Your search keyword '"Eva L Feldman"' showing total 44 results

1. Epigenetic age acceleration is associated with occupational exposures, sex, and survival in amyotrophic lateral sclerosisResearch in context

Author

Yue Zhao, Xiayan Li, Kai Wang, Gayatri Iyer, Stacey A. Sakowski, Lili Zhao, Samuel Teener, Kelly M. Bakulski, John F. Dou, Bryan J. Traynor, Alla Karnovsky, Stuart A. Batterman, Eva L. Feldman, Maureen A. Sartor, and Stephen A. Goutman

Subjects

Amyotrophic lateral sclerosis (ALS), Epigenetic clock, Occupational risk, Immune cell proportions, Sex, Ageing, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: Amyotrophic lateral sclerosis (ALS) is linked to ageing and genetic and environmental risk factors, yet underlying mechanisms are incompletely understood. We aimed to evaluate epigenetic age acceleration (EAA), i.e., DNA methylation (DNAm) age acceleration, and its association with ALS case status and survival. Methods: In this study, we included 428 ALS and 288 control samples collected between 2011 and 2021. We calculated EAA using the GrimAge residual method from ALS and control blood samples and grouped participants with ALS into three ageing groups (fast, normal, slow). We associated EAA with ALS case status and survival, stratified by sex, and correlated it with environmental and biological factors through occupational exposure assessments, immune cell proportions, and transcriptome changes. Findings: Participants with ALS had higher average EAA by 1.80 ± 0.30 years (p

Published

2024

2. IGF-I prevents glutamate-induced motor neuron programmed cell death

Author

Andrea M Vincent, Bret C Mobley, Andrew Hiller, and Eva L Feldman

Subjects

Amyotrophic lateral sclerosis, Apoptosis, Drug screening, Gene therapy, Insulin-like growth factor-I, Programmed cell death (PCD), Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Insulin-like growth factor I (IGF-I) is currently in clinical trials for treatment of amyotrophic lateral sclerosis (ALS), but little is known about how it promotes the survival of motor neurons. In the current study, we examined IGF-I-mediated neuroprotection in an in vitro model of ALS utilizing enriched cultures of embryonic rat spinal cord motor neurons. IGF-I binds to the IGF-I receptor (IGF-IR) in motor neurons and activates MAPK and the downstream effector of phosphatidylinositol 3-kinase (PI-3K) signaling, Akt. IGF-I:IGF-IR signaling involves phosphorylation of IRS-1 and Shc, but not IRS-2. Glutamate, which is elevated in the cerebrospinal fluid of ALS patients, induced DNA fragmentation and caspase-3 cleavage in the spinal cord motor neurons. These effects of glutamate were blocked by co-treatment with IGF-I. However, a delay of IGF-I treatment for as little as 30 min eliminated its neuroprotective effect. Finally, alone, neither the MAPK pathway inhibitor PD98059 nor the PI-3K inhibitor LY294002 blocked the neuroprotective effect of IGF-I, but both inhibitors together were effective in this regard. These results suggest that the dose and timing of IGF-I administration are critical for producing a neuroprotective effect, and also suggest that both the MAPK and PI-3K/Akt pathways can promote the survival of motor neurons. We discuss our results in terms of novel strategies for ALS therapy.

Published

2004

3. Adeno-associated viral vector gene expression in the adult rat spinal cord following remote vector delivery

Author

Nicholas M Boulis, Aaron J Noordmans, Debbie K Song, Michael J Imperiale, Adam Rubin, Paola Leone, Matthew During, and Eva L Feldman

Subjects

Spinal cord, Sciatic nerve, Adeno-associated virus, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The current investigation tests whether adeno-associated viral vectors (rAAV) undergo remote delivery to the spinal cord via peripheral nerve injection as previously demonstrated with adenoviral vectors. The sciatic nerves of adult rats (n = 10) were injected with either an rAAV (rAAVCMV-lacZ) or adenoviral (AdCMV-lacZ) vector (1.4 × 107 particles/ml). After 21 days, the rAAV group demonstrated significantly higher spinal cord viral expression than the adenoviral group (P < 0.024). A second group of rats was injected with rAAV expressing the green fluorescence protein (GFP) reporter gene. GFP was detected 21 days after unilateral sciatic nerve injection in the neurons of the dorsal root ganglion and spinal cord. The codistribution of the viral genome and transgene in CNS neurons was confirmed with in situ hybridization. In summary, rAAV genes are expressed in CNS neurons following peripheral nerve injection at levels exceeding those seen following remote adenovirus injection.

Published

2003

4. Stem cell therapeutics and gene therapy for neurologic disorders

Author

Kevin S. Chen, Emily J. Koubek, Stacey A. Sakowski, and Eva L. Feldman

Subjects

Gene therapy, Genetically modified cell therapy, Genome editing, Stem cells, Stem cell therapy, Transplantation, Neurology. Diseases of the nervous system, RC346-429

Abstract

Rapid advances in biological knowledge and technological innovation have greatly advanced the fields of stem cell and gene therapies to combat a broad spectrum of neurologic disorders. Researchers are currently exploring a variety of stem cell types (e.g., embryonic, progenitor, induced pluripotent) and various transplantation strategies, each with its own advantages and drawbacks. Similarly, various gene modification techniques (zinc finger, TALENs, CRISPR-Cas9) are employed with various delivery vectors to modify underlying genetic contributors to neurologic disorders. While these two individual fields continue to blaze new trails, it is the combination of these technologies which enables genetically engineered stem cells and vastly increases investigational and therapeutic opportunities. The capability to culture and expand stem cells outside the body, along with their potential to correct genetic abnormalities in patient-derived cells or enhance cells with extra gene products, unleashes the full biological potential for innovative, multifaceted approaches to treat complex neurological disorders. In this review, we provide an overview of stem cell and gene therapies in the context of neurologic disorders, highlighting recent advances and current shortcomings, and discuss prospects for future therapies in clinical settings.

Published

2024

5. Contributors

Author

Samira Abdulai-Saiku, Stanley H. Appel, Arthur P. Arnold, Lisa M. Arnold, Robert M. Arnold, Alexa Bacha, Miroslav 'Misha' Backonja, Zinzi D. Bailey, Lucinda Bateman, David R. Beers, Anna Berti, Mamta Bhatnagar, Devin K. Binder, Marina Boido, Maura Boldrini, David Borsook, Xandra O. Breakefield, Robert H. Brown, Rami Burstein, Eduardo R. Butelman, Louis R. Caplan, S. Chen, Marie-Françoise Chesselet, Stefan Clemens, Paula R. Clemens, Joseph T. Coyle, John C. DeWitt, Dena B. Dubal, Veljko Dubljević, Eva L. Feldman, Beth A. Fischer, M.C. Flux, J.S. Fortin, Angelisa Frasca, Francesca Garbarini, Thomas Gasser, Charles F. Gillespie, Michael S. Gold, Stefan M. Gold, Randi Hagerman, Regan Hamel, Craig Haney, James C. Harris, Sara Hassani, Norman J. Haughey, Vibol Heng, J. Horn, Rosana-Bristena Ionescu, Raffaele Iorio, David J. Irwin, Henry J. Kaminski, Dalia Khammash, Vikram Khurana, Charlotte Kilstrup-Nielsen, Bhumsoo Kim, Boram Kim, Marieke Klein, Nastassja Koen, Glenn T. Konopaske, Joanna A. Korecka, Birgitte Rahbek Kornum, Mary Jeanne Kreek, Krister Kristensson, Grzegorz Krzak, Linda L. Kusner, Nicoletta Landsberger, Edward B. Lee, Tong Li, Paweł P. Liberski, Christine Lochner, Christopher A. Lowry, J. John Mann, Clara Marincowitz, E.A. Mayer, E.D. Mayer, Iris Coates McCall, Louise D. McCullough, Michael J. Meaney, Claudio Melo de Gusmao, Abhishek L. Menesgere, Emmanuel Mignot, William C. Mobley, Mayra Montalvo, Alisha R. Moreland-Capuia, Marco Neppi-Modona, Alexandra M. Nicaise, Rae Nishi, Orna O'Toole, Cassia Overk, Laurie Ozelius, Matthew P. Parsons, H.B. Penticoff, Luca Peruzzotti-Jametti, Owen M. Peters, Allison Peterson, Jessica M. Phan, Sean J. Pittock, Stefano Pluchino, Thad A. Polk, Araya Puwanant, Shreya K. Rajagopal, Vijayalakshmi Ravindranath, Lynn A. Raymond, Brian Reed, Kerry J. Ressler, Diane L. Ritchie, Leah H. Rubin, Stacey A. Sakowski, Mario A. Saporta, Alena V. Savonenko, Helen E. Scharfman, Bruce K. Shapiro, Nutan Sharma, Cayce K. Shaw, Michael E. Shy, Beata Sikorska, Ethan J. Silverman, Roger P. Simon, Kristina Simonyan, Catrina Sims-Robinson, Richard Jay Smeyne, Clay Smith, Colin Smith, Sharan R. Srinivasan, Dan J. Stein, Christopher D. Stephen, Indu Subramanian, Edina Szabo, Alissa A. Thomas, Luis B. Tovar-y-Romo, Arshya Vahabzadeh, Alessandro Vercelli, Ashley Viera-Ortiz, Mitchell T. Wallin, Donna M. Werling, Thomas Wichmann, Clayton A. Wiley, David R. Williams, Cory Willis, Philip C. Wong, Vadim Yuferov, Weihua Zhao, Michael J. Zigmond, and Saša A. Živković

