Interdepartmental Training Program in Virology - Patricia Spear

Abstract

Funding Agency

Agency: National Institute of Health (NIH)
Institute: National Institute of Allergy and Infectious Diseases (NIAID)
Type: Institutional National Research Service Award (T32)
Project #: 5T32AI007182-07
Application #: 3530949
Study Section: Microbiology and Infectious Diseases Research Committee (MID)

Project Start: 1979-07-01
Project End: 1989-06-30
Budget Start: 1985-07-01
Budget End: 1986-06-30
Support Year: 7
Fiscal Year: 1985
Total Cost
Indirect Cost

Institution

Name: University of Chicago
Department
Type: Schools of Medicine
DUNS #: 225410919

City: Chicago
State: IL
Country: United States
Zip Code: 60637

Related projects


NIH 1988 T32 AI	Virology Roizman, Bernard / University of Chicago
NIH 1987 T32 AI	Interdepartmental Training Program in Virology Spear, Patricia G. / University of Chicago
NIH 1986 T32 AI	Interdepartmental Training Program in Virology Spear, Patricia G. / University of Chicago
NIH 1985 T32 AI	Interdepartmental Training Program in Virology Spear, Patricia G. / University of Chicago

Publications

Longnecker, R; Roizman, B (1987) Clustering of genes dispensable for growth in culture in the S component of the HSV-1 genome. Science 236:573-6

Kwong, A D; Frenkel, N (1987) Herpes simplex virus-infected cells contain a function(s) that destabilizes both host and viral mRNAs. Proc Natl Acad Sci U S A 84:1926-30

Purves, F C; Longnecker, R M; Leader, D P et al. (1987) Herpes simplex virus 1 protein kinase is encoded by open reading frame US3 which is not essential for virus growth in cell culture. J Virol 61:2896-901

Hummel, M; Berry, J K; Dunnick, W (1987) Switch region content of hybridomas: the two spleen cell Igh loci tend to rearrange to the same isotype. J Immunol 138:3539-48

Pellett, P E; Jenkins, F J; Ackermann, M et al. (1986) Transcription initiation sites and nucleotide sequence of a herpes simplex virus 1 gene conserved in the Epstein-Barr virus genome and reported to affect the transport of viral glycoproteins. J Virol 60:1134-40

Longnecker, R; Roizman, B (1986) Generation of an inverting herpes simplex virus 1 mutant lacking the L-S junction a sequences, an origin of DNA synthesis, and several genes including those specifying glycoprotein E and the alpha 47 gene. J Virol 58:583-91

Silver, S; Roizman, B (1985) gamma 2-Thymidine kinase chimeras are identically transcribed but regulated a gamma 2 genes in herpes simplex virus genomes and as beta genes in cell genomes. Mol Cell Biol 5:518-28

Kwong, A D; Frenkel, N (1985) The herpes simplex virus amplicon. IV. Efficient expression of a chimeric chicken ovalbumin gene amplified within defective virus genomes. Virology 142:421-5

Pellett, P E; Kousoulas, K G; Pereira, L et al. (1985) Anatomy of the herpes simplex virus 1 strain F glycoprotein B gene: primary sequence and predicted protein structure of the wild type and of monoclonal antibody-resistant mutants. J Virol 53:243-53

Pellett, P E; Biggin, M D; Barrell, B et al. (1985) Epstein-Barr virus genome may encode a protein showing significant amino acid and predicted secondary structure homology with glycoprotein B of herpes simplex virus 1. J Virol 56:807-13

Showing the most recent 10 out of 11 publications

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