Your search keyword '"Hurtig, H."' showing total 266 results

51. TDP?43 pathology occurs infrequently in multiple system atrophy.

Author

Geser, F., Malunda, J. A., Hurtig, H. I., Duda, J. E., Wenning, G. K., Gilman, S., Low, P. A., Lee, V. M.-Y., and Trojanowski, J. Q.

Subjects

ATROPHY, NEUROLOGICAL disorders, NEUROBIOLOGY, SARCOMA, DNA

Abstract

F. Geser, J. A. Malunda, H. I. Hurtig, J. E. Duda, G. K. Wenning, S. Gilman, P. A. Low, V. M.?Y. Lee and J. Q. Trojanowski (2011) Neuropathology and Applied Neurobiology 358-365 ? The ??synucleinopathy multiple system atrophy (MSA) and diseases defined by pathological 43?kDa transactive response DNA?binding protein (TDP?43) or fused in sarcoma (FUS) aggregates such as amyotrophic lateral sclerosis and frontotemporal lobar degeneration show overlapping clinico?pathological features. Consequently, we examined MSA for evidence of TDP?43 or FUS pathology utilizing immunohistochemical studies in autopsy material from 29 MSA patients. TDP?43 pathology was generally rare, and there were no FUS lesions. The TDP?43 lesions were located predominantly in medio?temporal lobe and subcortical brain areas and were comprised mainly of dystrophic processes and perivascular (and subpial) lesions. The multisystem clinical symptoms and signs of MSA, and in particular the neurobehavioural/cognitive and pyramidal features, appear not to result from concomitant TDP?43 or FUS pathology, but rather from widespread white matter ??synuclein positive glial cytoplasmic inclusions and neurodegeneration in keeping with a primary ??synuclein?mediated oligodendrogliopathy. The gliodegenerative disease MSA evidently results from different pathogenetic mechanisms than neurodegenerative diseases linked to pathological TDP?43. [ABSTRACT FROM AUTHOR]

Published

2011

52. Who was the man who discovered the "Lewy bodies"?

Author

Rodrigues e Silva AM, Geldsetzer F, Holdorff B, Kielhorn FW, Balzer-Geldsetzer M, Oertel WH, Hurtig H, Dodel R, Rodrigues e Silva, Antonio M, Geldsetzer, Felix, Holdorff, Bernd, Kielhorn, Friedrich W, Balzer-Geldsetzer, Monika, Oertel, Wolfgang H, Hurtig, Howard, and Dodel, Richard

Abstract

In 1912, Fritz Heinrich Lewy described neuronal inclusions in the brain of patients who had suffered from Paralysis agitans (i.e., Parkinson's disease). Later, these findings became the so-called "Lewy bodies." However, little is known about the man who made this discovery. Our aim was to investigate Lewy's private and professional life and to gather information for a detailed biography. We contacted over 100 archives, libraries, and museums in Germany, Poland, Switzerland, United Kingdom, and United States. Over 300 documents, publications, and photos were collected. Lewy was born in Berlin, Germany in 1885 and lived there until 1933. After his dismissal on racial grounds by the Nazis, Lewy emigrated to England in 1933 and to the United States of America in 1934, where he lived and worked until his death in 1950. This article gives a summary of Lewy's life and briefly presents his contribution to German and American neurology. [ABSTRACT FROM AUTHOR]

Published

2010

53. Sentence comprehension and praxis deficits in Parkinson's disease

Author

MD, M. G., primary, Carvell, S., additional, Gollomp, S., additional, Stern, M. B., additional, RN, G. V., additional, and Hurtig, H. I., additional

Published

1991

54. Neuromythology IX and DATATOP

Author

Hurtig, H. I., primary

Published

1991

55. Unexpected abundance of pathological tau in progressive supranuclear palsy white matter.

Author

Zhukareva V, Joyce S, Schuck T, Van Deerlin V, Hurtig H, Albin R, Gilman S, Chin S, Miller B, Trojanowski JQ, and Lee VM

Published

2006

56. Fluphenazine and postherpetic neuralgia

Author

Hurtig, H. I., primary

Published

1990

57. [99mTc]TRODAT-1 SPECT imaging correlates with odor identification in early Parkinson disease.

