Your search keyword '"Bailer, Robert T"' showing total 12 results

1. Neutralizing antibody VRC01 failed to select for HIV-1 mutations upon viral rebound

Author

Cale, Evan M., Bai, Hongjun, Bose, Meera, Messina, Michael A., Colby, Donn J., Sanders-Buell, Eric, Dearlove, Bethany, Li, Yifan, Engeman, Emily, Silas, Daniel, O'Sullivan, Anne Marie, Mann, Brendan, Pinyakorn, Suteeraporn, Intasan, Jintana, Benjapornpong, Khunthalee, Sacdalan, Carlo, Kroon, Eugene, Phanuphak, Nittaya, Gramzinski, Robert, Vasan, Sandhya, Robb, Merlin L., Michael, Nelson L., Lynch, Rebecca M., Bailer, Robert T., Pagliuzza, Amelie, Chomont, Nicolas, Pegu, Amarendra, Doria-Rose, Nicole A., Trautmann, Lydie, Crowell, Trevor A., Mascola, John R., Ananworanich, Jintanat, Tovanabutra, Sodsai, and Rolland, Morgane

Subjects

Highly active antiretroviral therapy -- Health aspects, HIV -- Genetic aspects -- Prevention, Antiretroviral agents -- Health aspects, Antibodies -- Genetic aspects -- Health aspects, Antigenic determinants -- Genetic aspects -- Health aspects, Health care industry

Abstract

Infusion of the broadly neutralizing antibody VRC01 has been evaluated in individuals chronically infected with HIV-1. Here, we studied how VRC01 infusions affected viral rebound after cessation of antiretroviral therapy (ART) in 18 acutely treated and durably suppressed individuals. Viral rebound occurred in all individuals, yet VRC01 infusions modestly delayed rebound and participants who showed a faster decay of VRC01 in serum rebounded more rapidly. Participants with strains most sensitive to VRC01 or with VRC01 epitope motifs similar to known VRC01- susceptible strains rebounded later. Upon rebound, HIV-1 sequences were indistinguishable from those sampled at diagnosis. Across the cohort, participant-derived Env showed different sensitivity to VRC01 neutralization (including 2 resistant viruses), yet neutralization sensitivity was similar at diagnosis and after rebound, indicating the lack of selection for VRC01 resistance during treatment interruption. Our results showed that viremia rebounded despite the absence of HIV-1 adaptation to VRC01 and an average VRC01 trough of 221 micro]g/mL. Although VRC01 levels were insufficient to prevent a resurgent infection, knowledge that they did not mediate Env mutations in acute-like viruses is relevant for antibody-based strategies in acute infection., Introduction Analytic treatment interruption (ATI) studies can help evaluate strategies to mediate long-term remission in HIV-1-infected persons. An ATI study tested the impact of the administration of the broadly neutralizing [...]

Published

2020

2. Broad and potent HIV-1 neutralization by a human antibody that binds the gp41-gp120 interface

Author

Huang, Jinghe, Kang, Byong H., Pancera, Marie, Lee, Jeong Hyun, Tong, Tommy, Feng, Yu, Imamichi, Hiromi, Georgiev, Ivelin S., Chuang, Gwo-Yu, Druz, Aliaksandr, Doria-Rose, Nicole A., Laub, Leo, Sliepen, Kwinten, van Gils, Marit J., de la Pena, Alba Torrents, Derking, Ronald, Klasse, Per-Johan, Migueles, Stephen A., Bailer, Robert T., Alam, Munir, Pugach, Pavel, Haynes, Barton F., Wyatt, Richard T., Sanders, Rogier W., Binley, James M., Ward, Andrew B., Mascola, John R., Kwong, Peter D., and Connors, Mark

Subjects

Viral antibodies -- Physiological aspects -- Research, Antigenic determinants -- Physiological aspects -- Research, Antibodies -- Physiological aspects -- Research, HIV infection -- Genetic aspects -- Care and treatment -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

The isolation of human monoclonal antibodies is providing important insights into the specificities that underlie broad neutralization of HIV-1 (reviewed in ref. 1). Here we report a broad and extremely potent HIV-specific monoclonal antibody, termed 35O22, which binds a novel HIV-1 envelope glycoprotein (Env) epitope. 35O22 neutralized 62% of 181 pseudoviruses with a half-maximum inhibitory concentration ([IC.sub.50]), Induction of a potent neutralizing antibody response capable of recognizing highly diverse isolates of HIV-1 is one of the most important goals of HIV vaccine research. This represents a considerable [...]

