Your search keyword '"Watkins, David I."' showing total 54 results

1. Plasmablast Expansion Following the Tetravalent, Live-Attenuated Dengue Vaccine Butantan-DV in DENV-Naïve and DENV-Exposed Individuals in a Brazilian Cohort.

Author

Silveira, Cássia G. T., Magnani, Diogo M., Costa, Priscilla R., Avelino-Silva, Vivian I., Ricciardi, Michael J., Timenetsky, Maria do Carmo S. T., Goulart, Raphaella, Correia, Carolina A., Marmorato, Mariana P., Ferrari, Lilian, Nakagawa, Zelinda B., Tomiyama, Claudia, Tomiyama, Helena, Kalil, Jorge, Palacios, Ricardo, Precioso, Alexander R., Watkins, David I., and Kallás, Esper G.

Subjects

DENGUE, DENGUE viruses, VACCINE effectiveness, VACCINES, VACCINATION

Abstract

An effective vaccine against the dengue virus (DENV) should induce a balanced, long-lasting antibody (Ab) response against all four viral serotypes. The burst of plasmablasts in the peripheral blood after vaccination may reflect enriched vaccine-specific Ab secreting cells. Here we characterize the acute plasmablast responses from naïve and DENV-exposed individuals following immunization with the live attenuated tetravalent (LAT) Butantan DENV vaccine (Butantan-DV). The frequency of circulating plasmablasts was determined by flow cytometric analysis of fresh whole blood specimens collected from 40 participants enrolled in the Phase II Butantan-DV clinical trial (NCT01696422) before and after (days 6, 12, 15 and 22) vaccination. We observed a peak in the number of circulating plasmablast at day 15 after vaccination in both the DENV naïve and the DENV-exposed vaccinees. DENV-exposed vaccinees experienced a significantly higher plasmablast expansion. In the DENV-naïve vaccinees, plasmablasts persisted for approximately three weeks longer than among DENV-exposed volunteers. Our findings indicate that the Butantan-DV can induce plasmablast responses in both DENV-naïve and DENV-exposed individuals and demonstrate the influence of pre-existing DENV immunity on Butantan DV-induced B-cell responses. [ABSTRACT FROM AUTHOR]

Published

2022

2. Non-neutralizing Antibodies May Contribute to Suppression of SIVmac239 Viremia in Indian Rhesus Macaques.

Author

Pedreño-Lopez, Nuria, Rosen, Brandon C., Flores, Walter J., Gorman, Matthew J., Voigt, Thomas B., Ricciardi, Michael J., Crosno, Kristin, Weisgrau, Kim L., Parks, Christopher L., Lifson, Jeffrey D., Alter, Galit, Rakasz, Eva G., Magnani, Diogo M., Martins, Mauricio A., and Watkins, David I.

Subjects

RHESUS monkeys, SIMIAN immunodeficiency virus, IMMUNOGLOBULINS, BACTERIAL vaccines, HUMORAL immunity, FC receptors

Abstract

The antiviral properties of broadly neutralizing antibodies against HIV are well-documented but no vaccine is currently able to elicit protective titers of these responses in primates. While current vaccine modalities can readily induce non-neutralizing antibodies against simian immunodeficiency virus (SIV) and HIV, the ability of these responses to restrict lentivirus transmission and replication remains controversial. Here, we investigated the antiviral properties of non-neutralizing antibodies in a group of Indian rhesus macaques (RMs) that were vaccinated with vif , rev, tat, nef , and env , as part of a previous study conducted by our group. These animals manifested rapid and durable control of viral replication to below detection limits shortly after SIVmac239 infection. Although these animals had no serological neutralizing activity against SIVmac239 prior to infection, their pre-challenge titers of Env-binding antibodies correlated with control of viral replication. To assess the contribution of anti-Env humoral immune responses to virologic control in two of these animals, we transiently depleted their circulating antibodies via extracorporeal plasma immunoadsorption and inhibition of IgG recycling through antibody-mediated blockade of the neonatal Fc receptor. These procedures reduced Ig serum concentrations by up to 80% and temporarily induced SIVmac239 replication in these animals. Next, we transferred purified total Ig from the rapid controllers into six vaccinated RMs one day before intrarectal challenge with SIVmac239. Although recipients of the hyperimmune anti-SIV Ig fraction were not protected from infection, their peak and chronic phase viral loads were significantly lower than those in concurrent unvaccinated control animals. Together, our results suggest that non-neutralizing Abs may play a role in the suppression of SIVmac239 viremia. [ABSTRACT FROM AUTHOR]

Published

2021

3. Immunophenotyping of Rhesus CMV‐Specific CD8 T‐Cell Populations.

Author

Pomplun, Nicholas L., Vosler, Logan, Weisgrau, Kim L., Furlott, Jessica, Weiler, Andrea M., Abdelaal, Hadia M., Evans, David T., Watkins, David I., Matano, Tetsuro, Skinner, Pamela J., Friedrich, Thomas C., and Rakasz, Eva G.

Abstract

A vaccine to ameliorate cytomegalovirus (CMV)‐related pathogenicity in transplantation patients is considered a top priority. A therapeutic vaccine must include components that elicit both neutralizing antibodies, and highly effective CD8 T‐cell responses. The most important translational model of vaccine development is the captive‐bred rhesus macaque (Macaca mulatta) of Indian origin. There is a dearth of information on rhesus cytomegalovirus (rhCMV)‐specific CD8 T cells due to the absence of well‐defined CD8 T‐cell epitopes presented by classical MHC‐I molecules. In the current study, we defined two CD8 T‐cell epitopes restricted by high‐frequency Mamu alleles: the Mamu‐A1*002:01 restricted VY9 (VTTLGMALY aa291‐299) epitope of protein IE‐1, and the Mamu‐A1*008:01 restricted NP8 (NPTDRPIP aa96‐103) epitope of protein phosphoprotein 65‐2. We developed tetramers and determined the level, phenotype, and functional capability of the two epitope‐specific T‐cell populations in circulation and various tissues. We demonstrated the value of these tetramers for in situ tetramer staining. Here, we first provided critical reagents and established a flow cytometric staining strategy to study rhCMV‐specific T‐cell responses in up to 40% of captive‐bred rhesus macaques. © 2020 The Authors. Cytometry Part A published by Wiley Periodicals LLC on behalf of International Society for Advancement of Cytometry. [ABSTRACT FROM AUTHOR]

Published

2021

4. Rhesus Cytomegalovirus-Specific CD8+ Cytotoxic T Lymphocytes Do Not Become Functionally Exhausted in Chronic SIVmac239 Infection.

Author

Rosen, Brandon C., Pedreño-Lopez, Nuria, Ricciardi, Michael J., Reed, Jason S., Sacha, Jonah B., Rakasz, Eva G., and Watkins, David I.

Subjects

CYTOMEGALOVIRUSES, CYTOTOXIC T cells, HIV infections, HUMAN cytomegalovirus, RHESUS monkeys, INFECTION

Abstract

CD8+ cytotoxic T lymphocytes (CTLs) exert potent antiviral activity after HIV/SIV infection. However, efforts to harness the antiviral efficacy of CTLs for HIV/SIV prophylaxis and therapy have been severely hindered by two major problems: viral escape and exhaustion. By contrast, CTLs directed against human cytomegalovirus (HCMV), a ubiquitous chronic herpesvirus, seldom select for escape mutations and remain functional and refractory to exhaustion during chronic HCMV and HIV infection. Recently, attempts have been made to retarget HCMV-specific CTLs for cancer immunotherapy. We speculate that such a strategy may also be beneficial in the context of HIV/SIV infection, facilitating CTL-mediated control of HIV/SIV replication. As a preliminary assessment of the validity of this approach, we investigated the phenotypes and functionality of rhesus CMV (RhCMV)-specific CTLs in SIVmac239-infected Indian rhesus macaques (RMs), a crucial HIV animal model system. We recently identified two immunodominant, Mamu-A∗02 -restricted CTL epitopes derived from RhCMV proteins and sought to evaluate the phenotypic and functional characteristics of these CTL populations in chronic SIVmac239 infection. We analyzed and directly compared RhCMV- and SIVmac239-specific CTLs during SIVmac239 infection in a cohort of Mamu-A∗01 + and Mamu-A∗02 + RMs. CTL populations specific for at least one of the RhCMV-derived CTL epitopes were detected in ten of eleven Mamu-A∗02 + animals tested, and both populations were detected in five of these animals. Neither RhCMV-specific CTL population exhibited significant changes in frequency, memory phenotype, granzyme B expression, exhaustion marker (PD-1 and CTLA-4) expression, or polyfunctionality between pre- and chronic SIVmac239 infection timepoints. In chronic SIVmac239 infection, RhCMV-specific CTLs exhibited higher levels of granzyme B expression and polyfunctionality, and lower levels of exhaustion marker expression, than SIVmac239-specific CTLs. Additionally, compared to SIVmac239-specific CTLs, greater proportions of RhCMV-specific CTLs were of the terminally differentiated effector memory phenotype (CD28– CCR7–) during chronic SIVmac239 infection. These results suggest that, in contrast to SIVmac239-specific CTLs, RhCMV-specific CTLs maintain their phenotypes and cytolytic effector functions during chronic SIVmac239 infection, and that retargeting RhCMV-specific CTLs might be a promising SIV immunotherapeutic strategy. [ABSTRACT FROM AUTHOR]

Published

2020

5. Longitudinal dynamics of the human B cell response to the yellow fever 17D vaccine.

Author

Wec, Anna Z., Haslwanter, Denise, Abdiche, Yasmina N., Shehata, Laila, Pedreño-Lopez, Nuria, Moyer, Crystal L., Bornholdt, Zachary A., Lilov, Asparouh, Nett, Juergen H., Jangra, Rohit K., Brown, Michael, Watkins, David I., Ahlm, Clas, Forsell, Mattias N., Rey, Félix A., Barba-Spaeth, Giovanna, Chandran, Kartik, and Walker, Laura M.