Published

2023

6. Diabetes and cognitive dysfunction

Author

Bhumsoo Kim, Catrina Sims-Robinson, Stacey A. Sakowski, and Eva L. Feldman

Published

2023

7. List of contributors

Author

Gulcin Akinci, Henning Andersen, Andrew J.M. Boulton, Frank Lee Bowling, Vera Bril, Nigel A. Calcutt, Brian C. Callaghan, Josie Carmichael, Krish Chandrasekaran, Joseph Colombo, Niels Ejskjaer, Hassan Fadavi, Eva L. Feldman, Keeley Jane Foley, Gary Gallagher, Hanna Harno, Fukashi Ishibashi, Páll Karlsson, Venu Kavarthapu, Joyce Lim, Andrew G. Marshall, Anne Marshall, Deepak Menon, Kalliopi Pafili, Nikolaos Papanas, Amanda C. Peltier, Brendan N. Putko, Beatriz Rodríguez-Sánchez, Johan Røikjer, Milla Rosengård-Bärlund, James W. Russell, Masha G. Savelieff, Dinesh Selvarajah, Angela C. Shore, Alan Sinclair, Anders Stouge, Mitra Tavakoli, Solomon Tesfaye, Prashanth R.J. Vas, Soroku Yagihashi, Dilek Gogas Yavuz, Mark Yorek, Lindsay A. Zilliox, and Douglas W. Zochodne

Published

2022

8. Diabetic neuropathy in children and youth

Author

Gulcin Akinci, Masha G. Savelieff, Gary Gallagher, Brian C. Callaghan, and Eva L. Feldman

Published

2022

9. Metabolism, cognition, and the brain throughout life

Author

Fergus J. Cameron, Eva L. Feldman, and Stacey A. Sakowski

Subjects

Aging, Central nervous system, lcsh:RC321-571, Cognition, Diabetes mellitus, medicine, Animals, Humans, Autism spectrum disorder, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Metabolic Syndrome, business.industry, Diabetes, Brain, Metabolism, Alzheimer's disease, medicine.disease, Obesity, medicine.anatomical_structure, Neurology, Metabolic syndrome, business, Neuroscience

Published

2020

10. The effects of insulin and insulin-like growth factor I on amyloid precursor protein phosphorylation in in vitro and in vivo models of Alzheimer's disease

Author

Sarah Elzinga, Rosemary E. Henn, Eva L. Feldman, Lisa M. McGinley, and Bhumsoo Kim

Subjects

0301 basic medicine, medicine.medical_specialty, medicine.medical_treatment, Diet, High-Fat, Article, lcsh:RC321-571, Rats, Sprague-Dawley, Dephosphorylation, Amyloid beta-Protein Precursor, Mice, 03 medical and health sciences, Insulin-like growth factor, 0302 clinical medicine, Insulin resistance, Alzheimer Disease, Internal medicine, medicine, Amyloid precursor protein, Animals, Insulin, Obesity, Insulin-Like Growth Factor I, Phosphorylation, Protein kinase B, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Cells, Cultured, Cerebral Cortex, biology, business.industry, Alzheimer's disease, medicine.disease, Rats, IGF-I, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, Neurology, biology.protein, Metabolic syndrome, business, 030217 neurology & neurosurgery

Abstract

Alzheimer’s disease (AD) is a growing problem worldwide, and there are currently no effective treatments for this devastating disease. The neurotrophic growth factors insulin and insulin-like growth factor-I (IGF-I) are currently being investigated as potential therapeutic approaches for AD in preclinical and clinical studies. However, given that the metabolic syndrome (MetS) and diabetes are risk factors for AD, it is unknown how associated insulin resistance (IR) in the brain may impact the effectiveness of these therapies for AD. In this report, we therefore investigated the mechanisms underlying the effects of insulin and IGF-I on AD-associated pathology in the context of IR, with particular emphasis on phosphorylation of amyloid precursor protein (APP), a key step in promoting amyloid plaque formation in AD. Both insulin and IGF-I decreased APP phosphorylation in cultured primary cortical neurons, supporting their therapeutic use in AD. Induction of IR blocked the beneficial effect of insulin and reduced the effect of IGF-I on APP dephosphorylation. These effects were mediated by the phosphatidylinositol 3- kinase (PI3-K)/protein kinase B (Akt) pathway, as inhibition of this pathway during IR restored the effect of IGF-I on APP dephosphorylation. Finally, we explored the translational relevance of these results in vivo by demonstrating that high fat diet fed mice, a robust model of IR and MetS, exhibited the expected increased brain APP phosphorylation. Overall, these data suggest that the beneficial therapeutic effect of insulin and IGF-I on APP phosphorylation is negatively impacted by IR, and suggest that insulin and IGF-I alone may not be appropriate therapies for AD patients with IR, MetS, or diabetes.