Published

2014

3. Structure and immune recognition of trimeric pre-fusion HIV-1 Env

Author

Pancera, Marie, Zhou, Tongqing, Druz, Aliaksandr, Georgiev, Ivelin S., Soto, Cinque, Gorman, Jason, Huang, Jinghe, Acharya, Priyamvada, Chuang, Gwo-Yu, Ofek, Gilad, Stewart-Jones, Guillaume B.E., Stuckey, Jonathan, Bailer, Robert T., Joyce, M. Gordon, Louder, Mark K., Tumba, Nancy, Yang, Yongping, Zhang, Baoshan, Cohen, Myron S., Haynes, Barton F., Mascola, John R., Morris, Lynn, Munro, James B., Blanchard, Scott C., Mothes, Walther, Connors, Mark, and Kwong, Peter D.

Subjects

HIV antibodies -- Physiological aspects, Viral proteins -- Structure -- Health aspects, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

The human immunodeficiency virus type 1 (HIV-1) envelope (Env) spike, comprising three gp120 and three gp41 sub-units, is a conformational machine that facilitates HIV-1 entry by rearranging from a mature unliganded state, through receptor-bound intermediates, to a post-fusion state. As the sole viral antigen on the HIV-1 virion surface, Env is both the target of neutralizing antibodies and a focus of vaccine efforts. Here we report the structure at 3.5 A resolution for an HIV-1 Env trimer captured in a mature closed state by antibodies PGT122 and 35O22. This structure reveals the prefusion conformation of gp41, indicates rearrangements needed for fusion activation, and defines parameters of immune evasion and immune recognition. Pre-fusion gp41 encircles amino- and carboxy- terminal strands of gp120 with four helices that form a membrane-proximal collar, fastened by insertion of a fusion peptide-proximal methionine into a gp41-tryptophan clasp. Spike rearrangements required for entry involve opening the clasp and expelling the termini. N-linked glycosylation and sequence- variable regions cover the pre-fusion closed spike; we used chronic cohorts to map the prevalence and location of effective HIV-1-neutralizing responses, which were distinguished by their recognition of N-linked glycan and tolerance for epitope-sequence variation., Over the last 50 years, more than 70 million people have been infected or killed by the human immunodeficiency virus type 1 (HIV-1) (1). A dominant contributing factor has been [...]

Published

2014

4. Immunological and virological mechanisms of vaccine-mediated protection against SIV and HIV

Author

Roederer, Mario, Keele, Brandon F., Schmidt, Stephen D., Mason, Rosemarie D., Welles, Hugh C., Fischer, Will, Labranche, Celia, Foulds, Kathryn E., Louder, Mark K., Yang, Zhi-Yong, Todd, John-Paul M., Buzby, Adam P., Mach, Linh V., Shen, Ling, Seaton, Kelly E., Ward, Brandy M., Bailer, Robert T., Gottardo, Raphael, Gu, Wenjuan, Ferrari, Guido, Alam, S. Munir, Denny, Thomas N., Montefiori, David C., Tomaras, Georgia D., Korber, Bette T., Nason, Martha C., Seder, Robert A., Koup, Richard A., Letvin, Norman L., Rao, Srinivas S., Nabel, Gary J., and Mascola, John R.

