range of intermediate to high-grade gliomas that each harbor multiple driver mutations. Pilocytic astrocytoma (PA), the most common childhood brain tumor, is a low-grade glioma. PAs frequently harbor oncogenic KIAA1549-BRAF fusions, and exhibit low rates of other driver mutations. While PAs exhibit a favorable prognosis compared to the higher-grade gliomas, treatment morbidity and tumor recurrence can represent major challenges for some PA patients. We performed scRNAseq of both tumor and non-tumor cells in newly-diagnosed PAs that contained KIAA1549-BRAF rearrangements. To confidently distinguish tumor cells from nontumor cells, we sorted cells by glial progenitor marker A2B5 status and profiled KIAA1549-BRAF fusion status of cells using a sensitive quantitative PCR-based assay. Results were validated using RNA in situ hybridization. When compared to higher-grade gliomas, a higher proportion of the PA tumor cells exhibited a differentiated, astrocyte-like phenotype. A smaller proportion of cells exhibited a progenitor-like phenotype with evidence of proliferation. These progenitor-like tumor cells expressed a mitogen-activated protein kinase (MAPK) program that was absent from higher-grade gliomas. Similar patterns of expression of genes associated with the astrocyte-like and MAPK gene programs were also seen in formalin fixed, paraffin embedded PA tissues using RNA in situ hybridization. Immune cells, especially microglia, comprised almost half of all cells in the PAs and accounted for differences in bulk expression profiles between tumor locations and subtypes. These single cell transcriptional data reveal a transcriptional developmental hierarchy in a pediatric low grade glioma that is skewed towards more mature brain cells compared to higher-grade gliomas. The results indicate that future analyses of bulk PA tissues should attempt to account for considerable infiltration by nontumor cells. Finally, the finding that a MAPK gene program is not uniformly expressed in PA tumor cells has implications for ongoing clinical investigations of therapies directed at the MAPK pathway for the treatment of PA. Citation Format: Zachary J. Reitman, Brenton Paolella, Guillaume Bergthold, Kristine Pelton, Robert Jones, Sarah Becker, Claire E. Sinai, Haley Malkin, Ying Huang, Leslie Grimmett, Zachary T. Herbert, Yu Sun, Jessica Weatherbee, John Alberta, John Daley, Orit Rozenblatt-Rosen, Rosalind Segal, Daphne Haas-Kogan, Mariella G. Filbin, Mario L. Suva, Aviv Regev, Charles Stiles, Mark W. Kieran, Liliana Goumnerova, Keith L. Ligon, Alex K. Shalek, Pratiti Bandopadhayay, Rameen Beroukhim. Single cell RNA sequencing reveals mitogenic and progenitor gene programs inBRAF-rearranged pilocytic astrocytomas [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 3647.

Published

2019

42. Target-Derived Neurotrophins Coordinate Transcription and Transport of Bclw to Prevent Axonal Degeneration

Author

Maria F. Pazyra-Murphy, Rosalind A. Segal, Sara J. Fenstermacher, and Katharina E. Cosker

Subjects

Male, Sensory Receptor Cells, Transcription, Genetic, bcl-X Protein, Apoptosis, Stimulation, Caspase 6, Biology, Axonal Transport, Mice, Pregnancy, Transcription (biology), Ganglia, Spinal, medicine, Animals, Humans, Nerve Growth Factors, RNA, Messenger, Axon, Cells, Cultured, General Neuroscience, Proteins, Articles, Axons, Rats, Cell biology, Nerve growth factor, medicine.anatomical_structure, nervous system, Nerve Degeneration, Axoplasmic transport, Retrograde signaling, biology.protein, Female, Apoptosis Regulatory Proteins, Neuroscience, Neurotrophin

Abstract

Establishment of neuronal circuitry depends on both formation and refinement of neural connections. During this process, target-derived neurotrophins regulate both transcription and translation to enable selective axon survival or elimination. However, it is not known whether retrograde signaling pathways that control transcription are coordinated with neurotrophin-regulated actions that transpire in the axon. Here we report that target-derived neurotrophins coordinate transcription of the antiapoptotic genebclwwith transport ofbclwmRNA to the axon, and thereby prevent axonal degeneration in rat and mouse sensory neurons. We show that neurotrophin stimulation of nerve terminals elicits newbclwtranscripts that are immediately transported to the axons and translated into protein. Bclw interacts with Bax and suppresses the caspase6 apoptotic cascade that fosters axonal degeneration. The scope ofbclwregulation at the levels of transcription, transport, and translation provides a mechanism whereby sustained neurotrophin stimulation can be integrated over time, so that axonal survival is restricted to neurons connected within a stable circuit.