Author

Siderowf A, Newberg A, Chou KL, Lloyd M, Colcher A, Hurtig HI, Stern MB, Doty RL, Mozley PD, Wintering N, Duda JE, Weintraub D, Moberg PJ, Siderowf, A, Newberg, A, Chou, K L, Lloyd, M, Colcher, A, Hurtig, H I, and Stern, M B

Published

2005

58. Alpha-synuclein cortical Lewy bodies correlate with dementia in Parkinson's disease.

Author

Hurtig, H I, Trojanowski, J Q, Galvin, J, Ewbank, D, Schmidt, M L, Lee, V M, Clark, C M, Glosser, G, Stern, M B, Gollomp, S M, and Arnold, S E

Published

2000

59. Cerebral hemodynamics in the diagnosis of normal pressure hydrocephalus.

Author

Kushner, Michael, Younkin, Donald, Weinberger, Jesse, Hurtig, Howard, Goldberg, Herbert, Reivich, Martin, Kushner, M, Younkin, D, Weinberger, J, Hurtig, H, Goldberg, H, and Reivich, M

Published

1984

60. Regional cerebral blood flow in stroke: hemispheric effects of cognitive activity.

Author

Gur, R C, Gur, R E, Silver, F L, Obrist, W D, Skolnick, B E, Kushner, M, Hurtig, H I, and Reivich, M

Published

1987

61. Posey and Spiller and progressive supranuclear palsy: an incorrect attribution.

Author

Siderowf, Andrew D., Galetta, Steven L., Hurtig, Howard I., Liu, Grant T., Siderowf, A D, Galetta, S L, Hurtig, H I, and Liu, G T

Published

1998

62. Slowly progressive aphasia without generalized dementia: studies with positron emission tomography.

Author

Chawluk, John B., Mesulam, M.-Marsel, Hurtig, Howard, Kushner, Michael, Weintraub, Sandra, Saykin, Andrew, Rubin, Nan, Alavi, Abass, Reivich, Martin, Chawluk, J B, Mesulam, M M, Hurtig, H, Kushner, M, Weintraub, S, Saykin, A, Rubin, N, Alavi, A, and Reivich, M

Published

1986

63. Corticobasal syndrome and primary progressive aphasia as manifestations of LRRK2gene mutationsSYMBOLSYMBOL

Author

Chen-Plotkin, A S., Yuan, W, Anderson, C, Wood, E McCarty, Hurtig, H I., Clark, C M., Miller, B L., Lee, V M.-Y., Trojanowski, J Q., Grossman, M, and Deerlin, V M. Van

Abstract

Mutations in the LRRK2gene are an important cause of familial and nonfamilial parkinsonism. Despite pleomorphic pathology, LRRK2mutations are believed to manifest clinically as typical Parkinson disease (PD). However, most genetic screens have been limited to PD clinic populations.

Published

2008

64. Dopamine supports sentence comprehension in Parkinson`s Disease

Author

Grossman, M., Glosser, G., Kalmanson, J., Morris, J., Stern, M. B., and Hurtig, H. I.

Published

2001

65. A multicenter trial of ropinirole as adjunct treatment for Parkinson's disease

Author

Lieberman, A., Olanow, C. W., Sethi, K., Swanson, P., Waters, C. H., Fahn, S., Hurtig, H., and Yahr, M.

Abstract

To evaluate the nonergot dopamine agonist ropinirole as an adjunct to L-dopa in a randomized, double-blind trial in PD patients with motor fluctuations.

Published

1998

66. The Decision-Making Process and Insect Control

Author

Hurtig, H.

