Your search keyword '"Redfield, Robert R."' showing total 18 results

1. Monotherapy with either dolutegravir or raltegravir fails to durably suppress HIV viraemia in humanized mice.

Author

Heredia, Alonso, Hassounah, Said, Medina-Moreno, Sandra, Zapata, Juan C., Le, Nhut M., Yingshan Han, Foulke Jr, James S., Davis, Charles, Bryant, Joseph, Redfield, Robert R., Wainberg, Mark A., Han, Yingshan, and Foulke, James S Jr

Subjects

HIV infections, THERAPEUTICS, VIREMIA, RALTEGRAVIR, VIRAL mutation, POLYMERASE chain reaction, SUPPRESSOR mutation, HETEROCYCLIC compounds, ANTI-HIV agents, HIV integrase inhibitors, ANIMAL experimentation, HIV, MICE, GENETIC mutation, RNA, GENOTYPES

Abstract

Objectives: To compare the effectiveness of HIV integrase inhibitor monotherapy between raltegravir and dolutegravir as an approach to simplify therapy.Methods: We evaluated and compared the efficacy of 20 week monotherapy with dolutegravir or raltegravir in humanized mice (HSC-NSG) infected with HIVBaL. Plasma HIV RNA was measured by quantitative RT-PCR (limit of detection of 150 copies/45 μL of plasma) and drug levels by LC-MS/MS. Escape viruses were genotyped and analysed for replication capacity and drug susceptibility in tissue culture.Results: Drug-untreated control mice maintained constant viraemia throughout the study. Virus isolates from these mice were susceptible to both raltegravir (EC50 of <8 nM) and dolutegravir (EC50 of <1 nM). Mice treated with raltegravir or dolutegravir had plasma drug levels comparable to those in humans. Monotherapy with raltegravir initially suppressed HIV viraemia, but failed to maintain suppression in 4/4 mice. Viruses from raltegravir failing mice developed mutations G140G/S and Q148H/K, and were resistant to both raltegravir (EC50 values of >100 nM) and dolutegravir (EC50 values ranging from 8.8 to 13.3 nM). Monotherapy with dolutegravir suppressed viraemia in 5/5 of mice, but viraemia rebounded in one animal. The virus from this mouse had mutations E138K, G140S, Q148H, N155H and S230R, was highly resistant to both raltegravir (EC50 of >1000 nM) and dolutegravir (EC50 of 550 nM), and replicated to levels similar to those of control viruses in PBMCs.Conclusions: Monotherapy with either raltegravir or dolutegravir does not consistently maintain HIV suppression, suggesting that dual therapy may be required in simplification strategies. [ABSTRACT FROM AUTHOR]

Published

2017

2. The mode of sensitization and its influence on allograft outcomes in highly sensitized kidney transplant recipients.

Author

Redfield, Robert R., Scalea, Joseph R., Zens, Tiffany J., Mandelbrot, Didier A., Leverson, Glen, Kaufman, Dixon B., and Djamali, Arjang

Subjects

*SENSITIZATION (Neuropsychology), *HOMOGRAFTS, *KIDNEY transplant patients, *REGRESSION analysis

Abstract

Background. We sought to determine whether the mode of sensitization in highly sensitized patients contributed to kidney allograft survival. Methods. An analysis of the United Network for Organ Sharing dataset involving all kidney transplants between 1997 and 2014 was undertaken. Highly sensitized adult kidney transplant recipients [panel reactive antibody (PRA) ≥98%] were compared with adult, primary non-sensitized and re-transplant recipients. Kaplan-Meier survival analyses were used to determine allograft survival rates. Cox proportional hazards regression analyses were conducted to determine the association of graft loss with key predictors. Results. Fifty-three percent of highly sensitized patients transplanted were re-transplants. Pregnancy and transfusion were the only sensitizing event in 20 and 5%, respectively. The 10-year actuarial graft survival for highly sensitized recipients was 43.9% compared with 52.4% for non-sensitized patients, P < 0.001. The combination of being highly sensitized by either pregnancy or blood transfusion increased the risk of graft loss by 23%[hazard ratio (HR) 1.230, confidence interval (CI) 1.150-1.315, P < 0.001], and the combination of being highly sensitized from a prior transplant increased the risk of graft loss by 58.1%(HR1.581, CI 1.473- 1.698, P < 0.001). Conclusions. The mode of sensitization predicts graft survival in highly sensitized kidney transplant recipients (PRA ≥98%). Patients who are highly sensitized from re-transplants have inferior graft survival compared with patients who are highly sensitized from other modes of sensitization. [ABSTRACT FROM AUTHOR]