Subjects

YELLOW fever, B cells, ANTIBODY formation, IMMUNOGLOBULIN M, GERMINAL centers

Abstract

A comprehensive understanding of the development and evolution of human B cell responses induced by pathogen exposure will facilitate the design of next-generation vaccines. Here, we utilized a highthroughput single B cell cloning technology to longitudinally track the human B cell response to the yellow fever virus 17D (YFV-17D) vaccine. The earlymemory B cell (MBC) response wasmediated by both classical immunoglobulin M (IgM) (IgM+CD27+) and switched immunoglobulin (swIg+) MBC populations; however, classical IgM MBCs waned rapidly, whereas swIg+ and atypical IgM+ and IgD+ MBCs were stable over time. Affinity maturation continued for 6 to 9mo following vaccination, providing evidence for the persistence of germinal center activity long after the period of active viral replication in peripheral blood. Finally, a substantial fraction of the neutralizing antibody response was mediated by public clones that recognize a fusion loop-proximal antigenic site within domain II of the viral envelope glycoprotein. Overall, our findings provide a framework for understanding the dynamics and complexity of human B cell responses elicited by infection and vaccination. [ABSTRACT FROM AUTHOR]

Published

2020

6. THE VACCINE SEARCH GOES ON.

Author

Watkins, David I.

Subjects

AIDS vaccines, VACCINE research, HIV infections, PREVENTIVE medicine, VACCINATION

Abstract

The article discusses the development of a vaccine for HIV. Background is given on the invention and function of vaccines. A history of attempted HIV vaccines is provided, noting the reasons for each vaccine's failure. Also discussed are the possibilities for future research, including studies into the behavior of HIV in order to discover new strategies for vaccine development.

Published

2008

7. Vaccine protection against SIVmac239 acquisition.

Author

Martins, Mauricio A., Bischof, Georg F., Shin, Young C., Lauer, William A., Gonzalez-Nieto, Lucas, Watkins, David I., Rakasz, Eva G., Lifson, Jeffrey D., and Desrosiers, Ronald C.

Subjects

SIV antibodies, IMMUNE response, VACCINATION, IMMUNIZATION, VIRAL antibodies

Abstract

The biological characteristics of HIV pose serious difficulties for the success of a preventive vaccine. Molecularly cloned SIVmac239 is difficult for antibodies to neutralize, and a variety of vaccine approaches have had great difficulty achieving protective immunity against it in rhesus monkey models. Here we report significant protection against i.v. acquisition of SIVmac239 using a long-lasting approach to vaccination. The vaccine regimen includes a replicationcompetent herpesvirus engineered to contain a near-full-length SIV genome that expresses all nine SIV gene products, assembles noninfectious SIV virion particles, and is capable of eliciting long-lasting effector-memory cellular immune responses to all nine SIV gene products. Vaccinated monkeys were significantly protected against acquisition of SIVmac239 following repeated marginal dose i.v. challenges over a 4-month period. Further work is needed to define the critical components necessary for eliciting this protective immunity, evaluate the breadth of the protection against a variety of strains, and explore how this approach may be extended to human use. [ABSTRACT FROM AUTHOR]

Published

2019

8. A recombinant herpesviral vector containing a near-full-length SIVmac239 genome produces SIV particles and elicits immune responses to all nine SIV gene products.

Author

Shin, Young C., Bischof, Georg F., Lauer, William A., Gonzalez-Nieto, Lucas, Rakasz, Eva G., Hendricks, Gregory M., Watkins, David I., Martins, Mauricio A., and Desrosiers, Ronald C.

Subjects

HIV, VACCINES, RHESUS monkeys, ELECTRON microscopy, PROTEOMICS, GENETICS

Abstract

The properties of the human immunodeficiency virus (HIV) pose serious difficulties for the development of an effective prophylactic vaccine. Here we describe the construction and characterization of recombinant (r), replication-competent forms of rhesus monkey rhadinovirus (RRV), a gamma-2 herpesvirus, containing a near-full-length (nfl) genome of the simian immunodeficiency virus (SIV). A 306-nucleotide deletion in the pol gene rendered this nfl genome replication-incompetent as a consequence of deletion of the active site of the essential reverse transcriptase enzyme. Three variations were constructed to drive expression of the SIV proteins: one with SIV’s own promoter region, one with a cytomegalovirus (cmv) immediate-early promoter/enhancer region, and one with an RRV dual promoter (p26 plus PAN). Following infection of rhesus fibroblasts in culture with these rRRV vectors, synthesis of the early protein Nef and the late structural proteins Gag and Env could be demonstrated. Expression levels of the SIV proteins were highest with the rRRV-SIVcmv-nfl construct. Electron microscopic examination of rhesus fibroblasts infected with rRRV-SIVcmv-nfl revealed numerous budding and mature SIV particles and these infected cells released impressive levels of p27 Gag protein (>150 ng/ml) into the cell-free supernatant. The released SIV particles were shown to be incompetent for replication. Monkeys inoculated with rRRV-SIVcmv-nfl became persistently infected, made readily-detectable antibodies against SIV, and developed T-cell responses against all nine SIV gene products. Thus, rRRV expressing a near-full-length SIV genome mimics live-attenuated strains of SIV in several important respects: the infection is persistent; >95% of the SIV proteome is naturally expressed; SIV particles are formed; and CD8+ T-cell responses are maintained indefinitely in an effector-differentiated state. Although the magnitude of anti-SIV immune responses in monkeys infected with rRRV-SIVcmv-nfl falls short of what is seen with live-attenuated SIV infection, further experimentation seems warranted. [ABSTRACT FROM AUTHOR]

Published

2018

9. Postnatal Zika virus infection is associated with persistent abnormalities in brain structure, function, and behavior in infant macaques.

Author

Mavigner, Maud, Raper, Jessica, Kovacs-Balint, Zsofia, Gumber, Sanjeev, O'Neal, Justin T., Bhaumik, Siddhartha K., Zhang, Xiaodong, Habib, Jakob, Mattingly, Cameron, McDonald, Circe E., Avanzato, Victoria, Burke, Mark W., Magnani, Diogo M., Bailey, Varian K., Watkins, David I., Vanderford, Thomas H., Fair, Damien, Earl, Eric, Feczko, Eric, and Styner, Martin

Subjects

ZIKA virus infections, LYMPHOID tissue, RHESUS monkeys, CENTRAL nervous system, GLIOSIS, NEURODEGENERATION

Abstract

Zika virus infection early after birth has deleterious effects on the developing brain and long-term behavioral changes in rhesus macaques. Postnatal perturbation by Zika virus: Much of the concern surrounding Zika virus infections focuses on fetuses infected in utero. Mavigner et al. reasoned that this neurotropic virus may have deleterious effects even after birth, so they set up a postnatal infection model to investigate. They found that infant rhesus macaques infected with Zika virus also had peripheral and central nervous system pathology. Longitudinal magnetic resonance imaging studies revealed that macaques that had been infected with Zika virus had structural and functional abnormalities and also altered emotional responses. These differences persisted months after the virus had been cleared. Although the work involved a small number of animals, their results suggest that infants and young children exposed to Zika virus should undergo more than just routine monitoring. The Zika virus (ZIKV) epidemic is associated with fetal brain lesions and other serious birth defects classified as congenital ZIKV syndrome. Postnatal ZIKV infection in infants and children has been reported; however, data on brain anatomy, function, and behavioral outcomes following infection are absent. We show that postnatal ZIKV infection of infant rhesus macaques (RMs) results in persistent structural and functional alterations of the central nervous system compared to age-matched controls. We demonstrate ZIKV lymphoid tropism and neurotropism in infant RMs and histopathologic abnormalities in the peripheral and central nervous systems including inflammatory infiltrates, astrogliosis, and Wallerian degeneration. Structural and resting-state functional magnetic resonance imaging (MRI/rs-fMRI) show persistent enlargement of lateral ventricles, maturational changes in specific brain regions, and altered functional connectivity (FC) between brain areas involved in emotional behavior and arousal functions, including weakened amygdala-hippocampal connectivity in two of two ZIKV-infected infant RMs several months after clearance of ZIKV RNA from peripheral blood. ZIKV infection also results in distinct alterations in the species-typical emotional reactivity to acute stress, which were predicted by the weak amygdala-hippocampal FC. We demonstrate that postnatal ZIKV infection of infants in this model affects neurodevelopment, suggesting that long-term clinical monitoring of pediatric cases is warranted. [ABSTRACT FROM AUTHOR]

Published

2018

10. SECTION VII: GENETICS OF THE ANTIMICROBIAL HOST RESPONSE: Chapter 39: Immunogenetics of Virus Pathogenesis.

Author

WILTSHIRE, SEAN, WATKINS, DAVID I., SKAMENE, EMIL, and VIDAL, SILVIA M.