Published

2013

43. Can the referring surgeon enhance accrual of breast cancer patients to medical and radiation oncology trials? The ENHANCE study

Author

Mark Clemons, Stan Z. Gertler, Xinni Song, Angel Arnaout, Femina Kanji, Nathaniel Bouganim, Rosalind A. Segal, Susan Dent, Iryna Kuchuk, Gregory R. Pond, and S. Verma

Subjects

medicine.medical_specialty, Accrual, business.industry, accrual strategies, Short Communication, General surgery, digestive, oral, and skin physiology, Psychological intervention, Newly diagnosed, medicine.disease, Clinical trial, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Primary outcome, Clinical trials, 030220 oncology & carcinogenesis, Radiation oncology, medicine, Physical therapy, 030212 general & internal medicine, business

Abstract

The accrual rate to clinical trials in oncology remains low. In this exploratory pilot study, we prospectively assessed the role that engaging a referring surgeon plays in enhancing nonsurgical oncologic clinical trial accrual. Newly diagnosed breast cancer patients were seen by a surgeon who actively introduced specific patient-and physician-centred strategies to increase clinical trial accrual. Patient-centred strategies included providing patients, before their oncology appointment, with information about specific clinical trials for which they might be eligible, as evaluated by the surgeon. The attitudes of the patients about clinical trials and the interventions used to improve accrual were assessed at the end of the study. The primary outcome was the clinical trial accrual rate during the study period. Overall clinical trial enrolment during the study period among the 34 participating patients was 15% (5 of 34), which is greater than the institution&rsquo, s historical average of 7%. All patients found the information delivered by the surgeon before the oncology appointment to be very helpful. Almost three quarters of the patients (73%) were informed about clinical trials by their oncologist. The top reasons for nonparticipation reported by the patients who did not participate in clinical trials included lack of interest (35%), failure of the oncologist to mention clinical trials (33%), and inconvenience (19%). Accrual of patients to clinical trials is a complex multistep process with multiple potential barriers. The findings of this exploratory pilot study demonstrate a potential role for the referring surgeon in enhancing nonsurgical clinical trial accrual.

Published

2016

44. LG-47TYPE II RAF INHIBITORS INHIBIT BRAF MUTATIONS AND TRUNCATED FUSIONS IN PEDIATRIC LOW-GRADE GLIOMAS

Author

Liliana Goumnerova, Charles D. Stiles, Peter E. Manley, Karen Wright, Yu Sun, Shakti Ramkissoon, Michael F. Kane, David Calligaris, Mark W. Kieran, Veronica Matia Garcia, Susan N. Chi, Nathanael S. Gray, Sara J. Buhrlage, Catherine Pilarz, Pratiti Bandopadhayay, Rosalind A. Segal, Michael J. Eck, Lori A. Ramkissoon, Emily J. Chadwick, Nathalie Y. R. Agar, Rameen Beroukhim, John A. Alberta, Keith L. Ligon, Levi A. Garraway, Kim Wilkinson, and Geoffrey Kannan

Subjects

Cancer Research, Mutation, Kinase, business.industry, Melanoma, Point mutation, Wild type, medicine.disease, medicine.disease_cause, Molecular biology, Abstracts, Oncology, Tumor progression, medicine, Cancer research, Neurology (clinical), business, Ex vivo, V600E

