Your search keyword '"CNS disorders"' showing total 301 results

1. Blood‐brain barrier dysfunction and decreased transcription of tight junction proteins in epileptic dogs

Author

Erez Hanael, Shelly Baruch, Rotem Kalev Altman, Orit Chai, Kira Rapoport, Dana Peery, Alon Friedman, and Merav H. Shamir

Subjects

blood‐brain barrier, claudin 5, CNS disorders, epilepsy, Kir 4.1, MMP9, Veterinary medicine, SF600-1100

Abstract

Abstract Background Epilepsy in dogs and humans is associated with blood‐brain barrier (BBB) dysfunction (BBBD), which may involve dysfunction of tight junction (TJ) proteins, matrix metalloproteases, and astrocytes. Imaging techniques to assess BBB integrity, to identify potential treatment strategies, have not yet been evaluated in veterinary medicine. Hypothesis Some dogs with idiopathic epilepsy (IE) will exhibit BBBD. Identifying BBBD may improve antiepileptic treatment in the future. Animals Twenty‐seven dogs with IE and 10 healthy controls. Methods Retrospective, prospective cohort study. Blood‐brain barrier permeability (BBBP) scores were calculated for the whole brain and piriform lobe of all dogs by using dynamic contrast enhancement (DCE) magnetic resonance imaging (MRI) and subtraction enhancement analysis (SEA). Matrix metalloproteinase‐9 (MMP9) activity in serum and cerebrospinal fluid (CSF) was measured and its expression in the piriform lobe was examined using immunofluorescent staining. Gene expression of TJ proteins and astrocytic transporters was analyzed in the piriform lobe. Results The DCE‐MRI analysis of the piriform lobe identified higher BBBP score in the IE group when compared with controls (34.5% vs 26.5%; P = .02). Activity and expression of MMP9 were increased in the serum, CSF, and piriform lobe of IE dogs as compared with controls. Gene expression of Kir4.1 and claudin‐5 in the piriform lobe of IE dogs was significantly lower than in control dogs. Conclusions and Clinical Importance Our findings demonstrate BBBD in dogs with IE and were supported by increased MMP9 activity and downregulation of astrocytic potassium channels and some TJ proteins. Blood brain barrier dysfunction may be a novel antiepileptic therapy target.

Published

2024

2. Blood‐brain barrier dysfunction and decreased transcription of tight junction proteins in epileptic dogs.

Author

Hanael, Erez, Baruch, Shelly, Altman, Rotem Kalev, Chai, Orit, Rapoport, Kira, Peery, Dana, Friedman, Alon, and Shamir, Merav H.

Subjects

*MAGNETIC resonance imaging, *POTASSIUM channels, *CARRIER proteins, *TIGHT junctions, *GENE expression

Abstract

Background: Epilepsy in dogs and humans is associated with blood‐brain barrier (BBB) dysfunction (BBBD), which may involve dysfunction of tight junction (TJ) proteins, matrix metalloproteases, and astrocytes. Imaging techniques to assess BBB integrity, to identify potential treatment strategies, have not yet been evaluated in veterinary medicine. Hypothesis: Some dogs with idiopathic epilepsy (IE) will exhibit BBBD. Identifying BBBD may improve antiepileptic treatment in the future. Animals: Twenty‐seven dogs with IE and 10 healthy controls. Methods: Retrospective, prospective cohort study. Blood‐brain barrier permeability (BBBP) scores were calculated for the whole brain and piriform lobe of all dogs by using dynamic contrast enhancement (DCE) magnetic resonance imaging (MRI) and subtraction enhancement analysis (SEA). Matrix metalloproteinase‐9 (MMP9) activity in serum and cerebrospinal fluid (CSF) was measured and its expression in the piriform lobe was examined using immunofluorescent staining. Gene expression of TJ proteins and astrocytic transporters was analyzed in the piriform lobe. Results: The DCE‐MRI analysis of the piriform lobe identified higher BBBP score in the IE group when compared with controls (34.5% vs 26.5%; P =.02). Activity and expression of MMP9 were increased in the serum, CSF, and piriform lobe of IE dogs as compared with controls. Gene expression of Kir4.1 and claudin‐5 in the piriform lobe of IE dogs was significantly lower than in control dogs. Conclusions and Clinical Importance: Our findings demonstrate BBBD in dogs with IE and were supported by increased MMP9 activity and downregulation of astrocytic potassium channels and some TJ proteins. Blood brain barrier dysfunction may be a novel antiepileptic therapy target. [ABSTRACT FROM AUTHOR]

Published

2024

3. Orexins in apoptosis: a dual regulatory role.

Author

Cavalu, Simona, Saber, Sameh, Hamad, Rabab S., Abdel-Reheim, Mustafa Ahmed, Elmorsy, Elsayed A., and Youssef, Mahmoud E.

Subjects

OREXINS, APOPTOSIS, PERIPHERAL nervous system, SLEEP-wake cycle, LUNGS, CENTRAL nervous system, NEUROPEPTIDES

Abstract

The orexins, also referred to as hypocretins, are neuropeptides that originate from the lateral hypothalamus (LH) region of the brain. They are composed of two small peptides, orexin-A, and orexin-B, which are broadly distributed throughout the central and peripheral nervous systems. Orexins are recognized to regulate diverse functions, involving energy homeostasis, the sleep-wake cycle, stress responses, and reward-seeking behaviors. Additionally, it is suggested that orexin-A deficiency is linked to sleepiness and narcolepsy. The orexins bind to their respective receptors, the orexin receptor type 1 (OX1R) and type 2 (OX2R), and activate different signaling pathways, which results in the mediation of various physiological functions. Orexin receptors are widely expressed in different parts of the body, including the skin, muscles, lungs, and bone marrow. The expression levels of orexins and their receptors play a crucial role in apoptosis, which makes them a potential target for clinical treatment of various disorders. This article delves into the significance of orexins and orexin receptors in the process of apoptosis, highlighting their expression levels and their potential contributions to different diseases. The article offers an overview of the existing understanding of the orexin/receptor system and how it influences the regulation of apoptosis. [ABSTRACT FROM AUTHOR]

Published

2024

4. MicroRNA-based interventions in aberrant cell cycle diseases: Therapeutic strategies for cancers, central nervous system disorders and comorbidities

Author

Xiaojuan Tang, Yuan Ren, Wen Zeng, Xiaoting Feng, Min He, Yuan Lv, Yongmin Li, and Yongheng He

Subjects

MicroRNA, Aberrant cell cycle, Cancer, CNS Disorders, Exosome, Signaling pathways, Therapeutics. Pharmacology, RM1-950

Abstract

Malignant tumors and central nervous system (CNS) disorders are intricately linked to a process known as ''aberrant cell cycle re-entry,'' which plays a critical role in the progression of these diseases. Addressing the dysregulation in cell cycles offers a promising therapeutic approach for cancers and CNS disorders. MicroRNAs (miRNAs) play a crucial role as regulators of gene expression in cell cycle transitions, presenting a promising therapeutic avenue for treating these disorders and their comorbidities. This review consolidates the progress made in the last three years regarding miRNA-based treatments for diseases associated with aberrant cell cycle re-entry. It encompasses exploring fundamental mechanisms and signaling pathways influenced by miRNAs in cancers and CNS disorders, particularly focusing on the therapeutic effects of exosome-derived miRNAs. The review also identifies specific miRNAs implicated in comorbidity of cancers and CNS disorders, discusses the future potential of miRNA reagents in managing cell cycle-related diseases.

Published

2024

5. Plant-derived bioactive compounds and their novel role in central nervous system disorder treatment via ATF4 targeting: A systematic literature review

Author

Nan Zhang, Shun Zhang, and Xiaoyu Dong

Subjects

ATF4, plant-derived bioactive compounds, CNS disorders, neuroprotection, systematic review, Therapeutics. Pharmacology, RM1-950

Abstract

Central nervous system (CNS) disorders exhibit exceedingly intricate pathogenic mechanisms. Pragmatic and effective solutions remain elusive, significantly compromising human life and health. Activating transcription factor 4 (ATF4) participates in the regulation of multiple pathophysiological processes, including CNS disorders. Considering the widespread involvement of ATF4 in the pathological process of CNS disorders, the targeted regulation of ATF4 by plant-derived bioactive compounds (PDBCs) may become a viable strategy for the treatment of CNS disorders. However, the regulatory relationship between PDBCs and ATF4 remains incompletely understood. Here, we aimed to comprehensively review the studies on PDBCs targeting ATF4 to ameliorate CNS disorders, thereby offering novel directions and insights for the treatment of CNS disorders. A computerized search was conducted on PubMed, Embase, Web of Science, and Google Scholar databases to identify preclinical experiments related to PDBCs targeting ATF4 for the treatment of CNS disorders. The search timeframe was from the inception of the databases to December 2023. Two assessors conducted searches using the keywords ''ATF4,'' ''Central Nervous System,'' ''Neurological,'' ''Alzheimer's disease,'' ''Parkinson's Disease,'' ''Stroke,'' ''Spinal Cord Injury,'' ''Glioblastoma,'' ''Traumatic Brain Injury,'' and ''Spinal Cord Injury.'' Overall, 31 studies were included, encompassing assessments of 27 PDBCs. Combining results from in vivo and in vitro studies, we observed that these PDBCs, via ATF4 modulation, prevent the deposition of amyloid-like fibers such as Aβ, tau, and α-synuclein. They regulate ERS, reduce the release of inflammatory factors, restore mitochondrial membrane integrity to prevent oxidative stress, regulate synaptic plasticity, modulate autophagy, and engage anti-apoptotic mechanisms. Consequently, they exert neuroprotective effects in CNS disorders. Numerous PDBCs targeting ATF4 have shown potential in facilitating the restoration of CNS functionality, thereby presenting expansive prospects for the treatment of such disorders. However, future endeavors necessitate high-quality, large-scale, and comprehensive preclinical and clinical studies to further validate this therapeutic potential.