Published

2011

11. Immunogenicity of Seven New Recombinant Yellow Fever Viruses 17D Expressing Fragments of SIVmac239 Gag, Nef, and Vif in Indian Rhesus Macaques.

Author

Martins, Mauricio A., Bonaldo, Myrna C., Rudersdorf, Richard A., Piaskowski, Shari M., Rakasz, Eva G., Weisgrau, Kim L., Furlott, Jessica R., Eernisse, Christopher M., de Santana, Marlon G. Veloso, Hidalgo, Bertha, Friedrich, Thomas C., Chiuchiolo, Maria J., Parks, Christopher L., Wilson, Nancy A., Allison, David B., Galler, Ricardo, and Watkins, David I.

Subjects

AIDS vaccines, IMMUNE response, YELLOW fever vaccines, ADENOVIRUS diseases, T cells, IMMUNOSUPPRESSION

Abstract

An effective vaccine remains the best solution to stop the spread of human immunodeficiency virus (HIV). Cellular immune responses have been repeatedly associated with control of viral replication and thus may be an important element of the immune response that must be evoked by an efficacious vaccine. Recombinant viral vectors can induce potent T-cell responses. Although several viral vectors have been developed to deliver HIV genes, only a few have been advanced for clinical trials. The live-attenuated yellow fever vaccine virus 17D (YF17D) has many properties that make it an attractive vector for AIDS vaccine regimens. YF17D is well tolerated in humans and vaccination induces robust T-cell responses that persist for years. Additionally, methods to manipulate the YF17D genome have been established, enabling the generation of recombinant (r)YF17D vectors carrying genes from unrelated pathogens. Here, we report the generation of seven new rYF17D viruses expressing fragments of simian immunodeficiency virus (SIV)mac239 Gag, Nef, and Vif. Studies in Indian rhesus macaques demonstrated that these live-attenuated vectors replicated in vivo, but only elicited low levels of SIV-specific cellular responses. Boosting with recombinant Adenovirus type-5 (rAd5) vectors resulted in robust expansion of SIV-specific CD8+ T-cell responses, particularly those targeting Vif. Priming with rYF17D also increased the frequency of CD4+ cellular responses in rYF17D/rAd5-immunized macaques compared to animals that received rAd5 only. The effect of the rYF17D prime on the breadth of SIV-specific T-cell responses was limited and we also found evidence that some rYF17D vectors were more effective than others at priming SIV-specific T-cell responses. Together, our data suggest that YF17D -- a clinically relevant vaccine vector -- can be used to prime AIDS virus-specific T-cell responses in heterologous prime boost regimens. However, it will be important to optimize rYF17D-based vaccine regimens to ensure maximum delivery of all immunogens in a multivalent vaccine. [ABSTRACT FROM AUTHOR]

Published

2013

12. Highly potent HIV-specific antibody neutralization in vitro translates into effective protection against mucosal SHIV challenge in vivo.

Author

Moldt, Brian, Rakasz, Eva G., Schultz, Niccole, Po-Ving Chan-Hui, Swiderek, Kristine, Weisgrau, Kimberly L., Piaskowski, Shari M., Bergman, Zachary, Watkins, David I., Poignard, Pascal, and Burton, Dennis R.

Subjects

HIV, MONOCLONAL antibodies, PREVENTIVE health services, RHESUS monkeys, IMMUNITY, VACCINATION, NEUTRALIZATION (Chemistry)

Abstract

Most animal studies using passive administration of HIV broadly neutralizing monoclonal antibodies (bnMAbs) have associated protection against high-dose mucosal viral challenge with relatively high serum concentrations of antibody. We recently identified several bnMAbs remarkable for their in vitro potency against HIV. Of these bnMAbs, PGT121 is one of the most broad and potent antibodies isolated to date and shows 10to 100-fold higher neutralizing activity than previously characterized bnMAbs. To evaluate the protective potency of PGT121 in viva, we performed a protection study in rhesus macaques. Animals were i.v. administered 5 mg/kg, 1 mg/kg, or 0.2 mg/kg PGT121 24 h before being vaginally challenged with a single high dose of chimeric simianhuman immunodeficiency virus (SHIV)SF162P3. Sterilizing immunity was achieved in all animals administered 5 mg/kg and 1 mg/kg and three of five animals administered 0.2 mg/kg PGT121, with corresponding average antibody serum concentrations of 95 μg/mL, 15 μg/mL, and 1.8 μg/mL, respectively. The results suggest that a protective serum concentration for PGT121 is in the single-digit μg/mL for SHIVSF162P3, showing that PGT121 can mediate sterilizing immunity at serum concentrations that are significantly lower than those observed in previous studies and that may be achievable through vaccination with the development of a suitable immunogen. [ABSTRACT FROM AUTHOR]

Published

2012

13. Protection against High-Dose Highly Pathogenic Mucosal SIV Challenge at Very Low Serum Neutralizing Titers of the Antibody-Like Molecule CD4-IgG2.

Author

Poignard, Pascal, Moldt, Brian, Maloveste, Karla, Campos, Noëlie, Olson, William C., Rakasz, Eva, Watkins, David I., and Burton, Dennis R.

Subjects

MONOCLONAL antibodies, SIMIAN immunodeficiency virus, IMMUNOGLOBULINS, MOLECULES, IMMUNITY, T cells

Abstract

Passive transfer studies using monoclonal or polyclonal antibodies in the macaque model have been valuable for determining conditions for antibody protection against immunodeficiency virus challenge. Most studies have employed hybrid simian/human immunodeficiency virus (SHIV) challenge in conjunction with neutralizing human monoclonal antibodies. Passive protection against SIV, particularly the pathogenic prototype virus SIVmac239, has been little studied because of the paucity of neutralizing antibodies to this virus. Here, we show that the antibody-like molecule CD4-IgG2 potently neutralizes SIVmac239 in vitro. When administered by an osmotic pump to maintain concentrations given the short half-life of CD4-IgG2 in macaques, the molecule provided sterilizing immunity/protection against high-dose mucosal viral challenge to a high proportion of animals (5/7 at a 200 mg dose CD4-IgG2 and 3/6 at a 20 mg dose) at serum concentrations below 1.5 μg/ml. The neutralizing titers of such sera were predicted to be very low and indeed sera at a 1:4 dilution produced no neutralization in a pseudovirus assay. Macaque anti-human CD4 titers did develop weakly at later time points in some animals but were not associated with the level of protection against viral challenge. The results show that, although SIVmac239 is considered a highly pathogenic virus for which vaccine-induced T cell responses in particular have provided limited benefit against high dose challenge, the antibody-like CD4-IgG2 molecule at surprisingly low serum concentration affords sterilizing immunity/protection to a majority of animals. [ABSTRACT FROM AUTHOR]

Published

2012

14. Understanding animal models of elite control: windows on effective immune responses against immunodeficiency viruses.

Author

Mudd, Philip A and Watkins, David I

Published

2011

15. Simian immunodeficiency virus-specific CD4+ T cells from successful vaccinees target the SIV Gag capsid.

Author

Giraldo-Vela, Juan P., Bean, Alex T., Rudersdorf, Richard, Wallace, Lyle T., Loffredo, John T., Erickson, Priscilla, Wilson, Nancy A., and Watkins, David I.

Subjects

MAJOR histocompatibility complex, T cells, RHESUS monkeys, VIRAL replication, TRANSPLANTATION immunology

Abstract

We recently demonstrated that vaccinated rhesus macaques controlled viral replication of a heterologous SIV challenge. Here, we analyzed anamnestic SIV-specific CD4+ T-cell responses expanding immediately after challenge and show that successful vaccinees consistently targeted a short region of the Gag-p27 Capsid (amino acids 249-291). We have also defined the major histocompatibility complex class II (MHC-II) restricting alleles for several of these responses and show that DQ-restricted CD4+ T-cells depend on unique combinations of both the DQA and DQB alleles. Analysis of SIV-specific CD4+ T-cell responses elicited by a successful vaccine may have important implications in the understanding of vaccine design. [ABSTRACT FROM AUTHOR]

Published

2010

16. The live-attenuated yellow fever vaccine 17D induces broad and potent T cell responses against several viral proteins in Indian rhesus macaques—implications for recombinant vaccine design.

