Zobrazeno 1 - 10
of 172
pro vyhledávání: '"L G, GOLDFARB"'
Autor:
D G, Tikhonov, L G, Goldfarb, T S, Neustroeva, N V, Yakovleva, L F, Timofeev, I P, Luckan, F A, Platonov
Publikováno v:
Problemy sotsial'noi gigieny, zdravookhraneniia i istorii meditsiny. (6)
The article presents results of investigation of certain unclear aspects of mortality of patients with spinocerebellar ataxia type I including patients with the same number of CAG-repetitions. The analysis of mortality of patients observed from 1993
Autor:
Stephen J. O'Brien, Taras K. Oleksyk, A. P. Danilova, Tatyana M. Sivtseva, L. G. Goldfarb, Michael W. Smith, Sadeep Shrestha, Vladimir L. Osakovsky
Publikováno v:
European Journal of Immunogenetics. 31:121-128
Since the discovery of Viliuisk encephalomyelitis (VE) in 1887, scientists have tried to understand the natural history and aetiology of this endemic neurological disorder among the native Sakha population of Central Siberia. Familial aggregation and
Autor:
L. G. Goldfarb, Yong-Xing Zhou, Shoji Tsuji, B.-X. Yang, D.-A. Wang, N. Sambuughin, Hee-Suk Lee, G.-X. Wang, W.-D. Li, L.-S. Zhou, B.-S. Tang
Publikováno v:
Neurology. 51:595-598
Sixteen patients from nine Chinese families with spinocerebellar ataxia type 2 (SCA2) were heterozygous for a CAG repeat expansion in the SCA2 gene containing 37 to 56 repeats, whereas the normal alleles carried 14 to 28 repeats. One or two CAA tripl
Autor:
J. Estupinan, Hee-Suk Lee, Amos D. Korczyn, D. C. Gajdusek, Larisa Cervenakova, Patrick O. Brown, Cindy L. Vnencak-Jones, S. Richardson, J. Chapman, Robert B. Petersen, L. G. Goldfarb
Publikováno v:
Neurology. 51:548-553
Background:TheAPOEgenotype has been shown to influence the risk of developing sporadic and familial AD. This effect is isoform-dependent, theAPOEϵ4 allele increasing susceptibility and theAPOEϵ2 allele providing protection. Amyloid formation is an
Autor:
C. A. McLean, V. A. Vladimirtsev, I. A. Prokhorova, L. G. Goldfarb, D. M. Asher, A. I. Vladimirtsev, V. P. Alekseev, D. C. Gajdusek
Publikováno v:
Neuropathology and Applied Neurobiology. 23:212-217
Autor:
David A. Bennett, B. Bernard, L. G. Goldfarb, Larisa Cervenakova, P. Brown, Norman L. Foster, Elizabeth J. Cochran, K. Kenney, D. F. Benson
Publikováno v:
Neurology. 47:727-733
We report a familial form of Creutzfeldt-Jakob disease, associated with a unique insert mutation of the PRNP gene in an American family of Ukrainian origin. Ten family members exhibited early age at onset and longduration illnesses characterized prim
Autor:
A. Arlazoroff, Amos D. Korczyn, D. C. Gajdusek, Larisa Cervenakova, Miriam Y. Neufeld, M. Herbert, E. Werber, Patrick O. Brown, Joab Chapman, L. G. Goldfarb
Publikováno v:
Neurology. 46:758-761
Fatal familial insomnia (FFI) has been exclusively associated with a pathogenic mutation at codon 178 in the PRNP gene coupled with methionine (Met) at codon 129. We now describe a subject with familial Creutzfeldt-Jakob disease, heterozygous for the
Autor:
K. Pettrone, Patrick O. Brown, James W. Nagle, D. C. Gajdusek, Richard Rubenstein, C. J. Gibbs, L. G. Goldfarb, M Dubnick, Larisa Cervenakova
Publikováno v:
Proceedings of the National Academy of Sciences. 91:12159-12162
Based on the analysis of genomic DNA from single healthy animals of each of five primate species, nucleotide and predicted amino acid sequences of the infectious amyloid precursor gene of higher apes (Gorilla and Pan) and Old World (Macaca) and New W
Publikováno v:
European Journal of Epidemiology. 7:494-500
In 1974-1984 30 patients died with a diagnosis of Creutzfeldt-Jakob disease (CJD) in Finland (annual mortality rate of CJD 0.9 per million population for the years 1979-1984). Six of these patients (20%) were familial, all belonging to the same kindr
Publikováno v:
The Lancet. 337:1019-1022