Published

2024

6. Impact of NQO1 dysregulation in CNS disorders

Author

Li Yuhan, Maryam Khaleghi Ghadiri, and Ali Gorji

Subjects

Brain, CNS disorders, Inflammation, Neurodegeneration, Neuronal excitability, NQO1, Medicine

Abstract

Abstract NAD(P)H Quinone Dehydrogenase 1 (NQO1) plays a pivotal role in the regulation of neuronal function and synaptic plasticity, cellular adaptation to oxidative stress, neuroinflammatory and degenerative processes, and tumorigenesis in the central nervous system (CNS). Impairment of the NQO1 activity in the CNS can result in abnormal neurotransmitter release and clearance, increased oxidative stress, and aggravated cellular injury/death. Furthermore, it can cause disturbances in neural circuit function and synaptic neurotransmission. The abnormalities of NQO1 enzyme activity have been linked to the pathophysiological mechanisms of multiple neurological disorders, including Parkinson's disease, Alzheimer's disease, epilepsy, multiple sclerosis, cerebrovascular disease, traumatic brain injury, and brain malignancy. NQO1 contributes to various dimensions of tumorigenesis and treatment response in various brain tumors. The precise mechanisms through which abnormalities in NQO1 function contribute to these neurological disorders continue to be a subject of ongoing research. Building upon the existing knowledge, the present study reviews current investigations describing the role of NQO1 dysregulations in various neurological disorders. This study emphasizes the potential of NQO1 as a biomarker in diagnostic and prognostic approaches, as well as its suitability as a target for drug development strategies in neurological disorders.

Published

2024

7. Impact of NQO1 dysregulation in CNS disorders.

Author

Yuhan, Li, Khaleghi Ghadiri, Maryam, and Gorji, Ali

Subjects

*ALZHEIMER'S disease, *NEUROLOGICAL disorders, *CENTRAL nervous system, *PARKINSON'S disease, *BRAIN injuries

Abstract

NAD(P)H Quinone Dehydrogenase 1 (NQO1) plays a pivotal role in the regulation of neuronal function and synaptic plasticity, cellular adaptation to oxidative stress, neuroinflammatory and degenerative processes, and tumorigenesis in the central nervous system (CNS). Impairment of the NQO1 activity in the CNS can result in abnormal neurotransmitter release and clearance, increased oxidative stress, and aggravated cellular injury/death. Furthermore, it can cause disturbances in neural circuit function and synaptic neurotransmission. The abnormalities of NQO1 enzyme activity have been linked to the pathophysiological mechanisms of multiple neurological disorders, including Parkinson's disease, Alzheimer's disease, epilepsy, multiple sclerosis, cerebrovascular disease, traumatic brain injury, and brain malignancy. NQO1 contributes to various dimensions of tumorigenesis and treatment response in various brain tumors. The precise mechanisms through which abnormalities in NQO1 function contribute to these neurological disorders continue to be a subject of ongoing research. Building upon the existing knowledge, the present study reviews current investigations describing the role of NQO1 dysregulations in various neurological disorders. This study emphasizes the potential of NQO1 as a biomarker in diagnostic and prognostic approaches, as well as its suitability as a target for drug development strategies in neurological disorders. [ABSTRACT FROM AUTHOR]

Published

2024

8. Nose-to-Brain (N2B) Delivery: An Alternative Route for the Delivery of Biologics in the Management and Treatment of Central Nervous System Disorders.

Author

Patharapankal, Elizabeth J., Ajiboye, Adejumoke Lara, Mattern, Claudia, and Trivedi, Vivek

Subjects

*CENTRAL nervous system, *SKIN permeability, *DRUG administration routes, *CENTRAL nervous system diseases, *BIOLOGICALS, *NASAL cavity

Abstract

In recent years, there have been a growing number of small and large molecules that could be used to treat diseases of the central nervous system (CNS). Nose-to-brain delivery can be a potential option for the direct transport of molecules from the nasal cavity to different brain areas. This review aims to provide a compilation of current approaches regarding drug delivery to the CNS via the nose, with a focus on biologics. The review also includes a discussion on the key benefits of nasal delivery as a promising alternative route for drug administration and the involved pathways or mechanisms. This article reviews how the application of various auxiliary agents, such as permeation enhancers, mucolytics, in situ gelling/mucoadhesive agents, enzyme inhibitors, and polymeric and lipid-based systems, can promote the delivery of large molecules in the CNS. The article also includes a discussion on the current state of intranasal formulation development and summarizes the biologics currently in clinical trials. It was noted that significant progress has been made in this field, and these are currently being applied to successfully transport large molecules to the CNS via the nose. However, a deep mechanistic understanding of this route, along with the intimate knowledge of various excipients and their interactions with the drug and nasal physiology, is still necessary to bring us one step closer to developing effective formulations for nasal–brain drug delivery. [ABSTRACT FROM AUTHOR]

Published

2024

9. Orexins in apoptosis: a dual regulatory role

Author

Simona Cavalu, Sameh Saber, Rabab S. Hamad, Mustafa Ahmed Abdel-Reheim, Elsayed A. Elmorsy, and Mahmoud E. Youssef

Subjects

orexins, apoptosis, CNS disorders, neuroprotection, cell signaling, new therapeutic target, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The orexins, also referred to as hypocretins, are neuropeptides that originate from the lateral hypothalamus (LH) region of the brain. They are composed of two small peptides, orexin-A, and orexin-B, which are broadly distributed throughout the central and peripheral nervous systems. Orexins are recognized to regulate diverse functions, involving energy homeostasis, the sleep-wake cycle, stress responses, and reward-seeking behaviors. Additionally, it is suggested that orexin-A deficiency is linked to sleepiness and narcolepsy. The orexins bind to their respective receptors, the orexin receptor type 1 (OX1R) and type 2 (OX2R), and activate different signaling pathways, which results in the mediation of various physiological functions. Orexin receptors are widely expressed in different parts of the body, including the skin, muscles, lungs, and bone marrow. The expression levels of orexins and their receptors play a crucial role in apoptosis, which makes them a potential target for clinical treatment of various disorders. This article delves into the significance of orexins and orexin receptors in the process of apoptosis, highlighting their expression levels and their potential contributions to different diseases. The article offers an overview of the existing understanding of the orexin/receptor system and how it influences the regulation of apoptosis.

Published

2024

10. Presumptive phenobarbital‐induced systemic lupus erythematosus in a domestic dog

Author

Erin Phillips, Matthew Kornya, Allison Collier, Maureen Barry, Katherine Morrison, and Felipe Reggeti

Subjects

autoimmunity, CNS disorders, drug reaction, epilepsy, immunology, lupus, Veterinary medicine, SF600-1100

Abstract

Abstract Case Description We describe a case of presumptive acquired systemic lupus erythematosus secondary to phenobarbital administration in a dog, which resolved with withdrawal of the drug. Clinical Findings A 3.5 year‐old poodle presented to a veterinary teaching hospital for Tier 1 idiopathic epilepsy and was treated with phenobarbital. The dog experienced fever, multiple cytopenias, and proteinuria in conjunction with a positive antinuclear antibody (ANA) titer. Diagnostics Serial CBCs, urine protein : creatinine ratios, and sternal bone marrow aspirates were performed to evaluate improvement. Treatment and Outcome Phenobarbital was withdrawn and levetiracetam initiated. All abnormalities resolved with supportive care, without initiation of immunosuppressive drugs. All cytopenias and proteinuria resolved and ANA test results became negative within 3 months. The patient recovered and did well clinically. Clinical Relevance Systemic lupus erythematosus is a disease of multiple autoimmune syndromes occurring concurrently or sequentially in conjunction with the presence of circulating ANA. It has been well described in dogs as an idiopathic condition, but in human medicine may occur secondary to drug reactions (drug‐associated lupus) including as a reaction to phenobarbital. The findings in our case are consistent with the criteria for drug‐induced lupus in humans and we suggest it as the first report of phenobarbital‐induced lupus in a dog.

Published

2023

11. The T2‐FLAIR mismatch sign as an imaging biomarker for oligodendrogliomas in dogs

Author

Josefa Garcia‐Mora, Rell L. Parker, Thomas Cecere, John L. Robertson, and John H. Rossmeisl

Subjects

brain tumor, CNS disorders, magnetic resonance imaging, neuroimaging, neurology, oncology‐diagnosis, Veterinary medicine, SF600-1100

Abstract

Abstract Background In humans, the T2‐weighted (T2W)—fluid‐attenuated inversion recovery (FLAIR) mismatch sign (T2FMM) is a specific imaging biomarker for the isocitrate dehydrogenase 1 (IDH1)‐mutated, 1p/19q non‐codeleted low‐grade astrocytomas (LGA). The T2FMM is characterized by a homogeneous hyperintense T2W signal and a hypointense signal with a hyperintense peripheral rim on FLAIR sequences. In gliomas in dogs, the T2FMM has not been described. Hypotheses/Objectives In dogs with focal intra‐axial brain lesions, T2FMM will discriminate gliomas from other lesions. The T2FMM will be associated with the LGA phenotype and presence of microcysts on histopathology. Interobserver agreement for T2FMM magnetic resonance imaging (MRI) features will be high. Animals One hundred eighty‐six dogs with histopathologically diagnosed focal intra‐axial lesions on brain MRI including oligodendrogliomas (n = 90), astrocytomas (n = 47), undefined gliomas (n = 9), cerebrovascular accidents (n = 33), and inflammatory lesions (n = 7). Methods Two blinded raters evaluated the 186 MRI studies and identified cases with the T2FMM. Histopathologic and immunohistochemical slides of T2FMM cases were evaluated for morphologic features and IDH1‐mutations and compared to cases without the T2FMM. Gene expression analyses were performed on a subset of oligodendrogliomas (n = 10) with and without T2FMM. Results The T2FMM was identified in 14/186 (8%) of MRI studies, and all dogs with T2FMM had oligodendrogliomas (n = 12 low‐grade [LGO], n = 2 high‐grade [HGO]; P

Published

2023

12. Presumptive phenobarbital‐induced systemic lupus erythematosus in a domestic dog.

Author

Phillips, Erin, Kornya, Matthew, Collier, Allison, Barry, Maureen, Morrison, Katherine, and Reggeti, Felipe

Subjects

*SYSTEMIC lupus erythematosus, *DOGS, *DRUG side effects, *EPILEPSY, *IMMUNOSUPPRESSIVE agents, *ANTINUCLEAR factors