Subjects

Antigen-antibody reactions -- Research, Immune complexes -- Research, AIDS (Disease) -- Research, AIDS research, Monoclonal antibodies -- Health aspects -- Analysis -- Physiological aspects, AIDS vaccines -- Health aspects -- Analysis -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

A major challenge for the development of a highly effective AIDS vaccine is the identification of mechanisms of protective immunity. To address this question, we used a nonhuman primate challenge model with simian immunodeficiency virus (SIV). We show that antibodies to the SIV envelope are necessary and sufficient to prevent infection. Moreover, sequencing of viruses from breakthrough infections revealed selective pressure against neutralization-sensitive viruses; we identified a two-amino-acid signature that alters antigenicity and confers neutralization resistance. A similar signature confers resistance of human immunodeficiency virus (HIV)-1 to neutralization by monoclonal antibodies against variable regions 1 and 2 (V1V2), suggesting that SIV and HIV share a fundamental mechanism of immune escape from vaccine-elicited or naturally elicited antibodies. These analyses provide insight into the limited efficacy seen in HIV vaccine trials., Among the five human efficacy trials of HIV-1 vaccines, only one has shown some success in preventing HIV infection. In the RV144 trial, a combination viral vector and protein immunization [...]

Published

2014

5. Safety and pharmacokinetics of the Fc-modified HIV-1 human monoclonal antibody VRC01LS: A Phase 1 open-label clinical trial in healthy adults

Author

Gaudinski, Martin R., Coates, Emily E., Houser, Katherine V., Chen, Grace L., Yamshchikov, Galina, Saunders, Jamie G., Holman, LaSonji A., Gordon, Ingelise, Plummer, Sarah, Hendel, Cynthia S., Conan-Cibotti, Michelle, Lorenzo, Margarita Gomez, Sitar, Sandra, Carlton, Kevin, Laurencot, Carolyn, Bailer, Robert T., Narpala, Sandeep, McDermott, Adrian B., Namboodiri, Aryan M., Pandey, Janardan P., Schwartz, Richard M., Hu, Zonghui, Koup, Richard A., Capparelli, Edmund, Graham, Barney S., Mascola, John R., and Ledgerwood, Julie E.

Subjects

United States. National Institutes of Health, HIV (Viruses) -- Research -- Drug therapy -- Prevention, Clinical trials -- Analysis, Adults -- Health aspects, Vaccines -- Health aspects, Monoclonal antibodies -- Health aspects, HIV infection -- Health aspects -- Prevention, Biological sciences

Abstract

Background VRC01 is a human broadly neutralizing monoclonal antibody (bnMAb) against the CD4-binding site of the HIV-1 envelope glycoprotein (Env) that is currently being evaluated in a Phase IIb adult HIV-1 prevention efficacy trial. VRC01LS is a modified version of VRC01, designed for extended serum half-life by increased binding affinity to the neonatal Fc receptor. Methods and findings This Phase I dose-escalation study of VRC01LS in HIV-negative healthy adults was conducted by the Vaccine Research Center (VRC) at the National Institutes of Health (NIH) Clinical Center (Bethesda, MD). The age range of the study volunteers was 21-50 years; 51% of study volunteers were male and 49% were female. Primary objectives were safety and tolerability of VRC01LS intravenous (IV) infusions at 5, 20, and 40 mg/kg infused once, 20 mg/kg given three times at 12-week intervals, and subcutaneous (SC) delivery at 5 mg/kg delivered once, or three times at 12-week intervals. Secondary objectives were pharmacokinetics (PK), serum neutralization activity, and development of antidrug antibodies. Enrollment began on November 16, 2015, and concluded on August 23, 2017. This report describes the safety data for the first 37 volunteers who received administrations of VRC01LS. There were no serious adverse events (SAEs) or dose-limiting toxicities. Mild malaise and myalgia were the most common adverse events (AEs). There were six AEs assessed as possibly related to VRC01LS administration, and all were mild in severity and resolved during the study. PK data were modeled based on the first dose of VRC01LS in the first 25 volunteers to complete their schedule of evaluations. The mean (±SD) serum concentration 12 weeks after one IV administration of 20 mg/kg or 40 mg/kg were 180 ± 43 [mu]g/mL (n = 7) and 326 ± 35 [mu]g/mL (n = 5), respectively. The mean (±SD) serum concentration 12 weeks after one IV and SC administration of 5 mg/kg were 40 ± 3 [mu]g/mL (n = 2) and 25 ± 5 [mu]g/mL (n = 9), respectively. Over the 5-40 mg/kg IV dose range (n = 16), the clearance was 36 ± 8 mL/d with an elimination half-life of 71 ± 18 days. VRC01LS retained its expected neutralizing activity in serum, and anti-VRC01 antibody responses were not detected. Potential limitations of this study include the small sample size typical of Phase I trials and the need to further describe the PK properties of VRC01LS administered on multiple occasions. Conclusions The human bnMAb VRC01LS was safe and well tolerated when delivered intravenously or subcutaneously. The half-life was more than 4-fold greater when compared to wild-type VRC01 historical data. The reduced clearance and extended half-life may make it possible to achieve therapeutic levels with less frequent and lower-dose administrations. This would potentially lower the costs of manufacturing and improve the practicality of using passively administered monoclonal antibodies (mAbs) for the prevention of HIV-1 infection. Trial registration ClinicalTrials.gov NCT02599896, Author(s): Martin R. Gaudinski 1, Emily E. Coates 1, Katherine V. Houser 1, Grace L. Chen 1, Galina Yamshchikov 1, Jamie G. Saunders 1, LaSonji A. Holman 1, Ingelise Gordon [...]

