The Molecular Epidemiology and Evolution of Epstein‐Barr Virus: Sequence Variation and Genetic Recombination in the Latent Membrane Protein‐1 Gene

Abstract: The phylogeny and evolution of Epstein-Barr virus (EBV) genetic variation are poorly understood. EBV latent membrane protein-1 (LMP-1) gene sequences are especially heterogeneous and may be useful as a tool for EBV genotype identification. Therefore, LMP-1 sequences obtained directly from EBV-infected human tissues were examined by PCR amplification and cloning. EBV genotypes were defined as "strains" from among 22 identified LMP-1 sequence patterns. Three molecular mechanisms were identified by which genetic … Show more

“…Similar substitution within the DG-SXXS motif in I B␣ abrogated the ability of I B␣ to recruit ␤-TrCP/HOS (66). Furthermore, substitutions of Ser-366 (such as S366T, S366A, and S366N) are observed more frequently in LMP1 isolates from EBV-associated tumors than in LMP1 from peripheral blood lymphocytes from apparently healthy individuals (30,39,65,67,68). G212S mutation may not be as common as substitution of Ser-366 (65, 67).…”

“…In addition to 30-bp deletions, these mutations may include D349A substitution (65). Similar substitution within the DG-SXXS motif in I B␣ abrogated the ability of I B␣ to recruit ␤-TrCP/HOS (66).…”

Interaction of Epstein-Barr Virus Latent Membrane Protein 1 with SCFHOS/β-TrCP E3 Ubiquitin Ligase Regulates Extent of NF-κB Activation

“…Similar substitution within the DG-SXXS motif in I B␣ abrogated the ability of I B␣ to recruit ␤-TrCP/HOS (66). Furthermore, substitutions of Ser-366 (such as S366T, S366A, and S366N) are observed more frequently in LMP1 isolates from EBV-associated tumors than in LMP1 from peripheral blood lymphocytes from apparently healthy individuals (30,39,65,67,68). G212S mutation may not be as common as substitution of Ser-366 (65, 67).…”

“…In addition to 30-bp deletions, these mutations may include D349A substitution (65). Similar substitution within the DG-SXXS motif in I B␣ abrogated the ability of I B␣ to recruit ␤-TrCP/HOS (66).…”

Interaction of Epstein-Barr Virus Latent Membrane Protein 1 with SCFHOS/β-TrCP E3 Ubiquitin Ligase Regulates Extent of NF-κB Activation

“…The association of specific LMP-1 sequences with disease has been extensively studied. Some studies reveal no relationship between specific EBV strains and disease (11,27,50), whereas others have shown that sequence variation in LMP-1 (compared to the B95-8 reference strain) is associated with more oncogenic phenotypes (21-24, 29-31, 44, 49). Thus, the ATGto-ATT/ACC substitution in the LMP-1 gene in tumor-associated strains may not be representative of virus found in healthy individuals.…”

Unexpected Absence of the Epstein-Barr Virus (EBV) lyLMP-1 Open Reading Frame in Tumor Virus Isolates: Lack of Correlation between Met129 Status and EBV Strain Identity

“…12 In addition, LMP1-BNLF1 gene polymorphisms, the most discriminating genetic locus, reflect intrastrain diversity. 13,14 EBV primary B-cell infection is polyclonal, always corresponding to an infection by a mixture of different EBV strains regarding the polymorphism of EBNAs and/or LMP1-BNLF1 genes. 15 Hodgkin's lymphoma shows a monoclonal pattern of infection which persists throughout the course of the disease, 16 suggesting that a selection pressure is exerted on the virus during the oncogenic process and raising the question of its role in the pathogenesis of Hodgkin's lymphoma.…”

Comparative analysis of oncogenic properties and nuclear factor- B activity of latent membrane protein 1 natural variants from Hodgkin's lymphoma's Reed-Sternberg cells and normal B-lymphocytes