Abstract

LG-47. TYPE II RAF INHIBITORS INHIBIT BRAF MUTATIONS AND TRUNCATED FUSIONS IN PEDIATRIC LOW-GRADE GLIOMAS Mark W. Kieran1,2, Yu Sun1, Catherine Pilarz1, David Calligaris3, Emily J. Chadwick1, John A. Alberta1, Shakti H. Ramkissoon1,2, Lori A. Ramkissoon1, Veronica Matia Garcia1, Kim Wilkinson1, Michael Kane1, Liliana Goumnerova1,2, Susan N. Chi1,2, Peter Manley1,2, Karen D. Wright1,2, Nathalie Y. Agar1,3, Keith L. Ligon1,3, Rameen Beroukhim1,3, Pratiti Bandopadhayay1,2, Geoffrey Kannan1,2, Rosalind A. Segal1, Levi A. Garraway1, Nathanael S. Gray1, Michael Eck1, Charles D. Stiles1, and Sara J. Buhrlage1; Dana-Farber/Harvard Cancer Center, Boston, MA, USA; Boston Children’s Hospital/Harvard Medical School, Boston, MA, USA; BrighamandWomen’sHospital/HarvardMedical School,Boston,MA,USA PURPOSE: Abnormal signaling of the ras/raf pathway predominates in pediatric low-grade gliomas (PLGGs). Most (75%) non-NF1 low-grade gliomas have Ras-independent BRAF activation, either due to KIAA1549:BRAF truncated fusion duplication or V600E point mutation. While the latter BRAF oncoprotein functions as a monomer, the truncated fusion form requires dimerization. Type I BRAF V600E inhibitors approved for melanoma effectively abrogate monomeric signaling by targeting the “DFG-in” kinase conformation but paradoxically activate wild type RAF dimers. We therefore evaluated Type II RAF inhibitor activity (targeting the “DFG-out” kinase conformation). METHODS: We developed multiple pathway relevant model systems for different BRAF point mutations and KIAA1549 variants using neural progenitor cells from mouse embryos for in vitro, in vivo and mass spectrometry analysis. Additionally, we developed an organoid ex vivo avatar assay from direct patient samples to identify drugs inhibiting these targets. We subsequently treated a single patient with one of two identified compounds. RESULTS: Two different type II BRAF inhibitors capable of inhibiting downstream activation of pERK and tumor progression in vivo for multiple point mutations and BRAF truncated fusion forms were identified. One compound was active on authentic human PLGA cells ex vivo and showed excellent CNS penetration. CONCLUSIONS: Type II BRAF inhibitors possess a unique mechanism of action targeting the BRAF/MEK complex and inhibiting both BRAF point mutations and common structural abnormalities (KIAA1549) in PLGGs. These results have led to the development of a phase I/0/II trial. Neuro-Oncology 18:iii78–iii96, 2016. doi:10.1093/neuonc/now075.47 #The Author(s) 2016. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.

Published

2016

45. There and back again: coordinated transcription, translation and transport in axonal survival and regeneration

Author

Ozge E. Tasdemir-Yilmaz and Rosalind A. Segal

Subjects

0301 basic medicine, Neurons, General Neuroscience, Stimulation, Dendrites, Biology, Axonal Transport, Axons, Article, Nerve Regeneration, Protein content, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, nervous system, Transcription (biology), Axoplasmic transport, biology.protein, medicine, Sensory cue, Neuroscience, Nucleus, Intracellular, Neurotrophin

Abstract

Neurons are highly polarized cells with axonal and dendritic projections that extend over long distances. Target-derived neurotrophins provide local axonal cues that function in developing neurons, while physical or chemical injuries to long axons initiate local environmental cues in mature neurons. In both instances initial responses at the location of stimulation or injury must be coordinated with changes in the transcriptional program and subsequent changes in axonal protein content. To achieve this coordination, intracellular signals move 'there and back again' between axons and the nucleus. Here, we review new findings on neuronal responses to growth factors and injury and highlight the coordination of transcription, translation and transport required to mediate communication between axons and cell bodies.

Published

2016

46. From Synapse to Nucleus and Back Again—Communication over Distance within Neurons: Figure 1

Author

Mike Fainzilber, Michael R. Kreutz, Vivian Budnik, and Rosalind A. Segal

Subjects

General Neuroscience, Dynein, Importin, Biology, Cell biology, medicine.anatomical_structure, nervous system, Synaptic plasticity, Second messenger system, Axoplasmic transport, medicine, Soma, Axon, Neuroscience, Nucleus

Abstract

How do neurons integrate intracellular communication from synapse to nucleus and back? Here we briefly summarize aspects of this topic covered by a symposium at Neuroscience 2011. A rich repertoire of signaling mechanisms link both dendritic terminals and axon tips with neuronal soma and nucleus, using motor-dependent transport machineries to traverse the long intracellular distances along neuronal processes. Activation mechanisms at terminals include localized translation of dendritic or axonal RNA, proteolytic cleavage of receptors or second messengers, and differential phosphorylation of signaling moieties. Signaling complexes may be transported in endosomes, or as non-endosomal complexes associated with importins and dynein. Anterograde transport of RNA granules from the soma to neuronal processes, coupled with retrograde transport of proteins translated locally at terminals or within processes, may fuel ongoing bidirectional communication between soma and synapse to modulate synaptic plasticity as well as neuronal growth and survival decisions.

