Critical Role of Human T-Lymphotropic Virus Type 1 Accessory Proteins in Viral Replication and Pathogenesis

doi:10.1128/MMBR.66.3.396-406.2002

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Microbiology and Molecular Biology Reviews, September 2002, p. 396-406, Vol. 66, No. 3
1092-2172/02/$04.00+0 DOI: 10.1128/MMBR.66.3.396-406.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

Critical Role of Human T-Lymphotropic Virus Type 1 Accessory Proteins in Viral Replication and Pathogenesis

Björn Albrecht¹^,2^, and Michael D. Lairmore¹^,2^,3^,4^,5^*

Center for Retrovirus Research,¹ Department of Veterinary Biosciences,² Comprehensive Cancer Center and Arthur G. James Cancer Hospital,³ Solove Research Center,⁴ Department of Molecular Virology, Immunology, and Medical Genetics, The Ohio State University, Columbus, Ohio 43210⁵

Human T-cell lymphotropic virus type 1 (HTLV-1) infection isassociated with a diverse range of lymphoproliferative and neurodegenerativediseases, yet pathogenic mechanisms induced by the virus remainobscure. This complex retrovirus contains typical structuraland enzymatic genes but also unique regulatory and accessorygenes in four open reading frames (ORFs) of the pX region ofthe viral genome (pX ORFs I to IV). The regulatory proteinsencoded by pX ORFs III and IV, Tax and Rex, respectively, havebeen extensively characterized. In contrast the contributionof the four accessory proteins p12^I, p27^I, p13^II, and p30^II,encoded by pX ORFs I and II, to viral replication and pathogenesisremained unclear. Proviral clones that are mutated in eitherpX ORF I or II, while fully competent in cell culture, are severelylimited in their replicative capacity in a rabbit model. Emergingevidence indicates that the HTLV-1 accessory proteins are criticalfor establishment of viral infectivity, enhance T-lymphocyteactivation, and potentially alter gene transcription and mitochondrialfunction. HTLV-1 pX ORF I expression is critical to the viralinfectivity in resting primary lymphocytes, suggesting a rolefor p12^I in lymphocyte activation. The endoplasmic reticulumand cis-Golgi localizing p12^I, encoded from pX ORF I, activatesNFAT, a key T-cell transcription factor, through calcium-mediatedsignaling pathways and may lower the threshold of lymphocyteactivation via the JAK/STAT pathway. In contrast p30^II localizesto the nucleus and represses viral promoter activity, but mayregulate cellular gene expression through p300/CBP or relatedcoactivators of transcription. p13^II targets mitochondrial proteins,where it alters the organelle morphology and may influence energymetabolism. Collectively, studies of the molecular functionsof the HTLV-1 accessory proteins provide insight into strategiesused by retroviruses that are associated with lymphoproliferativediseases.

* Corresponding author. Mailing address: The Ohio State University, Center for Retrovirus Research and Department of Veterinary Biosciences, 1925 Coffey Rd., Columbus, OH 43210. Phone: (614) 292-4489. Fax: (614) 292-6473. E-mail: lairmore.1{at}osu.edu.

Present address: Howard Hughes Medical Institute, MolecularPathogenesis Program, Skirball Institute of Biomolecular Medicine,New York University Medical Center, New York, NY 10016.

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