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223 results on '"Paul A. Morton"'

203. Carcinoid of the rectum

Author

Robert W. Fraser and Paul C. Morton

Subjects
medicine.medical_specialty, Pathology, Carcinoid tumors, Rectum, Carcinoid Tumor, digestive system, Lesion, medicine, Carcinoma, Humans, Barium enema, Rectal Neoplasms, business.industry, Mucous membrane, General Medicine, Anus, medicine.disease, digestive system diseases, Carcinoma, Neuroendocrine, medicine.anatomical_structure, Rectum neoplasm, Surgery, Radiology, medicine.symptom, business
Abstract

1. 1. Three cases of carcinoid of rectum are reported. 2. 2. All small lesions of rectum should be completely removed and entire specimen considered biopsy material. 3. 3. Periodic examinations of patients from whom carcinoid tumors have been removed are indicated and should include barium enema with air contrast. 4. 4. All tissue removed from anus and rectum should be subjected to pathologic examination to insure proper diagnosis and subsequent treatment. 5. 5. Carcinoid of the rectum must be considered in any pathologic report of a rectal lesion showing intact mucous membrane with underlying tumor tissue suggesting carcinoma of rectum. A correct evaluation of the lesion may avoid unnecessary resection of the rectum.

Published
1953

205. Ionization Currents in Non-Uniform Electric Fields

Author

Paul L. Morton

Subjects
Materials science, Ionization, Electric field, General Physics and Astronomy, Electric potential, Atomic physics, Voltage, Electric discharge in gases
Published
1946

207. GAS GANGRENE OF WOUND OF WRIST

Author

Paul C. Morton

Subjects
medicine.medical_specialty, medicine.anatomical_structure, business.industry, Medicine, Surgery, Wrist, Antitoxin, business, medicine.disease, Gas gangrene
Published
1936

208. Backpropagation and EEG Data

Author

Glenn F. Wilson and Paul E. Morton

Subjects
Complex data type, Focus (computing), Point (typography), Artificial neural network, business.industry, Computer science, Machine learning, computer.software_genre, Backpropagation, Field (computer science), Work (electrical), The Internet, Artificial intelligence, business, computer
Abstract

The development of neural networks has pursued a myriad of different courses reflecting the interests of a large number of researchers from highly varied backgrounds. This paper would like to focus on one point of this 'many faceted gem', as Stephen Grossberg described the field. The point of focus will be to address some of the practical results of applying a backpropagation trained net to raw electroencephalogram (EEG) data. Much important work on more efficient training rules has been done; however, equally critical is consideration of the information content of the data, the net size, number of hidden nodes and order of training data. This paper explores some of the training issues raised by applying backpropagation to this very complex data.

Published
1988

209. 1975 Memorial Award Paper. Image generation and display techniques for CT scan data. Thin transverse and reconstructed coronal and sagittal planes

Author

Raymond J. Johnston, William V. Glenn, Samuel J. Dwyer, and Paul E. Morton

Subjects
Adult, Male, Image generation, Adolescent, Computed tomography, Radiation Dosage, Imaging phantom, Plane (Unicode), medicine, Humans, Radiology, Nuclear Medicine and imaging, Technology, Radiologic, Brain Diseases, medicine.diagnostic_test, business.industry, Computers, Tomography, X-Ray, General Medicine, Middle Aged, Sagittal plane, Transverse plane, medicine.anatomical_structure, Coronal plane, Deconvolution, Nuclear medicine, business, Geology, Biomedical engineering
Abstract

The various limitations to computerized axial tomographic (CT) interpretation are due in part to the 8-13 mm standard tissue plane thickness and in part to the absence of alternative planes of view, such as coronal or sagittal images. This paper describes a method for gathering multiple overlapped 8 mm transverse sections, subjecting these data to a deconvolution process, and then displaying thin (1 mm) transverse as well as reconstructed coronal and sagittal CT images. Verification of the deconvolution technique with phantom experiments is described. Application of the phantom results to human post mortem CT scan data illustrates this method's faithful reconstruction of coronal and sagittal tissue densities when correlated with actual specimen photographs of a sectioned brain. A special CT procedure, limited basal overlap scanning, is proposed for use on current first generation CT scanners without hardware modification.