Published

2011

47. Numb Links Extracellular Cues to Intracellular Polarity Machinery to Promote Chemotaxis

Author

Marimelia Porcionatto, Rosalind A. Segal, Pengcheng Zhou, Xuesong Zhao, Jose Alfaro, and Eun Hyuk Chang

Subjects

animal structures, Endocytic cycle, Mice, Transgenic, Nerve Tissue Proteins, Tropomyosin receptor kinase B, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Mice, Cell Movement, Cell polarity, Extracellular, Animals, Receptor, trkB, Molecular Biology, Cells, Cultured, Protein Kinase C, Mice, Inbred BALB C, Chemotactic Factors, fungi, Cell Polarity, Membrane Proteins, Signal transducing adaptor protein, Chemotaxis, Cell Biology, Cell biology, nervous system, embryonic structures, NUMB, Intracellular, hormones, hormone substitutes, and hormone antagonists, Developmental Biology

Abstract

SummaryCell polarization is essential throughout development for proliferation, migration, and differentiation. However, it is not known how extracellular cues correctly orient cell polarity at distinct stages of development. Here, we show that the endocytic adaptor protein Numb, previously characterized for its role in cell proliferation, subsequently plays an important role in cell migration. In neural precursors stimulated with the chemotactic factor BDNF, Numb binds to activated TrkB, the BDNF receptor, and functions both as an endocytic regulator for TrkB and as a scaffold for aPKC (aPKC). Thus, Numb promotes BDNF-dependent aPKC activation. Interestingly, Numb is also a substrate of aPKC. When phosphorylated, Numb exhibits increased efficacy in binding TrkB and in promoting a chemotactic response to BDNF. Therefore, Numb functions in a feed-forward loop to promote chemotaxis of neural precursors, linking BDNF, an extracellular cue, to aPKC, a critical component of the intrinsic polarity machinery.

Published

2011

48. Sensory Neuropathy Attributable to Loss of Bcl-w

Author

Stephanie L. Courchesne, Rosalind A. Segal, Maria F. Pazyra-Murphy, and Christoph Karch

Subjects

Denervation, Membrane potential, medicine.medical_specialty, General Neuroscience, Sensory system, Degeneration (medical), Mitochondrion, Biology, Nociception, Endocrinology, nervous system, Sensory threshold, Internal medicine, medicine, Nociceptor, Neuroscience

Abstract

Small fiber sensory neuropathy is a common disorder in which progressive degeneration of small-diameter nociceptors causes decreased sensitivity to thermal stimuli and painful sensations in the extremities. In the majority of patients, the cause of small fiber sensory neuropathy is unknown, and treatment options are limited. Here, we show that Bcl-w (Bcl-2l2) is required for the viability of small fiber nociceptive sensory neurons.Bcl-w−/−mice demonstrate an adult-onset progressive decline in thermosensation and a decrease in nociceptor innervation of the epidermis. This denervation occurs without cell body loss, indicating that lack of Bcl-w results in a primary axonopathy. Consistent with this phenotype, we show that Bcl-w, in contrast to the closely related Bcl-2 and Bcl-xL, is enriched in axons of sensory neurons and that Bcl-w prevents the dying back of axons.Bcl-w−/−sensory neurons exhibit mitochondrial abnormalities, including alterations in axonal mitochondrial size, axonal mitochondrial membrane potential, and cellular ATP levels. Collectively, these data establishbcl-w−/−mice as an animal model of small fiber sensory neuropathy and provide new insight regarding the role of Bcl-w and of mitochondria in preventing axonal degeneration.