Published

2016

3. λ Light Chain Bias Associated With Enhanced Binding and Function of Anti-HIV Env Glycoprotein Antibodies.

Author

Sajadi, Mohammad M., Farshidpour, Maham, Brown, Eric P., Xin Ouyang, Seaman, Michael S., Pazgier, Marzena, Ackerman, Margaret E., Robinson, Harriet, Tomaras, Georgia, Parsons, Matthew S., Charurat, Manhattan, DeVico, Anthony L., Redfield, Robert R., Lewis, George K., and Ouyang, Xin

Subjects

BINDING sites, ANTI-HIV agents, GLYCOPROTEINS, HUMORAL immunity, GENETIC mutation, HIV infection epidemiology, HIV, HIV infections, IMMUNOGLOBULINS, LONGITUDINAL method, PROTEINS, RESEARCH funding, VIRAL antibodies, ANTIBODY formation

Abstract

The humoral response to human immunodeficiency virus (HIV) remains incompletely understood. In this report, we describe biased λ light chain use during the HIV Env glycoprotein (Env) response in HIV infection and vaccination. We examined HIV Env binding (and neutralization) in the context of light chain use in subjects with acute HIV infection, chronic HIV infection, and among HIV vaccinees. In all populations tested, there was a λ chain bias for HIV Env binding antibodies, compared with other HIV antigens (such as p24) or tetanus toxoid. In subjects with chronic HIV infection, a λ bias was noted for neutralization, with λ antibodies accounting for up to 90% of all neutralization activity observed. This is the first report of antibody function in a human infection being tied to light chain use. In HIV infection, antibodies expressing λ light chains tended to have longer CDRL3s, increased light chain contact with HIV Env, and less hypermutation in the heavy chain, compared with antibodies using the κ light chain. These data also support an evolutionary model for the understanding the various κ to λ light chain ratios observed across species and suggest that the λ light chain bias against HIV provides the host an advantage in developing a more efficient humoral response. [ABSTRACT FROM AUTHOR]

Published

2016

4. Is Mycobacterium avium paratuberculosis the Trigger in the Crohn's Disease Spectrum?

Author

Oken, Harry A., Saleeb, Paul G., Redfield, Robert R., and Schimpff, Stephen C.

Subjects

CROHN'S disease, INFLAMMATORY bowel diseases, HISTORY of medicine

Abstract

We present and discuss a 30-month investigation of a patient that presented with abdominal pain, postprandial diarrhea, bloating, and night sweats and was treated for Crohn's disease without significant improvement. The patient underwent an ileocecetomy with removal of an atonic segment with resolution of functional gastrointestinal symptoms, but profound night sweats continued postoperatively. The patient was presumptively treated for a mixed mycobacterial infection, blood cultures later grew Mycobacterium avium paratuberculosis (MAP), and she improved over time. We discuss MAP and its possible relationship to Crohn's disease. [ABSTRACT FROM AUTHOR]

Published

2017

5. Targeting of the Purine Biosynthesis Host Cell Pathway Enhances the Activity of Tenofovir Against Sensitive and Drug-Resistant HIV-1.

Author

Heredia, Alonso, Davis, Charles E., Reitz, Marvin S., Le, Nhut M., Wainberg, Mark A., Foulke, James S., Wang, Lai-Xi, and Redfield, Robert R.