Abstract

Case Description: We describe a case of presumptive acquired systemic lupus erythematosus secondary to phenobarbital administration in a dog, which resolved with withdrawal of the drug. Clinical Findings: A 3.5 year‐old poodle presented to a veterinary teaching hospital for Tier 1 idiopathic epilepsy and was treated with phenobarbital. The dog experienced fever, multiple cytopenias, and proteinuria in conjunction with a positive antinuclear antibody (ANA) titer. Diagnostics: Serial CBCs, urine protein : creatinine ratios, and sternal bone marrow aspirates were performed to evaluate improvement. Treatment and Outcome: Phenobarbital was withdrawn and levetiracetam initiated. All abnormalities resolved with supportive care, without initiation of immunosuppressive drugs. All cytopenias and proteinuria resolved and ANA test results became negative within 3 months. The patient recovered and did well clinically. Clinical Relevance: Systemic lupus erythematosus is a disease of multiple autoimmune syndromes occurring concurrently or sequentially in conjunction with the presence of circulating ANA. It has been well described in dogs as an idiopathic condition, but in human medicine may occur secondary to drug reactions (drug‐associated lupus) including as a reaction to phenobarbital. The findings in our case are consistent with the criteria for drug‐induced lupus in humans and we suggest it as the first report of phenobarbital‐induced lupus in a dog. [ABSTRACT FROM AUTHOR]

Published

2023

13. Quantitative analysis of magnetic resonance images for characterization of blood‐brain barrier dysfunction in dogs with brain tumors

Author

Erez Hanael, Shelly Baruch, Orit Chai, Liron Lishitsky, Tal Blum, Kira Rapoport, Marco Ruggeri, Zahi Aizenberg, Dana Peery, Nina Meyerhoff, Holger Andreas Volk, Steven De Decker, Andrea Tipold, Wolfgang Baumgaertner, Alon Friedman, and Merav Shamir

Subjects

blood‐brain barrier, CNS disorders, epilepsy, glioma, meningioma, neurology, Veterinary medicine, SF600-1100

Abstract

Abstract Background Blood‐brain barrier (BBB) permeability can be assessed quantitatively using advanced imaging analysis. Hypothesis/Objectives Quantification and characterization of blood‐brain barrier dysfunction (BBBD) patterns in dogs with brain tumors can provide useful information about tumor biology and assist in distinguishing between gliomas and meningiomas. Animals Seventy‐eight hospitalized dogs with brain tumors and 12 control dogs without brain tumors. Methods In a 2‐arm study, images from a prospective dynamic contrast‐enhanced (DCE; n = 15) and a retrospective archived magnetic resonance imaging study (n = 63) were analyzed by DCE and subtraction enhancement analysis (SEA) to quantify BBB permeability in affected dogs relative to control dogs (n = 6 in each arm). For the SEA method, 2 ranges of postcontrast intensity differences, that is, high (HR) and low (LR), were evaluated as possible representations of 2 classes of BBB leakage. BBB score was calculated for each dog and was associated with clinical characteristics and tumor location and class. Permeability maps were generated, using the slope values (DCE) or intensity difference (SEA) of each voxel, and analyzed. Results Distinctive patterns and distributions of BBBD were identified for intra‐ and extra‐axial tumors. At a cutoff of 0.1, LR/HR BBB score ratio yielded a sensitivity of 80% and specificity of 100% in differentiating gliomas from meningiomas. Conclusions and Clinical Importance Blood‐brain barrier dysfunction quantification using advanced imaging analyses has the potential to be used for assessment of brain tumor characteristics and behavior and, particularly, to help differentiating gliomas from meningiomas.

Published

2023

14. Editorial: Neuroimaging of neuroinflammation in neurological disorders

Author

Md Nasir Uddin, Madalina E. Tivarus, Giovanni Schifitto, and David A. Rudko

Subjects

neuroimaging, neuroinflammation, CNS disorders, MRI, brain, Neurology. Diseases of the nervous system, RC346-429

Published

2023

15. Editorial: Spatiotemporal regulation of central nervous system disorders: molecular mechanisms and emerging techniques

Author

Yanrong Zheng and Weiwei Hu

Subjects

CNS disorders, spatiotemporal regulation, cell subpopulation, cell type-specific, neurodevelopment, spatially resolved transcriptomics, Biology (General), QH301-705.5

Published

2023

16. The Impact of Microbiota on the Gut–Brain Axis: Examining the Complex Interplay and Implications.

Author

Chaudhry, Tuba Shahid, Senapati, Sidhartha Gautam, Gadam, Srikanth, Mannam, Hari Priya Sri Sai, Voruganti, Hima Varsha, Abbasi, Zainab, Abhinav, Tushar, Challa, Apurva Bhavana, Pallipamu, Namratha, Bheemisetty, Niharika, and Arunachalam, Shivaram P.

Subjects

*ENTERIC nervous system, *CENTRAL nervous system, *GASTROINTESTINAL system, *LITERATURE reviews, *SENSORY perception, *SUBMUCOUS plexus

Abstract

The association and interaction between the central nervous system (CNS) and enteric nervous system (ENS) is well established. Essentially ENS is the second brain, as we call it. We tried to understand the structure and function, to throw light on the functional aspect of neurons, and address various disease manifestations. We summarized how various neurological disorders influence the gut via the enteric nervous system and/or bring anatomical or physiological changes in the enteric nervous system or the gut and vice versa. It is known that stress has an effect on Gastrointestinal (GI) motility and causes mucosal erosions. In our literature review, we found that stress can also affect sensory perception in the central nervous system. Interestingly, we found that mutations in the neurohormone, serotonin (5-HT), would result in dysfunctional organ development and further affect mood and behavior. We focused on the developmental aspects of neurons and cognition and their relation to nutritional absorption via the gastrointestinal tract, the development of neurodegenerative disorders in relation to the alteration in gut microbiota, and contrariwise associations between CNS disorders and ENS. This paper further summarizes the synergetic relation between gastrointestinal and neuropsychological manifestations and emphasizes the need to include behavioral therapies in management plans. [ABSTRACT FROM AUTHOR]

Published

2023

17. The T2‐FLAIR mismatch sign as an imaging biomarker for oligodendrogliomas in dogs.

Author

Garcia‐Mora, Josefa, Parker, Rell L., Cecere, Thomas, Robertson, John L., and Rossmeisl, John H.

Subjects

*OLIGODENDROGLIOMAS, *MAGNETIC resonance imaging, *STROKE, *DOGS, *ISOCITRATE dehydrogenase

Abstract

Background: In humans, the T2‐weighted (T2W)—fluid‐attenuated inversion recovery (FLAIR) mismatch sign (T2FMM) is a specific imaging biomarker for the isocitrate dehydrogenase 1 (IDH1)‐mutated, 1p/19q non‐codeleted low‐grade astrocytomas (LGA). The T2FMM is characterized by a homogeneous hyperintense T2W signal and a hypointense signal with a hyperintense peripheral rim on FLAIR sequences. In gliomas in dogs, the T2FMM has not been described. Hypotheses/Objectives: In dogs with focal intra‐axial brain lesions, T2FMM will discriminate gliomas from other lesions. The T2FMM will be associated with the LGA phenotype and presence of microcysts on histopathology. Interobserver agreement for T2FMM magnetic resonance imaging (MRI) features will be high. Animals: One hundred eighty‐six dogs with histopathologically diagnosed focal intra‐axial lesions on brain MRI including oligodendrogliomas (n = 90), astrocytomas (n = 47), undefined gliomas (n = 9), cerebrovascular accidents (n = 33), and inflammatory lesions (n = 7). Methods: Two blinded raters evaluated the 186 MRI studies and identified cases with the T2FMM. Histopathologic and immunohistochemical slides of T2FMM cases were evaluated for morphologic features and IDH1‐mutations and compared to cases without the T2FMM. Gene expression analyses were performed on a subset of oligodendrogliomas (n = 10) with and without T2FMM. Results: The T2FMM was identified in 14/186 (8%) of MRI studies, and all dogs with T2FMM had oligodendrogliomas (n = 12 low‐grade [LGO], n = 2 high‐grade [HGO]; P <.001). Microcystic change was significantly associated with the T2FMM (P <.00001). In oligodendrogliomas with T2FMM, IDH1‐mutations or specific differentially expressed genes were not identified. Conclusion and Clinical Importance: The T2FMM can be readily identified on routinely obtained MRI sequences. It is a specific biomarker for oligodendroglioma in dogs, and was significantly associated with non‐enhancing LGO. [ABSTRACT FROM AUTHOR]

Published

2023

18. Quantitative analysis of magnetic resonance images for characterization of blood‐brain barrier dysfunction in dogs with brain tumors.

Author

Hanael, Erez, Baruch, Shelly, Chai, Orit, Lishitsky, Liron, Blum, Tal, Rapoport, Kira, Ruggeri, Marco, Aizenberg, Zahi, Peery, Dana, Meyerhoff, Nina, Volk, Holger Andreas, De Decker, Steven, Tipold, Andrea, Baumgaertner, Wolfgang, Friedman, Alon, and Shamir, Merav

Subjects

*BRAIN tumors, *BLOOD-brain barrier, *MAGNETIC resonance imaging, *DOGS, *QUANTITATIVE research

Abstract

Background: Blood‐brain barrier (BBB) permeability can be assessed quantitatively using advanced imaging analysis. Hypothesis/Objectives: Quantification and characterization of blood‐brain barrier dysfunction (BBBD) patterns in dogs with brain tumors can provide useful information about tumor biology and assist in distinguishing between gliomas and meningiomas. Animals: Seventy‐eight hospitalized dogs with brain tumors and 12 control dogs without brain tumors. Methods: In a 2‐arm study, images from a prospective dynamic contrast‐enhanced (DCE; n = 15) and a retrospective archived magnetic resonance imaging study (n = 63) were analyzed by DCE and subtraction enhancement analysis (SEA) to quantify BBB permeability in affected dogs relative to control dogs (n = 6 in each arm). For the SEA method, 2 ranges of postcontrast intensity differences, that is, high (HR) and low (LR), were evaluated as possible representations of 2 classes of BBB leakage. BBB score was calculated for each dog and was associated with clinical characteristics and tumor location and class. Permeability maps were generated, using the slope values (DCE) or intensity difference (SEA) of each voxel, and analyzed. Results: Distinctive patterns and distributions of BBBD were identified for intra‐ and extra‐axial tumors. At a cutoff of 0.1, LR/HR BBB score ratio yielded a sensitivity of 80% and specificity of 100% in differentiating gliomas from meningiomas. Conclusions and Clinical Importance: Blood‐brain barrier dysfunction quantification using advanced imaging analyses has the potential to be used for assessment of brain tumor characteristics and behavior and, particularly, to help differentiating gliomas from meningiomas. [ABSTRACT FROM AUTHOR]

