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Dive into the research topics where Ehounou R. Ekpini is active.

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Featured researches published by Ehounou R. Ekpini.


The Lancet | 2002

HIV-1/AIDS and maternal and child health in Africa

François Dabis; Ehounou R. Ekpini

Every day, 1900 children acquire HIV-1 infection from their mother in Africa. The 25-45% risk of mother-to-child transmission can be reduced in several ways: prevention of sexual transmission for women of child-bearing age, access to HIV-1 testing, reduction of unwanted pregnancies by education of HIV-1-infected women, and antiretroviral-based prevention. All antiretroviral regimens of proven efficacy can be used in a minimum package of care for HIV-1-infected pregnant women. At present, programmes in 13 countries reach less than 3% of HIV-1-infected African women. 35-59% of African children infected with HIV-1 die by their second birthday. Infectious complications are preventable by primary prophylaxis with co-trimoxazole. A rapid scaling-up and comprehensive continuum of care is needed for all members of affected families, including access to antiretroviral treatment and community-based responses to the increasing number of orphans. Prevention of mother-to-child transmission should become a universal standard of care in Africa, and research should continue to reduce the transmission risk to well below 5%.


AIDS Research and Human Retroviruses | 1999

Predominance of human immunodeficiency virus type 2 subtype B in Abidjan, Ivory Coast.

Danuta Pieniazek; Dennis Ellenberger; Luiz Mario Janini; Artur Ramos; John N. Nkengasong; Madeleine Sassan-Morokro; Dale J. Hu; Issa-Malick Coulibally; Ehounou R. Ekpini; Claudiu I. Bandea; Amilcar Tanuri; Alan E. Greenberg; Stefan Z. Wiktor; Mark Rayfield

We analyzed the genetic variability and phylogenetic relationships among 28 HIV-2 strains collected from patients enrolled in an HIV epidemiologic study in Abidjan, Ivory Coast, during 1995-1996. Although both subtype A (n = 8; 29%) and subtype B (n = 20; 71%) were present in this sampling, the majority of infections were caused by subtype B viruses. These findings contrasted with the reported predominance of HIV-2 subtype A in other African countries. The broad genetic diversity identified among protease gene sequences for HIV-2 subtype A (6%; range 3-15%) and subtype B (7%; range, 2-12%), and their presence in Abidjan during the 1980s, document a long coexistence of two viral subtypes in Ivory Coast. Our data indicate that viruses of subtypes A and B have contributed to the HIV-2 epidemic in Ivory Coast.


AIDS Research and Human Retroviruses | 1999

Genetic Analysis of Human Immunodeficiency Virus in Abidjan, Ivory Coast Reveals Predominance of HIV Type 1 Subtype A and Introduction of Subtype G

Dennis Ellenberger; Danuta Pieniazek; John N. Nkengasong; Chi-Cheng Luo; Sushil G. Devare; Chantal Maurice; Mario Janini; Artur Ramos; Carol Fridlund; Dale J. Hu; Issa-Malick Coulibaly; Ehounou R. Ekpini; Stefan Z. Wiktor; Alan E. Greenberg; Gerald Schochetman; Mark Rayfield

To better understand the molecular epidemiology of HIV genetic diversity in Abidjan, Ivory Coast, we performed a genetic analysis of 170 HIV-1-seropositive specimens representing newly diagnosed tuberculosis patients (n = 143) and women monitored in a mother-to-child transmission cohort study (n = 27). Preliminary screening with RFLP presumptively classified 162 (95.3%) of these as subtype A. The envelope region of 108 specimens was subtyped by sequence analysis: 102 (94.4%) were subtype A, 2 (1.9%) were subtype D, and 4 (3.7%) were subtype G. Subtyping gag and env regions of the genome suggested that five of the six nonsubtype A isolates exhibited a potentially mosaic structure. A comparative phylogenetic analysis of HIV-1 subtype A C2V3 from 27 Ivory Coast and 21 Ugandan sequences revealed a striking clustering among Ivory Coast variants, and an independent segregation from Ugandan subtype A. Despite independent clustering with other subtype A specimens, limited variability of the V3 loop apex was observed; the globally predominant V3 motif, GPGQ, represented 90.1% of the HIV-1 strains. This study demonstrates that clade A is the predominant HIV-1 subtype in HIV-seropositive individuals in Abidjan, Ivory Coast and that these strains are phylogenetically distinct from other subtype A strains observed in East Africa.


Journal of Acquired Immune Deficiency Syndromes | 2000

Lower HIV-2 plasma viral loads may explain differences between the natural histories of HIV-1 and HIV-2 infections.

Vedapuri Shanmugam; William M. Switzer; John N. Nkengasong; Gerardo J. Garcia-Lerma; Timothy A. Green; Ehounou R. Ekpini; Madeleine Sassan-Morokro; Francisco Antunes; Kamal Manshino; Vincent Soriano; Stefan Z. Wiktor; Walid Heneine