Author

Mudd, Philip A., Piaskowski, Shari M., Costa Neves, Patricia C., Rudersdorf, Richard, Kolar, Holly L., Eernisse, Christopher M., Weisgrau, Kim L., Veloso de Santana, Marlon G., Wilson, Nancy A., Bonaldo, Myrna C., Galler, Ricardo, Rakasz, Eva G., and Watkins, David I.

Subjects

YELLOW fever vaccines, VACCINATION, T cells, VIRAL proteins, RHESUS monkeys, ENDOPLASMIC reticulum, FLAVIVIRUSES, CYTOPLASM

Abstract

The yellow fever vaccine 17D (YF17D) is one of the most effective vaccines. Its wide use and favorable safety profile make it a prime candidate for recombinant vaccines. It is believed that neutralizing antibodies account for a large measure of the protection afforded to YF17D-vaccinated individuals, however cytotoxic T lymphocyte (CTL) responses have been described in the setting of YF17D vaccination. YF17D is an ssRNA flavivirus that is translated as a full-length polyprotein, several domains of which pass into the lumen of the endoplasmic reticulum (ER). The processing and presentation machinery for MHC class I-restricted CTL responses favor cytoplasmic peptides that are transported into the ER by the transporter associated with antigen presentation proteins. In order to inform recombinant vaccine design, we sought to determine if YF17D-induced CTL responses preferentially targeted viral domains that remain within the cytoplasm. We performed whole YF17D proteome mapping of CTL responses in six Indian rhesus macaques vaccinated with YF17D using overlapping YF17D peptides. We found that the ER luminal E protein was the most immunogenic viral protein followed closely by the cytoplasmic NS3 and NS5 proteins. These results suggest that antigen processing and presentation in this model system is not preferentially affected by the subcellular location of the viral proteins that are the source of CTL epitopes. The data also suggest potential immunogenic regions of YF17D that could serve as the focus of recombinant T cell vaccine development. [ABSTRACT FROM AUTHOR]

Published

2010

17. Unexpected Diversity of Cellular Immune Responses against Nef and Vif in HIV-1-Infected Patients Who Spontaneously Control Viral Replication.

Author

Tarosso, Leandro F., Sauer, Mariana M., Sanabani, Sabri, Giret, Maria Teresa, Tomiyama, Helena I., Sidney, John, Piaskowski, Shari M., Diaz, Ricardo S., Sabino, Ester C., Sette, Alessandro, Kalil-Filho, Jorge, Watkins, David I., and Kallas, Esper G.

Subjects

CELLULAR immunity, HIV-positive persons, VIRAL replication, IMMUNOREGULATION, AIDS vaccines, AMINO acids, EPITOPES, PEPTIDES, ANTIRETROVIRAL agents

Abstract

Background: HIV-1-infected individuals who spontaneously control viral replication represent an example of successful containment of the AIDS virus. Understanding the anti-viral immune responses in these individuals may help in vaccine design. However, immune responses against HIV-1 are normally analyzed using HIV-1 consensus B 15-mers that overlap by 11 amino acids. Unfortunately, this method may underestimate the real breadth of the cellular immune responses against the autologous sequence of the infecting virus. Methodology and Principal Findings: Here we compared cellular immune responses against nef and vif-encoded consensus B 15-mer peptides to responses against HLA class I-predicted minimal optimal epitopes from consensus B and autologous sequences in six patients who have controlled HIV-1 replication. Interestingly, our analysis revealed that three of our patients had broader cellular immune responses against HLA class I-predicted minimal optimal epitopes from either autologous viruses or from the HIV-1 consensus B sequence, when compared to responses against the 15-mer HIV-1 type B consensus peptides. Conclusion and Significance: This suggests that the cellular immune responses against HIV-1 in controller patients may be broader than we had previously anticipated. [ABSTRACT FROM AUTHOR]

Published

2010

18. Gag- and Nef-specific CD4+ T cells recognize and inhibit SIV replication in infected macrophages early after infection.

Author

Sacha, Jonah B., GiraIdo-Vela, Juan P., Buechler, Matthew B., Martins, Mauricio A., Maness, Nicholas J., Chungwon Chung, Wallace, Lyle T., León, Enrique J., Friedrich, Thomas C., Wilson, Nancy A., Hiraoka, Atsunobu, and Watkins, David I.

Subjects

T cells, MACROPHAGES, RETROVIRUS diseases, IMMUNE response, EXPERIMENTAL design, EPITOPES

Abstract

The precise immunological role played by CD4+ T cells in retroviral infections is poorly defined. Here, we describe a new function of these cells, the elimination of retrovirus-infected macrophages. After experimental CD8+ cell depletion, elite controlling macaques with set-point viral loads ≤500 viral RNA copies/mL mounted robust Gag-and Nef-specific CD4+ T cell responses during reestablishment of control with ≥54% of all virus-specific CD4+ T cells targeting these 2 proteins. Ex vivo, these simian immunodeficiency virus (SIV)-specific CD4+ T cells neither recognized nor suppressed viral replication in SIV-infected CD4+ T cells. In contrast, they recognized SIV-infected macrophages as early as 2 h postinfection because of presentation of epitopes derived from virion-associated Gag and Nef proteins. Furthermore, virus-specific CD4+ T cells displayed direct effector function and eliminated SIV-infected macrophages. These results suggest that retrovirus-specific CD4+ T cells may contribute directly to elite control by inhibiting viral replication in macrophages. [ABSTRACT FROM AUTHOR]

Published

2009

19. Broadly Neutralizing Human Anti-HIV Antibody 2G12 Is Effective in Protection against Mucosal SHIV Challenge Even at Low Serum Neutralizing Titers.

Author

Hessell, Ann J., Rakasz, Eva G., Poignard, Pascal, Hangartner, Lars, Landucci, Gary, Forthal, Donald N., Koff, Wayne C., Watkins, David I., and Burton, Dennis R.

Subjects

VIRAL antibodies, HIV infections, THERAPEUTICS, VACCINE research, T cells, MACAQUES, VIRAL replication, EPITOPES

Abstract

Developing an immunogen that elicits broadly neutralizing antibodies (bNAbs) is an elusive but important goal of HIV vaccine research, especially after the recent failure of the leading T cell based HIV vaccine in human efficacy trials. Even if such an immunogen can be developed, most animal model studies indicate that high serum neutralizing concentrations of bNAbs are required to provide significant benefit in typical protection experiments. One possible exception is provided by the anti-glycan bNAb 2G12, which has been reported to protect macaques against CXCR4-using SHIV challenge at relatively low serum neutralizing titers. Here, we investigated the ability of 2G12 administered intravenously (i.v.) to protect against vaginal challenge of rhesus macaques with the CCR5-using SHIVSF162P3. The results show that, at 2G12 serum neutralizing titers of the order of 1:1 (IC90), 3/5 antibody-treated animals were protected with sterilizing immunity, i.e. no detectable virus replication following challenge; one animal showed a delayed and lowered primary viremia and the other animal showed a course of infection similar to 4 control animals. This result contrasts strongly with the typically high titers observed for protection by other neutralizing antibodies, including the bNAb b12. We compared b12 and 2G12 for characteristics that might explain the differences in protective ability relative to neutralizing activity. We found no evidence to suggest that 2G12 transudation to the vaginal surface was significantly superior to b12. We also observed that the ability of 2G12 to inhibit virus replication in target cells through antibody-mediated effector cell activity in vitro was equivalent or inferior to b12. The results raise the possibility that some epitopes on HIV may be better vaccine targets than others and support targeting the glycan shield of the envelope. [ABSTRACT FROM AUTHOR]

Published

2009

20. Localized Populations of CD8low/- MHC Class I Tetramer+ SIV-Specific T Cells in Lymphoid Follicles and Genital Epithelium.

Author

Jung Joo Hong, Reynolds, Matthew R., Mattila, Teresa L., Hage, Aaron, Watkins, David I., Miller, Christopher J., and Skinner, Pamela J.