Abstract

AbstractThe decision-making process in insect control at the practical level involves not only the complex relationships between pests and their environment, but also equally complex human relationships and values. The actions advantageous to one of our resources may be harmful to another. Ultimately, the process of decision-making, at the individual problem level, must be integrated with economic factors, public health and sociological considerations. Calculated risks must be taken, but decision-making should he based on the evaluation of data bearing on efficiency, economy and safety of use of any method, including pesticides. Integrated control as a newly repopularized concept is examined in relation to the economics of its potential application in Canada. The concept of safety of pesticide residues in food is discussed and related to “good agricultural practices.” Three operative levels of decision-making are examined; the regulatory, quarantine and pest suppression activities and the role of the local advisory committees on pest control. The author expresses concern that the current public preoccupation with establishing safeguards for pesticide use does not begin and end merely with legislative action and strengthening of enforcement agencies. A desirable parallel result likely to be overlooked would be administrative and financial support for research on how the use of pesticides may be developed in the best interests of the community as a whole.

Published

1964

67. Magnetic resonance imaging in Parkinson's disease and parkinsonian syndromes.

Author

Stern, M. B., Braffman, B. H., Skolnick, B. E., Hurtig, H. I., and Grossman, R. I.

Published

1989

68. Persistent cerebellar ataxia after exposure to toluene.

Author

Boor, John William, Hurtig, Howard I., Boor, J W, and Hurtig, H I

Published

1977

69. Emboli and open heart surgery

Author

Hurtig, H. I., primary and Gonzalez-Scarano, F., additional

Published

1983

70. Neurologic complications of coronary artery bypass grafting: Case-control study

Author

Gonzalez-Scarano, F., primary and Hurtig, H. I., additional

Published

1981

71. Recent Developments in Parkinson's Disease

Author

Hurtig, H. I., primary

Published

1987

72. "Locked-In" State With Bilateral Midbrain Infarcts

Author

Karp, J. S., primary and Hurtig, H. I., additional

Published

1974

73. Superficial temporal-middle cerebral artery anastomosis: Effects on vascular, neurologic, and neuropsychological functions

Author

Younkin, D., primary, Hungerbuhler, J. P., additional, O'Connor, M., additional, Goldberg, H., additional, Burke, A., additional, Kushner, M., additional, Hurtig, H., additional, Obrist, W., additional, Gordon, J., additional, Gur, R., additional, and Reivich, M., additional

Published

1985

74. Long-distance Transport of Pesticides

Author

Hurtig, H., primary

Published

1971

75. Report of the Committee on Establishment of Standard Test Methods for Determination of Insect Resistance

Author

Hurtig, H., primary, Lindquist, A. W., additional, Ludvik, G. F., additional, Quarterman, K. D., additional, and Reynolds, H. T., additional