Published

2019

11. List of contributors

Author

Dayo O. Adewole, Elham Afjeh-Dana, Ehsaneh Daghigh Ahmadi, Nessar Ahmed, Osama A. Alkhalili, Ali Amadikuchaksaraei, Naser Amini, Moein Amoupour, Ilida Ortega Asencio, Khadijeh Ashtari, Amish Asthana, Anthony Atala, Cynthia A. Batchelder, Francois Berthiaume, Michael J. Brenner, Beyza Bulutoglu, Justin C. Burrell, Hannes Campo, Irene Cervelló, Deborah Chaimov, Munmun Chattopadhyay, Yibin Chen, Phil Coates, D. Kacy Cullen, Suradip Das, Petra de Graaf, Vincent F. de Kemp, Laetitia M.O. de Kort, Khangembam Sangeeta Devi, Rukmani Dewangan, Adam K. Ekenseair, Sarah Elzinga, Gholam Ali Farzi, Eva L. Feldman, Soon Chin Fhong, Christine Finck, Christopher Foster, Michaela Gaffley, Anil Kumar Gangwar, Carlo Gazia, Saudah Hafeji, Ehab Hafiz, Zoe Hancox, John E. Hanks, Debels Heidi, Michael D. House, Ji-Young Hwang, Maria Jaramillo, Todd Jensen, Binata Joddar, Inho Jo, Eyone Jones, Sung-Chul Jung, Ninad S. Kanetkar, Hwan June Kang, Saied Kargozar, Kritika S. Katiyar, Sarah S. Kelangi, Saeed Heidari Keshel, Seyed Ali Khaghani, Sangeeta Devi Khangembam, Han Su Kim, Bouchra Koullali, Naveen Kumar, Suneel Kumar, Vineet Kumar, Joerg Lahann, Yunki Lee, Jennifer L. Long, Renata S. Magalhaes, Swapan Kumar Maiti, Peiman Brouki Milan, Adam Mitchell, Majid Momeni-Moghadam, Masoud Mozafari, Ayșe Jane Muñiz, Chaman Naeem, Karthik Nair, Se-Young Oh, Jeremie D. Oliver, Hazem Orabi, Giuseppe Orlando, Ki Dong Park, Yoon Shin Park, Dmitriy Petrov, P.D.S. Raghuvanshi, Alireza Rezapour, Xavier Santamaria, Sonal Saxena, Wael Sayej, Farshid Sefat, Tejal Shah, Shahryar Shakeri, Ishna Sharma, Sameer Shrivastava, Carlos Simón, Ajit Kumar Singh, Karam Pal Singh, Naresh Kumar Singh, S.L. Sing, Aaron W. Stebbins, E.Y.S. Tan, Alice F. Tarantal, Nishat Tasnim, Tuğba Topal, Herminio M. Torres, George Tsachouridis, Basak E. Uygun, Krishna S. Vyas, Heather Wanczyk, Hongjun Wang, Morrison Wayne, W.Y. Yeong, Safiyya Yousaf, Mansour Youseffi, and Wei Zhang

Published

2019

12. Disorders of mitochondrial dynamics in peripheral neuropathy: Clues from hereditary neuropathy and diabetes

Author

Masha G. Savelieff, Stacey A. Sakowski, Eva L. Feldman, and Amy E. Rumora

Subjects

business.industry, Mitochondrion, medicine.disease, Bioinformatics, 03 medical and health sciences, 0302 clinical medicine, Peripheral neuropathy, Apoptosis, Diabetes mellitus, medicine, Prediabetes, business, Complication, 030217 neurology & neurosurgery, Dyslipidemia, Mitochondrial transport

Abstract

Peripheral neuropathy is a common and debilitating complication of diabetes and prediabetes. Recent clinical studies have identified an association between the development of neuropathy and dyslipidemia in prediabetic and diabetic patients. Despite the prevalence of this complication, studies identifying molecular mechanisms that underlie neuropathy progression in prediabetes or diabetes are limited. However, dysfunctional mitochondrial pathways in hereditary neuropathy provide feasible molecular targets for assessing mitochondrial dysfunction in neuropathy associated with prediabetes or diabetes. Recent studies suggest that elevated levels of dietary saturated fatty acids (SFAs) associated with dyslipidemia impair mitochondrial dynamics in sensory neurons by inducing mitochondrial depolarization, compromising mitochondrial bioenergetics, and impairing axonal mitochondrial transport. This causes lower neuronal ATP and apoptosis. Conversely, monounsaturated fatty acids (MUFAs) restore nerve and sensory mitochondrial function. Understanding the mitochondrial pathways that contribute to neuropathy progression in prediabetes and diabetes may provide therapeutic targets for the treatment of this debilitating complication.

Published

2019

13. Emerging understanding of the genotype–phenotype relationship in amyotrophic lateral sclerosis

Author

Eva L. Feldman, Stephen A. Goutman, Ximena Paez-Colasante, and Kevin S. Chen

Subjects

0301 basic medicine, Mutation, business.industry, Genetic heterogeneity, Genetic counseling, SOD1, Disease, medicine.disease_cause, Bioinformatics, medicine.disease, TARDBP, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, C9orf72, medicine, Amyotrophic lateral sclerosis, business, 030217 neurology & neurosurgery

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive, noncurable neurodegenerative disorder of the upper and lower motor neurons causing weakness and death within a few years of symptom onset. About 10% of patients with ALS have a family history of the disease; however, ALS-associated genetic mutations are also found in sporadic cases. There are over 100 ALS-associated mutations, and importantly, several genetic mutations, including C9ORF72, SOD1, and TARDBP, have led to mechanistic insight into this complex disease. In the clinical realm, knowledge of ALS genetics can also help explain phenotypic heterogeneity, aid in genetic counseling, and in the future may help direct treatment efforts.

Published

2018

14. Stem Cell Therapy for Amyotrophic Lateral Sclerosis

Author

Eva L. Feldman and Kevin S. Chen

Subjects

business.industry, medicine.medical_treatment, Mesenchymal stem cell, Stem-cell therapy, medicine.disease, Embryonic stem cell, Neural stem cell, Transplantation, Medicine, Respiratory function, Amyotrophic lateral sclerosis, Stem cell, business, Neuroscience

Abstract

Amyotrophic lateral sclerosis (ALS) is a challenging disease characterized by progressive loss of motor neurons. This is manifested in deterioration of strength, gait, speech, swallowing, respiratory function, and eventually leads to death. A major hurdle in development of effective therapy is rooted in the multifactorial nature of ALS pathophysiology. Cell-based therapies, in particular stem cells, have emerged as a promising therapeutic option. Stem cells have the capacity to modulate the local environment by multiple simultaneous mechanisms and promote survival of motor neurons. In this chapter, we describe various stem cell types that have been used in ALS and the underlying rationale. We also review early clinical trials using these diverse types of stem cells. Advances in stem cell therapy are moving forward at breakneck pace, and if approached with attention to methodology and regulation, have the potential to significantly improve the care of patients with ALS.

Published

2017

15. Intraspinal transplantation of neurogenin-expressing stem cells generates spinal cord neural progenitors

Author

Stacey A. Sakowski, Sue O'Shea, Eva L. Feldman, J. Matthew Velkey, J. Simon Lunn, Crystal Pacut, and Emily R. Stern

Subjects

Embryonic stem cells, Cellular differentiation, Neurogenesis, Transplantation, Heterologous, Nerve Tissue Proteins, Biology, Article, Spinal Cord Diseases, Cell Line, lcsh:RC321-571, Rats, Sprague-Dawley, Mice, Neural Stem Cells, medicine, Basic Helix-Loop-Helix Transcription Factors, Animals, Progenitor cell, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Spinal cord, Neural specification, Neurogenin1, Embryonic stem cell, Neural stem cell, Cell biology, Rats, Transplantation, medicine.anatomical_structure, Neurology, Stem cell, Neuroscience, Stem Cell Transplantation

Abstract

Embryonic stem (ES) cells and their derivatives are an important resource for developing novel cellular therapies for disease. Controlling proliferation and lineage selection, however, are essential to circumvent the possibility of tumor formation and facilitate the safe translation of ES-based therapies to man. Expression of appropriate transcription factors is one approach to direct the differentiation of ES cells towards a specific lineage and stop proliferation. Neural differentiation can be initiated in ES cells by expression of Neurogenin1 (Ngn1). In this study we investigate the effects of controlled Ngn1 expression on mouse ES (mES) cell differentiation in vitro and following grafting into the rat spinal cord. In vitro, Ngn1 expression in mES cells leads to rapid and specific neural differentiation, and a concurrent decrease in proliferation. Similarly transplantation of Ngn1-expressing mES cells into the spinal cord lead to in situ differentiation and spinal precursor formation. These data demonstrate that Ngn1 expression in mES cells is sufficient to promote neural differentiation and inhibit proliferation, thus establishing an approach to safely graft ES cells into the spinal cord.