Subjects

AIDS prevention, NATURAL products, PLANT products, NUCLEOSIDES, HIV

Abstract

Background. Targeting host-cell pathways to increase the potency of nucleoside/nucleotide analog reverse transcriptase inhibitors (NRTIs) is an important strategy for clinical investigation. Resveratrol is a natural product that inhibits cellular ribonucleotide reductase, prolonging the S phase of the cell cycle and preferentially lowering dATP levels.Methods. We performed in vitro evaluation of resveratrol on the antiviral activity of adenosine analog tenofovir (TFV) against sensitive and drug-resistant human immunodeficiency virus type 1 (HIV-1), from subtypes B and C, in primary cells.Results. Resveratrol enhanced the antiviral activity of TFV by up to 10-fold and restored susceptibility of TFV-resistant viruses. Resveratrol prevented wild-type HIV-1 from developing phenotypic resistance to TFV. Notably, resveratrol enhanced TFV activity against sensitive and resistant HIV-1 from both subtypes B and C.Conclusions. Prolonged wide-scale use of thymidine analogs in the setting of viral failure has limited the efficacy of second-line NRTI-based regimens in Africa. Moreover, the extensive use of ddI and d4T has led to high frequencies of the K65R mutation, further compromising TFV efficacy. In light of increasing resistance to commonly used NRTIs in global HIV treatment programs, targeting nucleoside biosynthesis with resveratrol, or derivatives with improved bioavailabilities, is a potential strategy to maintain, enhance, and restore susceptibility of commonly used NRTIs. [ABSTRACT FROM PUBLISHER]

Published

2013

6. Impact of persistent HIV replication on CD4 negative Vγ2Vδ2 T cells.

Author

Boudová S, Li H, Sajadi MM, Redfield RR, Pauza CD, Boudová, Sarah, Li, Haishan, Sajadi, Mohammad M, Redfield, Robert R, and Pauza, C David

Abstract

Background: CD4- Vγ2Vδ2 T cells are depleted during human immunodeficiency virus (HIV) infection but can recover to near normal levels in patients who spontaneously control viremia in the absence of therapy. By contrasting Vγ2Vδ2 T-cell numbers, phenotype, and T-cell receptor (TCR) repertoire, we investigate the dynamic tension between active immunity and progressive T-cell destruction during persistent viremia.Methods: Peripheral blood Vγ2Vδ2 T-cell levels and phenotypes were characterized by flow cytometry. Lymphoproliferation assays measured functional responses. Spectratyping characterized damage to the TCR repertoire.Results: Levels, responses to antigen and the proportion of T effector memory Vγ2Vδ2 T cells in patients with persistent viremia, were intermediate between patients with natural virus suppression (NVS) and patients receiving antiretroviral therapy. Damage to the TCR γ-2 chain repertoire and depletion of CD56+ Vγ2Vδ2 T cells were more pronounced in viremic patients, compared with antiretroviral therapy recipients and patients with natural virus suppression.Conclusions: Characteristics of Vγ2Vδ2 T cells in viremic patients reflect both active responses (increasing cell numbers, better antigen responses, and higher proportion of effector memory cells) and ongoing damage (repertoire changes and loss of CD56+ cells). Unlike patients who control viremia to undetectable levels, Vγ2Vδ2 T cells are diminished during persistent viremia and may eventually be lost because of progressive destruction of the TCR repertoire. [ABSTRACT FROM AUTHOR]

Published

2012

7. Antiviral Activity of Single-Dose PRO 140, a CCR5 Monoclonal Antibody, in HIV-Infected Adults.

Author

Jacobson, Jeffrey M., Saag, Michael S., Thompson, Melanie A., Fischl, Margaret A., Liporace, Ralph, Reichman, Richard C., Redfield, Robert R., Fichtenbaum, Carl J., Zingman, Barry S., Patel, Mahesh C., Murga, Jose D., Pemrick, Suzanne M., d'Ambrosio, Paul, Michael, Marti, Kroger, Hans, Hieu Ly, Rotshteyn, Yakov, Buice, Robert, Morris, Stephen A., and Stavola, Joseph J.

