Valeri, Valerio William (2009) Role of Human T-cell Leukemia Virus Type I (HTLV-I) Regulatory Proteins in Viral Replication. [Tesi di dottorato] (Inedito)

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Tipologia del documento:	Tesi di dottorato
Lingua:	English
Titolo:	Role of Human T-cell Leukemia Virus Type I (HTLV-I) Regulatory Proteins in Viral Replication
Autori:	Autore Email Valeri, Valerio William [non definito]
Data:	30 Novembre 2009
Numero di pagine:	63
Istituzione:	Università degli Studi di Napoli Federico II
Dipartimento:	Biologia e patologia cellullare e molecolare "L. Califano"
Scuola di dottorato:	Medicina molecolare
Dottorato:	Oncologia ed endocrinologia molecolare
Ciclo di dottorato:	22
Coordinatore del Corso di dottorato:	nome email Vecchio, Giancarlo [non definito]
Tutor:	nome email Ciminale, Vincenzo v.ciminale@unipd.it Franchini, Genoveffa franchinig@mail.nih.gov
Data:	30 Novembre 2009
Numero di pagine:	63
Parole chiave:	HTLV
Settori scientifico-disciplinari del MIUR:	Area 05 - Scienze biologiche > BIO/11 - Biologia molecolare Area 05 - Scienze biologiche > BIO/19 - Microbiologia generale
Depositato il:	12 Ott 2010
Ultima modifica:	30 Apr 2014 19:41
URI:	http://www.fedoa.unina.it/id/eprint/5031

Abstract

The pX region at the 3’ end of the HTLV-1 genome encodes alternatively spliced mRNAs for nonstructural proteins such as HBZ, p12/8, and p30. In vitro studies have demonstrated that ectopic expression of these proteins results in decreased viral replication: HBZ directly antagonizes Tax transcriptional activity by competing with CREB/ATF; p30 decreases viral replication by a post transcriptional mechanism and retains the Tax/Rex mRNA in the nucleus. p12 modulates T-cell proliferation and downregulates the major histocompatibility class I heavy chain complex expression. p8 affects viral replication indirectly by dampening TCR signaling. In the present study, we generated mutants that selectively ablate expression of p12/8, p30, and HBZ (Δp12, Δp8, Δp30, ΔHBZ). We inoculated a total of 30 rabbits (5 rabbits per group). Control animals were inoculated with lethally irradiated 729 uninfected human B cell line. The remaining groups received ~1x108 lethally irradiated cells harboring wild-type (WT) or Δp12, Δp8, Δp30, ΔHBZ Within four weeks all animals inoculated with the wt or mutant viruses seroconverted, and all where either positive by virus isolation from PBMC or by PCR for proviral DNA. Quantitative assessment of virus load in blood of all animals revealed between 1 log decrease for Δp30 and Δp12 and 2 logs decrease for animals infected with the ΔHBZ virus. Interestingly, the Δp8 mutant, produced a proviral load which was higher than that in animals infected with the WT virus.

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