Published

2012

16. Oxidative injury and neuropathy in diabetes and impaired glucose tolerance

Author

Kelli A. Sullivan, Eva L. Feldman, Alison Berent-Spillson, Andrea M. Vincent, Catherine L. Freimann, and James W. Russell

Subjects

Blood Glucose, medicine.medical_specialty, endocrine system diseases, Type 2 diabetes, medicine.disease_cause, Article, lcsh:RC321-571, Impaired glucose tolerance, Diabetes mellitus genetics, Dorsal root ganglion, Diabetic Neuropathies, Internal medicine, Diabetes mellitus, Ganglia, Spinal, Glucose Intolerance, medicine, Diabetes Mellitus, Animals, Dorsal root ganglia, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, business.industry, Diabetes, Snap, nutritional and metabolic diseases, medicine.disease, Axons, Rats, Rats, Zucker, Neuropathy, medicine.anatomical_structure, Endocrinology, Neurology, Oxidative stress, Female, business, Sensory nerve

Abstract

Clinical studies suggest that impaired glucose tolerance (IGT) is associated with the development of neuropathy. The aim of the current study was to determine if neuropathy developed in the female Zucker Diabetic Fatty (ZDF) rat, an animal model of IGT and type 2 diabetes. The ZDF rat develops impaired glucose tolerance (IGT) when fed a control diet, and frank diabetes when fed a high fat diet. Following 10 weeks of hyperglycemia, sensory nerve action potentials (SNAP) and compound motor action potentials (CMAP) were reduced and sensory conduction velocities were slowed (distal > proximal) in the tail and hind limb in ZDF animals with IGT and frank diabetes (p

Published

2008

17. Degradation and Dephosphorylation of Focal Adhesion Kinase During Okadaic Acid-Induced Apoptosis in Human Neuroblastoma Cells

Author

Cynthia M. van Golen, Bhumsoo Kim, and Eva L. Feldman

Subjects

Cancer Research, Biology, lcsh:RC254-282, Focal adhesion, Dephosphorylation, 03 medical and health sciences, chemistry.chemical_compound, Neuroblastoma, 0302 clinical medicine, okadaic acid, insulin-like growth factor-I, Protein kinase B, 030304 developmental biology, 0303 health sciences, PTK2B, focal adhesion kinase, apoptosis, Tyrosine phosphorylation, 15. Life on land, Actin cytoskeleton, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Protein ubiquitination, Cell biology, chemistry, 030220 oncology & carcinogenesis, Phosphorylation, biological phenomena, cell phenomena, and immunity

Abstract

Focal adhesion kinase (FAK) prevents apoptosis in many cell types. We have reported that tyrosine residues in FAK are dephosphorylated and FAK is degraded during mannitol-induced apoptosis in human neuroblastoma cells. Several studies suggest that FAK dephosphorylation and degradation are separate events. The current study defines the relationship between FAK dephosphorylation and degradation in neuroblastoma cells using okadaic acid (OA). OA, a serine phosphatase inhibitor, promotes serine/threonine phosphorylation, which in turn blocks tyrosine phosphorylation. OA induced focal adhesion loss, actin cytoskeleton disorganization, and cellular detachment, which corresponded to a loss of FAK Tyr397 phosphorylation. These changes preceded caspase-3 activation, Akt and MAP kinase activity loss, protein ubiquitination, and cellular apoptosis. Insulin-like growth factor-I prevented mannitol-induced, but not OA-induced, substrate detachment and FAK Tyr397 dephosphorylation, and the effects of OA on FAK Tyr397 phosphorylation were irreversible. The proteolytic degradation of FAK is temporally distinct from its tyrosine dephosphorylation, occurring when apoptotic pathways are already initiated and during a generalized destruction of signaling proteins. Therefore, agents resulting in the dephosphorylation of FAK may be beneficial for therapeutic treatment, irrespective of FAK protein levels, as this may result in apoptosis, which cannot be prevented by growth factor signaling.

Published

2003

18. Therapy for diabetic neuropathy

Author

Bernadette Calabek, Brian C. Callaghan, and Eva L. Feldman

Subjects

medicine.medical_specialty, Type 1 diabetes, Diabetic neuropathy, business.industry, Type 2 diabetes, medicine.disease, Clinical trial, Internal medicine, Anesthesia, Diabetes mellitus, Neuropathic pain, medicine, Complication, business, Glycemic

Abstract

Neuropathy is a highly prevalent complication of diabetes that is only likely to increase as the diabetic epidemic continues. Unfortunately, the only disease-modifying treatment is to address the underlying diabetes with enhanced glucose control. In patients with type 1 diabetes, improved glycemic control dramatically reduces the incidence of neuropathy. In contrast, in patients with type 2 diabetes, better glucose control has only a marginal effect on the prevention of neuropathy. However, recognition and treatment of neuropathic pain is also important. An ever expanding number of randomized, controlled clinical trials support multiple medications for the reduction of pain. This includes medications such as calcium channel agonists, tricyclic antidepressants, and selective serotonin/norepinephrine reuptake inhibitors. However, the precise order and combination of these medications remains unclear. Furthermore, several new promising medications are being developed. Overall, the cornerstones of the treatment of diabetic neuropathy are improved glycemic control and initiation of a neuropathic pain medication with high levels of evidence to support its use when pain is present.

Published

2014

19. Biology of diabetic neuropathy

Author

Eva L. Feldman, Bernadette Calabek, Laurel Roberts, and Andrea M. Vincent

Subjects

medicine.medical_specialty, Diabetic neuropathy, business.industry, Disease, Type 2 diabetes, medicine.disease, Bioinformatics, Insulin resistance, Peripheral neuropathy, Endocrinology, Diabetes mellitus, Internal medicine, medicine, business, Polyneuropathy, Glycemic

Abstract

More than half of all patients with diabetes develop neuropathic disorders affecting the distal sensory and/or motor nerves, or autonomic or cranial nerve functions. Glycemic control can decrease the incidence of neuropathy but is not adequate alone to prevent or treat the disease. This chapter introduces diabetic neuropathy with a morphological description of the disease then describes our current understanding of metabolic and molecular mechanisms that contribute to neurovascular dysfunctions. Key mechanisms include glucose and lipid imbalances and insulin resistance that are interconnected via oxidative stress, inflammation, and altered gene expression. These complex interactions should be considered for the development of new treatment strategies against the onset or progression of neuropathy. Advances in understanding the combined metabolic stressors and the novel study of epigenetics suggest new therapeutic targets to combat this morbid and intractable disease affecting millions of patients with type 1 or type 2 diabetes.

Published

2013

20. Contributors

Author

Gary M. Abrams, Gregory W. Albers, Bradley L. Allen, Michael J. Aminoff, Bruce O. Berg, Joseph R. Berger, Timothy G. Berger, Adil E. Bharucha, Charles F. Bolton, David L. Brown, Christine E. Burness, Michael Camilleri, Vinay Chaudhry, Chadwick W. Christine, Kimberly P. Cockerham, Gary M. Cox, G.A.B. Davies-Jones, Larry E. Davis, Lisa M. Deangelis, Philip R. Delio, William P. Dillon, Christopher F. Dowd, AdrÉ J. Du Plessis, David T. Durack, Jacob S. Elkins, John W. Engstrom, Randolph W. Evans, Eva L. Feldman, Bruce J. Fisch, Joseph M. Furman, Douglas J. Gelb, David J. Gladstone, Douglas S. Goodin, Sean A. Grimm, John J. Halperin, J. Claude Hemphill, John R. Hotson, Cheryl A. Jay, S. Claiborne Johnston, Charles H. King, Nerissa U. Ko, Allan Krumholz, Colin D. Lambert, J. William Langston, John M. Leonard, Catherine Limperopoulos, Alan H. Lockwood, W.T. Longstreth, Elliott L. Mancall, Frank L. Mastaglia, Una D. Mccann, Robert O. Messing, Andrea Olmos, Richard K. Olney, Jack M. Parent, Gareth J. Parry, Roy A. Patchell, John R. Perfect, Ann Noelle Poncelet, Rodica Pop-Busui, Jerome B. Posner, Jeffrey W. Ralph, William J. Ravich, George A. Ricaurte, Jack E. Riggs, Karen L. Roos, Andrew P. Rose-Innes, Richard B. Rosenbaum, Thomas D. Sabin, Robert A. Salata, Hyman M. Schipper, Pamela J. Shaw, Roger P. Simon, Michele B. St. Martin, Barney J. Stern, Kelli A. Sullivan, Jon D. Sussman, Michael Swash, Thomas R. Swift, Michael R. Trimble, Angela T. Truong, Alex C. Tselis, David B. VoduŠek, Kevin C. Wang, Linda S. Williams, Marc D. Winkelman, G. Bryan Young, and Jonathan G. Zaroff