Published

2023

19. Intraosseous administration into the skull: Potential blood–brain barrier bypassing route for brain drug delivery.

Author

Kang, Ji Hee and Ko, Young Tag

Subjects

*BLOOD-brain barrier, *SKULL, *CENTRAL nervous system, *BRAIN diseases, *BONE marrow, *DRUG administration

Abstract

Progress in treating central nervous system (CNS) disorders is retarded owing to a limited understanding of brain disease pathology. Additionally, the blood–brain barrier (BBB) limits molecular entry into the brain. Many approaches for brain drug delivery to overcome the BBB, such as BBB permeability enhancement, transient BBB disruption, and direct surgical administration have been explored with limited success. Recent research has shown that direct vascular channels exist between the skull bone marrow and the meninges, allowing myeloid and lymphoid cells to migrate. We hypothesized that these direct channels may also allow brain drug delivery from the skull bone marrow to the brain. In this study, for the first time we propose intraosseous administration of drugs into the skull (intracalvariosseous [ICO]) as a novel approach for brain drug delivery via BBB bypassing routes. We tested the feasibility of the approach by applying nine representative compounds over thinned mouse skulls to simulate ICO and measuring the compound entry level in the brain compared to that after systemic administration. Surprisingly, we found that the skull is not completely impermeable to drug penetration into the brain and the tested compounds reached the brain tissue several tens‐to‐hundred times higher by ICO than systemic application. These findings suggest a role for the BBB bypassing route from skull to brain, apart from the systemic route, in the drug entry into the brain after ICO. This approach should be applicable to other CNS drugs and even BBB impermeable drugs. Overall ICO provides an innovative and advantageous pathway for effective treatment of brain diseases. [ABSTRACT FROM AUTHOR]

Published

2023

20. Nose-to-Brain (N2B) Delivery: An Alternative Route for the Delivery of Biologics in the Management and Treatment of Central Nervous System Disorders

Author

Elizabeth J. Patharapankal, Adejumoke Lara Ajiboye, Claudia Mattern, and Vivek Trivedi

Subjects

CNS disorders, nasal delivery, biologics, nose-to-brain, Pharmacy and materia medica, RS1-441

Abstract

In recent years, there have been a growing number of small and large molecules that could be used to treat diseases of the central nervous system (CNS). Nose-to-brain delivery can be a potential option for the direct transport of molecules from the nasal cavity to different brain areas. This review aims to provide a compilation of current approaches regarding drug delivery to the CNS via the nose, with a focus on biologics. The review also includes a discussion on the key benefits of nasal delivery as a promising alternative route for drug administration and the involved pathways or mechanisms. This article reviews how the application of various auxiliary agents, such as permeation enhancers, mucolytics, in situ gelling/mucoadhesive agents, enzyme inhibitors, and polymeric and lipid-based systems, can promote the delivery of large molecules in the CNS. The article also includes a discussion on the current state of intranasal formulation development and summarizes the biologics currently in clinical trials. It was noted that significant progress has been made in this field, and these are currently being applied to successfully transport large molecules to the CNS via the nose. However, a deep mechanistic understanding of this route, along with the intimate knowledge of various excipients and their interactions with the drug and nasal physiology, is still necessary to bring us one step closer to developing effective formulations for nasal–brain drug delivery.

Published

2023

21. Editorial: Neuroimaging of neuroinflammation in neurological disorders.

Author

Uddin, Md Nasir, Tivarus, Madalina E., Schifitto, Giovanni, and Rudko, David A.

Subjects

NEUROLOGICAL disorders, NEUROINFLAMMATION, BRAIN imaging

Published

2023

22. Intraosseous administration into the skull: Potential blood–brain barrier bypassing route for brain drug delivery

Author

Ji Hee Kang and Young Tag Ko

Subjects

BBB‐bypassing route, brain drug delivery, brain uptake, CNS disorders, intraclavariosseous, Chemical engineering, TP155-156, Biotechnology, TP248.13-248.65, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Progress in treating central nervous system (CNS) disorders is retarded owing to a limited understanding of brain disease pathology. Additionally, the blood–brain barrier (BBB) limits molecular entry into the brain. Many approaches for brain drug delivery to overcome the BBB, such as BBB permeability enhancement, transient BBB disruption, and direct surgical administration have been explored with limited success. Recent research has shown that direct vascular channels exist between the skull bone marrow and the meninges, allowing myeloid and lymphoid cells to migrate. We hypothesized that these direct channels may also allow brain drug delivery from the skull bone marrow to the brain. In this study, for the first time we propose intraosseous administration of drugs into the skull (intracalvariosseous [ICO]) as a novel approach for brain drug delivery via BBB bypassing routes. We tested the feasibility of the approach by applying nine representative compounds over thinned mouse skulls to simulate ICO and measuring the compound entry level in the brain compared to that after systemic administration. Surprisingly, we found that the skull is not completely impermeable to drug penetration into the brain and the tested compounds reached the brain tissue several tens‐to‐hundred times higher by ICO than systemic application. These findings suggest a role for the BBB bypassing route from skull to brain, apart from the systemic route, in the drug entry into the brain after ICO. This approach should be applicable to other CNS drugs and even BBB impermeable drugs. Overall ICO provides an innovative and advantageous pathway for effective treatment of brain diseases.

Published

2023

23. The benefits of hesperidin in central nervous system disorders, based on the neuroprotective effect

Author

Xinyu Li, Wei Huang, Rongrong Tan, Caijuan Xu, Xi Chen, Sixin Li, Ying Liu, Huiwen Qiu, Hui Cao, and Quan Cheng

Subjects

Hesperidin, CNS disorders, Mental disorders, Anti-depression, Therapeutics. Pharmacology, RM1-950

Abstract

Disorders of central nervous system (CNS) disorders are considered serious health issues. The most common CNS diseases include neurodegenerative diseases, mental disorders, demyelinating disease, ischemia-reperfusion injury, and neuroinflammation. As a natural phenolic compound, hesperidin is a flavanone glycoside with various biological effects. Increasing evidence show that the growth of CNS diseases is hindered by hesperidin. Here, we have reviewed the related literature on neuropharmacological mechanisms for the preventive and therapeutic effects of hesperidin on CNS diseases. Several cellular and animal models have been developed to evaluate the underlying neuropharmacological mechanisms of hesperidin. Additionally, clinical evidence has confirmed its neuroprotective function. Hesperidin exerts its neuroprotective properties by decreasing neuro-inflammatory and apoptotic pathways. Hesperidin function has been studied in preclinical models for CNS diseases, but little is known about its definite effect in humans. Hesperidin can effectively alleviate depression and improve cognition and memory. It is urgent to explore and discover clinical trials for further confirmation of the neuroprotective efficacy of hesperidin and to evaluate its safety profile.

Published

2023

24. Tumor Treating Fields (TTFields) Induce Cell Junction Alterations in a Human 3D In Vitro Model of the Blood-Brain Barrier.

Author

Salvador, Ellaine, Köppl, Theresa, Hörmann, Julia, Schönhärl, Sebastian, Bugaeva, Polina, Kessler, Almuth F., Burek, Malgorzata, Ernestus, Ralf-Ingo, Löhr, Mario, and Hagemann, Carsten

Subjects

*BLOOD-brain barrier, *ELECTRIC field therapy, *CELL junctions, *ENDOTHELIAL cells, *TIGHT junctions, *PERICYTES, *HUMAN origins

Abstract

In a recent study, we showed in an in vitro murine cerebellar microvascular endothelial cell (cerebEND) model as well as in vivo in rats that Tumor-Treating Fields (TTFields) reversibly open the blood–brain barrier (BBB). This process is facilitated by delocalizing tight junction proteins such as claudin-5 from the membrane to the cytoplasm. In investigating the possibility that the same effects could be observed in human-derived cells, a 3D co-culture model of the BBB was established consisting of primary microvascular brain endothelial cells (HBMVEC) and immortalized pericytes, both of human origin. The TTFields at a frequency of 100 kHz administered for 72 h increased the permeability of our human-derived BBB model. The integrity of the BBB had already recovered 48 h post-TTFields, which is earlier than that observed in cerebEND. The data presented herein validate the previously observed effects of TTFields in murine models. Moreover, due to the fact that human cell-based in vitro models more closely resemble patient-derived entities, our findings are highly relevant for pre-clinical studies. [ABSTRACT FROM AUTHOR]

Published

2023

25. Critical factors responsible for the therapeutic effect of mesenchymal stem/stromal cells in central nervous system disorders

Author

Anna Figiel-Dąbrowska, Monika Sypecka, Magdalena Chodkowska, and Anna Sarnowska

Subjects

mesenchymal stem/stromal cells, cns disorders, intrathecal injection, immunomodulatory properties, therapeutic effect, cell therapy, Medicine

Abstract

Nowadays it is observed that the number of stem-cell based experimental therapies in neurodegenerative disorders is massively increasing. Most of the clinical trials registered to date have been based on autologous mesenchymal stem/stromal cells (MSC) obtained from somatic tissues. In the conducted clinical trials neither serious side effects, nor statistically significant improvement were observed. The lack of statistical significance could result from a relatively small number of patients involved in clinical trials or highly incoherent study protocols. However, most clinical groups describe a trend towards improvement in MSC-treated patients. Hence, the question arises which factors associated with MSC-based therapy may be the key and result in better therapeutic response. In the presented paper, we summarize, in our opinion, the most important factors that could increase the effectiveness of this therapy.