Published

2018

6. Broad and potent neutralization of HIV-1 by a gp41-specific human antibody

Author

Huang, Jinghe, Ofek, Gilad, Laub, Leo, Louder, Mark K., Doria-Rose, Nicole A., Longo, Nancy S., Imamichi, Hiromi, Bailer, Robert T., Chakrabarti, Bimal, Sharma, Shailendra K., Alam, S. Munir, Wang, Tao, Yang, Yongping, Zhang, Baoshan, Migueles, Stephen A., Wyatt, Richard, Haynes, Barton F., Kwong, Peter D., Mascola, John R., and Connors, Mark

Subjects

Viral antibodies -- Properties -- Research, Vaccines -- Research, Antibodies -- Properties -- Research, HIV infection -- Prevention -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Characterization of human monoclonal antibodies is providing considerable insight into mechanisms of broad HIV-1 neutralization. Here we report an HIV-1 gp41 membrane-proximal external region (MPER)-specific antibody, named 10E8, which neutralizes ~98% of tested viruses. An analysis of sera from 78 healthy HIV-1-infected donors demonstrated that 27% contained MPER-specific antibodies and 8% contained 10E8-like specificities. In contrast to other neutralizing MPER antibodies, 10E8 did not bind phospholipids, was not autoreactive, and bound cell-surface envelope. The structure of 10E8 in complex with the complete MPER revealed a site of vulnerability comprising a narrow stretch of highly conserved gp41-hydrophobic residues and a critical arginine or lysine just before the transmembrane region. Analysis of resistant HIV-1 variants confirmed the importance of these residues for neutralization. The highly conserved MPER is a target of potent, non-self-reactive neutralizing antibodies, suggesting that HIV-1 vaccines should aim to induce antibodies to this region of HIV-1 envelope glycoprotein., Induction of an antibody response capable of neutralizing diverse HIV-1 isolates is a critical goal for vaccines that protect against HIV-1 infection. Potentially the greatest obstacle to achieving this goal [...]

Published

2012

7. Safety, pharmacokinetics, and immunological activities of multiple intravenous or subcutaneous doses of an anti-HIV monoclonal antibody, VRC01, administered to HIV-uninfected adults: Results of a phase 1 randomized trial

Author

Mayer, Kenneth H., Seaton, Kelly E., Huang, Yunda, Grunenberg, Nicole, Isaacs, Abby, Allen, Mary, Ledgerwood, Julie E., Frank, Ian, Sobieszczyk, Magdalena E., Baden, Lindsey R., Rodriguez, Benigno, Van Tieu, Hong, Tomaras, Georgia D., Deal, Aaron, Goodman, Derrick, Bailer, Robert T., Ferrari, Guido, Jensen, Ryan, Hural, John, Graham, Barney S., Mascola, John R., Corey, Lawrence, and Montefiori, David C.