Published
1975

211. Treatment of rectal and rectosigmoid polyps; funnel tip suction as an aid in their removal

Author

Paul C. Morton

Subjects
Tip suction, medicine.medical_specialty, Local excision, business.industry, Rectal Neoplasms, Rectum, Suction, digestive system, Surgery, Lesion, Sigmoid Neoplasms, medicine.anatomical_structure, Posterior commissure, Polyps, Colon, Sigmoid, Neoplasms, Medicine, Sphincter, Proper treatment, Humans, medicine.symptom, business
Abstract

The removal of polyps of the upper part of the rectum and rectosigmoid presents technical difficulties of some magnitude if performed through a proctoscope. The proper and complete removal of such a lesion through the anal outlet may give accurate data for proper diagnosis and prognosis and information as to the need for further operation. Piecemeal removal of such lesions should be avoided, because the gross appearance of the polyp, together with sections through the base or pedicle, is most important in determining the proper treatment of the patient. These lesions can be removed by several technics. David 1 advocated section of the sphincter in the posterior commissure with prolapse of the mucous membrane with the polyp and local excision. Others have approached the lesion through the ischiorectal space with local excision and without sphincter section. Removal through a proctoscope with an electric snare provides a simpler form of treatment

Published
1948

212. Primary intussusception of appendix with endometrial implants

Author

Paul C. Morton and Carl S. Oakman

Subjects
medicine.medical_specialty, business.industry, General surgery, Appendix wall, General Medicine, Appendix, bacterial infections and mycoses, medicine.disease, digestive system, digestive system diseases, Appendicitis, Surgery, surgical procedures, operative, medicine.anatomical_structure, Intussusception (medical disorder), medicine, Etiology, Humans, business, neoplasms, Intussusception
Abstract

The writers present a case of primary intussusception of the appendix, gangrenous appendicitis and endometrial implants within the appendix wall. References to the literature and a brief consideration of etiology are given.

Published
1952

213. CHRONIC, DISSEMINATED, NONLIPOID RETICULOENDOTHELIOSIS (HISTIOCYTOSIS X): TREATMENT WITH CORTICOTROPIN AND ANTIBIOTICS, WITH REPORT OF TWO CASES

Author

Paul H. Morton

Subjects
medicine.medical_specialty, Severe combined immunodeficiency, Langerhans cell, PULMONARY HISTIOCYTOSIS, medicine.drug_class, business.industry, Histiocytosis X, Antibiotics, Genetic Diseases, X-Linked, General Medicine, medicine.disease, Dermatology, Anti-Bacterial Agents, Histiocytosis, Langerhans-Cell, Histiocytosis, medicine.anatomical_structure, Adrenocorticotropic Hormone, Immunology, Internal Medicine, medicine, Severe Combined Immunodeficiency, business, Antibiotics, Antitubercular, Mononuclear Phagocyte System
Abstract

Excerpt During the last few years occasional reports have appeared in the literature concerning a group of diseases of the reticuloendothelial system which have the appearance of inflammatory granu...

Published
1957

214. TROPICAL EOSINOPHILIA WITH REPORT OF A CASE TREATED WITH PENICILLIN

Author

Paul H. Morton and Carl C. Jones

Subjects
medicine.medical_specialty, medicine.drug_class, business.industry, Antibiotics, Penicillins, General Medicine, medicine.disease, Dermatology, Tropical eosinophilia, Microbiology, Eosinophils, Penicillin, Leukocyte Count, Tropical Medicine, Eosinophilia, Tropical medicine, Internal Medicine, medicine, medicine.symptom, business, Beta lactam antibiotics, medicine.drug
Abstract

Excerpt Several articles and case reports have recently appeared in the literature concerning this disease which was first described in 1919,5and was given the name tropical eosinophilia by Weingar...

Published
1949

215. A New Differential Analyzer

Author

H. P. Kuehni, H. A. Peterson, and Paul L. Morton

Subjects
Differential analyser, Materials science, Optics, business.industry, law, business, law.invention
Published
1945

216. The California Digital Computer

Author

Paul L. Morton

Subjects
Computational Mathematics, Digital computer, Algebra and Number Theory, Applied Mathematics, Computer graphics (images), Mathematics
Published
1951

217. Chip-based soliton microcomb module using a hybrid semiconductor laser

Author

John E. Bowers, Paul A. Morton, Junqiu Liu, Rui Ning Wang, Tobias J. Kippenberg, Romain Bouchand, Arslan S. Raja, Erwan Lucas, Nicolas Volet, and Jijun He