Subjects

T cells, LYMPHOCYTES, CELL-mediated lympholysis, SUPPRESSOR cells, LYMPHOID tissue, IMMUNE system, LYMPHATICS, IMMUNOGLOBULINS, EPITHELIUM

Abstract

CD8 T cells play an important role in controlling viral infections. We investigated the in situ localization of simian immunodeficiency virus (SIV)-specific T cells in lymph and genital tissues from SIV-infected macaques using MHC-class I tetramers. The majority of tetramer-binding cells localized in T cell zones and were CD8+. Curiously, small subpopulations of tetramer-binding cells that had little to no surface CD8 were detected in situ both early and late post-infection, and in both vaginally and rectally inoculated macaques. These tetramer+CD8low/- cells were more often localized in apparent B cell follicles relative to T cell zones and more often found near or within the genital epithelium than the submucosa. Cells analyzed by flow cytometry showed similar populations of cells. Further immunohistological characterization revealed small populations of tetramer+CD20- cells inside B cell follicles and that tetramer+ cells did not stain with γδ-TCR nor CD4 antibodies. Negative control tetramer staining indicated that tetramer+CD8low/2 cells were not likely NK cells nonspecifically binding to MHC tetramers. These findings have important implications for SIV-specific and other antigen-specific T cell function in these specific tissue locations, and suggest a model in which antigen-specific CD8+ T cells down modulate CD8 upon entering B cell follicles or the epithelial layer of tissues, or alternatively a model in which only antigen-specific CD8 T cells that down-modulate CD8 can enter B cell follicles or the epithelium. [ABSTRACT FROM AUTHOR]

Published

2009

21. Impact of MHC class I diversity on immune control of immunodeficiency virus replication.

Author

Goulder, Philip J. R. and Watkins, David I.

Subjects

MAJOR histocompatibility complex, T-cell receptor genes, VIRAL replication, AIDS vaccines, IMMUNOGENETICS, HIV prevention, HISTOCOMPATIBILITY antigens, HIV, HIV infections, PRIMATES, RESEARCH funding, T cells, VIRAL vaccines, RNA virus infections, PREVENTION, PHYSIOLOGY

Abstract

The recent failure of the T-cell-based HIV vaccine trial led by Merck & Co., Inc. prompts the urgent need to refocus on the question of which T-cell responses are required to control HIV replication. The well-described association between the expression of particular MHC class I molecules and successful containment of HIV or, in the macaque model, SIV replication provide a valuable starting point from which to evaluate more precisely what might constitute effective CD8(+) T-cell responses. Here, we review recent studies of T-cell-mediated control of HIV and SIV infection, and offer insight for the design of a successful T-cell-based HIV vaccine in the future. [ABSTRACT FROM AUTHOR]

Published

2008

22. Nonhuman primate models and the failure of the Merck HIV-1 vaccine in humans.

Author

Watkins, David I., Burton, Dennis R., Kallas, Esper G., Moore, John P., and Koff, Wayne C.

Subjects

ADENOVIRUSES, VACCINES, DNA viruses, HIV, HIV infections, SIMIAN viruses, T cells

Abstract

The adenovirus type 5 (Ad5)-based vaccine developed by Merck failed to either prevent HIV-1 infection or suppress viral load in subsequently infected subjects in the STEP human Phase 2b efficacy trial. Analogous vaccines had previously also failed in the simian immunodeficiency virus (SIV) challenge–rhesus macaque model. In contrast, vaccine protection studies that used challenge with a chimeric simian-human immunodeficiency virus (SHIV89.6P) in macaques did not predict the human trial results. Ad5 vector–based vaccines did not protect macaques from infection after SHIV89.6P challenge but did cause a substantial reduction in viral load and a preservation of CD4+ T cell counts after infection, findings that were not reproduced in the human trials. Although the SIV challenge model is incompletely validated, we propose that its expanded use can help facilitate the prioritization of candidate HIV-1 vaccines, ensuring that resources are focused on the most promising candidates. Vaccine designers must now develop T cell vaccine strategies that reduce viral load after heterologous challenge. [ABSTRACT FROM AUTHOR]

Published

2008

23. Wanted: correlates of vaccine-induced protection against simian immunodeficiency virus.

Author

Friedrich, Thomas C and Watkins, David I

Published

2008

24. Molecular typing of major histocompatibility complex class I alleles in the Indian rhesus macaque which restrict SIV CD8+ T cell epitopes.

Author

Kaizu, Masahiko, Borchardt, Gretta J., Glidden, Chrystal E., Fisk, Debra L., Loffredo, John T., Watkins, David I., and Rehrauer, William M.

Subjects

MAJOR histocompatibility complex, RHESUS monkeys, EPITOPES, ANIMAL models in research, IMMUNOGENETICS

Abstract

The utility of the rhesus macaque as an animal model in both HIV vaccine development and pathogenesis studies necessitates the development of accurate and efficient major histocompatibility complex (MHC) genotyping technologies. In this paper, we describe the development and application of allele-specific polymerase chain reaction (PCR) amplification for the simultaneous detection of eight MHC class I alleles from the rhesus macaque ( Macaca mulatta) of Indian descent. These alleles were selected, as they have been implicated in the restriction of CD8+ T cell epitopes of simian immunodeficiency virus (SIV). Molecular typing of Mamu- A*01, Mamu-A*02, Mamu-A*08, Mamu-A*11, Mamu-B*01, Mamu-B*03, Mamu-B*04, and Mamu-B*17 was conducted in a high throughput fashion using genomic DNA. Our amplification strategy included a conserved internal control target to minimize false negative results and can be completed in less than 5 h. We have genotyped over 4,000 animals to establish allele frequencies from colonies all over the western hemisphere. The ability to identify MHC-defined rhesus macaques will greatly enhance investigation of the immune responses, which are responsible for the control of viral replication. Furthermore, application of this technically simple and accurate typing method should facilitate selection, utilization, and breeding of rhesus macaques for AIDS virus pathogenesis and vaccine studies. [ABSTRACT FROM AUTHOR]

Published

2007

25. Polymorphisms in eight host genes associated with control of HIV replication do not mediate elite control of viral replication in SIV-infected Indian rhesus macaques.

Author

Weiler, Andrea, May, Gemma E., Ying Qi, Wilson, Nancy, and Watkins, David I.

Subjects

GENETIC polymorphisms, HIV, VIRAL replication, RHESUS monkeys, POPULATION genetics, REPRODUCTION

Abstract

Polymorphisms in several host genes in HIV-infected individuals facilitate slow progression to AIDS. We have identified several SIV-infected Indian rhesus macaques that naturally control viral replication. We investigated whether spontaneous control of SIV in any of these animals could be explained by mutations in host genes. Such variables could confound studies of associations between MHC class I alleles and control of viral replication. We searched for polymorphisms in CCR5, CXCR6, GPR15, RANTES, IL-10, APOBEC3G, TNF-α, and TSG101 and looked for associations with decreased viral replication. We did not detect any correlations between plasma viral concentration and polymorphisms in host genes examined in this study. In addition, we did not find the polymorphisms present in humans in any of our macaques. [ABSTRACT FROM AUTHOR]

Published

2006

26. Initiation of antiretroviral therapy during chronic SIV infection leads to rapid reduction in viral loads and the level of T-cell immune response.

Author

Boyer, Jean D., Kumar, Sanjeev, Robinson, Tara, Parkinson, Rose, Ling Wu, Lewis, Mark, Watkins, David I., and Weiner, David B.

Subjects

SIMIAN viruses, ANTIRETROVIRAL agents, HIV, IMMUNE response, AIDS

Abstract

In the present era of increasing resistance of human immunodeficiency virus (HIV) to antiviral drugs, exploration of adjunct therapies directed at immune responses in combination with antiretroviral drugs may be of value for the treatment of acquired immunodeficiency syndrome. In this study, we designed a model for immune therapy using SIVmac251 infection in rhesus macaques. We explored the outcomes of primary infection on viral loads and the resulting T-cell immune responses in primates. The SIV-infected rhesus macaque model exhibited features similar to those observed in HIV-1 infection of humans. Major histocompatibility complex (MHC) segregation with viral loads were found to associate with viral containment and hence the duration of the disease-free latency period. Thus a better understanding of the relative roles of MHC class I allele in control of viral replication may provide important information for prophylactic or therapeutic vaccine designs. Mamu-A01 is significantly associated with higher immune response and control of viral replication. This allele is frequent in rhesus macaques of Indian origin (22%). Interestingly, Mamu-B01 (26% animals) was associated with lower immune responses and higher viral loads. Another allele, A08 was also predominantly present in 37% of the animals in this study. We observed higher viral replication in individual SIV-infected rhesus monkeys that did not demonstrate strong cellular immune responses. The results are important for understanding SIV disease progression in different MHC Mamu alleles and also for improving the interpretation and quality of pre-clinical studies in rhesus monkeys. [ABSTRACT FROM AUTHOR]

Published

2006

27. Premature Induction of an Immunosuppressive Regulatory T Cell Response during Acute Simian Immunodeficiency Virus Infection.

Author

Estes, Jacob D., Qingsheng Li, Reynolds, Matthew R., Wietgrefe, Stephen, Duan, Lijie, Schacker, Timothy, Picker, Louis J., Watkins, David I., Lifson, Jeffrey D., Reilly, Cavan, Carlis, John, and Haase, Ashley T.