Subjects

AIDS (Disease) -- Research, AIDS research, Monoclonal antibodies -- Testing, HIV infection -- Care and treatment, Biological sciences

Abstract

Background VRC01 is an HIV-1 CD4 binding site broadly neutralizing antibody (bnAb) that is active against a broad range of HIV-1 primary isolates in vitro and protects against simian-human immunodeficiency virus (SHIV) when delivered parenterally to nonhuman primates. It has been shown to be safe and well tolerated after short-term administration in humans; however, its clinical and functional activity after longer-term administration has not been previously assessed. Methods and findings HIV Vaccine Trials Network (HVTN) 104 was designed to evaluate the safety and tolerability of multiple doses of VRC01 administered either subcutaneously or by intravenous (IV) infusion and to assess the pharmacokinetics and in vitro immunologic activity of the different dosing regimens. Additionally, this study aimed to assess the effect that the human body has on the functional activities of VRC01 as measured by several in vitro assays. Eighty-eight healthy, HIV-uninfected, low-risk participants were enrolled in 6 United States clinical research sites affiliated with the HVTN between September 9, 2014, and July 15, 2015. The median age of enrollees was 27 years (range, 18-50); 52% were White (non-Hispanic), 25% identified as Black (non-Hispanic), 11% were Hispanic, and 11% were non-Hispanic people of diverse origins. Participants were randomized to receive the following: a 40 mg/kg IV VRC01 loading dose followed by five 20 mg/kg IV VRC01 doses every 4 weeks (treatment group 1 [T1], n = 20); eleven 5 mg/kg subcutaneous (SC) VRC01 (treatment group 3 [T3], n = 20); placebo (placebo group 3 [P3], n = 4) doses every 2 weeks; or three 40 mg/kg IV VRC01 doses every 8 weeks (treatment group 2 [T2], n = 20). Treatment groups T4 and T5 (n = 12 each) received three 10 or 30 mg/kg IV VRC01 doses every 8 weeks, respectively. Participants were followed for 32 weeks after their first VRC01 administration and received a total of 249 IV infusions and 208 SC injections, with no serious adverse events, dose-limiting toxicities, nor evidence for anti-VRC01 antibodies observed. Serum VRC01 levels were detected through 12 weeks after final administration in all participants who received all scheduled doses. Mean peak serum VRC01 levels of 1,177 [mu]g/ml (95% CI: 1,033, 1,340) and 420 [mu]g/ml (95% CI: 356, 494) were achieved 1 hour after the IV infusion series of 30 mg/kg and 10 mg/kg doses, respectively. Mean trough levels at week 24 in the IV infusion series of 30 mg/kg and 10 mg/kg doses, respectively, were 16 [mu]g/ml (95% CI: 10, 27) and 6 [mu]g/ml (95% CI: 5, 9) levels, which neutralize a majority of circulating strains in vitro (50% inhibitory concentration [IC50] > 5 [mu]g/ml). Post-infusion/injection serum VRC01 retained expected functional activity (virus neutralization, antibody-dependent cellular cytotoxicity, phagocytosis, and virion capture). The limitations of this study include the relatively small sample size of each VRC01 administration regimen and missing data from participants who were unable to complete all study visits. Conclusions VRC01 administered as either an IV infusion (10-40 mg/kg) given monthly or bimonthly, or as an SC injection (5 mg/kg) every 2 weeks, was found to be safe and well tolerated. In addition to maintaining drug concentrations consistent with neutralization of the majority of tested HIV strains, VRC01 concentrations from participants' sera were found to avidly capture HIV virions and to mediate antibody-dependent cellular phagocytosis, suggesting a range of anti-HIV immunological activities, warranting further clinical trials. Trial registration Clinical Trials Registration: NCT02165267, Author(s): Kenneth H. Mayer 1,*, Kelly E. Seaton 2, Yunda Huang 3, Nicole Grunenberg 3, Abby Isaacs 3, Mary Allen 4, Julie E. Ledgerwood 5, Ian Frank 6, Magdalena E. [...]

Published

2017

8. Safety and immunogenicity of a gag-pol candidate HIV-1 DNA vaccine administered by a needle-free device in HIV-1-seronegative subjects

Author

Tavel, Jorge A., Martin, Julie E., Kelly, Grace G., Enama, Mary E., Shen, Jean M., Gomez, Phillip L., Andrews, Charla A., Koup, Richard A., Bailer, Robert T., Stein, Judy A., Roederer, Mario, Nabel, Gary J., and Graham, Barney S.