Published

1963

76. Report of the Program Committee for 1963

Author

Bray, D. F., primary, Carman, G. E., additional, Stone, P. C., additional, Peterson, D. G., additional, Davis, L. G., additional, Mcgregor, W. S., additional, Jones, L. S., additional, Blake, G., additional, Stitt, L. L., additional, Kenaga, E. E., additional, Sternburg, J. G., additional, Forgash, A. J., additional, Dawsey, L. H., additional, Borror, D. J., additional, Byers, G. W., additional, Rosen, J. G., additional, Walle, G. S., additional, Sabrosky, C. W., additional, Art, R. M. B., additional, Hardy, D. E., additional, Philip, C. B., additional, Usinger, R. L., additional, Becker, E. C., additional, Ebeling, W., additional, Johnson, P. C., additional, Kowal, R. J., additional, Laffoon, J. L., additional, Lilly, J. H., additional, Morrison, F. O., additional, Spangler, R. J., additional, Slater, J. A., additional, Baker, H., additional, Mcalister, L. C., additional, Osmun, J. V., additional, Pepper, J. O., additional, Hurtig, H., additional, Billings, S. C., additional, Cowan, F. T., additional, Hughes, J. H., additional, Knutson, H., additional, Magner, J. M., additional, Petty, H. B., additional, Simanton, W. A., additional, Whiteside, J. M., additional, Anderson, W. H., additional, Holway, R. T., additional, Dorward, K., additional, Iverson, L. G. K., additional, Knight, K. L., additional, Mccauley, W. E., additional, Eden, W. G., additional, Ritcher, P. O., additional, Michener, C. D., additional, Reed, W. D., additional, Cole, A. C., additional, Dahm, P. A., additional, Knipling, E. F., additional, West, A. S., additional, Wolfenbarger, D. O., additional, Richmond, R. G., additional, Rathbone, R. B., additional, Budd, M. R., additional, Hall, D. G., additional, Chapman, P. J., additional, Gunderson, H., additional, Hansberry, R., additional, Linsley, E. G., additional, Travis, B. V., additional, and Hoffmann, C. H., additional

Published

1964

77. Statement of the Entomological Society of America Regarding the Adoption of Common Names for Chemicals

Author

Baker, H., primary, Osmun, J. V., additional, Hurtig, H., additional, McAlister, L. C., additional, Pepper, J. O., additional, and Billings, S. C., additional

Published

1963

78. Report of the Committee on Insecticide Terminology

Author

Baker, H., primary, Brogdon, J. E., additional, Bussart, J. E., additional, Hurtig, H., additional, Osmun, J. V., additional, and Billings, S. C., additional

Published

1963

79. Reports of Special Committees for 1961

Author

Mills, A. S., primary, Porter, J. E., additional, King, J. R., additional, Baranowski, R. M., additional, Berner, L., additional, Smith, C. N., additional, Mayeux, H. W., additional, Dekle, G. W., additional, Maxwell, L. S., additional, Butcher, G. F., additional, Bellows, J. M., additional, Haynie, J. D., additional, Stains, G. S., additional, Walker, T. J., additional, Wood, R. J., additional, Dowling, C. F., additional, Kriner, R. R., additional, Mead, F. W., additional, Murphey, M., additional, Morris, S. R., additional, Mayeux, H. S., additional, Cory, E. N., additional, Guyton, F. E., additional, Howell, D. E., additional, Knight, H. H., additional, Hansberry, R., additional, Jones, L. S., additional, Slater, J. A., additional, Greyson, J. M., additional, Hurtig, H., additional, Lindquist, A. W., additional, Ludvik, G. F., additional, Quarterman, K. D., additional, Reynolds, H. D., additional, Carruth, L. A., additional, Painter, R. H., additional, Davidson, R. H., additional, Newsom, L. D., additional, Steinhaus, E. A., additional, and Philip, C. B., additional

Published

1962

80. TOXICITY OF SELECTED ORGANIC COMPOUNDS TO INSECTS: PART I. TESTS FOR GENERAL TOXICITY ON LARVAE OF MUSCA, TRIBOLIUM, AND EPHESTIA, AND ADULTS OF SITOPHILUS

Author

Brown, A. W. A., primary, Robinson, D. B. W., additional, Hurtig, H., additional, and Wenner, B. J., additional

Published

1948

81. CHARACTERISTICS OF SPRAY DEPOSITS RESULTING FROM AIRCRAFT APPLICATION OF OIL-CARRIER SPRAYS

Author

Sexsmith, J. J., primary, Anderson, D. T., additional, Russell, G. C., additional, Hopewell, W. W., additional, and Hurtig, H., additional

Published

1957

82. Slide Coatings for Aerosol Droplet Collection and Preservation

Author

Hurtig, H., primary and Perry, A. S., additional

Published

1950

83. Transport de pesticides à longue distance

Author

Hurtig, H., primary

Published

1971

84. Specification for Pesticides: Insecticides, Rodenticidea, Molluscicides, Herbicides, Auxiliary Chemicals, Spraying and Dusting Apparatus. Second Edition, 1961; 523 pages, 31 figures, 2 tables. World Health Organization, Palais des Nations, Geneva. Price $10.00 (Clothbound).