Subjects

ANTIVIRAL agents, HIV, MONOCLONAL antibodies, VIRAL replication, BLOOD plasma, IMMUNOGLOBULINS, CETUXIMAB, RNA, PLACEBOS

Abstract

Background. The current goal of human immunodeficiency virus type 1 (HIV-1) therapy is to maximally suppress viral replication. Securing this goal requires new drugs and treatment classes. The chemokine receptor CCR5 provides an entry portal for HIV-1, and PRO 140 is a humanized monoclonal antibody that binds to CCR5 and potently inhibits CCR5-tropic (R5) HIV-1 in vitro. Methods. A randomized, double-blind, placebo-controlled, dose-escalating study was conducted in 39 individuals with HIV-1 RNA levels ⩾5000 copies/mL, CD4+ cell counts ⩾250 cells/μL, no antiretroviral therapy for 3 months, and only R5 HIV-1 detectable. Cohorts were randomized 3:10 to receive placebo or doses of PRO 140 of 0.5, 2, or 5 mg/kg. Subjects were monitored for 58 days for safety, antiviral effects, and serum concentrations of PRO 140. Results. PRO 140 was generally well tolerated and demonstrated potent, rapid, prolonged, and dose-dependent antiviral activity. Mean reductions in HIV-1RNAlevel of 0.58 log10, 1.20 log10 (P = .0002) and 1.83 log10 (P < .0001) were observed for the 0.5-, 2-, and 5-mg/kg dose groups, respectively. Reductions in mean viral load of ⩾10-fold were observed within 4 days and persisted for 2-3 weeks after treatment. Conclusions. This trial established clear proof of concept for PRO 140 as a potent antiretroviral agent with extended activity after a single dose. Trial registration. ISRCTN Register: ISRCTN45537485. [ABSTRACT FROM AUTHOR]

Published

2008

8. Prospective Analyses of HIV-1--Specific Proliferative Responses, Recall Antigen Proliferative Responses, and Clinical Outcomes in an HIV-1--Seropositive Cohort.

Author

Ratto-Kim, Silvia, Garner, Robin P., Kim, Jerome H., Jagodzinski, Linda L., Michael, Nelson L., Paris, Robert, Redfield, Robert R., and Birx, Deborah L.

Subjects

HIV, VIRAL antigens, HIV infections, RNA, VIRAL load, LYMPHOPROLIFERATIVE disorders

Abstract

In cross-sectional studies of chronically infected individuals, lymphoproliferative responses to human immunodeficiency virus (HIV) type 1 p24 Gag antigen have previously been associated with lower virus load. It was not known whether this association would be predictive of better clinical outcome in longitudinal studies. Although response to recall antigens did not correlate with clinical indices of disease progression, positive baseline lymphoproliferative responses to p24 and TT were associated with lower plasma levels of HIV- 1 RNA. Persistently positive lymphoproliferative responses to the antigens also inversely correlated with repeated measurements of virus load, although the significance was lost once the measurements were adjusted for virus load and CD4+ cell count at baseline, by use of generalized estimating equation analysis. These observations suggest that the effect of the association between lymphoproliferative response and virus load is established early during HIV-1 infection and does not increase over time and suggest that antigen- specific lymphoproliferative responses reflect the dynamic state of HIV-1 infection and are inversely associated with virus load. [ABSTRACT FROM AUTHOR]

Published

2004

9. Association between Longer Duration of HIV-Suppressive Therapy and Partial Recovery of the V.... 2 T Cell Receptor Repertoire.

Author

Bordon, Jose, Evans, Peter S., Propp, Nadia, David Jr., Charles E., Redfield, Robert R., and Pauza, C. David

Subjects

HIV infections, T cell receptors, CELLS, IMMUNITY, VIRAL replication, VIROLOGY

Abstract

Human immunodeficiency virus (HIV) infection alters the function and repertoire of peripheral blood γδ T cells expressing the Vγ2/Vδ2 T cell receptor (TCR). A cross-sectional comparison of the Vγ2 TCR repertoire was performed for 56 HIV-infected subjects, 51 of whom were receiving highly active antiretroviral therapy (HAART), to measure changes in the Vγ2 TCR repertoire. Longer durations of HAART were associated with partial recovery of the normal TCR repertoire, and recovery was greatest in subjects with complete virus suppression. Changes in the Vγ2 TCR repertoire are sensitive measures for the effects of HAART and of residual HIV replication. [ABSTRACT FROM AUTHOR]

Published

2004

10. Repeated Immunization with Recombinant gp160 Human Immunodeficiency Virus (HIV) Envelope Protein...

Author

Ratto-Kim, Silvia, Sitz, Karl V., Garner, Robin P., Kim, Jerome H., Davis, Charles, Aronson, Naomi, Ruiz, Nancy, Tencer, Kathleen, Redfield, Robert R., and Birx, Deborah L.