Subjects
spectroscopy, diode, Physics::Optics, Soliton (optics), 02 engineering and technology, DIODE, 01 natural sciences, Noise (electronics), law.invention, high-power, 010309 optics, law, generation, 0103 physical sciences, Diode, Physics, SPECTROSCOPY, Spectrometer, Laser diode, business.industry, Amplifier, 021001 nanoscience & nanotechnology, Laser, Atomic and Molecular Physics, and Optics, HIGH-POWER, Optoelectronics, 0210 nano-technology, business, Ultrashort pulse, GENERATION
Abstract

Photonic chip-based soliton microcombs have shown rapid progress and have already been used in many system-level applications. There has been substantial progress in realizing soliton microcombs that rely on compact laser sources, culminating in devices that only utilize a semiconductor gain chip or a self-injection-locked laser diode as the pump source. However, generating single solitons with electronically detectable repetition rates from a compact laser module has remained challenging. Here we demonstrate a current-initiated, Si(3)N(4 )chip-based, 99-GHz soliton microcomb driven directly by a compact, semiconductor-based laser. This approach does not require any complex soliton tuning techniques, and single solitons can be accessed by tuning the laser current. Further, we demonstrate a generic, simple, yet reliable, packaging technique to facilitate the fiber-chip interface, which allows building a compact soliton microcomb package that can benefit from the fiber systems operating at high power (> 100 mW). Both techniques can exert immediate impact on chip-based nonlinear photonic applications that require high input power, high output power, and interfacing chip-based devices to mature fiber systems. (C) 2020 Optical Society of America under the terms of the OSA Open Access Publishing Agreement

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218. Early Influences of Microbiota on White Matter Development in Germ-Free Piglets

Author

Sadia Ahmed, Sierrah D. Travis, Francisca V. Díaz-Bahamonde, Demisha D. L. Porter, Sara N. Henry, Julia Mykins, Aditya Ravipati, Aryn Booker, Jing Ju, Hanzhang Ding, Ashwin K. Ramesh, Alicia M. Pickrell, Maosen Wang, Stephen LaConte, Brittany R. Howell, Lijuan Yuan, and Paul D. Morton

Subjects
microbiota, brain, white matter, oligodendrocyte, myelin, germ-free, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Abnormalities in the prefrontal cortex (PFC), as well as the underlying white matter (WM) tracts, lie at the intersection of many neurodevelopmental disorders. The influence of microorganisms on brain development has recently been brought into the clinical and research spotlight as alterations in commensal microbiota are implicated in such disorders, including autism spectrum disorders, schizophrenia, depression, and anxiety via the gut-brain axis. In addition, gut dysbiosis is common in preterm birth patients who often display diffuse WM injury and delayed WM maturation in critical tracts including those within the PFC and corpus callosum. Microbial colonization of the gut aligns with ongoing postnatal processes of oligodendrogenesis and the peak of brain myelination in humans; however, the influence of microbiota on gyral WM development remains elusive. Here, we develop and validate a neonatal germ-free swine model to address these issues, as piglets share key similarities in WM volume, developmental trajectories, and distribution to humans. We find significant region-specific reductions, and sexually dimorphic trends, in WM volume, oligodendrogenesis, and mature oligodendrocyte numbers in germ-free piglets during a key postnatal epoch of myelination. Our findings indicate that microbiota plays a critical role in promoting WM development during early life when the brain is vulnerable to environmental insults that can result in an array of disabilities manifesting later in life.

Published
2021
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219. PINK1/Parkin Influences Cell Cycle by Sequestering TBK1 at Damaged Mitochondria, Inhibiting Mitosis

Author

Shireen A. Sarraf, Dionisia P. Sideris, Nikolaos Giagtzoglou, Lina Ni, Mark W. Kankel, Anindya Sen, Lauren E. Bochicchio, Chiu-Hui Huang, Samuel C. Nussenzweig, Stuart H. Worley, Paul D. Morton, Spyros Artavanis-Tsakonas, Richard J. Youle, and Alicia M. Pickrell