Published

2008

21. Diabetes and the Nervous System

Author

Eva L. Feldman, Kelli A. Sullivan, and Rodica Pop-Busui

Subjects

Nervous system, medicine.anatomical_structure, business.industry, Diabetes mellitus, Medicine, business, medicine.disease, Neuroscience

Published

2008

22. Editors

Author

Sid Gilman, John C.M. Brust, John J. Caronna, Kenneth L. Casey, Eva L. Feldman, Christopher Gomez, Richard T. Johnson, Michael V. Johnston, John J. Laterra, Phillip A. Low, John C. Mazziotta, Emmanuel Mignot, Lewis B. Morgenstern, Hugo W. Moser, Timothy A. Pedley, Anthony T. Reder, James W. Russell, Charles A. Thornton, and Gregor K. Wenning

Published

2007

23. Diabetic Nerve Disease, Neuropathy

Author

Kelli A. Sullivan and Eva L. Feldman

Subjects

Nervous system, Diabetic neuropathy, business.industry, Cranial nerves, Sensory system, medicine.disease, Peripheral, Autonomic nervous system, medicine.anatomical_structure, Anesthesia, Peripheral nervous system, Diabetes mellitus, medicine, business

Abstract

Diabetic neuropathy consists of a set of clinical syndromes, the signs and symptoms of which depend on the part of the nervous system damaged by chronic hyperglycemia. The most common type of diabetic neuropathy is distal symmetric sensorimotor polyneuropathy (DPN). DPN is characterized by progressive distal sensory and, in severe cases, motor dysfunction due to loss of sensory and motor axons. Diabetes also damages the autonomic nervous system, thoracic and lumbar nerve roots, isolated peripheral nerves, and cranial nerves. This article focuses on the sensory aspects of DPN.

Published

2004

24. Single-cell RNA sequencing identifies hippocampal microglial dysregulation in diet-induced obesity

Author

Rosemary E. Henn, Kai Guo, Sarah E. Elzinga, Mohamed H. Noureldein, Faye E. Mendelson, John M. Hayes, Diana M. Rigan, Masha G. Savelieff, Junguk Hur, and Eva L. Feldman

Subjects

Neuroscience, Physiology, Transcriptomics, Science

Abstract

Summary: Obesity is a growing global concern in adults and youth with a parallel rise in associated complications, including cognitive impairment. Obesity induces brain inflammation and activates microglia, which contribute to cognitive impairment by aberrantly phagocytosing synaptic spines. Local and systemic signals, such as inflammatory cytokines and metabolites likely participate in obesity-induced microglial activation. However, the precise mechanisms mediating microglial activation during obesity remain incompletely understood. Herein, we leveraged our mouse model of high-fat diet (HFD)-induced obesity, which mirrors human obesity, and develops hippocampal-dependent cognitive impairment. We assessed hippocampal microglial activation by morphological and single-cell transcriptomic analysis to evaluate this heterogeneous, functionally diverse, and dynamic class of cells over time after 1 and 3 months of HFD. HFD altered cell-to-cell communication, particularly immune modulation and cellular adhesion signaling, and induced a differential gene expression signature of protein processing in the endoplasmic reticulum in a time-dependent manner.

Published

2023

25. Disrupted axon-glia communication leads to neurodegeneration in metabolic diseases

Author

Stacey A. Sakowski, Masha G. Savelieff, and Eva L. Feldman

Subjects

Alzheimer's disease, Astrocyte, Diabetes, Metabolic crosstalk, Metabolic syndrome, Neuron, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2023

26. Glial-neuron crosstalk in health and disease: A focus on metabolism, obesity, and cognitive impairment

Author

Rosemary E. Henn, Mohamed H. Noureldein, Sarah E. Elzinga, Bhumsoo Kim, Masha G. Savelieff, and Eva L. Feldman

Subjects

Astrocyte, Axon, Cognitive impairment, Dementia, Diabetes, Metabolic syndrome, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Dementia is a complex set of disorders affecting normal cognitive function. Recently, several clinical studies have shown that diabetes, obesity, and components of the metabolic syndrome (MetS) are associated with cognitive impairment, including dementias such as Alzheimer's disease. Maintaining normal cognitive function is an intricate process involving coordination of neuron function with multiple brain glia. Well-orchestrated bioenergetics is a central requirement of neurons, which need large amounts of energy but lack significant energy storage capacity. Thus, one of the most important glial functions is to provide metabolic support and ensure an adequate energy supply for neurons. Obesity and metabolic disease dysregulate glial function, leading to a failure to respond to neuron energy demands, which results in neuronal damage. In this review, we outline evidence for links between diabetes, obesity, and MetS components to cognitive impairment. Next, we focus on the metabolic crosstalk between the three major glial cell types, oligodendrocytes, astrocytes, and microglia, with neurons under physiological conditions. Finally, we outline how diabetes, obesity, and MetS components can disrupt glial function, and how this disruption might impair glia-neuron metabolic crosstalk and ultimately promote cognitive impairment.

Published

2022

27. Neurological sequela and disruption of neuron-glia homeostasis in SARS-CoV-2 infection

Author

Masha G. Savelieff, Eva L. Feldman, and Amro M. Stino

Subjects

Axon, Astrocyte, COVID-19, Cytokine storm, Extracellular vesicles, Immune system, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The coronavirus disease 2019 (COVID-19) pandemic is responsible for 267 million infections and over 5 million deaths globally. COVID-19 is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), a single-stranded RNA beta-coronavirus, which causes a systemic inflammatory response, multi-organ damage, and respiratory failure requiring intubation in serious cases. SARS-CoV-2 can also trigger neurological conditions and syndromes, which can be long-lasting and potentially irreversible. Since COVID-19 infections continue to mount, the burden of SARS-CoV-2-induced neurologic sequalae will rise in parallel. Therefore, understanding the spectrum of neurological clinical presentations in SARS-CoV-2 is needed to manage COVID-19 patients, facilitate diagnosis, and expedite earlier treatment to improve outcomes. Furthermore, a deeper knowledge of the neurological SARS-CoV-2 pathomechanisms could uncover potential therapeutic targets to prevent or mitigate neurologic damage secondary to COVID-19 infection. Evidence indicates a multifaceted pathology involving viral neurotropism and direct neuroinvasion along with cytokine storm and neuroinflammation leading to nerve injury. Importantly, pathological processes in neural tissue are non-cell autonomous and occur through a concerted breakdown in neuron-glia homeostasis, spanning neuron axonal damage, astrogliosis, microgliosis, and impaired neuron-glia communication. A clearer mechanistic and molecular picture of neurological pathology in SARS-CoV-2 may lead to effective therapies that prevent or mitigate neural damage in patients contracting and developing severe COVID-19 infection.