To explain the low transmissibility and pathogenicity of HIV-2 infections plasma viral loads in both HIV-1- and HIV-2-infected persons were compared by using the polymerase chain reaction (PCR)-based Amp-RT assay to measure levels of reverse transcriptase (RT) activity. The study comprised a total of 155 HIV-infected-people including 58 who were infected with HIV-2 with CD4+ cell counts <500 x 106/L (n = 15), CD4+ cell counts >500 x 106/L (n = 26), or with tuberculosis (TB; n = 17), and 97 HIV-1-infected people with CD4+ cell counts <500 x 106/L (n = 32), CD4+ cell counts >500 x 106/L (n = 25), or TB (n = 40). Among persons with CD4+ cell counts <500 x 106/L, 11 (73.3%) of 15 HIV-2-infected persons had detectable plasma RT activity compared with 25 (78.1%) of 32 HIV-1-infected persons (p =.725). However, the median HIV-2 plasma RT activity in this group was significantly lower (2561 x 10-10 U/ml; p =.036; detectable range, 1712-644,868 x 10-10 U/ml) than the RT activity of HIV-1-infected persons with similar CD4+ cell counts (13,241 x 10-10 U/ml; detectable range, 8482-1,478,880 x 10-10 U/ml). Among TB patients, 10 (58.8%) of 17 HIV-2-infected persons had detectable plasma RT activity compared with 30 (75%) of 40 HIV-1-infected persons (p =.342). In contrast, among patients with CD4+ cell counts >500 x 106/L, none of 26 HIV-2-infected persons had detectable RT activity compared with 13 (52%) of 25 HIV-1-infected persons (p <.001). Our data suggest that unlike HIV-1 infection, HIV-2 infections with CD4+ cell counts >500 x 106/L are associated with a low level of viral replication, which may explain the longer clinical latency and lower transmissibility seen in HIV-2 infection.


The Journal of Infectious Diseases | 1998

Evidence of Nef Truncation in Human Immunodeficiency Virus Type 2 Infection

William M. Switzer; Stefan Z. Wiktor; Vincent Soriano; Antonio Silva-Graça; Kamal Mansinho; Issa Malik Coulibaly; Ehounou R. Ekpini; Alan E. Greenberg; Thomas M. Folks; Walid Heneine

Human immunodeficiency virus (HIV)-2 differs from HIV-1 in its relative lower transmissibility and pathogenicity. To understand the virologic basis of these differences, the nef gene from HIV-2-seropositive persons was analyzed because of its importance for disease progression in the genetically related simian immunodeficiency virus (SIV[MAC]). Proviral nef sequences from 60 HIV-2-infected persons were amplified from peripheral blood lymphocytes, and nef open-reading frames were screened by a transcription and translation assay for the presence of full-length (32- to 36-kDa) or truncated (<32 kDa) Nef proteins. Overall, 6 (10%) of 60 persons had truncated Nef proteins; of these, 5 were among the 36 asymptomatic subjects (13.9%) and only 1 was among the 24 symptomatic subjects (4.2%) (P =.23). The results of this study document the presence of defective nef genes in HIV-2 infections with a prevalence higher than that previously seen in HIV-1-infected cohorts of long-term nonprogressors or patients with AIDS.


International Journal of Gynecology & Obstetrics | 1994

Retrospective study of maternal HIV-1 and HIV-2 infections and child survival in Abidjan, Cote d'Ivoire

K.M. De Cock; F. Zadi; Georgette Adjorlolo; Mamadou O. Diallo; Madeleine Sassan-Morokro; Ehounou R. Ekpini; Toussaint S. Sibailly; Ronan Doorly; V. Batter; Kari Brattegaard; H D Gayle

and serum triglycerides were assayed. Results There was a strong positive correlation between serum concentrations of triglyceride, basal insulin, and abdominal obesity on the one hand, and plasminogen activator inhibitor, fibrinogen, and von Willebrand factor on the other, among women with PCOS as well as among referents. There were significantly higher mean concentrations of fibrinogen and factor VII:Ag among referents, but the mean values of most hemostatic variables studied showed no differences between the groups. Conclusion -Women with an altered metabolic profile were also found to have affected hemostatic factors, but PcoS in itself did not seem to influence them.


The Lancet | 1999

Short-course oral zidovudine for prevention of mother-to-child transmission of HIV-1 in Abidjan, Côte d'Ivoire: a randomised trial

Stefan Z. Wiktor; Ehounou R. Ekpini; John M. Karon; John N. Nkengasong; Chantal Maurice; Sibailly T Severin; Thierry H. Roels; Moïse K Kouassi; Eve M. Lackritz; Issa-Malick Coulibaly; Alan E. Greenberg


JAMA | 1993

Epidemiology and transmission of HIV-2 : why there is no HIV-2 pandemic

Kevin M. De Cock; Georgette Adjorlolo; Ehounou R. Ekpini; Toussaint S. Sibailly; Justin Kouadio; Matthieu Maran; Kari Brattegaard; Kathleen M. Vetter; Ronan Doorly; Helene D Gayle


JAMA | 1994

Prospective Comparison of Mother-to-Child Transmission of HIV-1 and HIV-2 in Abidjan, Ivory Coast

Georgette T Adjorlolo-Johnson; Kevin M. De Cock; Ehounou R. Ekpini; Kathleen M. Vetter; Toussaint S. Sibailly; Kari Brattegaard; Daniel Yavo; Ronan Doorly; J. Patrick Whitaker; Luc Kestens; Chin-Yih Ou; J. Richard George; Helene D Gayle


The Lancet | 1997

Late postnatal mother-to-child transmission of HIV-1 in Abidjan, Côte d'Ivoire

Ehounou R. Ekpini; Stefan Z. Wiktor; Glen A. Satten; Georgette T Adjorlolo-Johnson; Toussaint S. Sibailly; Chin-Yih Ou; John M. Karon; Kari Brattegaard; J. Patrick Whitaker; Emmanuel Gnaore; Kevin M. De Cock; Alan E. Greenberg

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Stefan Z. Wiktor

Centers for Disease Control and Prevention

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Toussaint S. Sibailly

Centers for Disease Control and Prevention

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Alan E. Greenberg

George Washington University

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Thierry H. Roels

Centers for Disease Control and Prevention

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John N. Nkengasong

Centers for Disease Control and Prevention

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Kari Brattegaard

Centers for Disease Control and Prevention

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John M. Karon

Centers for Disease Control and Prevention

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Kevin M. De Cock

Centers for Disease Control and Prevention

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Chin-Yih Ou

Centers for Disease Control and Prevention

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