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Dive into the research topics where Elena Dukhovlinova is active.

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Featured researches published by Elena Dukhovlinova.


Addiction | 2009

Hepatitis C virus infection among drug injectors in St Petersburg, Russia: social and molecular epidemiology of an endemic infection

Elijah Paintsil; Sergei V. Verevochkin; Elena Dukhovlinova; Linda M. Niccolai; Russell Barbour; Edward White; Olga V. Toussova; Louis Alexander; Andrei P. Kozlov; Robert Heimer

AIMS To understand the epidemiology and transmission patterns of hepatitis C virus (HCV), the predominant blood borne-pathogen infecting injection drug users (IDUs), in a part of the former Soviet Union. DESIGN Cross-sectional respondent-driven sample of IDUs. SETTING St Petersburg, Russia. PARTICIPANTS A total of 387 IDUs were recruited in late 2005 and throughout 2006. MEASUREMENTS Participants were surveyed to collect demographic, medical and both general and dyad-specific drug injection and sexual behaviors. A blood sample was collected to detect antibodies to hepatitis C and to amplify viral RNA for molecular analysis. The molecular data, including genotypes, were analyzed spatially and linkage patterns were compared to the social linkages obtained by respondent-driven sampling (RDS) for chains of respondents and among the injection dyads. FINDINGS HCV infection was all but ubiquitous: 94.6% of IDUs were HCV-seropositive. Among the 209 viral sequences amplified, genotype 3a predominated (n = 119, 56.9%), followed by 1b (n = 61, 29.2%) and 1a (n = 25, 11.9%). There was no significant clustering of genotypes spatially. Neither genotypes nor closely related sequences were clustered within RDS chains. Analysis of HCV sequences from dyads failed to find associations of genotype or sequence homology within pairs. CONCLUSIONS Genotyping reveals that there have been at least five unique introductions of HCV genotypes into the IDU community in St Petersburg. Analysis of prevalent infections does not appear to correlate with the social networks of IDUs, suggesting that simple approaches to link these networks to prevalent infections, rather than incident transmission, will not prove meaningful. On a more positive note, the majority of IDUs are infected with 3a genotype that is associated with sustained virological response to antiviral therapy.


The Journal of Infectious Diseases | 2010

A Substantial Transmission Bottleneck among Newly and Recently HIV-1-Infected Injection Drug Users in St Petersburg, Russia

Alexey Masharsky; Elena Dukhovlinova; Sergei V. Verevochkin; Olga V. Toussova; Roman V. Skochilov; Jeffrey A. Anderson; Irving Hoffman; Myron S. Cohen; Ronald Swanstrom; Andrei P. Kozlov

There are limited data on the genetic complexity of human immunodeficiency virus type 1 (HIV-1) after transmission among a cohort of injection drug users (IDUs). We used single-genome amplification of HIV-1 env to determine the genotypic characteristics of virus among IDUs with acute infection in St Petersburg, Russia. Our results indicate that a single variant was transmitted in a majority of cases (9 of 13 participants), which is analogous to what is observed in sexual transmission. These data are most consistent with a genetic bottleneck during transmission by injection drug use that is due to a small inoculum, which most often results in the transmission of a low-complexity viral population.


Current Hiv\/aids Reports | 2015

Compartmentalization, Viral Evolution, and Viral Latency of HIV in the CNS

Maria M. Bednar; Christa Buckheit Sturdevant; Lauren A. Tompkins; Kathryn T. Arrildt; Elena Dukhovlinova; Laura P. Kincer; Ronald Swanstrom

Human immunodeficiency virus type 1 (HIV-1) infection occurs throughout the body and can have dramatic physical effects, such as neurocognitive impairment in the central nervous system (CNS). Furthermore, examining the virus that resides in the CNS is challenging due to its location and can only be done using samples collected either at autopsy, indirectly form the cerebral spinal fluid (CSF), or through the use of animal models. The unique milieu of the CNS fosters viral compartmentalization as well as evolution of viral sequences, allowing for new cell types, such as macrophages and microglia, to be infected. Treatment must also cross the blood–brain barrier adding additional obstacles in eliminating viral populations in the CNS. These long-lived infected cell types and treatment barriers may affect functional cure strategies in people on highly active antiretroviral therapy (HAART).


Journal of Acquired Immune Deficiency Syndromes | 2017

Treatment as Prevention: Characterization of partner infections in the HIV Prevention Trials Network 052 trial.