Published

2022

28. Chain length of saturated fatty acids regulates mitochondrial trafficking and function in sensory neurons

Author

Amy E. Rumora, Giovanni LoGrasso, Julia A. Haidar, Justin J. Dolkowski, Stephen I. Lentz, and Eva L. Feldman

Subjects

diabetes, dyslipidemias, apoptosis, palmitate, stearate, laurate, Biochemistry, QD415-436

Abstract

Dyslipidemia associated with T2D leads to diabetic neuropathy, a complication characterized by sensory neuronal dysfunction and peripheral nerve damage. Sensory dorsal root ganglion (DRG) neurons are dependent on axonal mitochondrial energy production facilitated by mitochondrial transport mechanisms that distribute mitochondria throughout the axon. Because long-chain saturated FAs (SFAs) damage DRG neurons and medium-chain SFAs are reported to improve neuronal function, we evaluated the impact of SFA chain length on mitochondrial trafficking, mitochondrial function, and apoptosis. DRG neurons were exposed to SFAs with C12:0−C18:0 chain lengths and evaluated for changes in mitochondrial trafficking, mitochondrial polarization, and apoptosis. DRG neurons treated with C16:0 and C18:0 SFAs showed a significant decrease in the percentage of motile mitochondria and velocity of mitochondrial trafficking, whereas C12:0 and C14:0 SFAs had no impact on motility. Treatment with C16:0 and C18:0 SFAs exhibited mitochondrial depolarization correlating with impaired mitochondrial motility; the C12:0- and C14:0-treated neurons retained mitochondrial polarization. The reduction in mitochondrial trafficking and function in C16:0- and C18:0-treated DRG neurons correlated with apoptosis that was blocked in C12:0 and C14:0 SFA treatments. These results suggest that SFA chain length plays an important role in regulating axonal mitochondrial trafficking and function in DRG neurons.

Published

2019

29. Metabolism, cognition, and the brain throughout life

Author

Stacey A. Sakowski, Fergus Cameron, and Eva L. Feldman

Subjects

Aging, Alzheimer's disease, Autism spectrum disorder, Central nervous system, Cognition, Diabetes, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2020

30. Shared and distinct lipid-lipid interactions in plasma and affected tissues in a diabetic mouse model

Author

Kelli M. Sas, Jiahe Lin, Thekkelnaycke M. Rajendiran, Tanu Soni, Viji Nair, Lucy M. Hinder, Hosagrahar V. Jagadish, Thomas W. Gardner, Steven F. Abcouwer, Frank C. Brosius, III, Eva L. Feldman, Matthias Kretzler, George Michailidis, and Subramaniam Pennathur

Subjects

diabetes, eye, kidney, mass spectrometry, nerve, systems biology, Biochemistry, QD415-436

Abstract

Lipids are ubiquitous metabolites with diverse functions; abnormalities in lipid metabolism appear to be related to complications from multiple diseases, including type 2 diabetes. Through technological advances, the entire lipidome has been characterized and researchers now need computational approaches to better understand lipid network perturbations in different diseases. Using a mouse model of type 2 diabetes with microvascular complications, we examined lipid levels in plasma and in renal, neural, and retinal tissues to identify shared and distinct lipid abnormalities. We used correlation analysis to construct interaction networks in each tissue, to associate changes in lipids with changes in enzymes of lipid metabolism, and to identify overlap of coregulated lipid subclasses between plasma and each tissue to define subclasses of plasma lipids to use as surrogates of tissue lipid metabolism. Lipid metabolism alterations were mostly tissue specific in the kidney, nerve, and retina; no lipid changes correlated between the plasma and all three tissue types. However, alterations in diacylglycerol and in lipids containing arachidonic acid, an inflammatory mediator, were shared among the tissue types, and the highly saturated cholesterol esters were similarly coregulated between plasma and each tissue type in the diabetic mouse. Our results identified several patterns of altered lipid metabolism that may help to identify pathogenic alterations in different tissues and could be used as biomarkers in future research into diabetic microvascular tissue damage.

Published

2018

31. The effects of insulin and insulin-like growth factor I on amyloid precursor protein phosphorylation in in vitro and in vivo models of Alzheimer's disease

Author

Bhumsoo Kim, Sarah E. Elzinga, Rosemary E. Henn, Lisa M. McGinley, and Eva L. Feldman

Subjects

Alzheimer's disease, IGF-I, Insulin, Amyloid precursor protein, Insulin resistance, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Alzheimer's disease (AD) is a growing problem worldwide, and there are currently no effective treatments for this devastating disease. The neurotrophic growth factors insulin and insulin-like growth factor-I (IGF-I) are currently being investigated as potential therapeutic approaches for AD in preclinical and clinical studies. However, given that the metabolic syndrome (MetS) and diabetes are risk factors for AD, it is unknown how associated insulin resistance (IR) in the brain may impact the effectiveness of these therapies for AD. In this report, we therefore investigated the mechanisms underlying the effects of insulin and IGF-I on AD-associated pathology in the context of IR, with particular emphasis on phosphorylation of amyloid precursor protein (APP), a key step in promoting amyloid plaque formation in AD. Both insulin and IGF-I decreased APP phosphorylation in cultured primary cortical neurons, supporting their therapeutic use in AD. Induction of IR blocked the beneficial effect of insulin and reduced the effect of IGF-I on APP dephosphorylation. These effects were mediated by the phosphatidylinositol 3-kinase (PI3-K)/protein kinase B (Akt) pathway, as inhibition of this pathway during IR restored the effect of IGF-I on APP dephosphorylation. Finally, we explored the translational relevance of these results in vivo by demonstrating that high fat diet fed mice, a robust model of IR and MetS, exhibited the expected increased brain APP phosphorylation. Overall, these data suggest that the beneficial therapeutic effect of insulin and IGF-I on APP phosphorylation is negatively impacted by IR, and suggest that insulin and IGF-I alone may not be appropriate therapies for AD patients with IR, MetS, or diabetes.

Published

2019

32. The dual roles of immunity in ALS: Injury overrides protection

Author

Benjamin J. Murdock, Diane E. Bender, Benjamin M. Segal, and Eva L. Feldman

Subjects

Amyotrophic lateral sclerosis, Central nervous system, Immune response, Mutant SOD1, Debris clearance, Repair, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive, fatal neurodegenerative disease affecting motor neurons. Disease progression is accompanied by a multi-phased immune response, and recent studies indicate that the immune system is not simply a bystander during disease, but plays an active role in shaping ALS pathology. The role of the immune system during ALS progression is highly complex, however, as it has been found to have a role in both enhancing neurodegeneration as well as protecting the central nervous system. Previous reports have established that the immune response can therefore be separated into two distinct phases: a protective Type 2 response followed by a neurotoxic Type 1 response. This review will address the two phases of the immune response in ALS and describe their roles during disease progression. More importantly, it will also examine the likely sources of immune polarization that are responsible for shifting immunity from the protective T2 phase to the neurotoxic T1 phase.

Published

2015

33. BTBR ob/ob mice as a novel diabetic neuropathy model: Neurological characterization and gene expression analyses

Author

Phillipe D. O'Brien, Junguk Hur, John M. Hayes, Carey Backus, Stacey A. Sakowski, and Eva L. Feldman

Subjects

Type-2 diabetes, Obesity, Diabetic neuropathy, Mouse model, Leptin, Gene expression analysis, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Given the lack of treatments for diabetic neuropathy (DN), a common diabetic complication, accurate disease models are necessary. Characterization of the leptin-deficient BTBR ob/ob mouse, a type 2 diabetes model, demonstrated that the mice develop robust diabetes coincident with severe neuropathic features, including nerve conduction deficits and intraepidermal nerve fiber loss by 9 and 13 weeks of age, respectively, supporting its use as a DN model. To gain insight into DN mechanisms, we performed microarray analysis on sciatic nerve from BTBR ob/ob mice, identifying 1503 and 642 differentially expressed genes associated with diabetes at 5 and 13 weeks, respectively. Further analyses identified overrepresentation of inflammation and immune-related functions in BTBR ob/ob mice, which interestingly were more highly represented at 5 weeks, an observation that may suggest a contributory role in DN onset. To complement the gene expression analysis, we demonstrated that protein levels of select cytokines were significantly upregulated at 13 weeks in BTBR ob/ob mouse sciatic nerve. Furthermore, we compared our array data to that from an established DN model, the C57BKS db/db mouse, which reflected a common dysregulation of inflammatory and immune-related pathways. Together, our data demonstrate that BTBR ob/ob mice develop rapid and robust DN associated with dysregulated inflammation and immune-related processes.