Subjects

IMMUNOSUPPRESSION, T cells, HIV, RHESUS monkeys, VIRAL replication, LYMPHOID tissue

Abstract

Here we report the results of an investigation into the possibility that one mechanism responsible for the establishment of persistent human immunodeficiency virus infection is an early regulatory T (Treg) cell response that blunts virus-specific responses. Using the simian immunodeficiency virus (SIV)-infected rhesus macaque model, we show that, indeed, viral replication and immune activation in lymphatic tissue drive a premature immunosuppressive response, with dramatic increases in the frequencies of CD4+CD25+FOXP3+ Treg cells, transforming growth factor-β1+ cells, interleukin-10+ cells, and indoleamine 2,3-dioxygenase+CD3+ cells. When we compared SIV infection with rhesus cytomegalovirus (RhCMV) infection, we found that the frequency of Treg cells paralleled the magnitude of immune activation during both infections but that the magnitude of immune activation and of the Treg cell response were lower and peaked much later during RhCMV infection. Importantly, the frequency of Treg cells inversely correlated with the magnitude of the SIV-specific cytotoxic T lymphocyte response. We conclude that an early Treg cell response during acute SIV infection may contribute to viral persistence by prematurely limiting the antiviral immune response before infection is cleared. [ABSTRACT FROM AUTHOR]

Published

2006

28. HIV vaccine design: insights from live attenuated SIV vaccines.

Author

Koff, Wayne C., Johnson, Philip R., Watkins, David I., Burton, Dennis R., Lifson, Jeffrey D., Hasenkrug, Kim J., McDermott, Adrian B., Schultz, Alan, Zamb, Timothy J., Boyle, Rosanne, and Desrosiers, Ronald C.

Subjects

AIDS vaccines, VIRAL vaccines, HIV, PREVENTIVE medicine, IMMUNE response, IMMUNOLOGY

Abstract

The International AIDS Vaccine Initiative has established a consortium to elucidate mechanisms of protection conferred by live attenuated simian immunodeficiency virus vaccines in monkeys. Here, the strategies defining key components of the protective immune response elicited by these vaccines are discussed. [ABSTRACT FROM AUTHOR]

Published

2006

29. The pigtail macaque MHC class I allele Mane-A* 10 presents an immundominant SIV Gag epitope: identification, tetramer development and implications of immune escape and reversion.

Author

Smith, Miranda Z., Fernandez, Caroline S., Chung, Amy, Dale, C. Jane, De Rose, Robert, Jie Lin, Brooks, Andrew G., Krebs, Kendall C., Watkins, David I., O'Connor, David H., Davenport, Miles P., and Kent, Stephen J.

Subjects

HIV, HTLV, MAJOR histocompatibility complex, AIDS, HLA histocompatibility antigens, PIG-tailed macaque, SIMIAN viruses

Abstract

The pigtail macaque ( Macaca nemestrina) is a common model for the study of AIDS. The pigtail major histocompatibility complex class I allele Mane-A* 10 restricts an immunodominant simian immunodeficiency virus (SIV) Gag epitope (KP9) which rapidly mutates to escape T cell recognition following acute simian/human immunodeficiency virus infection. Two technologies for the detection of Mane-A* 10 in outbred pigtail macaques were developed: reference strand-mediated conformational analysis and sequence-specific primer polymerase chain reaction. A Mane-A*10/KP9 tetramer was then developed to quantify CD8+ T lymphocytes primed by multigenic DNA vaccination, which have previously been difficult to detect using standard interferon- γ-based T cell assays. We also demonstrate mutational escape at KP9 following acute SIV infection. Mane-A* 10+ animals have lower set point SIV levels than Mane-A* 10− animals, suggesting a significant fitness cost of escape. These studies pave the way for a more robust understanding of HIV vaccines in pigtail macaques. [ABSTRACT FROM AUTHOR]

Published

2005

30. Automated generation and evaluation of specific MHC binding predictive tools: ARB matrix applications.

Author

Huynh-Hoa Bui, Sidney, John, Peters, Bjoern, Sathiamurthy, Muthuraman, Sinichi, Asabe, Purton, Kelly-Anne, Mothé, Bianca R., Chisari, Francis V., Watkins, David I., and Sette, Alessandro

Subjects

PEPTIDES, MAJOR histocompatibility complex, IMMUNOGENETICS, EPITOPES, T cells, BINDING sites, MATRICES (Mathematics), COMPUTER software

Abstract

Prediction of which peptides can bind major histocompatibility complex (MHC) molecules is commonly used to assist in the identification of T cell epitopes. However, because of the large numbers of different MHC molecules of interest, each associated with different predictive tools, tool generation and evaluation can be a very resource intensive task. A methodology commonly used to predict MHC binding affinity is the matrix or linear coefficients method. Herein, we described Average Relative Binding (ARB) matrix methods that directly predict IC50 values allowing combination of searches involving different peptide sizes and alleles into a single global prediction. A computer program was developed to automate the generation and evaluation of ARB predictive tools. Using an in-house MHC binding database, we generated a total of 85 and 13 MHC class I and class II matrices, respectively. Results from the automated evaluation of tool efficiency are presented. We anticipate that this automation framework will be generally applicable to the generation and evaluation of large numbers of MHC predictive methods and tools, and will be of value to centralize and rationalize the process of evaluation of MHC predictions. MHC binding predictions based on ARB matrices were made available at web server. [ABSTRACT FROM AUTHOR]

Published

2005

31. Unparalleled complexity of the MHC class I region in rhesus macaques.

Author

Otting, Nel, Heijmans, Corrine M. C., Noort, Riet C., de Groot, Natasja G., Doxiadis, Gaby G. M., van Rood, Jon J., Watkins, David I., and Bontrop, Ronald E.

Subjects

GENES, RHESUS monkeys, GENETICS, CELL nuclei, POLYMORPHISM (Zoology), AIDS vaccines, PREVENTIVE medicine

Abstract

The highly polymorphic gene products of the classical MHC class I genes in humans (HLA-A, HLA-B, and HLA-C) play a critical role in the immune defense against intracellular infections. Because non- human primates are important models for AIDS vaccine research, rhesus monkeys from a thoroughly pedigreed and serotyped colony were subjected to full-length cDNA analysis of MHC class 1 gene transcripts. Rhesus macaques express multiple dominant Mamu-A and Mamu-B transcripts (majors) per chromosome, which are characterized by high expression levels. The presence of additional cDNAs with low levels of expression (minors) suggests evidence for transcriptional control of MHC class I genes. More-over, phylogenetic analyses illustrate that most of the Mamu-A and Mamu-B loci/lineages identified display no or only limited levels of allelic polymorphism. Thus, MHC class 1 diversity in rhesus macaques is typified by the existence of an unmatched high number of Mamu-A and Mamu-B region configurations that exhibit polymorphism with regard to the number and combination of transcribed loci present per chromosome. [ABSTRACT FROM AUTHOR]

Published

2005

32. HIV and SIV CTL escape: implications for vaccine design.

Author

Goulder, Philip J. R. and Watkins, David I.

Subjects

LYMPHOCYTES, VIRUS diseases, GENETIC mutation, VACCINES, HIV

Abstract

Cytotoxic T lymphocytes (CTLs) have a central role in the successful control of immunodeficiency virus infection. Evasion of this immune response through CTL escape is therefore an important factor in HIV and simian immunodeficiency virus pathogenesis. During the course of an infection, the precise timing of the occurrence of escape mutations and their location in the viral genome can indicate the efficacy of certain CTL specificities and the cost to viral fitness of particular escape mutations - factors that are highly relevant to vaccine design. Also crucial for vaccine design is the extent to which CTL escape is driving the evolution of HIV at the population level. Here, we highlight the important lessons that can be learned from immunodeficiency virus CTL escape. [ABSTRACT FROM AUTHOR]

Published

2004

33. Reversion of CTL escape-variant immunodeficiency viruses in vivo.

Author

Friedrich, Thomas C., Dodds, Elizabeth J., Yant, Levi J., Vojnov, Lara, Rudersdorf, Richard, Cullen, Candice, Evans, David T., Desrosiers, Ronald C., Mothé, Bianca R., Sidney, John, Sette, Alessandro, Kunstman, Kevin, Wolinsky, Steven, Piatak, Michael, Lifson, Jeffrey, Hughes, Austin L., Wilson, Nancy, O'Connor, David H., and Watkins, David I.

Subjects

T cells, ANTINEOPLASTIC agents, LYMPHOCYTES, CELL-mediated lympholysis, HIV, IMMUNODEFICIENCY

Abstract

Engendering cytotoxic T-lymphocyte (CTL) responses is likely to be an important goal of HIV vaccines. However, CTLs select for viral variants that escape immune detection. Maintenance of such escape variants in human populations could pose an obstacle to HIV vaccine development. We first observed that escape mutations in a heterogeneous simian immunodeficiency virus (SIV) isolate were lost upon passage to new animals. We therefore infected macaques with a cloned SIV bearing escape mutations in three immunodominant CTL epitopes, and followed viral evolution after infection. Here we show that each mutant epitope sequence continued to evolve in vivo, often re-establishing the original, CTL-susceptible sequence. We conclude that escape from CTL responses may exact a cost to viral fitness. In the absence of selective pressure upon transmission to new hosts, these original escape mutations can be lost. This suggests that some HIV CTL epitopes will be maintained in human populations. [ABSTRACT FROM AUTHOR]

Published

2004

34. Cytotoxic T-Lymphocyte Escape Monitoring in Simian Immunodeficiency Virus Vaccine Challenge Studies.

Author

O'Connor, David H., Allen, Todd M., and Watkins, David I.

