Preferential infection of human Ad5-specific CD4 T cells by HIV in Ad5 naturally exposed and recombinant Ad5-HIV vaccinated individuals

Hu, Haitao; Eller, Michael A.; Zafar, Shah J.; Zhou, Yu; Gu, Mengnan; Wei, Zhi; Currier, Jeffrey R.; Marovich, Mary; Kibuuka, Hannah; Bailer, Robert T.; Koup, Richard A.; Robb, Merlin L.; Michael, Nelson L.; Kim, Jerome H.; Ratto‐Kim, Silvia

doi:10.1073/pnas.1400446111

Cited by 41 publications

(48 citation statements)

References 30 publications

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“…Second, no HPV genes are expressed from the pseudogenomes, so there is no potential reduction in immunity to the target antigen because of immunodominance of an HPV viral antigen. Third, the recent cessation of an HIV trial (HVTN 502) highlighted the risk of potentiating HIV infection through the induction of HIV-susceptible CD4 ϩ T cells (56). Because ivag genetic vaccination with HPV vectors results in highly skewed CD8 ϩ T cell responses, it should minimize the risk of…”

Section: Discussionmentioning

confidence: 99%

“…Occasionally, we observed a Ͻ2-fold increase in the level of CD4 ϩ T cells in HPV vector ivag-immunized groups, which is much less pronounced than the 20-fold increase in the level of CD8 ϩ T cells. Also, HPV vector ivag immunization did not induce expression of HIV coreceptor ␣4␤7 by cervicovaginal CD4 ϩ T cells (data not shown) (57,58), in contrast to marked induction of this coreceptor after vaccination with an adenovirus 5 vector (56). Finally, there are many human and animal papillomavirus types that are distinct serotypes.…”

Section: Figmentioning

confidence: 93%

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Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8⁺T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Çuburu

Wang

Goodman

et al. 2015

J Virol

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No herpes simplex virus 2 (HSV-2G enital herpes is a common sexually transmitted disease caused by herpes simplex virus 2 (HSV-2). Worldwide, more than 500 million individuals are chronically infected by HSV-2, and the prevalence of HSV-2 infection is twice as high in women as in men (1). In the United States, the seroprevalence of HSV-2 in 14-to 49-year-olds during the 2005-2010 period was 15.7% (2). During primary infection, HSV-2 infects and replicates in epithelial cells of the genital mucosa and spreads to the regional ganglia, where it establishes a lifelong latent infection. HSV-2 can undergo reactivation and shedding from the genital mucosa, where it can cause recurrent genital lesions, which are associated with an increased risk of HIV-1 acquisition (3, 4). Shedding of HSV-2 may also be subclinical, and HSV-2 transmission can occur in the absence of lesions (5, 6). Immunosuppression is associated with an increased risk of severe disseminated disease. In addition, transmission of HSV-2 from the genital mucosae of acutely infected pregnant women to neonates can cause severe infection.Several therapeutic and preventive interventions based on antiviral drugs, the use of condoms, abstinence, or circumcision can reduce the burden of HSV-2 infection at the individual level.However, these interventions have not controlled the HSV-2 epidemic (7). Therefore, a vaccine that could prevent primary acquisition of HSV-2 or reduce HSV-2 shedding and/or recurrent lesions in chronically infected individuals might have a substantial impact at both the individual and public health levels.

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Section: Discussionmentioning

confidence: 99%

Section: Figmentioning

confidence: 93%

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8⁺T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Çuburu

Wang

Goodman

et al. 2015

J Virol

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“…CD4+ and CD8+ T-cell responses are directed towards epitopes within conserved regions of the virus, particularly the immunodominant hexon, [73][74][75][76] and these can be cross-reactive among different Ad species groups. [75,77] In recent years, a number of studies have demonstrated that pre-existing anti-vector T-cells are boosted in vivo [74,[77][78][79] and ex vivo following vaccination/stimulation with Ad vectors. [80,81] Furthermore, in addition to issues with pre-existing anti-vector NAbs limiting transgene expression, cellular immunity can also eliminate vectortransduced cells, having a negative impact on vaccine immunogenicity.…”

Section: Challenges and Limitations Associated With Adenoviral Vaccinesmentioning

confidence: 99%

Adenoviral vectors as novel vaccines for influenza

Coughlan

Mullarkey

Gilbert

2015

Journal of Pharmacy and Pharmacology

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Objectives Influenza is a viral respiratory disease causing seasonal epidemics, with significant annual illness and mortality. Emerging viruses can pose a major pandemic threat if they acquire the capacity for sustained human-to-human transmission. Vaccination reduces influenza-associated mortality and is critical in minimising the burden on the healthcare system. However, current vaccines are not always effective in at-risk populations and fail to induce long-lasting protective immunity against a range of viruses. Key findings The development of 'universal' influenza vaccines, which induce heterosubtypic immunity capable of reducing disease severity, limiting viral shedding or protecting against influenza subtypes with pandemic potential, has gained interest in the research community. To date, approaches have focused on inducing immune responses to conserved epitopes within the stem of haemagglutinin, targeting the ectodomain of influenza M2e or by stimulating cellular immunity to conserved internal antigens, nucleoprotein or matrix protein 1. Summary Adenoviral vectors are potent inducers of T-cell and antibody responses and have demonstrated safety in clinical applications, making them an excellent choice of vector for delivery of vaccine antigens. In order to circumvent pre-existing immunity in humans, serotypes from non-human primates have recently been investigated. We will discuss the pre-clinical development of these novel vectors and their advancement to clinical trials.

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“…The increased infection rate in men with baseline Ad5 seropositivity in Step is further supported by observed Ad5-specific cellular immune boosting in vaccines [21,22], data that Ad5 exposure of PBMC from Ad5-seropositive persons causes proliferation of mucosal-homed HIV-1-susceptible CD4 þ T cells [23], and the observation that Ad5-specific CD4 þ T cells (generated either by natural infection or rAd5 vaccination) appear to be more susceptible to infection than cytomegalovirus (CMV)-specific CD4 þ T cells [24]. However, none of the trials included a control vector-only group to distinguish between contributions of responses against rAd5 versus HIV-1 inserts.…”

Section: Role Of Preexisting Adenovirus Immunity In Increased Hiv-1 Imentioning

confidence: 82%

Adenovirus vectors as HIV-1 vaccines

D’Souza

Yang²

2015

Aids

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Preferential infection of human Ad5-specific CD4 T cells by HIV in Ad5 naturally exposed and recombinant Ad5-HIV vaccinated individuals

Cited by 41 publications

References 30 publications

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8⁺T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8⁺T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Adenoviral vectors as novel vaccines for influenza

Adenovirus vectors as HIV-1 vaccines

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Preferential infection of human Ad5-specific CD4 T cells by HIV in Ad5 naturally exposed and recombinant Ad5-HIV vaccinated individuals

Cited by 41 publications

References 30 publications

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8+T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8+T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Adenoviral vectors as novel vaccines for influenza

Adenovirus vectors as HIV-1 vaccines

Contact Info

Product

Resources

About

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8⁺T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge

Topical Herpes Simplex Virus 2 (HSV-2) Vaccination with Human Papillomavirus Vectors Expressing gB/gD Ectodomains Induces Genital-Tissue-Resident Memory CD8⁺T Cells and Reduces Genital Disease and Viral Shedding after HSV-2 Challenge