Author

Hurtig, H., primary

Published

1961

85. Organic Insecticides for the Lesser Migratory Locust

Author

Brown, A. W. A., primary and Hurtig, H., additional

Published

1947

86. Insecticide Terminology Committee Announcement

Author

Baker, H., primary, Hurtig, H., additional, Mcalister, L. C., additional, Osmun, J. V., additional, Pepper, J. O., additional, and Billings, S. C., additional

Published

1963

87. Reports of Special Committees for 1963

Author

Hurtig, H., primary, Lindquist, A. W., additional, Ludvik, G. F., additional, Quarterman, K. D., additional, Reynolds, H. T., additional, Senechal, G., additional, Owens, H., additional, Travis, R. V., additional, Bickley, W. E., additional, Cochran, D. G., additional, Haeussler, G. J., additional, Gressitt, J. L., additional, Holloway, J. K., additional, Knipling, E. F., additional, Ortega, A. C., additional, Sabrosky, C. W., additional, Brown, A. W. A., additional, Beard, R. L., additional, Bushland, R. C., additional, Eisner, T., additional, Ferguson, G. R., additional, Hocking, B., additional, Kohls, G. M., additional, O'Brien, R. D., additional, Smallman, B. N., additional, Ross, H. H., additional, Sternburg, J., additional, Weber, N. A., additional, Richards, A. G., additional, Barnes, M. M., additional, Jones, G. D., additional, Smith, R. F., additional, Weiden, M. H. J., additional, Wharton, G. W., additional, and Oman, P., additional

Published

1964

88. Cerebral Atrophy Is Highly Correlated with the Severity of Alzheimer's Dementia: A Volumetric Computed Tomographic Study.

Author

Chawluk, J., Alavi, A., Hurtig, H., Dann, R., Bais, S., Zimmerman, R. A., and Reivich, M.

Published

1986

89. Regional Cerebral Blood Flow (rCBF) During Cognitive Activation in Focal Epilepsy.

Author

Gur, R. C., Skolnick, B. E., Susman, N. M., Hurtig, H., Barry, E., Gur, R. E., and Obrist, W. D.

Published

1985

90. Altered Patterns of Regional Cerebral Glucose Metabolism in Aging and Dementia.

Author

Chawluk, J., Alavi, A., Hurtig, H., Dann, R., Rosen, M., Kushner, M., Silver, F., and Reivich, M.

Published

1985

91. Effects of Cognitive Stimulation on Cerebral Blood Flow After Stroke and Transient Ischemic Attack.

Author

GUR, R. C., BURKE, A., GUR, R. E., YOUNKIN, D., HURTIG, H., SHAPIRO, H., PISTONE, L., and REIVICH, M.

Published

1982

92. Anticholinergics for Parkinson disease.

Author

Hurtig, Howard I. and Hurtig, H I

Published

1980

93. Correlates of Clinical Decline in Early Parkinson's Disease

Author

Fahn, S., Brin, M., Burke, R., Bressman, S., Tetrud, J., Langston, W., Jankovic, J., Kurlan, R., Plumb, S., Odoroff, C., Tanner, C., Goetz, C., Klawans, H., Shannon, K., Lang, A., Weiner, W., Ramos, J., Penney, J., Young, A., Starosta, S., Hurtig, H., Stern, M., Gollomp, S., Pfeiffer, R., Friedman, J., Olanow, W., Paulson, G., Tsui, J., Nutt, J., Rodnitzky, R., Grimes, D., Hassan, M., LeWitt, P., Hoehn, M., and Bennett, J.