Subjects

SIMIAN viruses, AIDS vaccines, CELL-mediated cytotoxicity, CELLULAR immunity, IMMUNODEFICIENCY, VACCINATION

Abstract

Several vaccine studies have ameliorated disease progression in simian–human immunodeficiency virus (SHIV) infections. The successes of these vaccines have been largely attributed to protective effects of cytotoxic T-lymphocyte (CTL) responses, although the precise correlates of immune protection remain poorly defined. It is now well established that vigorous CTL and antibody responses can rapidly select for viral escape variants after HIV and SIV infection. Here we suggest that viral variation analyses should be performed on viruses derived from vaccinated, SIV-, or SHIV-challenged animals as a routine component of vaccine evaluation to determine the contribution of immune responses to the success (or failure) of the vaccine regimen. To illustrate the importance of escape analysis, we show that rapid emergence of escape variants postchallenge contributed to the failure of a DNA prime/MVA boost vaccine regimen encoding SIV Tat. [ABSTRACT FROM AUTHOR]

Published

2002

35. Acute phase cytotoxic T lymphocyte escape is a hallmark of simian immunodeficiency virus infection.

Author

O'Connor, David H., Allen, Todd M., Vogel, Thorsten U., Jing, Peicheng, DeSouza, Ivna P., Dodds, Elizabeth, Dunphy, Edward J., Melsaether, Cheri, Mothé, Bianca, Yamamoto, Hiroshi, Horton, Helen, Wilson, Nancy, Hughes, Austin L., and Watkins, David I.

Subjects

T cells, SIMIAN viruses, INFECTION

Abstract

Cytotoxic T-lymphocyte (CTL) responses peak coincident with the decline in acute HIV viremia. Despite two reports of CTL-resistant HIV variants emerging during acute infection, the contribution of acute CTL escape to HIV pathogenesis remains unclear. Difficulties inherent in studying acute HIV infection can be overcome by modeling virus-host interactions in SIV-infected rhesus macaques. We sequenced 21 complete simian immunodeficiency virus (SIV)mac239 genomes at four weeks post-infection to determine the extent of acute CTL escape. Here we show that viruses from 19 of 21 macaques escaped from CTLs during acute infection and that these escape-selecting CTLs were responsive to lower concentrations of peptide than other SIV-specific CTLs. Interestingly, CTLs that require low peptide concentrations for stimulation (high 'functional avidity') are particularly effective at controlling other viral infections. Our results suggest that acute viral escape from CTLs is a hallmark of SIV infection and that CTLs with high functional avidity can rapidly select for escape variants. [ABSTRACT FROM AUTHOR]

Published

2002

36. Mucosal AIDS vaccine reduces disease and viral load in gut reservoir and blood after mucosal infection of macaques.

Author

Belyakov, Igor M., Hel, Zdenek, Kelsall, Brian, Kuznetsov, Vladimir A., Ahlers, Jeffrey D., Nacsa, Janos, Watkins, David I., Allen, Todd M., Sette, Alessandro, Altman, John, Woodward, Ruth, Markham, Phillip D., Clements, John D., Franchini, Genoveffa, Strober, Warren, and Berzofsky, Jay A.

Subjects

VACCINES, T cells, HIV, RHESUS monkeys

Abstract

Given the mucosal transmission of HIV-1, we compared whether a mucosal vaccine could induce mucosal cytotoxic T lymphocytes (CTLs) and protect rhesus macaques against mucosal infection with simian/human immunodeficiency virus (SHIV) more effectively than the same vaccine given subcutaneously. Here we show that mucosal CTLs specific for simian immunodeficiency virus can be induced by intrarectal immunization of macaques with a synthetic-peptide vaccine incorporating the LT(R192G) adjuvant. This response correlated with the level of T-helper response. After intrarectal challenge with pathogenic SHIV-Ku2, viral titers were eliminated more completely (to undetectable levels) both in blood and intestine, a major reservoir for virus replication, in intrarectally immunized animals than in subcutaneously immunized or control macaques. Moreover, CD4+ T cells were better preserved. Thus, induction of CTLs in the intestinal mucosa, a key site of virus replication, with a mucosal AIDS vaccine ameliorates infection by SHIV in non-human primates. [ABSTRACT FROM AUTHOR]

Published

2001

37. A common rhesus macaque MHC class I molecule which binds a cytotoxic T-lymphocyte epitope in Nef of simian immunodeficiency virus.

Author

Horton, Helen, Rehrauer, William, Meek, Eliabeth C., Shultz, Millicent A., Piekarczyk, Marian S., Jing, Peicheng, Carter, Donald K., Steffen, Susan R., Calore, Briana, Urvater, Julie A., Vogel, Thorsten U., Wilson, Nancy A., and Watkins, David I.

Subjects

SIMIAN viruses, IMMUNODEFICIENCY, HIV, RHESUS monkeys, HIV infections, VIRAL replication, VACCINES

Abstract

Focuses on the importance of simian immunodeficiency virus (SIV) infection of rhesus macaques as a model for the study of HIV infection in humans. Importance in controlling viral replication in infected hosts; Expansion on the utility of the rhesus macaque as a model for vaccine and pathogenesis study; Understanding on the importance of cytotoxic T lymphocytes responses during SIV infection.

Published

2001

38. Tat-specific cytotoxic T lymphocytes select for SIV escape variants during resolution of primary viraemia.

Author

Allen, Todd M., O'Connor, David H., Jing, Peicheng, Dzuris, John L., Mothe, Bianca R., Vogel, Thorsten U., Dunphy, Ed, Liebl, Max E., Emerson, Carol, Wilson, Nancy, Kuntsman, Kevin J., Wang, Xiaochi, Allison, David B., Hughes, Austin L., Desrosiers, Ronald C., Altman, John D., Wolinsky, Steven M., Sette, Alessandro, and Watkins, David I.

Subjects

T cells, HIV, SIMIAN viruses, VIROLOGY

Abstract

Presents a study which shows that Tat-specific CD8-positive T-lymphocyte responses select for new viral escape variants during the acute phase of HIV and the simian immunodeficiency virus (SIV) infections. What was revealed when the virus was sequenced immediately after the acute phase; Implications of this research for the development of an HIV vaccine.

Published

2000

39. Major histocompatibility complex class I diversity in a West African chimpanzee population: implications for HIV research.

Author

de Groot, Natasja G., Otting, N., Argüello, Rafael, Watkins, David I., Doxiadis, Gaby G. M., Madrigal, J. Alejandro, and Bontrop, R. E.

Subjects

HIV, MAJOR histocompatibility complex, CHIMPANZEES as laboratory animals, IMMUNOGENETICS, IMMUNOLOGY, GENETICS, SEROLOGY

Abstract

Human immunodefiency virus (HIV) poses a major threat to humankind. And though, like humans, chimpanzees are susceptible to HIV infection, they are considered to be resistant to the development of the acquired immune deficiency syndrome (AIDS). Little is known about major histocompatibility complex (MHC) class I diversity in chimpanzee populations and, moreover, whether qualitative aspects of Patr class I molecules may control resistance to AIDS. To address these questions, we assayed MHC class I diversity in a West African chimpanzee population and in some animals from other subspecies of chimpanzee. Application of different techniques allowed the detection of 17 full-length Patr-A, 19 Patr-B, and 10 Patr-C alleles. All Patr-A alleles cluster only into the HLA-A1/A3/A11 family, which supports the idea that chimpanzees have experienced a reduction in their repertoire of A locus alleles. The Patr-B alleles do not cluster in the same lineages as their human equivalents, due to frequent exchange of polymorphic sequence motifs. Furthermore, polymorphic motifs may have been exchanged between Patr-A and Patr-B loci, resulting in convergence. With regard to evolutionary stability, the Patr-C locus is more similar to the Patr-A locus than it is to the Patr-B locus. Despite the relatively low number of animals analyzed, humans and chimpanzees were ascertained as sharing similar degrees of diversity at the contact residues constituting the B and F pockets in the peptide-binding side of MHC class I molecules. Our results indicate that within a small sample of a West African chimpanzee population, a high degree of Patr class I diversity is encountered. This is in agreement with the fact that chimpanzees display more mitochondrial DNA variation than humans. In addition, population analyses demonstrated that particular Patr-B molecules, with the capacity to bind conserved HIV-1 epitopes, are characterized by high gene frequencies. These findings have important implications for evaluating immune responses in HIV vaccine studies and, more importantly, may help in understanding the relative resistance of chimpanzees to AIDS. [ABSTRACT FROM AUTHOR]

Published

2000

40. Isolation of the HLA-H orthologue in gorillas and chimpanzees.

Author

Urvater, Julie A. and Watkins, David I.