Subjects

HIV infections, IMMUNIZATION, IMMUNOTHERAPY

Abstract

Evaluates cellular immunity in early-stage, asymptomatic HIV-1 infected persons immunized with either recombinant gp160 or placebo every two months for five years. Proliferative responses; Reactivity to antigens and mitogens; Statistical differences between vaccine and placebo groups.

Published

1999

11. Establishment and Characterization of Human Immunodeficiency Virus Type 1 (HIV-1) Envelope-Specific CD4+ T Lymphocyte Lines from HIV-I-Seropositive Patients.

Author

Ratto, Silvia, Sitz, Karl V., Scherer, Aimée M., Manca, Fabrizio, Loomis, Lawrence D., Cox, Josephine H., Redfield, Robert R., and Birx, Deborah L.

Abstract

Human immunodeficiency virus type 1 (HIV-l) gpI60-, gpI20-, and tetanus toxoid-specific CD4+ T lymphocyte lines were developed from 11 HIV-l-seropositive volunteers enrolled in a vaccine therapy trial. Of the 20 HIV-1 envelope-specific T cell lines, 9 were challenged with a panel of overlapping peptides spanning the gp120LAI sequence. The most frequently recognized regions were amino acids 74–105 in the Cl region and 306–328 in the V3 region. When tested against a panel of divergent HIV-1 envelopes, 55% of the envelope-specific lines were able to recognize gp120MN, while only 22% recognized gp120SF2. Cytotoxicity testing with HIV-l envelope antigen or peptides demonstrated killing by all 3 envelope-specific lines tested. Supernatants from 2 of 9 lines had high titers of p24 gag antigen, which did not seem to interfere with functional properties. [ABSTRACT FROM PUBLISHER]

Published

1995

12. Correlation between Humoral Responses to Human Immunodeficiency Virus Type 1 Envelope and Disease Progression in Early-Stage Infection.

Author

Loomis-Price, Lawrence D., Cox, Josephine H., Mascola, John R., VanCott, Thomas C., Michael, Nelson L., Fouts, Timothy R., Redfield, Robert R., Robb, Merlin L., Wahren, Britta, Sheppard, Haynes W., and Birx, Deborah L.

Abstract

Human immunodeficiency virus (HIV)-1—infected rapid and slow progressors showed differential humoral responses against HIV envelope peptides and proteins early in infection. Sera from slow progressors reacted more strongly with short envelope peptides modeling gp160NL4-3, predominantly in gp41. Reactivity to six peptides (in constant regions C3, C4, and C5 of gp120 and in gp41) correlated with slower progression. In a novel association, reactivity to three peptides (in constant regions C1 and C3 and variable region V3 of gp120) correlated with faster progression. Envelope peptide reactivity correlated with subsequent course of disease progression as strongly as did reactivity to gag p24. Patients heterozygous for 32-bp deletions in the CCR5 coreceptor reacted more frequently to an epitope in gp41. Rapid progressors had greater gp120 native-to-denatured binding ratios than did slow progressors. While antibody-dependent cellular cytotoxicity against gp120 did not strongly differentiate the groups, slow progressors showed a broader neutralization pattern against 5 primary virus isolates. [ABSTRACT FROM PUBLISHER]

Published

1998

13. Delayed-Type Hypersensitivity Skin Testing using Third Variable Loop Peptides Identifies T Lymphocyte Epitopes in Human Immunodeficiency Virus-Infected Persons.

Author

Sitz, Karl V., Price, Lawrence D. Loomis, Kim, Silvia Ratto, Kenner, Julie R., Sau, Purnima, Eckels, Kenneth H., Redfield, Robert R., and Birx, Deborah L.