Published

1987

94. Book Review: Specification for Pesticides: Insecticides, Rodenticidea, Molluscicides, Herbicides, Auxiliary Chemicals, Spraying and Dusting Apparatus

Author

Hurtig, H.

Published

1961

95. Genetic and phenotypic characterization of Parkinson's disease at the clinic-wide level.

Author

Tropea TF, Hartstone W, Amari N, Baum D, Rick J, Suh E, Zhang H, Paul RA, Han N, Zack R, Brody EM, Albuja I, James J, Spindler M, Deik A, Aamodt WW, Dahodwala N, Hamedani A, Lasker A, Hurtig H, Stern M, Weintraub D, Vaswani P, Willis AW, Siderowf A, Xie SX, Van Deerlin V, and Chen-Plotkin AS

Abstract

Observational studies in Parkinson's disease (PD) deeply characterize relatively small numbers of participants. The Molecular Integration in Neurological Diagnosis Initiative seeks to characterize molecular and clinical features of every PD patient at the University of Pennsylvania (UPenn). The objectives of this study are to determine the feasibility of genetic characterization in PD and assess clinical features by sex and GBA1/LRRK2 status on a clinic-wide scale. All PD patients with clinical visits at the UPenn PD Center between 9/2018 and 12/2022 were eligible. Blood or saliva were collected, and a clinical questionnaire administered. Genotyping at 14 GBA1 and 8 LRRK2 variants was performed. PD symptoms were compared by sex and gene groups. 2063 patients were approached and 1,689 (82%) were enrolled, with 374 (18%) declining to participate. 608 (36%) females were enrolled, 159 (9%) carried a GBA1 variant, and 44 (3%) carried a LRRK2 variant. Compared with males, females across gene groups more frequently reported dystonia (53% vs 46%, p = 0.01) and anxiety (64% vs 55%, p < 0.01), but less frequently reported cognitive impairment (10% vs 49%, p < 0.01) and vivid dreaming (53% vs 60%, p = 0.01). GBA1 variant carriers more frequently reported anxiety (67% vs 57%, p = 0.04) and depression (62% vs 46%, p < 0.01) than non-carriers; LRRK2 variant carriers did not differ from non-carriers. We report feasibility for near-clinic-wide enrollment and characterization of individuals with PD during clinical visits at a high-volume academic center. Clinical symptoms differ by sex and GBA1, but not LRRK2, status., (© 2024. The Author(s).)

Published

2024

96. Whole Clinic Research Enrollment in Parkinson's Disease: The Molecular Integration in Neurological Diagnosis (MIND) Study.

Author

Tropea TF, Amari N, Han N, Rick J, Suh E, Akhtar RS, Dahodwala N, Deik A, Gonzalez-Alegre P, Hurtig H, Siderowf A, Spindler M, Stern M, Thenganatt MA, Weintraub D, Willis AW, Van Deerlin V, and Chen-Plotkin A

Subjects

Aged, Cohort Studies, Glucosylceramidase genetics, Humans, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 genetics, Mutation, Parkinson Disease diagnosis, Parkinson Disease genetics

Abstract

Background: Observational studies in Parkinson's disease (PD) have focused on relatively small numbers of research participants who are studied extensively. The Molecular Integration in Neurological Diagnosis Initiative at the University of Pennsylvania aims to characterize molecular and clinical features of PD in every patient in a large academic center., Objective: To determine the feasibility and interest in a global-capture biomarker research protocol. Additionally, to describe the clinical characteristics and GBA and LRRK2 variant carrier status among participants., Methods: All patients at UPenn with a clinical diagnosis of PD were eligible. Informed consent included options for access to the medical record, future recontact, and use of biosamples for additional studies. A blood sample and a completed questionnaire were obtained from participants. Targeted genotyping for four GBA and eight LRRK2 variants was performed, with plasma and DNA banked for future research., Results: Between September 2018 and December 2019, 704 PD patients were approached for enrollment; 652 (92.6%) enrolled, 28 (3.97%) declined, and 24 (3.41%) did not meet eligibility criteria. Median age was 69 (IQR 63&#95;75) years, disease duration was 5.41 (IQR 2.49&#95;9.95) years, and 11.10%of the cohort was non-white. Disease risk-associated variants in GBA were identified in 39 participants (5.98%) and in LRRK2 in 16 participants (2.45%)., Conclusions: We report the clinical and genetic characteristics of PD patients in an all-comers, global capture protocol from an academic center. Patient interest in participation and yield for identification of GBA and LRRK2 mutation carriers is high, demonstrating feasibility of PD clinic-wide molecular characterization.