Published

2011

49. A Retrograde Neuronal Survival Response: Target-Derived Neurotrophins Regulate MEF2D and bcl-w

Author

Heather M. Heerssen, Christoph Karch, Fiona L. Watson, Michael E. Greenberg, Tae Kyung Kim, Rosalind A. Segal, Stephanie L. Courchesne, Maria F. Pazyra-Murphy, Aymeric Hans, and Katharina E. Cosker

Subjects

Mef2, Sensory Receptor Cells, Cell Survival, Green Fluorescent Proteins, Nerve Tissue Proteins, Stimulation, Transfection, Article, Ganglia, Spinal, Chlorocebus aethiops, In Situ Nick-End Labeling, medicine, Animals, Nerve Growth Factors, RNA, Messenger, Enzyme Inhibitors, Cells, Cultured, Mitogen-Activated Protein Kinase 7, Regulation of gene expression, biology, General Neuroscience, Embryo, Mammalian, Protein Tyrosine Phosphatases, Non-Receptor, Sensory neuron, Rats, Cell biology, Nerve growth factor, medicine.anatomical_structure, Gene Expression Regulation, Proto-Oncogene Proteins c-bcl-2, nervous system, biology.protein, RNA Interference, Signal transduction, Signal Transduction, Neurotrophin

Abstract

Survival and maturation of dorsal root ganglia sensory neurons during development depend on target-derived neurotrophins. These target-derived signals must be transmitted across long distances to alter gene expression. Here, we address the possibility that long-range retrograde signals initiated by target-derived neurotrophins activate a specialized transcriptional program. The transcription factor MEF2D is expressed in sensory neurons; we show that expression of this factor is induced in response to target-derived neurotrophins that stimulate the distal axons. We demonstrate that MEF2D regulates expression of an anti-apoptoticbcl-2family member,bcl-w. Expression ofmef2dandbcl-wis stimulated in response to activation of a Trk-dependent ERK5/MEF2 pathway, and our data indicate that this pathway promotes sensory neuron survival. We find thatmef2dandbcl-ware members of a larger set of retrograde response genes, which are preferentially induced by neurotrophin stimulation of distal axons. Thus, activation of an ERK5/MEF2D transcriptional program establishes and maintains the cellular constituents of functional sensory circuits.

Published

2009

50. Proteoglycan interactions with Sonic Hedgehog specify mitogenic responses

Author

Margaret A. Thompson, Yoojin Choi, Jennifer A. Chan, Rosalind A. Segal, Carolyn O Walsh, Maria F. Pazyra-Murphy, Srividya Balasubramanian, Rochelle M. Witt, and Kellie J. Nazemi

Subjects

Central Nervous System, animal structures, Cell division, Glycosylphosphatidylinositols, Kruppel-Like Transcription Factors, Gene Expression, Mitosis, Mice, Transgenic, Nerve Tissue Proteins, Article, Histones, Mice, Fibrinolytic Agents, Zinc Finger Protein Gli3, Precursor cell, In Situ Nick-End Labeling, medicine, Animals, Hedgehog Proteins, Progenitor cell, Sonic hedgehog, Body Patterning, Cell Proliferation, Regulation of gene expression, biology, Heparin, Cell growth, Stem Cells, General Neuroscience, Gene Expression Regulation, Developmental, Embryo, Mammalian, Oligodendrocyte, medicine.anatomical_structure, Animals, Newborn, Bromodeoxyuridine, Proteoglycan, Mutation, embryonic structures, biology.protein, Proteoglycans, Neuroscience, Protein Binding

Abstract

Sonic Hedgehog (Shh) has dual roles in vertebrate development, promoting progenitor cell proliferation and inducing tissue patterning. We found that the mitogenic and patterning functions of Shh can be uncoupled from one another. Using a genetic approach to selectively inhibit Shh-proteoglycan interactions in a mouse model, we found that binding of Shh to proteoglycans was required for proliferation of neural stem/precursor cells, but not for tissue patterning. Shh-proteoglycan interactions regulated both spatial and temporal features of Shh signaling. Proteoglycans localized Shh to specialized mitogenic niches and also acted at the single-cell level to regulate the duration of Shh signaling, thereby promoting a gene expression program that is important for cell division. Because activation of the Shh pathway is a feature of diverse human cancers, selective stimulation of proliferation by Shh-proteoglycan interactions may also figure prominently in neoplastic growth.

Published

2009