Susan H. Eshleman; Sarah E. Hudelson; Andrew D. Redd; Ronald Swanstrom; San San Ou; Xinyi Cindy Zhang; Li Hua Ping; Estelle Piwowar-Manning; Stephen F. Porcella; Matthew F. Sievers; Craig Martens; Daniel P. Bruno; Elena Dukhovlinova; Marybeth McCauley; Theresa Gamble; Jessica M. Fogel; Devin Sabin; Thomas C. Quinn; Laurence Gunde; Madalitso Maliwichi; Nehemiah Nhando; Victor Akelo; Sikhulile Moyo; Ravindre Panchia; Nagalingeswaran Kumarasamy; Nuntisa Chotirosniramit; Marineide Gonçalves de Melo; José Henrique Pilotto; Beatriz Grinsztejn; Kenneth H. Mayer

Abstract: HIV Prevention Trials Network 052 demonstrated that antiretroviral therapy (ART) prevents HIV transmission in serodiscordant couples. HIV from index–partner pairs was analyzed to determine the genetic linkage status of partner infections. Forty-six infections were classified as linked, indicating that the index was the likely source of the partners infection. Lack of viral suppression and higher index viral load were associated with linked infection. Eight linked infections were diagnosed after the index started ART: 4 near the time of ART initiation and 4 after ART failure. Linked infections were not observed when the index participant was stably suppressed on ART.


Journal of Virology | 2015

Phenotypic Correlates of HIV-1 Macrophage Tropism

Kathryn T. Arrildt; Celia C. LaBranche; Sarah Joseph; Elena Dukhovlinova; William D. Graham; Li Hua Ping; Gretja Schnell; Christa Buckheit Sturdevant; Laura P. Kincer; Macpherson Mallewa; Robert S. Heyderman; Annelies Van Rie; Myron S. Cohen; Serena Spudich; Richard W. Price; David C. Montefiori; Ronald Swanstrom

ABSTRACT HIV-1 is typically CCR5 using (R5) and T cell tropic (T-tropic), targeting memory CD4+ T cells throughout acute and chronic infections. However, viruses can expand into alternative cells types. Macrophage-tropic (M-tropic) HIV-1 variants have evolved to infect macrophages, which have only low levels of surface CD4. Most M-tropic variants have been isolated from the central nervous system during late-stage chronic infection. We used the HIV-1 env genes of well-defined, subject-matched M-tropic and T-tropic viruses to characterize the phenotypic features of the M-tropic Env protein. We found that, compared to T-tropic viruses, M-tropic viruses infect monocyte-derived macrophages (MDMs) on average 28-fold more efficiently, use low-density CD4 more efficiently, have increased sensitivity to soluble CD4 (sCD4), and show trends toward sensitivity to some CD4 binding site antibodies but no difference in sensitivity to antibodies targeting the CD4-bound conformation. M-tropic viruses also displayed a trend toward resistance to neutralization by monoclonal antibodies targeting the V1/V2 region of Env, suggesting subtle changes in Env protein conformation. The paired M- and T-tropic viruses did not differ in autologous serum neutralization, temperature sensitivity, entry kinetics, intrinsic infectivity, or Env protein incorporation. We also examined viruses with modestly increased CD4 usage. These variants have significant sensitivity to sCD4 and may represent evolutionary intermediates. CD4 usage is strongly correlated with infectivity of MDMs over a wide range of CD4 entry phenotypes. These data suggest that emergence of M-tropic HIV-1 includes multiple steps in which a phenotype of increased sensitivity to sCD4 and enhanced CD4 usage accompany subtle changes in Env conformation. IMPORTANCE HIV-1 typically replicates in CD4+ T cells. However, HIV-1 can evolve to infect macrophages, especially within the brain. Understanding how CCR5-using macrophage-tropic viruses evolve and differ from CCR5-using T cell-tropic viruses may provide insights into viral evolution and pathogenesis within the central nervous system. We characterized the HIV-1 env viral entry gene from subject-matched macrophage-tropic and T cell-tropic viruses to identify entry features of macrophage-tropic viruses. We observed several differences between T cell-tropic and macrophage-tropic Env proteins, including functional differences with host CD4 receptor engagement and possible changes in the CD4 binding site and V1/V2 region. We also identified viruses with phenotypes between that of “true” macrophage-tropic and T cell-tropic viruses, which may represent evolutionary intermediates in a multistep process to macrophage tropism.