Published

2021

97. ADNC-RS, a clinical-genetic risk score, predicts Alzheimer's pathology in autopsy-confirmed Parkinson's disease and Dementia with Lewy bodies.

Author

Dai DL, Tropea TF, Robinson JL, Suh E, Hurtig H, Weintraub D, Van Deerlin V, Lee EB, Trojanowski JQ, and Chen-Plotkin AS

Subjects

Age of Onset, Aged, Aged, 80 and over, Alzheimer Disease pathology, Female, Genotype, Humans, Lewy Body Disease genetics, Male, Middle Aged, Parkinson Disease genetics, Polymorphism, Single Nucleotide, Risk Factors, Lewy Body Disease pathology, Neurofibrillary Tangles pathology, Parkinson Disease pathology, Plaque, Amyloid pathology

Abstract

Growing evidence suggests overlap between Alzheimer's disease (AD) and Parkinson's disease (PD) pathophysiology in a subset of patients. Indeed, 50-80% of autopsy cases with a primary clinicopathological diagnosis of Lewy body disease (LBD)-most commonly manifesting during life as PD-have concomitant amyloid-beta and tau pathology, the defining pathologies of AD. Here we evaluated common genetic variants in genome-wide association with AD as predictors of concomitant AD pathology in the brains of people with a primary clinicopathological diagnosis of PD or Dementia with Lewy Bodies (DLB), diseases both characterized by neuronal Lewy bodies. In the first stage of our study, 127 consecutive autopsy-confirmed cases of PD or DLB from a single center were assessed for AD neuropathological change (ADNC), and these same cases were genotyped at 20 single nucleotide polymorphisms (SNPs) found by genome-wide association study to associate with risk for AD. In these 127 training set individuals, we developed a logistic regression model predicting the presence of ADNC, using backward stepwise regression for model selection and tenfold cross-validation to estimate performance. The best-fit model generated a risk score for ADNC (ADNC-RS) based on age at disease onset and genotype at three SNPs (APOE, BIN1, and SORL1 loci), with an area under the receiver operating curve (AUC) of 0.751 in our training set. In the replication stage of our study, we assessed model performance in a separate test set of the next 81 individuals genotyped in our center. In the test set, the AUC was 0.781, and individuals with ADNC-RS in the top quintile had four-fold increased likelihood of having AD pathology at autopsy compared with those in each of the lowest two quintiles. Finally, in the validation stage of our study, we applied our ADNC-RS model to 70 LBD individuals from 20 Alzheimer's Disease Research Centers (ADRC) whose autopsy and genetic data were available in the National Alzheimer's Coordinating Center (NACC) database. In this validation set, the AUC was 0.754. Thus, in patients with autopsy-confirmed PD or DLB, a simple model incorporating three AD-risk SNPs and age at disease onset substantially enriches for concomitant AD pathology at autopsy, with implications for identifying LBD patients in which targeting amyloid-beta or tau is a therapeutic strategy.