Abstract

Cellular immune responses to human immunodeficiency virus type 1 (HIV-1) infection, particularly in vivo responses, have been difficult to study in large patient cohorts because of technical impediments. By use of small peptide fragments of the HIV-1 gp120 third variable loop, the CD4 T lymphocyte epitopes of 2 HIV-infected persons were mapped using a cutaneous delayed-type hypersensitivity (DTH) assay. The in vivo DTHresponses correlated with epitopes previously identified in vitro using CD4 T lymphocyte lines. The ability to determine CD4 T lymphocyte epitopes in large cohorts of patients using this simple in vivo technique would provide important diagnostic and prognostic data regarding effective immunoregulation of HIV-1. This technique should have broad applicability in HIV vaccine development and in the investigation of other immune-mediated human diseases. [ABSTRACT FROM PUBLISHER]

Published

1997

14. Proteosomes, Emulsomes, and Cholera Toxin B Improve Nasal Immunogenicity of Human Immunodeficiency Virus gp160 in Mice: Induction of Serum, Intestinal, Vaginal, and Lung IgA and IgG.

Author

Lowell, George H., Kaminski, Robert W., VanCott, Thomas C., Slike, Bonnie, Kersey, Kathryn, Zawoznik, Eduardo, Loomis-Price, Lawrence, Smith, Gale, Redfield, Robert R., Amselem, Shimon, and Birx, Deborah L.

Abstract

Intranasal immunization of mice with human immunodeficiency virus (HIV) rgp160 complexed to proteosomes improved anti-gp160 serum IgA and IgG titers, increased the number of gp160 peptides recognized, and stimulated anti-gp160 intestinal IgA compared with immunization with uncomplexed rgp160 in saline. These enhanced responses were especially evident when either a bioadhesive nanoemulsion (emulsomes) or cholera toxin B subunit (CTB) was added to the proteosome-rgp160 vaccine. Furthermore, anti-gp160 IgG and IgA in vaginal secretions and fecal extracts were induced after intranasal immunization with proteosome-rgp160 delivered either in saline or with emulsomes. Formulation of uncompiexed rgp160 with emulsomes or CTB also enhanced serum and selected mucosal IgA responses. Induction of serum, vaginal, bronchial, intestinal, and fecal IgA and IgG by intranasal proteosome-rgp160 vaccines delivered in saline or with emulsomes or CTB is encouraging for mucosal vaccine development to help control the spread of HIV transmission and AIDS. [ABSTRACT FROM PUBLISHER]

Published

1997

15. OCCUPATIONAL AND GEOGRAPHIC RISK FACTORS FOR HEPATITIS B AMONG US ARMY ENLISTED PERSONNEL DURING 1980.

Author

GARDNER, LYTT I., REDFIELD, ROBERT R., LEDNAR, WAYNE M., LEMON, STANLEY M., and MILLER, RICHARD N.

Published

1986

16. FREQUENCY OF ILLNESS ASSOCIATED WITH EPIDEMIC HEPATITIS A VIRUS INFECTIONS IN ADULTS.

Author

LEDNAR, WAYNE M., LEMON, STANLEY M., KIRKPATRICK, JAMES W., REDFIELD, ROBERT R., FIELDS, MIRIAM L., and KELLEY, PATRICK W.

Published

1985

17. Combination Antiretroviral Therapy with Tenofovir, Emtricitabine or Lamivudine, and Nevirapine.

Author

Redfield, Robert R. and Morrow, J. Scott

Subjects

*LETTERS to the editor, *ANTIVIRAL agents

Abstract

A letter to the editor is presented in response to the article about regimens that consist tenofovir, emtricitabine and nevirapine associated with a risk of early virologic failure in antiretroviral-naive, which appeared in the previous issue.

Published

2008

18. Reply to Hartjen et al.

Author

Boudova, Sarah, Li, Haishan, Sajadi, Mohammad M., Redfield, Robert R., Cairo, Cristiana, and David Pauza, C.

Subjects

HIV, T cells

Abstract

A letter to the editor in response to a study published in the earlier issue of the journal is presented.

Published

2013