Published

2022

26. Extensive Transduction and Enhanced Spread of a Modified AAV2 Capsid in the Non-human Primate CNS

Author

Naidoo, Jerusha, Stanek, Lisa M, Ohno, Kousaku, Trewman, Savanah, Samaranch, Lluis, Hadaczek, Piotr, O'Riordan, Catherine, Sullivan, Jennifer, San Sebastian, Waldy, Bringas, John R, Snieckus, Christopher, Mahmoodi, Amin, Mahmoodi, Amir, Forsayeth, John, Bankiewicz, Krystof S, and Shihabuddin, Lamya S

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Neurosciences, Neurodegenerative, Gene Therapy, Genetics, Neurological, Animals, Axonal Transport, Brain, Capsid Proteins, Central Nervous System, Dependovirus, Disease Models, Animal, Genetic Therapy, Genetic Vectors, Heparan Sulfate Proteoglycans, Humans, Infusions, Intraventricular, Motor Neurons, Neurons, Parvovirinae, Primates, Spinal Cord, Thalamus, AAV vectors, CNS disorders, brain, capsid modification, gene therapy, nervous system, non-human primate, spinal cord, transduction, viral vector, Biological Sciences, Technology, Medical and Health Sciences, Biotechnology, Clinical sciences, Medical biotechnology

Abstract

The present study was designed to characterize transduction of non-human primate brain and spinal cord with a modified adeno-associated virus serotype 2, incapable of binding to the heparan sulfate proteoglycan receptor, referred to as AAV2-HBKO. AAV2-HBKO was infused into the thalamus, intracerebroventricularly or via a combination of both intracerebroventricular and thalamic delivery. Thalamic injection of this modified vector encoding GFP resulted in widespread CNS transduction that included neurons in deep cortical layers, deep cerebellar nuclei, several subcortical regions, and motor neuron transduction in the spinal cord indicative of robust bidirectional axonal transport. Intracerebroventricular delivery similarly resulted in widespread cortical transduction, with one striking distinction that oligodendrocytes within superficial layers of the cortex were the primary cell type transduced. Robust motor neuron transduction was also observed in all levels of the spinal cord. The combination of thalamic and intracerebroventricular delivery resulted in transduction of oligodendrocytes in superficial cortical layers and neurons in deeper cortical layers. Several subcortical regions were also transduced. Our data demonstrate that AAV2-HBKO is a powerful vector for the potential treatment of a wide number of neurological disorders, and highlight that delivery route can significantly impact cellular tropism and pattern of CNS transduction.

Published

2018

27. Tumor Treating Fields (TTFields) Reversibly Permeabilize the Blood–Brain Barrier In Vitro and In Vivo.

Author

Salvador, Ellaine, Kessler, Almuth F., Domröse, Dominik, Hörmann, Julia, Schaeffer, Clara, Giniunaite, Aiste, Burek, Malgorzata, Tempel-Brami, Catherine, Voloshin, Tali, Volodin, Alexandra, Zeidan, Adel, Giladi, Moshe, Ernestus, Ralf-Ingo, Löhr, Mario, Förster, Carola Y., and Hagemann, Carsten

Subjects

*BLOOD-brain barrier, *ELECTRIC field therapy, *IMMUNOSTAINING, *TIGHT junctions

Abstract

Despite the availability of numerous therapeutic substances that could potentially target CNS disorders, an inability of these agents to cross the restrictive blood–brain barrier (BBB) limits their clinical utility. Novel strategies to overcome the BBB are therefore needed to improve drug delivery. We report, for the first time, how Tumor Treating Fields (TTFields), approved for glioblastoma (GBM), affect the BBB's integrity and permeability. Here, we treated murine microvascular cerebellar endothelial cells (cerebEND) with 100–300 kHz TTFields for up to 72 h and analyzed the expression of barrier proteins by immunofluorescence staining and Western blot. In vivo, compounds normally unable to cross the BBB were traced in healthy rat brain following TTFields administration at 100 kHz. The effects were analyzed via MRI and immunohistochemical staining of tight-junction proteins. Furthermore, GBM tumor-bearing rats were treated with paclitaxel (PTX), a chemotherapeutic normally restricted by the BBB combined with TTFields at 100 kHz. The tumor volume was reduced with TTFields plus PTX, relative to either treatment alone. In vitro, we demonstrate that TTFields transiently disrupted BBB function at 100 kHz through a Rho kinase-mediated tight junction claudin-5 phosphorylation pathway. Altogether, if translated into clinical use, TTFields could represent a novel CNS drug delivery strategy. [ABSTRACT FROM AUTHOR]

Published

2022

28. A comprehensive review on potential pharmacological activities of Morinda citrifolia Linn. for the treatment of central nervous system disorders.

Author

Begum, Asiya, Pandy, Vijayapandi, Chimakurthy, Jithendra, and Nadendla, Rama Rao

Subjects

*MORINDA citrifolia, *CENTRAL nervous system, *MONOAMINE oxidase, *CARDIOTONIC agents, *ANTIDEPRESSANTS, *ONLINE databases, *ALCOHOLISM

Abstract

Back ground: In brazil, the plant Morinda citrifolia, popularly known as noni, is widely utilized in traditional medicine. Many components of the noni tree, including the roots, leaves, and seeds, are used in these traditions. Because of its high antioxidant activity and established health advantages Morinda citrifolia (Noni) has been widely utilized as a complementary and alternative medicine in many countries. The noni plant has an ancient legacy of being used to cure a range of diseases including CNS abnormalities. It has historically used as an antidepressant, anxiolytic, antiepileptic activity, antipsychotic, nootropic activity, anticraving activity aganist alcohol dependence, antiemetic activity, neuroprotective agent. Objective: Based on preclinical research published in the literature, the current study underlines noni therapeutic potential activities for the treatment of cns disorders. The literature was collected from research gate, Wikipedia, medline, scholarly articles, online databases and academic search. The present review targeted on mostly receptors, enzyme transporters and invivo, invitro and insilico methods for different cns disorders. Conclusion:The monoamine oxidase (MAO) A and B bioassays were used to evaluate the antidepressant effects of Morinda citrifolia (noni) fruit extracts invitro. Nonifruit has a synergistic impact because of its active components, involved in inhibiting MAOA and MAOB enzymes. The methanolic extract of noni shows antipsychotic activity by inhibiting dopaminergic receptors. Administration of benzodiazepine and MMC attenuated anxiolytic activityin mouse models. Noni inhibits acetycholine esterase enzyme and exhibits nootropic activity. Noni exhibits anticraving activity against alcoholdependence by CPP test. Noni exhibits neuroprotective activity by decreasing the brain damage and dysfunction caused by reperfusion injury. [ABSTRACT FROM AUTHOR]

Published

2022

29. Quantifying Patient Investment in Novel Neurological Drug Development.

Author

MacPherson, Amanda, Gumnit, Elias, Ouimet, Charlotte, Hutchinson, Nora, Kieburtz, Karl, Pearson, Toni S., and Kimmelman, Jonathan

Abstract

While the drug development literature provides numerous estimates of the financial costs to bring a new drug to market, the investment of patient-participants in the research process has not been described. Trial participants and their caregivers, like companies, invest time and undertake risk when they participate in prelicense trials. We determined the average number of patient-participants needed to develop a novel neurological drug. We created a cohort of 108 unapproved drugs first tested for efficacy between 2006 and 2011 and used ClinicalTrials.gov to capture enrollment in all subsequent prelicense trials of these drugs over a 9-year period. Our primary outcome was the average number of patients enrolled in prelicense neurological drug trials per drug that ultimately attained FDA approval, including patients who participated in both successful and unsuccessful development efforts. Five drugs (4.6%) were FDA approved, and 66,751 patient-participants were enrolled across successful and unsuccessful drug development efforts, resulting in an average of 13,350 patients for each drug attaining approval (95% CI 7155 to 54,954). Our estimates reveal the substantial amount patients and their caregivers contribute to private drug development. [ABSTRACT FROM AUTHOR]

Published

2022

30. Intranasal delivery: An attractive route for the administration of nucleic acid based therapeutics for CNS disorders.

Author

Shah, Pranav, Lalan, Manisha, and Barve, Kalyani

Subjects

INTRANASAL administration, RETICULO-endothelial system, SMALL interfering RNA, MICRORNA, ANTISENSE RNA

Abstract

The etiologies of several cardiovascular, inflammatory, neurological, hereditary disorders, cancer, and infectious diseases have implicated changes in the genetic set up or genetic mutations as the root cause. Nucleic acid based therapeutics (NBTs) is a new class of biologics that are known to regulate gene expression at the transcriptional and post-transcriptional level. The NBTs include oligonucleotides, nucleosides, antisense RNA, small interfering RNAs, micro RNA etc. In recent times, this new category of biologics has found enormous potential in the management of cardiovascular, inflammatory, neurological disorders, cancer, infectious diseases and organ transplantation. However, the delivery of NBTs is highly challenging in terms of target specificity (intracellular delivery), mononuclear phagocyte system uptake, stability and biodistribution. Additionally, management of the above mentioned disorders require regular and intrusive therapy making non-invasive routes preferable in comparison to invasive routes like parenteral. The nasal route is garnering focus in delivery of NBTs to the brain in the management of several CNS disorders due to the associated merits such as non-invasiveness, possibility of chronic delivery, improved patient compliance, avoidance of hepatic and gastrointestinal metabolism as well as ability to bypass the BBB. Hence in recent times, this route has been sought by the reserachers as an alternative to parenteral therapy for the delivery of several NBTs. This review shall focus on an array of NBTs delivered through nasal route, their challenges, applications and opportunities. The novel delivery systems for incorporating NBTs; their targeting strategies shall be critically reviewed. The challenges towards regulatory approvals and commercialization shall also be discussed at large. Comparison of learnings derived from the success and barriers in nasal delivery of NBTs will help in identification of futuristic opportunities for their translation from bench to bedside. [ABSTRACT FROM AUTHOR]

Published

2022

31. The role of enriched environment in neural development and repair.

Author

Yu Han, Mei Yuan, Yi-Sha Guo, Xin-Ya Shen, Zhen-Kun Gao, and Xia Bi

Subjects

NEURAL development, NEUROLOGICAL disorders, CEREBRAL ischemia, NERVOUS system, HISTOLOGY, CENTRAL nervous system physiology, ADOLESCENCE