Subjects

DNA vaccines -- Dosage and administration, HIV infection -- Care and treatment, Hypodermic jet injectors -- Usage, Health

Abstract

The safety and immunogenicity of a candidate HIV DNA vaccine administered by using a needle-free device is evaluated. The results have shown that the HIV DNA vaccine is safe and well tolerated and it has led to the development of a 4-plasmid multiclade HIV DNA Vaccine Research Center vaccine candidate in which envelope genes expressing Env from clades A, B, and C and Nef gene from clade B is added.

Published

2007

9. A West Nile virus dna vaccine induces neutralizing antibody in healthy adults during a phase 1 clinical trial

Author

Martin, Julie E., Pierson, Theodore C., Hubka, Sarah, Rucker, Steve, Gordon, Ingelise J., Enama, Mary E., Andrews, Charla A., Xu, Qing, Davis, Brent S., Nason, Martha C., Fay, Michael P., Koup, Richard A., Roederer, Mario, Bailer, Robert T., Gomez, Phillip L., Mascola, John R., Chang, Gwong-Jen J., Nabel, Gary J., and Graham, Barney S.

Subjects

West Nile virus -- Physiological aspects, West Nile virus -- Research, DNA vaccines -- Dosage and administration, DNA vaccines -- Physiological aspects, DNA vaccines -- Research, Human immunogenetics -- Research, Clinical trials -- Reports, Health

Published

2007

10. Phase 1 safety and immunogenicity evaluation of a multiclade HIV-1 DNA candidate vaccine

Author

Graham, Barney S., Koup, Richard A., Roederer, Mario, Bailer, Robert T., Enama, Mary E., Moodie, Zoe, Martin, Julie E., McCluskey, Margaret M., Chakrabarti, Bimal K., Lamoreaux, Laurie, Andrews, Charla A., Gomez, Phillip L., Mascola, John R., and Nabel, Gary J.

Subjects

AIDS vaccines -- Research, Immunogenetics -- Research, Health

Published

2006

11. Phase 1 safety and immunogenicity evaluation of a multiclade HIV-1 candidate vaccine delivered by a replication-defective recombinant adenovirus vector

Author

Catanzaro, Andrew T., Koup, Richard A., Roederer, Mario, Bailer, Robert T., Enama, Mary E., Moodie, Zoe, Gu, Lin, Martin, Julie E., Novik, Laura, Chakrabarti, Bimal K., Butman, Bryan T., Gall, Jason G.D., King, C. Richter, Andrews, Charla A., Sheets, Rebecca, Gomez, Phillip L., Mascola, John R., Nabel, Gary J., and Graham, Barney S.

Subjects

AIDS vaccines -- Dosage and administration, AIDS vaccines -- Research, Adenoviruses, Human -- Research, Health

Published

2006

12. Fusion activity dissociated from replication ability in feline immunodeficiency virus (FIV) in human cells

Author

Tochikura, Tadafumi S., Tanabe-Tochikura, Akiko, Hayes, Kathleen A., Lazo, Aristides, Bailer, Robert T., Blakeslee, James R., Jr., Lafrado, Louis J., Roy-Burman, Pradip, Pandey, Rakesh, Olsen, Richard G., and Mathes, Lawrence E.

Subjects

Feline immunodeficiency virus, Human cell culture -- Analysis, Cell hybridization -- Analysis, Health

Abstract

Feline immunodeficiency virus (FIV) may be able to form viral DNA in human T-cell lines, but may not produce competent viruses. T-cell lines are precursors to the T-cells of the immune system. Researchers grew two HTLV-1-positive human cell lines and three HTLV-1-negative human cell lines with an FIV-positive feline cell line to evaluate the human cell lines' sensitivity to FIV-induced cell joining. Giant cells with multiple nuclei formed in four of the five human cell lines cultivated with FIV cells. In three human cell lines, giant cell formation was followed by cell death. None of the cultivated human cells or human cells treated with cell-free FIV produced proteins specific to FIV. Four of the human cell lines tested negative for the presence of FIV DNA or virus replication according to tests conducted after exposure to FIV. Subsequent analyses identified one human cell line that contained FIV DNA.

Published

1993