Published

2020

98. The Many Faces of Parkinson's Disease.

Author

Horn S and Hurtig H

Abstract

The total cost of Parkinson disease (PD), which affects nearly 1 million people in the US is $52 billion every year, with $25.4 billion attributable to direct medical costs such as hospitalizations and medication, and $26.5 billion in non-medical costs like missed work, lost wages, early forced retirement, and family caregiver time. The more we know about PD's non-motor symptoms-depression, dementia, fatigue, and others-the better we can treat, and perhaps find a cure, for this neurological disorder ., (Copyright 2019 The Dana Foundation All Rights Reserved.)

Published

2019

99. Drug-induced phospholipidosis caused by combinations of common drugs in vitro.

Author

Glock M, Muehlbacher M, Hurtig H, Tripal P, and Kornhuber J

Subjects

Cell Line, Tumor, Drug Interactions, Humans, Lipidoses metabolism, Drug Combinations, Drug-Related Side Effects and Adverse Reactions, Lipidoses chemically induced, Phospholipids metabolism

Abstract

Drug-induced phospholipidosis (DIPLD), characterized by the accumulation of phospholipids within lysosomes, is suspected to impair lysosomal function and considered an adverse side effect of the administered medication. The increasing use of polypharmacy and the resultant elevated risks of adverse drug reactions raise the need to explore the effects of drug combinations with respect to their influence on side effects, such as DIPLD. In this study, we utilized an in vitro assay to investigate DIPLD that was caused by 24 commonly used drugs applied alone and in binary combinations with each other. Moreover, we attempted to predict the extent of DIPLD resulting from the combinations using a simple additive approach based on the increase in phospholipid levels caused by the single drugs. The results suggest that DIPLD, which was caused by combinations of drugs, occurs in an additive manner, depending on total drug concentration. Furthermore, we show that the extent of DIPLD can be predicted from the DIPLD caused by the single drugs. Thus, the simultaneous use of multiple drugs with PLD-inducing properties increases the event risk, as well as the severity of drug-induced phospholipidosis. The findings underline the importance of considering the DIPLD-inducing properties of drugs, especially in the context of polypharmacy., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

100. The Penn Parkinson's Daily Activities Questionnaire-15: Psychometric properties of a brief assessment of cognitive instrumental activities of daily living in Parkinson's disease.

Author

Brennan L, Siderowf A, Rubright JD, Rick J, Dahodwala N, Duda JE, Hurtig H, Stern M, Xie SX, Rennert L, Karlawish J, Shea JA, Trojanowski JQ, and Weintraub D

Subjects

Activities of Daily Living, Aged, Cognition Disorders etiology, Female, Humans, Male, Parkinson Disease psychology, Cognition Disorders diagnosis, Parkinson Disease complications, Psychometrics methods, Surveys and Questionnaires

Abstract

Introduction: To describe the psychometric properties of the Penn Parkinson's Daily Activities Questionnaire-15 (PDAQ-15), a 15-item measure of cognitive instrumental activities of daily living for Parkinson's disease (PD) patients derived from the original 50-item PDAQ., Methods: PDAQ-15 items were chosen by expert consensus. Knowledgeable informants of PD participants (n = 161) completed the PDAQ-15. Knowledgeable informants were defined as an individual having regular contact with the PD participant. PD participants were assigned a diagnosis of normal cognition, mild cognitive impairment, or dementia based on expert consensus., Results: PDAQ-15 scores correlated strongly with global cognition (Dementia Rating Scale-2, r = 0.71, p < 0.001) and a performance-based functional measure (Direct Assessment of Functional Status, r = 0.83; p < 0.001). PDAQ-15 scores accurately discriminated between non-demented PD participants (normal cognition/mild cognitive impairment) and PD with dementia (ROC curve area = 0.91), participants with and without any cognitive impairment (normal cognition versus mild cognitive impairment/dementia, ROC curve area = 0.85) and between participants with mild cognitive impairment and dementia (ROC curve area = 0.84)., Conclusions: The PDAQ-15 shows good discriminant validity across cognitive stages, correlates highly with global cognitive performance, and appears suitable to assess daily cognitive functioning in PD., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016