AIDS Research and Human Retroviruses | 2014

Two Independent HIV Epidemics in Saint Petersburg, Russia Revealed by Molecular Epidemiology.

Elena Dukhovlinova; Alexey Masharsky; Olga V. Toussova; Sergei V. Verevochkin; Tatiana Solovyeva; Maria Meringof; Elijah Paintsil; Edward White; Russell Barbour; Robert Heimer; Andrei P. Kozlov

The HIV epidemic in Russia, one of the worlds fastest growing, has been concentrated mostly among people who inject drugs (PWID). We sought to explore the epidemiology of the epidemic in St. Petersburg by sampling from the highest risk groups of PWID and men who have sex with men (MSM) and use viral sequencing data to better understand the nature of the citys epidemic. Serological testing confirmed an HIV prevalence among PWID in excess of 40%. All but 1 of 110 PWID whose blood samples were tested for genetic diversity were infected by subtype A virus, specifically by the AFSU strain. The remaining person was infected with a CRF-06cpx recombinant. Analysis of pairwise genetic distance among all PWID studied revealed an average of 3.1% sequence divergence, suggesting clonal introduction of the AFSU strain and/or constraints on sequence divergence. The HIV prevalence was less than 10% among MSM. All 17 sequences from HIV-infected MSM were found to be a clade B virus with a much higher average sequence diversity of 15.7%. These findings suggest two independent epidemics with little overlap between the two highest at-risk populations, which will require different HIV prevention approaches.


Journal of Virology | 2015

R5 macrophage-tropic HIV-1 in the male genital tract

Maria M. Bednar; Blake M. Hauser; Li Hua Ping; Elena Dukhovlinova; Shuntai Zhou; Kathryn T. Arrildt; Irving Hoffman; Joseph J. Eron; Myron S. Cohen; Ronald Swanstrom

ABSTRACT The entry tropism of HIV-1 Env proteins from virus isolated from the blood and genital tract of five men with compartmentalized lineages was determined. The Env proteins isolated from the genital tract of subject C018 were macrophage-tropic proteins, while the remaining cloned env genes encoded R5 T cell-tropic proteins. The detection of a macrophage-tropic lineage of HIV-1 within the male genital tract strongly suggests that evolution of macrophage-tropic viruses can occur in anatomically isolated sites outside the central nervous system.


Vaccine | 2007

The feasibility of HIV vaccine efficacy trials among Russian injection drug users

Chris Beyrer; Stefan Baral; Alla V. Shaboltas; Elena Dukhovlinova; Alexey Masharsky; Sergey V. Verevochkin; Carl A. Latkin; Robert Heimer; Irving Hoffman; Andrei P. Kozlov


Biotechnology Journal | 2007

Immunogenicity of candidate DNA vaccine based on subtype A of human immunodeficiency virus type 1 predominant in Russia.

Boris V. Murashev; Elena Kazennova; Alexander Kozlov; Irina Murasheva; Elena Dukhovlinova; Yuri P Galachyants; Ekaterina Dorofeeva; Ilya V Dukhovlinov; Galina Smirnova; Alexey Masharsky; Nikolay Klimov; Andrei P. Kozlov


AIDS Research and Human Retroviruses | 2018

Characterization of the Transmitted Virus in an Ongoing HIV-1 Epidemic Driven by Injecting Drug Use

Elena Dukhovlinova; Alexey Masharsky; Aleksandra Vasileva; Alessandro Porrello; Shuntai Zhou; Olga V. Toussova; Sergei Verevochkin; Ekaterina B. Akulova; Dmitrij Frishman; David C. Montefiori; Celia C. LaBranche; Irving Hoffman; William C. Miller; Myron S. Cohen; Andrei Kozlov; Ronald Swanstrom

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Ronald Swanstrom

University of North Carolina at Chapel Hill

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Andrei P. Kozlov

Saint Petersburg State University

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Olga V. Toussova

Saint Petersburg State University

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Irving Hoffman

University of North Carolina at Chapel Hill

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Myron S. Cohen

University of North Carolina at Chapel Hill

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Sergei V. Verevochkin

Saint Petersburg State University

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Kathryn T. Arrildt

University of North Carolina at Chapel Hill

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Li Hua Ping

University of North Carolina at Chapel Hill

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Alla V. Shaboltas

Saint Petersburg State University

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