Abstract

In addition to genetic information, environmental factors play an important role in the structure and function of nervous system and the occurrence and development of some nervous system diseases. Enriched environment (EE) can not only promote normal neural development through enhancing neuroplasticity but also play a nerve repair role in restoring functional activities during CNS injury by morphological and cellular and molecular adaptations in the brain. Different stages of development after birth respond to the environment to varying degrees. Therefore, we systematically review the pro-developmental and anti-stress value of EE during pregnancy, pre- weaning, and "adolescence" and analyze the difference in the effects of EE and its sub-components, especially with physical exercise. In our exploration of potential mechanisms that promote neurodevelopment, we have found that not all sub-components exert maximum value throughout the developmental phase, such as animals that do not respond to physical activity before weaning, and that EE is not superior to its sub-components in all respects. EE affects the developing and adult brain, resulting in some neuroplastic changes in the microscopic and macroscopic anatomy, finally contributing to enhanced learning and memory capacity. These positive promoting influences are particularly prominent regarding neural repair after neurobiological disorders. Taking cerebral ischemia as an example, we analyzed the molecular mediators of EE promoting repair from various dimensions. We found that EE does not always lead to positive effects on nerve repair, such as infarct size. In view of the classic issues such as standardization and relativity of EE have been thoroughly discussed, we finally focus on analyzing the essentiality of the time window of EE action and clinical translation in order to devote to the future research direction of EE and rapid and reasonable clinical application. [ABSTRACT FROM AUTHOR]

Published

2022

32. Intranasal delivery: An attractive route for the administration of nucleic acid based therapeutics for CNS disorders

Author

Pranav Shah, Manisha Lalan, and Kalyani Barve

Subjects

CNS disorders, drug delivery, nasal route, regulatory challenges, toxicity, nucleic acid, Therapeutics. Pharmacology, RM1-950

Abstract

The etiologies of several cardiovascular, inflammatory, neurological, hereditary disorders, cancer, and infectious diseases have implicated changes in the genetic set up or genetic mutations as the root cause. Nucleic acid based therapeutics (NBTs) is a new class of biologics that are known to regulate gene expression at the transcriptional and post-transcriptional level. The NBTs include oligonucleotides, nucleosides, antisense RNA, small interfering RNAs, micro RNA etc. In recent times, this new category of biologics has found enormous potential in the management of cardiovascular, inflammatory, neurological disorders, cancer, infectious diseases and organ transplantation. However, the delivery of NBTs is highly challenging in terms of target specificity (intracellular delivery), mononuclear phagocyte system uptake, stability and biodistribution. Additionally, management of the above mentioned disorders require regular and intrusive therapy making non-invasive routes preferable in comparison to invasive routes like parenteral. The nasal route is garnering focus in delivery of NBTs to the brain in the management of several CNS disorders due to the associated merits such as non-invasiveness, possibility of chronic delivery, improved patient compliance, avoidance of hepatic and gastrointestinal metabolism as well as ability to bypass the BBB. Hence in recent times, this route has been sought by the reserachers as an alternative to parenteral therapy for the delivery of several NBTs. This review shall focus on an array of NBTs delivered through nasal route, their challenges, applications and opportunities. The novel delivery systems for incorporating NBTs; their targeting strategies shall be critically reviewed. The challenges towards regulatory approvals and commercialization shall also be discussed at large. Comparison of learnings derived from the success and barriers in nasal delivery of NBTs will help in identification of futuristic opportunities for their translation from bench to bedside.

Published

2022

33. MicroRNA-based interventions in aberrant cell cycle diseases: Therapeutic strategies for cancers, central nervous system disorders and comorbidities.

Author

Tang, Xiaojuan, Ren, Yuan, Zeng, Wen, Feng, Xiaoting, He, Min, Lv, Yuan, Li, Yongmin, and He, Yongheng

Subjects

*CELL cycle, *CENTRAL nervous system, *CENTRAL nervous system injuries, *TREATMENT effectiveness, *GENE expression, CENTRAL nervous system tumors

Abstract

Malignant tumors and central nervous system (CNS) disorders are intricately linked to a process known as "aberrant cell cycle re-entry," which plays a critical role in the progression of these diseases. Addressing the dysregulation in cell cycles offers a promising therapeutic approach for cancers and CNS disorders. MicroRNAs (miRNAs) play a crucial role as regulators of gene expression in cell cycle transitions, presenting a promising therapeutic avenue for treating these disorders and their comorbidities. This review consolidates the progress made in the last three years regarding miRNA-based treatments for diseases associated with aberrant cell cycle re-entry. It encompasses exploring fundamental mechanisms and signaling pathways influenced by miRNAs in cancers and CNS disorders, particularly focusing on the therapeutic effects of exosome-derived miRNAs. The review also identifies specific miRNAs implicated in comorbidity of cancers and CNS disorders, discusses the future potential of miRNA reagents in managing cell cycle-related diseases. [Display omitted] • Linking miRNAs to cell cycle dysregulation in cancers and CNS disorders. • Highlighting exosome-derived miRNAs in the treatment of cancers and CNS disorders. • Revealing the shared mechanism of miRNAs-based interventions in cancers and CNS disorders. • Identifying specific miRNAs in comorbidity of cancers and CNS disorders. • Discussing the challenges of miRNA reagents in disease management. [ABSTRACT FROM AUTHOR]

Published

2024

34. Plant-derived bioactive compounds and their novel role in central nervous system disorder treatment via ATF4 targeting: A systematic literature review.

Author

Zhang, Nan, Zhang, Shun, and Dong, Xiaoyu

Subjects

*CENTRAL nervous system, *CENTRAL nervous system injuries, *BIOACTIVE compounds, *TRANSCRIPTION factors, *ALZHEIMER'S disease, *PARKINSON'S disease

Abstract

Central nervous system (CNS) disorders exhibit exceedingly intricate pathogenic mechanisms. Pragmatic and effective solutions remain elusive, significantly compromising human life and health. Activating transcription factor 4 (ATF4) participates in the regulation of multiple pathophysiological processes, including CNS disorders. Considering the widespread involvement of ATF4 in the pathological process of CNS disorders, the targeted regulation of ATF4 by plant-derived bioactive compounds (PDBCs) may become a viable strategy for the treatment of CNS disorders. However, the regulatory relationship between PDBCs and ATF4 remains incompletely understood. Here, we aimed to comprehensively review the studies on PDBCs targeting ATF4 to ameliorate CNS disorders, thereby offering novel directions and insights for the treatment of CNS disorders. A computerized search was conducted on PubMed, Embase, Web of Science, and Google Scholar databases to identify preclinical experiments related to PDBCs targeting ATF4 for the treatment of CNS disorders. The search timeframe was from the inception of the databases to December 2023. Two assessors conducted searches using the keywords "ATF4," "Central Nervous System," "Neurological," "Alzheimer's disease," "Parkinson's Disease," "Stroke," "Spinal Cord Injury," "Glioblastoma," "Traumatic Brain Injury," and "Spinal Cord Injury." Overall, 31 studies were included, encompassing assessments of 27 PDBCs. Combining results from in vivo and in vitro studies, we observed that these PDBCs, via ATF4 modulation, prevent the deposition of amyloid-like fibers such as Aβ, tau, and α-synuclein. They regulate ERS, reduce the release of inflammatory factors, restore mitochondrial membrane integrity to prevent oxidative stress, regulate synaptic plasticity, modulate autophagy, and engage anti-apoptotic mechanisms. Consequently, they exert neuroprotective effects in CNS disorders. Numerous PDBCs targeting ATF4 have shown potential in facilitating the restoration of CNS functionality, thereby presenting expansive prospects for the treatment of such disorders. However, future endeavors necessitate high-quality, large-scale, and comprehensive preclinical and clinical studies to further validate this therapeutic potential. [Display omitted] • ATF4 is widely implicated in the pathological mechanisms of Central nervous system (CNS) disorders. • The studies of 27 plant-derived bioactive compounds (PDBCs) targeting ATF4 for the treatment of CNS disorders incorporated into the study. • The PDBCs exert their effects in the treatment of CNS disorders by modulating ATF4. [ABSTRACT FROM AUTHOR]

Published

2024

35. Complement cascade functions during brain development and neurodegeneration.

Author

Fatoba, Oluwaseun, Itokazu, Takahide, and Yamashita, Toshihide

Subjects

*NEURAL development, *COMPLEMENT activation, *PERILIPIN, *NEURODEGENERATION, *GLYCOSAMINOGLYCANS, *CENTRAL nervous system

Abstract

The complement system, an essential tightly regulated innate immune system, is a key regulator of normal central nervous system (CNS) development and function. However, aberrant complement component expression and activation in the brain may culminate into marked neuroinflammatory response, neurodegenerative processes and cognitive impairment. Over the years, complement‐mediated neuroinflammatory responses and complement‐driven neurodegeneration have been increasingly implicated in the pathogenesis of a wide spectrum of CNS disorders. This review describes how complement system contributes to normal brain development and function. We also discuss how pathologic insults such as misfolded proteins, lipid droplet/lipid droplet‐associated protein or glycosaminoglycan accumulation could trigger complement‐mediated neuroinflammatory responses and neurodegenerative process in neurodegenerative proteinopathies, age‐related macular degeneration and neurodegenerative lysosomal storage disorders. [ABSTRACT FROM AUTHOR]

Published

2022

36. Recent developments on PET radiotracers for TSPO and their applications in neuroimaging

Author

Lingling Zhang, Kuan Hu, Tuo Shao, Lu Hou, Shaojuan Zhang, Weijian Ye, Lee Josephson, Jeffrey H. Meyer, Ming-Rong Zhang, Neil Vasdev, Jinghao Wang, Hao Xu, Lu Wang, and Steven H. Liang

Subjects

TSPO, Microglial activation, Neuroinflammation, Positron emission tomography (PET), CNS disorders, Therapeutics. Pharmacology, RM1-950

Abstract

The 18 kDa translocator protein (TSPO), previously known as the peripheral benzodiazepine receptor, is predominately localized to the outer mitochondrial membrane in steroidogenic cells. Brain TSPO expression is relatively low under physiological conditions, but is upregulated in response to glial cell activation. As the primary index of neuroinflammation, TSPO is implicated in the pathogenesis and progression of numerous neuropsychiatric disorders and neurodegenerative diseases, including Alzheimer's disease (AD), amyotrophic lateral sclerosis (ALS), Parkinson's disease (PD), multiple sclerosis (MS), major depressive disorder (MDD) and obsessive compulsive disorder (OCD). In this context, numerous TSPO-targeted positron emission tomography (PET) tracers have been developed. Among them, several radioligands have advanced to clinical research studies. In this review, we will overview the recent development of TSPO PET tracers, focusing on the radioligand design, radioisotope labeling, pharmacokinetics, and PET imaging evaluation. Additionally, we will consider current limitations, as well as translational potential for future application of TSPO radiopharmaceuticals. This review aims to not only present the challenges in current TSPO PET imaging, but to also provide a new perspective on TSPO targeted PET tracer discovery efforts. Addressing these challenges will facilitate the translation of TSPO in clinical studies of neuroinflammation associated with central nervous system diseases.