Published

2015

34. Intraspinal transplantation of neurogenin-expressing stem cells generates spinal cord neural progenitors

Author

J. Simon Lunn, Crystal Pacut, Emily Stern, Stacey A. Sakowski, J. Matthew Velkey, Sue O'Shea, and Eva L. Feldman

Subjects

Embryonic stem cells, Neurogenin1, Neural specification, Spinal cord, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Embryonic stem (ES) cells and their derivatives are an important resource for developing novel cellular therapies for disease. Controlling proliferation and lineage selection, however, are essential to circumvent the possibility of tumor formation and facilitate the safe translation of ES-based therapies to man. Expression of appropriate transcription factors is one approach to direct the differentiation of ES cells towards a specific lineage and stop proliferation. Neural differentiation can be initiated in ES cells by expression of Neurogenin1 (Ngn1). In this study we investigate the effects of controlled Ngn1 expression on mouse ES (mES) cell differentiation in vitro and following grafting into the rat spinal cord. In vitro, Ngn1 expression in mES cells leads to rapid and specific neural differentiation, and a concurrent decrease in proliferation. Similarly transplantation of Ngn1-expressing mES cells into the spinal cord lead to in situ differentiation and spinal precursor formation. These data demonstrate that Ngn1 expression in mES cells is sufficient promote neural differentiation and inhibit proliferation, thus establishing an approach to safely graft ES cells into the spinal cord.

Published

2012

35. Nerve growth factor/p38 signaling increases intraepidermal nerve fiber densities in painful neuropathy of type 2 diabetes

Author

Hsinlin T. Cheng, Jacqueline R. Dauch, John M. Hayes, Brandon M. Yanik, and Eva L. Feldman

Subjects

Diabetic pain, Intraepidermal nerve fibers, Type 2 diabetes, Nerve growth factor, Peptidergic nerve fibers, Mechanical allodynia, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Painful diabetic neuropathy (PDN) is a common, yet devastating complication of type 2 diabetes. At this time, there is no objective test for diagnosing PDN. In the current study, we measured the peptidergic intraepidermal nerve fiber densities (IENFD) from hind paws of the db/db mouse, an animal model for type 2 diabetes, during the period of mechanical allodynia from 6 to 12 weeks of age. Intraepidermal nerve fibers (IENF) of the hind footpads were identified by protein gene product (PGP) 9.5 immunohistochemistry. The peptidergic IENF were determined by double immunofluorescence using anti-PGP9.5 and antibodies against tropomyosin-receptor-kinase (Trk) A. We observed a significant increase in PGP9.5-positive IENFD at 8 and 10 weeks of age. Similarly, Trk A-positive peptidergic IENF, which also express substance P and calcitonin gene related peptide in db/db mice, were observed to be elevated from 1.5 to 2 fold over controls. This upregulation ended at 16 weeks of age, in accordance with the reduction of mechanical allodynia. Anti-NGF treatment significantly inhibited the upregulation of peptidergic IENFD during the period of mechanical allodynia, suggesting that increased neurotrophism may mediate this phenomenon. In addition, SB203580, an inhibitor of p38, blocked the increase in peptidergic IENFD in db/db mice. The current results suggest that peptidergic IENFD could be a potential diagnostic indicator for PDN in type 2 diabetes. Furthermore, the inhibition of NGF-p38 signaling could be a potential therapeutic strategy for treating this painful condition.

Published

2012

36. Intraspinal cord delivery of IGF-I mediated by adeno-associated virus 2 is neuroprotective in a rat model of familial ALS

Author

Colin K. Franz, Thais Federici, Jun Yang, Carey Backus, Sang Su Oh, Qingshan Teng, Erin Carlton, Kathie M. Bishop, Mehdi Gasmi, Raymond T. Bartus, Eva L. Feldman, and Nicholas M. Boulis

Subjects

Amyotrophic lateral sclerosis, Insulin-like growth factor-I, Motor neuron, Neuroprotection, Spinal cord, Gene therapy, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Background: Amyotrophic lateral sclerosis (ALS) is a devastating disease that is characterized by the progressive loss of motor neurons. Patients with ALS usually die from respiratory failure due to respiratory muscle paralysis. Consequently, therapies aimed at preserving segmental function of the respiratory motor neurons could extend life for these patients. Insulin-like growth factor-I (IGF-I) is known to be a potent survival factor for motor neurons. In this study we induced high levels of IGF-I expression in the cervical spinal cord of hSOD1G93A rats with intraspinal cord (ISC) injections of an adeno-associated virus serotype 2 vector (CERE-130). This approach reduced the extent of motor neuron loss in the treated segments of the spinal cord. However, a corresponding preservation of motor function was observed in male, but not female, hSOD1G93A rats. We conclude that ISC injection of CERE-130 has the potential to protect motor neurons and preserve neuromuscular function in ALS.

Published

2009

37. Oxidative injury and neuropathy in diabetes and impaired glucose tolerance

Author

James W. Russell, Alison Berent-Spillson, Andrea M. Vincent, Catherine L. Freimann, Kelli A. Sullivan, and Eva L. Feldman

Subjects

Neuropathy, Diabetes, Impaired glucose tolerance, Oxidative stress, Axons, Dorsal root ganglia, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Clinical studies suggest that impaired glucose tolerance (IGT) is associated with the development of neuropathy. The aim of the current study was to determine if neuropathy developed in the female Zucker Diabetic Fatty (ZDF) rat, an animal model of IGT and type 2 diabetes. The ZDF rat develops impaired glucose tolerance (IGT) when fed a control diet, and frank diabetes when fed a high fat diet. Following 10 weeks of hyperglycemia, sensory nerve action potentials (SNAP) and compound motor action potentials (CMAP) were reduced and sensory conduction velocities were slowed (distal>proximal) in the tail and hind limb in ZDF animals with IGT and frank diabetes (p

Published

2008

38. Mouse models of diabetic neuropathy

Author

Kelli A. Sullivan, John M. Hayes, Timothy D. Wiggin, Carey Backus, Sang Su Oh, Stephen I. Lentz, Frank Brosius, III, and Eva L. Feldman

Subjects

BKS, Streptozotocin, B6Ins2Akita, Sciatic nerve, Dorsal root ganglia, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Diabetic neuropathy (DN) is a debilitating complication of type 1 and type 2 diabetes. Rodent models of DN do not fully replicate the pathology observed in human patients. We examined DN in streptozotocin (STZ)-induced [B6] and spontaneous type 1 diabetes [B6Ins2Akita] and spontaneous type 2 diabetes [B6-db/db, BKS-db/db]. Despite persistent hyperglycemia, the STZ-treated B6 and B6Ins2Akita mice were resistant to the development of DN. In contrast, DN developed in both type 2 diabetes models: the B6-db/db and BKS-db/db mice. The persistence of hyperglycemia and development of DN in the B6-db/db mice required an increased fat diet while the BKS-db/db mice developed severe DN and remained hyperglycemic on standard mouse chow. Our data support the hypothesis that genetic background and diet influence the development of DN and should be considered when developing new models of DN.