Subjects
Biology (General), QH301-705.5
Abstract

Summary: PINK1 and Parkin are established mediators of mitophagy, the selective removal of damaged mitochondria by autophagy. PINK1 and Parkin have been proposed to act as tumor suppressors, as loss-of-function mutations are correlated with enhanced tumorigenesis. However, it is unclear how PINK1 and Parkin act in coordination during mitophagy to influence the cell cycle. Here we show that PINK1 and Parkin genetically interact with proteins involved in cell cycle regulation, and loss of PINK1 and Parkin accelerates cell growth. PINK1- and Parkin-mediated activation of TBK1 at the mitochondria during mitophagy leads to a block in mitosis due to the sequestration of TBK1 from its physiological role at centrosomes during mitosis. Our study supports a diverse role for the far-reaching, regulatory effects of mitochondrial quality control in cellular homeostasis and demonstrates that the PINK1/Parkin pathway genetically interacts with the cell cycle, providing a framework for understanding the molecular basis linking PINK1 and Parkin to mitosis. : Sarraf et al. use mouse and fly genetics to discover that PINK1 and Parkin influence cell cycle progression. Mitophagy and mitosis independently activate TBK1 at damaged mitochondria and centrosomes, respectively, influencing whether the cell will address mitochondrial quality control or progress with proliferation. Keywords: PINK1, Parkin, mitosis, mitophagy, TBK1, cell cycle, ATM, centrosome, tank binding kinase 1, ik2

Published
2019
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220. Treatment With Tetrahydrobiopterin Improves White Matter Maturation in a Mouse Model for Prenatal Hypoxia in Congenital Heart Disease

Author

Jennifer Romanowicz, Camille Leonetti, Zaenab Dhari, Ludmila Korotcova, Shruti D. Ramachandra, Nemanja Saric, Paul D. Morton, Shivani Bansal, Amrita Cheema, Vittorio Gallo, Richard A. Jonas, and Nobuyuki Ishibashi

Subjects
congenital heart disease, hypoxia, neuroprotection, tetrahydrobiopterin, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background Reduced oxygen delivery in congenital heart disease causes delayed brain maturation and white matter abnormalities in utero. No treatment currently exists. Tetrahydrobiopterin (BH4) is a cofactor for neuronal nitric oxide synthase. BH4 availability is reduced upon NOS activation, such as during hypoxic conditions, and leads to toxin production. We hypothesize that BH4 levels are depleted in the hypoxic brain and that BH4 replacement therapy mitigates the toxic effects of hypoxia on white matter. Methods and Results Transgenic mice were used to visualize oligodendrocytes. Hypoxia was introduced during a period of white matter development equivalent to the human third trimester. BH4 was administered during hypoxia. BH4 levels were depleted in the hypoxic brain by direct quantification (n=7–12). The proliferation (n=3–6), apoptosis (n=3–6), and developmental stage (n=5–8) of oligodendrocytes were determined immunohistologically. Total oligodendrocytes increased after hypoxia, consistent with hypoxia‐induced proliferation seen previously; however, mature oligodendrocytes were less prevalent in hypoxia, and there was accumulation of immature oligodendrocytes. BH4 treatment improved the mature oligodendrocyte number such that it did not differ from normoxia, and accumulation of immature oligodendrocytes was not observed. These results persisted beyond the initial period of hypoxia (n=3–4). Apoptosis increased with hypoxia but decreased with BH4 treatment to normoxic levels. White matter myelin levels decreased following hypoxia by western blot. BH4 treatment normalized myelination (n=6–10). Hypoxia worsened sensory‐motor coordination on balance beam tasks, and BH4 therapy normalized performance (n=5–9). Conclusions Suboptimal BH4 levels influence hypoxic white matter abnormalities. Repurposing BH4 for use during fetal brain development may limit white matter dysmaturation in congenital heart disease.

Published
2019
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221. Endothelin-B Receptor Activation in Astrocytes Regulates the Rate of Oligodendrocyte Regeneration during Remyelination

Author

Timothy R. Hammond, Brian McEllin, Paul D. Morton, Matthew Raymond, Jeff Dupree, and Vittorio Gallo

Subjects
Biology (General), QH301-705.5
Abstract

Reactive astrogliosis is an essential and ubiquitous response to CNS injury, but in some cases, aberrant activation of astrocytes and their release of inhibitory signaling molecules can impair endogenous neural repair processes. Our lab previously identified a secreted intercellular signaling molecule, called endothelin-1 (ET-1), which is expressed at high levels by reactive astrocytes in multiple sclerosis (MS) lesions and limits repair by delaying oligodendrocyte progenitor cell (OPC) maturation. However, as ET receptors are widely expressed on neural cells, the cell- and receptor-specific mechanisms of OPC inhibition by ET-1 action remain undefined. Using pharmacological approaches and cell-specific endothelin receptor (EDNR) ablation, we show that ET-1 acts selectively through EDNRB on astrocytes—and not OPCs—to indirectly inhibit remyelination. These results demonstrate that targeting specific pathways in reactive astrocytes represents a promising therapeutic target in diseases with extensive reactive astrogliosis, including MS.