Published

2021

37. Mitochondrial Extracellular Vesicles in CNS Disorders: New Frontiers in Understanding the Neurological Disorders of the Brain

Author

Mary F. Nakamya, Susmita Sil, Shilpa Buch, and Ramin M. Hakami

Subjects

mitochondria, mitochondria-derived vesicles, extracellular vesicles, mitophagy, CNS disorders, mitochondrial dysfunction, Biology (General), QH301-705.5

Abstract

Recent findings have highlighted potential diagnostic and prognostic values of extracellular vesicles (EVs) that contain mitochondrial derived components for neurological disorders. Furthermore, functional influences of vesicles carrying mitochondrial components have been reported. In particular, this includes indications of crosstalk with mitophagy to influence progression of various CNS disorders. In this mini-review, we discuss the current state of knowledge about this intriguing class of vesicles in neurological disorders of the CNS, and outline the lacunae and thus scope of further development in this fascinating field of study.

Published

2022

38. Critical factors responsible for the therapeutic effect of mesenchymal stem/stromal cells in central nervous system disorders.

Author

Figiel-Dąbrowska, Anna, Sypecka, Monika, Chodkowska, Magdalena, and Sarnowska, Anna

Abstract

Nowadays it is observed that the number of stem-cell based experimental therapies in neurodegenerative disorders is massively increasing. Most of the clinical trials registered to date have been based on autologous mesenchymal stem/stromal cells (MSC) obtained from somatic tissues. In the conducted clinical trials neither serious side effects, nor statistically significant improvement were observed. The lack of statistical significance could result from a relatively small number of patients involved in clinical trials or highly incoherent study protocols. However, most clinical groups describe a trend towards improvement in MSC-treated patients. Hence, the question arises which factors associated with MSC-based therapy may be the key and result in better therapeutic response. In the presented paper, we summarize, in our opinion, the most important factors that could increase the effectiveness of this therapy. [ABSTRACT FROM AUTHOR]

Published

2022

39. Microglia as therapeutic target in central nervous system disorders

Author

Oluwaseun Fatoba, Takahide Itokazu, and Toshihide Yamashita

Subjects

Microglial activation, Phenotypes, Homeostasis, Heterogeneity, CNS disorders, Therapeutics. Pharmacology, RM1-950

Abstract

Chronic microglial activation is associated with the pathogenesis of several CNS disorders. Microglia show phenotypic diversity and functional complexity in diseased CNS. Thus, understanding the pathology-specific heterogeneity of microglial behavior is crucial for the future development of microglia-modulating therapy for variety of CNS disorders. This review summarizes up-to-date knowledge on how microglia contribute to CNS homeostasis during development and throughout adulthood. We discuss the heterogeneity of microglial phenotypes in the context of CNS disorders with an emphasis on neurodegenerative diseases, demyelinating diseases, CNS trauma, and epilepsy. We conclude this review with a discussion about the disease-specific heterogeneity of microglial function and how it could be exploited for therapeutic intervention.

Published

2020

40. Tumor Treating Fields (TTFields) Induce Cell Junction Alterations in a Human 3D In Vitro Model of the Blood-Brain Barrier

Author

Ellaine Salvador, Theresa Köppl, Julia Hörmann, Sebastian Schönhärl, Polina Bugaeva, Almuth F. Kessler, Malgorzata Burek, Ralf-Ingo Ernestus, Mario Löhr, and Carsten Hagemann

Subjects

blood-brain barrier, Tumor-Treating Fields (TTFields), CNS disorders, human brain microvascular endothelial cells (HBMVEC), human cells, 3D in vitro model, Pharmacy and materia medica, RS1-441

Abstract

In a recent study, we showed in an in vitro murine cerebellar microvascular endothelial cell (cerebEND) model as well as in vivo in rats that Tumor-Treating Fields (TTFields) reversibly open the blood–brain barrier (BBB). This process is facilitated by delocalizing tight junction proteins such as claudin-5 from the membrane to the cytoplasm. In investigating the possibility that the same effects could be observed in human-derived cells, a 3D co-culture model of the BBB was established consisting of primary microvascular brain endothelial cells (HBMVEC) and immortalized pericytes, both of human origin. The TTFields at a frequency of 100 kHz administered for 72 h increased the permeability of our human-derived BBB model. The integrity of the BBB had already recovered 48 h post-TTFields, which is earlier than that observed in cerebEND. The data presented herein validate the previously observed effects of TTFields in murine models. Moreover, due to the fact that human cell-based in vitro models more closely resemble patient-derived entities, our findings are highly relevant for pre-clinical studies.

Published

2023

41. cGAS- Stimulator of Interferon Genes Signaling in Central Nervous System Disorders.

Author

Fengjuan Li, Ningqun Wang, Yangmin Zheng, Yumin Luo, and Yongbo Zhang

Subjects

*INTERFERONS, *CENTRAL nervous system physiology, *NATURAL immunity

Abstract

Cytosolic nucleic acid sensors contribute to the initiation of innate immune responses by playing a critical role in the detection of pathogens and endogenous nucleic acids. The cytosolic DNA sensor cyclic-GMPAMP synthase (cGAS) and its downstream effector, stimulator of interferon genes (STING), mediate innate immune signaling by promoting the release of type I interferons (IFNs) and other inflammatory cytokines. These biomolecules are suggested to play critical roles in host defense, senescence, and tumor immunity. Recent studies have demonstrated that cGAS-STING signaling is strongly implicated in the pathogenesis of central nervous system (CNS) diseases which are underscored by neuroinflammatory-driven disease progression. Understanding and regulating the interactions between cGAS-STING signaling and the nervous system may thus provide an effective approach to prevent or delay late-onset CNS disorders. Here, we present a review of recent advances in the literature on cGAS-STING signaling and provide a comprehensive overview of the modulatory patterns of the cGAS-STING pathway in CNS disorders. [ABSTRACT FROM AUTHOR]

Published

2021

42. She Doesn't Even Go Here: The Role of Inflammatory Astrocytes in CNS Disorders.

Author

Reid, Jacqueline Kelsey and Kuipers, Hedwich Fardau

Subjects

ASTROCYTES, NEURODEGENERATION, PATHOGENESIS, NEUROLOGICAL disorders

Abstract

Astrocyte heterogeneity is a rapidly evolving field driven by innovative techniques. Inflammatory astrocytes, one of the first described subtypes of reactive astrocytes, are present in a variety of neurodegenerative diseases and may play a role in their pathogenesis. Moreover, genetic and therapeutic targeting of these astrocytes ameliorates disease in several models, providing support for advancing the development of astrocyte-specific disease modifying therapies. This review aims to explore the methods and challenges of identifying inflammatory astrocytes, the role these astrocytes play in neurological disorders, and future directions in the field of astrocyte heterogeneity. [ABSTRACT FROM AUTHOR]

Published

2021

43. A Review on Some Medicinal Plants of North- East India Region Used in the Treatment of Central Nervous System Disorders.

Author

Nath, Venessa, Buragohain, Parishmita, and Sharma, Hemanta Kr.

Subjects

CENTRAL nervous system, MEDICINAL plants, SPINAL cord, HUMAN body, NEUROLOGICAL disorders

Abstract

Background: Central nervous system (CNS) disorders are a group of neurological disorders concerned with behaviour, coordination and functioning of the brain and the spinal cord. The CNS is the site of processing various informations. It interprets and evaluates the information and as result, the CNS responds accordingly and controls the body. Any defects or disorders of the Central nervous system may cause degeneration of the organs and tissues associated with it, loss of coordination, paralysis, etc. These disorders may be hereditary or due to injuries to the brain and spinal cord. Although, these disorders are being cured with medicaments, many plant species are also seen to be effective in its treatment. Objective: the main objective of this article is to underline the potentials and the needs for the documentation of the ecological knowledge of herbal medicines of the north east India region, necessary for the greater well-being of mankind in the prevention and cure of CNS disorders. Methods: an extensive literature survey was carried out through various databases like Google Scholar, Pubmed, Sciencedirect etc to support this review. All the collected information was analyzed accordingly and the plants were enlisted based on the classes of CNS disorders for which they are used. Result and discussion: from the survey of the database being collected, it was found that many traditional and local plants of the northeast India region are therapeutically effective in the treatment and cure of many Central nervous system disorders. Conclusion:-It is now an accepted fact that many traditional plants found in the Northeast India have been acceptable within the human body and hence these can be used to replace many expensive medications available in the market. [ABSTRACT FROM AUTHOR]

Published

2021

44. She Doesn’t Even Go Here: The Role of Inflammatory Astrocytes in CNS Disorders

Author

Jacqueline Kelsey Reid and Hedwich Fardau Kuipers

Subjects

astrocytes, reactive astrogliosis, heterogeneity, neuroinflammation, immune mediators, CNS disorders, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Astrocyte heterogeneity is a rapidly evolving field driven by innovative techniques. Inflammatory astrocytes, one of the first described subtypes of reactive astrocytes, are present in a variety of neurodegenerative diseases and may play a role in their pathogenesis. Moreover, genetic and therapeutic targeting of these astrocytes ameliorates disease in several models, providing support for advancing the development of astrocyte-specific disease modifying therapies. This review aims to explore the methods and challenges of identifying inflammatory astrocytes, the role these astrocytes play in neurological disorders, and future directions in the field of astrocyte heterogeneity.