Subjects

ANTISENSE DNA, EXONS (Genetics), MAJOR histocompatibility complex, CHIMPANZEES, GORILLA (Genus), NUCLEOTIDES, IMMUNOGENETICS

Abstract

Describes the full-length complementary DNA sequence of Gogo-H, the likely donor of exon 2 in major histocompatibility complex class I A locus allele, Gogo-Oko, as well as Patr-H, the HLA-H orthologue in chimpanzees. Likelihood of H gene to contain a phenyl-alanine substitution for the conserved cysteine 164; Absence of single nucleotide deletion in exon 4; Possibility of nonfunctional gene Gogo-H to be rendered functional through the appropriate segmental exchange.

Published

2000

41. Major histocompatibility complex class I genes in primates: co-evolution with pathogens.

Author

Vogel, Thorsten U., Evans, David T., Urvater, Julie A., O'Connor, David H., Hughes, Austin L., and Watkins, David I.

Subjects

MAJOR histocompatibility complex, PRIMATES, PATHOGENIC microorganisms

Abstract

The major histocompatibility complex (MHC) is the most polymorphic genetic system known, playing a central role in the cellular immune response to pathogens. The relationship between the MHC of humans and non-human primates has increased our understanding of MHC evolution and how polymorphism of this gene family may have been generated. We will review MHC class I evolution in great apes and Old World and New World primates and discuss new data from the simian immunodeficiency virus/rhesus monkey animal model that demonstrate the role of MHC class I alleles in selecting for new populations of viruses. This suggests that certain pathogens co-evolve with the MHC class I molecules they encounter in a population. [ABSTRACT FROM AUTHOR]

Published

1999

42. Virus-specific cytotoxic T-lymphocyte responses select for amino-acid variation in simian immunodeficiency virus Env and Nef.

Author

Evans, David T., O'Connor, David H., Jing, Peicheng, Dzuris, John L., Sidney, John, da Silva, Jack, Allen, Todd M., Horton, Helen, Venham, John E., Rudersdorf, Richard A., Vogel, Thorsten, Pauza, C. David, Bontrop, Ronald E., DeMars, Robert, Sette, Alessandro, Hughes, Austin L., and Watkins, David I.

Subjects

LYMPHOCYTES, HIV, AMINO acids, SIMIAN viruses

Abstract

Cytotoxic T-lymphocyte (CTL) responses to human immunodeficiency virus arise early after infection, but ultimately fail to prevent progression to AIDS. Human immunodeficiency virus may evade the CTL response by accumulating amino-acid replacements within CTL epitopes. We studied 10 CTL epitopes during the course of simian immunodeficiency virus disease progression in three related macaques. All 10 of these CTL epitopes accumulated amino-acid replacements and showed evidence of positive selection by the time the macaques died. Many of the amino-acid replacements in these epitopes reduced or eliminated major histocompatibility complex class I binding and/or CTL recognition. These findings strongly support the CTL 'escape' hypothesis. [ABSTRACT FROM AUTHOR]

Published

1999

43. Identification of new Mamu-DRB alleles using DGGE and direct sequencing.

Author

Knapp, L. A., Cadavid, Luis F., Eberle, Mary E., Knechtle, Stuart J., Bontrop, Ronald E., and Watkins, David I.

Abstract

Rhesus macaques represent important animal models for biomedical research. The ability to identify macaque major histocompatibility complex ( Mhc) alleles is crucial for fully understanding these models of autoimmune and infectious disease. Here we describe a rapid and unambiguous way to distinguish DRB alleles in the rhesus macaque using the polymerase chain reaction, denaturing gradient gel electrophoresis (DGGE), and direct sequencing. The highly variable second exon of Mamu-DRB alleles was amplified using generic DRB primers and alleles were separated by DGGE. DNA was then reamplified from plugs removed from the gel and alleles were determined using fluorescent-based sequencing. Validity of this typing procedure was confirmed by identification of all DRB alleles for three macaques previously characterized by cloning and sequencing techniques. Importantly, our analysis revealed DRB alleles not previously identified in the three reference animals. Using this technique, we identified 40 alleles in fifteen unrelated macaques. On the basis of phylogenetic tree analyses, 14 new DRB alleles were assigned to 10 different Mhc-DRB lineages. Interestingly, two of the new DRB6 lineages had previously been identified in prosimians and pigtailed macaques. Whereas traditional DRB typing methods provide limited information, our new technique provides a simple and relatively rapid way of identifying DRB alleles for tissue typing, determining individual identification and studies of disease association and susceptibility. This new technique should also contribute to ongoing studies of Mhc function and evolution in many different species of nonhuman primates. [ABSTRACT FROM AUTHOR]

Published

1997

44. The T-cell receptor β chain-encoding gene repertoire of a New World primate species, the cotton-top tamarin.

Author

Allen, T. M., Lanchbury, Jerry S., Hughes, Austin L., and Watkins, David I.

Abstract

The New World primate, the cotton-top tamarin ( Saguinus oedipus), expresses major histocompatibility complex (MHC) class I molecules with limited diversity. The uniqueness of the cotton-top tamarin MHC class I loci may contribute to this species' unusual susceptibility to viral infections and high incidence of ulcerative colitis. As a prelude to examining the effect of this limited MHC class I diversity on the tamarin CD8 T-cell receptor (TCR) repertoire, we identified expressed tamarin TCR β chain ( TCRB) cDNAs by anchored and inverse polymerase chain reaction. Sequence alignments and phylogenetic comparisons with human and rhesus macaque sequences identified homologues of 21 human variable ( V) gene families. Only single variable region genes were identified in each of these tamarin VB families, with the exception of the VB 5, 9, and 13 families which were comprised of two or three distinct members. The multiple genes within these three VB families do not appear to have separate human homologues, but rather aligned equally well to a single human gene from their respective VB families. These genes appear to have arisen, therefore, by duplication of certain VB genes in the tamarin ancestors following their divergence from the lineage leading to Old World primates and hominoids. Homologues of 12 of the 13 human joining ( J) region genes were also identified in the tamarin. Comparison of the proportion of nonsynonymous (p) and synonymous (p) substitutions occurring per site within tamarin variable region genes demonstrated a reduction in p in the framework regions compared with p in the presumed MHC contact regions (CDR1 and CDR2). Taken together, these findings illustrate that the TCR β chain-encoding genes of the cotton-top tamarin are similar in structure and degree of complexity compared with their Old World primate and human counterparts. [ABSTRACT FROM AUTHOR]

Published

1996

45. Isoelectric focusing of bovine major histocompatibility complex class II molecules.

Author

Watkins, David I., Shadduck, John A., Rudd, Christopher E., Stone, Marc E., Lewin, Harris A., and Letvin, Norman L.

Published

1989

46. Major histocompatibility complex class I molecules of nonhuman primates.

Author

Watkins, David I., Kannagi, Mari, Stone, Marc E., and Letvin, Norman L.

Published

1988

47. HLA-A *8001 is a member of a newly discovered ancient family of HLA-A alleles.

Author

Wagner, Annette G., Hughes, Austin L., Iandoll, Mary L., Stawart, Dod, Herbert, Susie, Watkins, David I., Hurley, Carolyn Katovich, and Rosen-Bronson, Sandra

Published

1993

48. SPLIT TOLERANCE INDUCED BY IMMUNOTOXIN IN A RHESUS KIDNEY ALLOGRAFT MODEL.

Author

Fechner Jr., John H., Vargo, Daniel J., Geissler, Edward K., Graeb, Christian, Wang, Jue, Hanaway, Michael J., Watkins, David I., Piekarczyk, Marian, Neville Jr., David M., and Knechtle, Stuart J.

Published

1997

49. USE OF cDNA PROBES SPECIFIC FOR THE HUMAN MHC CLASS IIβ LOCI FOR TISSUE-TYPING NONHUMAN PRIMATES AT THEIR CLASS IIβ LOCI.

Author

Watkins, David I., Shadduck, John A., Hodi, F. Stephen, Stone, Marc E., and Letvin, Norman L.

Published

1989

50. Evolutionary instability of the major histocompatibility complex class I loci in New World primates.

Author

Cadavid, Luis F., Shufflebotham, Clare, Ruiz, Francisco J., Yeager, Meredith, Hughes, Austin L., and Watkins, David I.

Subjects

MAJOR histocompatibility complex, SAGUINUS

Abstract

Describes the presence of a major histocompatibility complex (MHC) class I processed pseudogene in the genome of several species of the genus Saguinus. Hallmarks of the MHC; Evolutionary stability of the loci; Materials and methods of the study; Details of the study.

Published

1997