Published
2015
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222. Microstructural Alterations and Oligodendrocyte Dysmaturation in White Matter After Cardiopulmonary Bypass in a Juvenile Porcine Model

Author

Gary R. Stinnett, Stephen Lin, Alexandru V. Korotcov, Ludmila Korotcova, Paul D. Morton, Shruti D. Ramachandra, Angeline Pham, Sonali Kumar, Kota Agematsu, David Zurakowski, Paul C. Wang, Richard A. Jonas, and Nobuyuki Ishibashi

Subjects
cardiopulmonary bypass, congenital heart disease, diffusion tensor imaging, thoracic surgery, white matter, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

BackgroundNewly developed white matter (WM) injury is common after cardiopulmonary bypass (CPB) in severe/complex congenital heart disease. Fractional anisotropy (FA) allows measurement of macroscopic organization of WM pathology but has rarely been applied after CPB. The aims of our animal study were to define CPB‐induced FA alterations and to determine correlations between these changes and cellular events after congenital heart disease surgery. Methods and ResultsNormal porcine WM development was first assessed between 3 and 7 weeks of age: 3‐week‐old piglets were randomly assigned to 1 of 3 CPB‐induced insults. FA was analyzed in 31 WM structures. WM oligodendrocytes, astrocytes, and microglia were assessed immunohistologically. Normal porcine WM development resembles human WM development in early infancy. We found region‐specific WM vulnerability to insults associated with CPB. FA changes after CPB were also insult dependent. Within various WM areas, WM within the frontal cortex was susceptible, suggesting that FA in the frontal cortex should be a biomarker for WM injury after CPB. FA increases occur parallel to cellular processes of WM maturation during normal development; however, they are altered following surgery. CPB‐induced oligodendrocyte dysmaturation, astrogliosis, and microglial expansion affect these changes. FA enabled capturing CPB‐induced cellular events 4 weeks postoperatively. Regions most resilient to CPB‐induced FA reduction were those that maintained mature oligodendrocytes. ConclusionsReducing alterations of oligodendrocyte development in the frontal cortex can be both a metric and a goal to improve neurodevelopmental impairment in the congenital heart disease population. Studies using this model can provide important data needed to better interpret human imaging studies.

Published
2017
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223. Inhibition of NADPH oxidase activation in oligodendrocytes reduces cytotoxicity following trauma.

Author

Joshua T Johnstone, Paul D Morton, Arumugam R Jayakumar, Andrea L Johnstone, Han Gao, Valerie Bracchi-Ricard, Damien D Pearse, Michael D Norenberg, and John R Bethea

Subjects
Medicine, Science
Abstract

Spinal cord injury is a debilitating neurological disorder that initiates a cascade of cellular events that result in a period of secondary damage that can last for months after the initial trauma. The ensuing outcome of these prolonged cellular perturbations is the induction of neuronal and glial cell death through excitotoxic mechanisms and subsequent free radical production. We have previously shown that astrocytes can directly induce oligodendrocyte death following trauma, but the mechanisms regulating this process within the oligodendrocyte remain unclear. Here we provide evidence demonstrating that astrocytes directly regulate oligodendrocyte death after trauma by inducing activation of NADPH oxidase within oligodendrocytes. Spinal cord injury resulted in a significant increase in oxidative damage which correlated with elevated expression of the gp91 phox subunit of the NADPH oxidase enzyme. Immunohistochemical analysis confirmed the presence of gp91 phox in oligodendrocytes in vitro and at 1 week following spinal cord injury. Exposure of oligodendrocytes to media from injured astrocytes resulted in an increase in oligodendrocyte NADPH oxidase activity. Inhibition of NADPH oxidase activation was sufficient to attenuate oligodendrocyte death in vitro and at 1 week following spinal cord injury, suggesting that excitotoxicity of oligodendrocytes after trauma is dependent on the intrinsic activation of the NADPH oxidase enzyme. Acute administration of the NADPH oxidase inhibitor apocynin and the alpha-amino-3-hydroxy-5-methylisoxazole-4-propionate channel blocker 2,3-dihydroxy-6-nitro-7-sulfamoyl-benzo[f]quinoxaline-2,3-dione significantly improved locomotor behavior and preserved descending axon fibers following spinal cord injury. These studies lead to a better understanding of oligodendrocyte death after trauma and identify potential therapeutic targets in disorders involving demyelination and oligodendrocyte death.

Published
2013
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