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Gholamreza Darai

Researcher at Heidelberg University

Publications -  183
Citations -  6077

Gholamreza Darai is an academic researcher from Heidelberg University. The author has contributed to research in topics: Gene & Virus. The author has an hindex of 41, co-authored 183 publications receiving 5961 citations.

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Journal ArticleDOI

Genome sequence of a human tumorigenic poxvirus: prediction of specific host response-evasion genes.

TL;DR: MCV possesses 59 genes that are predicted to encode previously uncharacterized proteins, including major histocompatibility complex class I, chemokine, and glutathione peroxidase homologs, which suggests that there are MCV-specific strategies for coexistence with the human host.
Reference BookDOI

The Springer index of viruses

TL;DR: This book covers virus reserach history, virion morphology, electron microscopic images, genome properties, replication strategy, properties of individual transcripts and proteins, biological properties in vitro and in vivo, and specific information about the individual virus species.
Journal ArticleDOI

The genome of molluscum contagiosum virus: Analysis and comparison with other poxviruses

TL;DR: Despite the acquisition of unique genes for host interactions and changes in GC content, the physical order and regulation of essential ancestral poxvirus genes have been largely conserved in MCV and OPV.
Journal ArticleDOI

The Complete DNA Sequence of Lymphocystis Disease Virus

TL;DR: Computer-assisted analyses of the deduced amino acid sequences led to the identification of several putative gene products with significant homologies to entries in protein data banks, such as the two major subunits of the viral DNA-dependent RNA polymerase, DNA polymerase and several protein kinases.
Journal ArticleDOI

Analysis of the primary structure of the long terminal repeat and the gag and pol genes of the human spumaretrovirus.

TL;DR: The data justify classifying the spumaretroviruses as a third subfamily of Retroviridae, and the HSRV genomic organization is more similar to that of human and simian immunodeficiency viruses.