Published

2007

39. Mitochondria in DRG neurons undergo hyperglycemic mediated injury through Bim, Bax and the fission protein Drp1

Author

Gina M. Leinninger, Carey Backus, Ann Marie Sastry, Yun-Bo Yi, Chia-Wei Wang, and Eva L. Feldman

Subjects

Dorsal root ganglion, Glucose, Bim, Bax, Drp1, IGF-I, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Dorsal root ganglia (DRG) neurons degenerate in diabetic neuropathy (DN) and exhibit mitochondrial damage. We studied mitochondria of cultured DRG neurons exposed to high glucose as an in vitro model of DN. High glucose sequentially increases the expression, activation and localization of the pro-apoptotic proteins Bim and Bax and the mitochondrial fission protein dynamin-regulated protein 1 (Drp1). High glucose causes association of Drp1/Bax, similar to other apoptotic stimuli. Collectively, these events promote mitochondrial fragmentation and reduce mitochondrial number, suggestive of apoptotic mitochondrial fission. Drp1 is also upregulated in DRG from experimentally diabetic rats, suggesting a role for mitochondrial fission in DN. Insulin-like growth factor-I (IGF-I) protects high glucose-treated DRG neurons by preventing mitochondrial accumulation of Bim and Bax but does not modulate Drp1 expression or localization. We propose that mitochondria are compromised by convergence of Bim/Bax proteins with Drp1, which contributes to high glucose-induced injury in DRG neurons.

Published

2006

40. Integrin Expression Regulates Neuroblastoma Attachment and Migration

Author

Amy Meyer, Cynthia M. van Golen, Bhumsoo Kim, Kenneth L. van Golen, and Eva L. Feldman

Subjects

Neuroblastoma, integrins, attachment, migration, fibronectin, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Neuroblastoma (NBL) is the most common malignant disease of infancy, and children with bone metastasis have a mortality rate greater than 90%. Two major classes of proteins, integrins and growth factors, regulate the metastatic process. We have previously shown that tumorigenic NBL cells express higher levels of the type I insulin-like growth factor receptor (IGF-IR) and that β1 integrin expression is inversely proportional to tumorigenic potential in NBL. In the current study, we analyze the effect of β1 integrin and IGF-IR on NBL cell attachment and migration. Nontumorigenic S-cells express high levels of β1 integrin, whereas tumorigenic N-cells express little β1 integrin. Alterations in (3, integrin are due to regulation at the protein level, as translation is decreased in N-type cells. Moreover, inhibition of protein synthesis shows that β1 integrin is degraded more slowly in S-type cells (SHEP) than in N-type cells (SH-SY5Y and IMR32). Inhibition of α5β1 integrin prevents SHEP (but not SH-SY5Y or IMR32) cell attachment to fibronectin and increases SHEP cell migration. Increases in IGF-IR decrease β1 integrin expression, and enhance SHEP cell migration, potentially through increased expression of αvβ3. These data suggest that specific classes of integrins in concert with IGF-IR regulate NBL attachment and migration.

Published

2004

41. Degradation and Dephosphorylation of Focal Adhesion Kinase During Okadaic Acid-Induced Apoptosis in Human Neuroblastoma Cells

Author

Bhumsoo Kim, Cynthia M. van Golen, and Eva L. Feldman

Subjects

Neuroblastoma, focal adhesion kinase, insulin-like growth factor-I, okadaic acid, apoptosis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Focal adhesion kinase (FAK) prevents apoptosis in many cell types. We have reported that tyrosine residues in FAK are dephosphorylated and FAK is degraded during mannitol-induced apoptosis in human neuroblastoma cells. Several studies suggest that FAK dephosphorylation and degradation are separate events. The current study defines the relationship between FAK dephosphorylation and degradation in neuroblastoma cells using okadaic acid (OA). OA, a serine phosphatase inhibitor, promotes serinetthreonine phosphorylation, which in turn blocks tyrosine phosphorylation. OA induced focal adhesion loss, actin cytoskeleton disorganization, cellular detachment, which corresponded to a loss of FAK Tyr397 phosphorylation. These changes preceded caspase-3 activation, Akt and MAP kinase activity loss, protein ubiquitination, cellular apoptosis. Insulin-like growth factor-I prevented mannitol-induced, but not OA-induced, substrate detachment and FAK Tyr397 dephosphorylation, the effects of OA on FAK Tyr397 phosphorylation were irreversible. The proteolytic degradation of FAK is temporally distinct from its tyrosine dephosphorylation, occurring when apoptotic pathways are already initiated and during a generalized destruction of signaling proteins. Therefore, agents resulting in the dephosphorylation of FAK may be beneficial for therapeutic treatment, irrespective of FAK protein levels, as this may result in apoptosis, which cannot be prevented by growth factor signaling.

Published

2003

42. Insulin-like Growth Factor-I in Muscle Metabolism and Myotherapies

Author

J.Robinson Singleton and Eva L. Feldman

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The critical anabolic and trophic role of signaling by insulin-like growth factors (IGF) I and II via the type-I IGF receptor (IGF-IR) is reviewed throughout the life of skeletal myocytes. The proliferative effects of IGF-IR stimulation, both during embryogenesis and during satellite cell proliferation following denervation or muscle injury, are mediated primarily through activation of mitogen-activated protein kinases. Signaling through phosphatidylinositol 3-kinase is essential to muscle protein synthesis and glucose uptake and may contribute to the observed resilience of mature muscle to programmed cell death. Degeneration or inhibition of the GH–IGF-I axis by aging, cachexia, sepsis, diabetes, drugs, and disuse all enhance muscle catabolism, and opposition of these effects by IGF-I may form the basis of effective myotherapy.

Published

2001

43. Neurons Undergo Apoptosis in Animal and Cell Culture Models of Diabetes

Author

James W. Russell, Kelli A. Sullivan, Anthony J. Windebank, David N. Herrmann, and Eva L. Feldman

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Recent clinical trials indicate that the severity of diabetic neuropathy is correlated with the level of patient glycemic control. In the current study, hyperglycemia induces apoptotic changes in dorsal root ganglion neurons and Schwann cells in vivo both in streptozotocin-treated diabetic rats and in rats made acutely hyperglycemic with infused glucose. Typical apoptotic nuclear and cytoplasmic changes are observed. In addition mitochondrial changes recently reported to occur as part of the apoptotic cascade, such as ballooning of mitochondria and disruption of the internal cristae, are seen in diabetic dorsal root ganglion neurons and Schwann cells. Similar changes have been reported in neurons in the presence of oxidative stress. In order to study the neurotoxic effects of high glucose we developed an in vitro model using rat dorsal root ganglion neurons. In dorsal root ganglion cultured in defined medium, addition of moderate glucose levels results in neurite degeneration and apoptosis. These changes are coupled with activation of caspase-3, dependent on the concentration of glucose. The apoptotic changes observed in vitro are similar to those observed in vivo. In contrast, addition of IGF-I, even at physiological concentrations, prevents activation of caspase-3 and neuronal apoptosis in vitro. We suggest that oxidative stress may promote the mitochondrial changes in diabetic animals and lead to activation of programmed cell death caspase pathways. These results imply a new pathogenetic mechanism for diabetic sensory neuropathy.

Published

1999

44. Insulin-like Growth Factors Regulate Neuronal Differentiation and Survival

Author

Eva L. Feldman, Kelli A. Sullivan, Bhumsoo Kim, and James W. Russell

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Insulin-like growth factor I (IGF-I) and IGF-II are potent trophic factors for motor and sensory neurons and glial cells. The actions of IGF-I and IGF-II are mediated via the IGF-I receptor (IGF-IR). IGF:IGF-IR binding activates distinct signaling cascades, which in turn mediate the trophic effects of the IGFs. We discuss three main IGF coupled events: growth cone motility, long-term neurite outgrowth, and neuroprotection. Our data suggest that IGF-I enhances growth cone motility by promoting reorganization of actin and activation of focal adhesion proteins via the phosphatidylinositol-3 kinase (PI-3K) pathway. Long-term treatment with IGF-I activates the mitogen-activated protein (MAP) kinase cascade and promotes neurite outgrowth. A separable, but likely linked, action of the IGFs via PI-3K is protection of neurons from apoptosis. These pleotrophic effects of IGFs suggest that this family of growth factors may have potential clinical utility in the treatment of neurological disorders.

Published

1997