Abstract

BackgroundKaposi sarcoma-associated herpes virus (KSHV) is one of the most common causal agents of Kaposi Sarcoma (KS) in individuals with HIV-infections. The virus has gained attention over the past few decades due to its remarkable pathogenic mechanisms. A group of genes, ORF71, ORF72, and ORF73, are expressed as polycistronic mRNAs and the functions of ORF71 and ORF72 in KSHV are already reported in the literature. However, the function of ORF73 has remained a mystery. The aim of this study is to conduct comprehensive exploratory experiments to clarify the role of ORF73 in KSHV pathology and discover markers of AIDS-associated KSHV-induced KS by bioinformatic approaches.Methods and ResultsWe searched for homologues of ORF-73 and attempted to predict protein-protein interactions (PPI) based on GeneCards and UniProtKB, utilizing Position-Specific Iterated BLAST (PSI-BLAST). We applied Gene Ontology (GO) and KEGG pathway analyses to identify highly conserved regions between ORF-73 and p53to help us identify potential markers with predominant hits and interactions in the KEGG pathway associated with host apoptosis and cell arrest. The protein p53 is selected because it is an important tumor suppressor antigen. To identify the potential roles of the candidate markers at the molecular level, we used PSIPRED keeping the conserved domains as the major parameters to predict secondary structures. We based the FUGE interpretation consolidations of the sequence-structure comparisons on distance homology, where the score for the amino acids matching the insertion/deletion (indels) detected were based on structures compared to the FUGE database of structural profiles. We also calculated the compatibility scores of sequence alignments accordingly. Based on the PSI-BLAST homologues, we checked the disordered structures predicted using PSI-Pred and DISO-Pred for developing a hidden Markov model (HMM). We further applied these HMMs models based on the alignment of constructed 3D models between the known structure and the HMM of our sequence. Moreover, stable homology and structurally conserved domains confirmed that ORF-73 maybe an important prognostic marker for AIDS-associated KS.ConclusionCollectively, similar variants of ORF-73 markers involved in the immune response may interact with targeted host proteins as predicted by our computational analysis. This work also suggests the existence of potential conformational changes that need to be further explored to help elucidate the role of immune signaling during KS towards the development of therapeutic applications.

Highlights

  • Pre-existing human immunodeficiency virus (HIV) infections affect the immune system increasing the risk for development of Kaposi sarcoma (KS)

  • We extracted ORF-73 sequences from the NCBI database search using the accession number AAC57158.1. These are the exact URLs of the searched databases we used to identify markers associated with KS : GeneCards https:// genecards.weizmann.ac.il/v3/index.php?path=/Search/keyword/ kaposi%20sarcoma%20markers/0/20; UniPortKB https://www. uniprot.org/uniprot/?query=kaposi+sarcoma&sort=score; and NCBI https://www.ncbi.nlm.nih.gov/protein/?term=ORF-73% 20kaposi%20sarcoma)

  • Annotations used to search for the KS-associated markers in the UniProtKB database quoted about 137 entries, which we screened to find those with computationally annotated data

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Summary

Introduction

Pre-existing human immunodeficiency virus (HIV) infections affect the immune system increasing the risk for development of Kaposi sarcoma (KS). Since the discovery of Kaposi sarcomaassociated herpesvirus (KSHV), termed human herpesvirus 8 (HHV8), the tumor development and oncogenesis were associated with co-expression of different genes (Barré-Sinoussi et al, 1983; Gelmann et al, 1983). Soon after the discovery of HIV-1, scientists discovered g-herpesvirus in KS lesions (Chang et al, 1994). KSHV is a key viral pathogen in cancer biology affecting humans and its discovery promoted clinical and epidemiological research into viral oncology (Chang et al, 1994). Kaposi sarcoma-associated herpes virus (KSHV) is one of the most common causal agents of Kaposi Sarcoma (KS) in individuals with HIV-infections. The aim of this study is to conduct comprehensive exploratory experiments to clarify the role of ORF73 in KSHV pathology and discover markers of AIDS-associated KSHV-induced KS by bioinformatic approaches

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