Published

2021

45. Tumor Treating Fields (TTFields) Reversibly Permeabilize the Blood–Brain Barrier In Vitro and In Vivo

Author

Ellaine Salvador, Almuth F. Kessler, Dominik Domröse, Julia Hörmann, Clara Schaeffer, Aiste Giniunaite, Malgorzata Burek, Catherine Tempel-Brami, Tali Voloshin, Alexandra Volodin, Adel Zeidan, Moshe Giladi, Ralf-Ingo Ernestus, Mario Löhr, Carola Y. Förster, and Carsten Hagemann

Subjects

blood–brain barrier, TTFields, CNS disorders, Microbiology, QR1-502

Abstract

Despite the availability of numerous therapeutic substances that could potentially target CNS disorders, an inability of these agents to cross the restrictive blood–brain barrier (BBB) limits their clinical utility. Novel strategies to overcome the BBB are therefore needed to improve drug delivery. We report, for the first time, how Tumor Treating Fields (TTFields), approved for glioblastoma (GBM), affect the BBB’s integrity and permeability. Here, we treated murine microvascular cerebellar endothelial cells (cerebEND) with 100–300 kHz TTFields for up to 72 h and analyzed the expression of barrier proteins by immunofluorescence staining and Western blot. In vivo, compounds normally unable to cross the BBB were traced in healthy rat brain following TTFields administration at 100 kHz. The effects were analyzed via MRI and immunohistochemical staining of tight-junction proteins. Furthermore, GBM tumor-bearing rats were treated with paclitaxel (PTX), a chemotherapeutic normally restricted by the BBB combined with TTFields at 100 kHz. The tumor volume was reduced with TTFields plus PTX, relative to either treatment alone. In vitro, we demonstrate that TTFields transiently disrupted BBB function at 100 kHz through a Rho kinase-mediated tight junction claudin-5 phosphorylation pathway. Altogether, if translated into clinical use, TTFields could represent a novel CNS drug delivery strategy.

Published

2022

46. Current State and Future Directions of Intranasal Delivery Route for Central Nervous System Disorders: A Scientometric and Visualization Analysis

Author

Haiyang Wu, Yan Zhou, Yulin Wang, Linjian Tong, Fanchen Wang, Sirong Song, Lixia Xu, Baolong Liu, Hua Yan, and Zhiming Sun

Subjects

scientometric, intranasal drug delivery, blood-brain barrier, CNS disorders, citespace, VOS viewer, Therapeutics. Pharmacology, RM1-950

Abstract

Background: The management of various central nervous system (CNS) disorders has been challenging, due to highly compact blood-brain barrier (BBB) impedes the access of most pharmacological agents to the brain. Among multiple strategies proposed to circumvent this challenge, intranasal delivery route has sparked great interest for brain targeting in the past decades. The aim of this study was to apply scientometric method to estimate the current status and future trends of the field from a holistic perspective.Methods: All relevant publications during 1998–2020 were retrieved from the Web of Science Core Collection (SCIE, 1998-present). Two different scientometric software including VOS viewer and CiteSpace, and one online platform were used to conduct co-authorship, co-citation, and co-occurrence analysis of journals, countries, institutes, authors, references and keywords.Results: A total of 2,928 documents, including 2,456 original articles and 472 reviews, were retrieved. Our analysis revealed a significant increasing trend in the total number of scientific publications over the past 2 decades (R2 = 0.98). The United States dominated the field, reflecting in the largest amount of publications (971), the highest H-index (99), and extensive international collaboration. Jamia Hamdard contributed to most publications. Frey WH and Illum L were key researchers with the highest number of publications and citations, respectively. The International Journal of Pharmaceutics was the most influential academic journal, and Pharmacology/Pharmacy and Neurosciences/Neurology were the hottest research categories in this field. Based on keywords occurrence analysis, four main topics were identified, and the current research focus of this field has shifted from cluster 4 (pathways and mechanisms of intranasal delivery) to cluster 2 (the study of nasal drug delivery systems), especially the nanostructured and nano-sized carrier systems. Keywords burst detection revealed that the research focus on oxidative stress, drug delivery, neuroinflammation, nanostructured lipid carrier, and formulation deserves our continued attention.Conclusion: To the authors’ knowledge, this is the first scientometric analysis regarding intranasal delivery research. This study has demonstrated a comprehensive knowledge map, development landscape and future directions of intranasal delivery research, which provides a practical and valuable reference for scholars and policymakers in this field.

Published

2021

47. Mutation of copper binding sites on cellular prion protein abolishes its inhibitory action on NMDA receptors in mouse hippocampal neurons.

Author

Huang, Sun, Black, Stefanie A., Huang, Junting, Stys, Peter K., and Zamponi, Gerald W.

Subjects

*METHYL aspartate receptors, *BINDING sites, *PRIONS, *NEURONS, *HIPPOCAMPUS (Brain), *CREUTZFELDT-Jakob disease

Abstract

We have previously reported that cellular prion protein (PrPC) can down-regulate NMDA receptor activity and in a copper dependent manner. Here, we employed AAV9 to introduce murine cellular prion protein into mouse hippocampal neurons in primary cultures from PrP null mice to determine the role of the six copper binding motifs located within the N-terminal domain of PrPC. The results demonstrate that viral expression of wild type PrPC lowers NMDAR activity in PrP null mouse hippocampal neurons by reducing the magnitude of non-desensitizing currents. Elimination of the last two copper binding sites alone, or in combination with the remaining four attenuates this protective effect. Thus our data suggest that copper ion interactions with specific binding sites on PrPC are critical for PrPC dependent modulation of NMDA receptor function. [ABSTRACT FROM AUTHOR]

Published

2021

48. Current State and Future Directions of Intranasal Delivery Route for Central Nervous System Disorders: A Scientometric and Visualization Analysis.

Author

Wu, Haiyang, Zhou, Yan, Wang, Yulin, Tong, Linjian, Wang, Fanchen, Song, Sirong, Xu, Lixia, Liu, Baolong, Yan, Hua, and Sun, Zhiming

Subjects

INTRANASAL administration, CENTRAL nervous system, BLOOD-brain barrier, DRUG delivery systems, SCHOLARLY periodicals, VISUALIZATION

Abstract

Background: The management of various central nervous system (CNS) disorders has been challenging, due to highly compact blood-brain barrier (BBB) impedes the access of most pharmacological agents to the brain. Among multiple strategies proposed to circumvent this challenge, intranasal delivery route has sparked great interest for brain targeting in the past decades. The aim of this study was to apply scientometric method to estimate the current status and future trends of the field from a holistic perspective. Methods: All relevant publications during 1998–2020 were retrieved from the Web of Science Core Collection (SCIE, 1998-present). Two different scientometric software including VOS viewer and CiteSpace, and one online platform were used to conduct co-authorship, co-citation, and co-occurrence analysis of journals, countries, institutes, authors, references and keywords. Results: A total of 2,928 documents, including 2,456 original articles and 472 reviews, were retrieved. Our analysis revealed a significant increasing trend in the total number of scientific publications over the past 2 decades (R 2 = 0.98). The United States dominated the field, reflecting in the largest amount of publications (971), the highest H-index (99), and extensive international collaboration. Jamia Hamdard contributed to most publications. Frey WH and Illum L were key researchers with the highest number of publications and citations, respectively. The International Journal of Pharmaceutics was the most influential academic journal, and Pharmacology/Pharmacy and Neurosciences/Neurology were the hottest research categories in this field. Based on keywords occurrence analysis, four main topics were identified, and the current research focus of this field has shifted from cluster 4 (pathways and mechanisms of intranasal delivery) to cluster 2 (the study of nasal drug delivery systems), especially the nanostructured and nano-sized carrier systems. Keywords burst detection revealed that the research focus on oxidative stress, drug delivery, neuroinflammation, nanostructured lipid carrier, and formulation deserves our continued attention. Conclusion: To the authors' knowledge, this is the first scientometric analysis regarding intranasal delivery research. This study has demonstrated a comprehensive knowledge map, development landscape and future directions of intranasal delivery research, which provides a practical and valuable reference for scholars and policymakers in this field. [ABSTRACT FROM AUTHOR]

Published

2021

49. Agmatine: A potential Neurotherapeutic Agent.

Author

Neha, Binjhade, Vinanti, Supare, Shailesh, Ghaywat, Sagar, Trivedi, Kamlesh, Wadher, and Milind, Umekar

Subjects

AGMATINE, DRUG target, PARKINSON'S disease, ALZHEIMER'S disease, NEUROLOGICAL disorders

Abstract

Agmatine, a natural polyamine disregarded almost for over 100 years, was discovered in year 1910. Almost after a decade, several researches on Agmatine indicated its modulatory action at multiple molecular targets such as, nitric oxide synthesis, neurotransmitter systems, and polyamine metabolism unbolt the new avenues for extensive therapeutic applications which includes neurotrauma and neurodegenerative diseases, antidepressant, cognitive disorders. Agmatine exerts its varied biological characteristics and therapeutic potential in diverse arena. Agmatine has been extensively researched for its neuroprotective effect in various types of neurological diseases, including stroke and trauma brain injury along with Parkinson's disease, Alzheimer's disease, Hypoxia/Ischemia. In the present review we have summarized the therapeutic potential of agmatine as protective and regenerative properties in the CNS. [ABSTRACT FROM AUTHOR]

Published

2021

50. Advances in Diagnostic and Treatment Modalities for Intracranial Tumors

Author

Dickinson, PJ

Subjects

Veterinary Sciences, Agricultural, Veterinary and Food Sciences, Brain Disorders, Orphan Drug, Rare Diseases, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Animals, Brain, Brain Neoplasms, Dog Diseases, Dogs, Immunoglobulin G, Melphalan, Brain tumor, CNS disorders, Neuroimaging, Neurology, Neurosurgery, Oncology, Oncology treatment, Veterinary sciences

Abstract

Intracranial neoplasia is a common clinical condition in domestic companion animals, particularly in dogs. Application of advances in standard diagnostic and therapeutic modalities together with a broad interest in the development of novel translational therapeutic strategies in dogs has resulted in clinically relevant improvements in outcome for many canine patients. This review highlights the status of current diagnostic and therapeutic approaches to intracranial neoplasia and areas of novel treatment currently in development.

Published

2014